LEFKO3
R package lefko3
is a complete environment for the
construction and analysis of matrix projection models (MPMs) and
integral projection models (IPMs) (Shefferson,
Kurokawa, and Ehrlén 2021). It was originally developed to
estimate and analyze historical size-classified matrix
projection models (hMPMs), which are matrices designed to include not
only current state but also past history in terms of previous states,
where stages are defined in terms of size. Such matrices are large,
typically having dimensions higher than their standard, ahistorical
counterparts (the latter will be hereafter referred to as ahistorical
MPMs, or ahMPMs, while the acronym MPM will be used to refer to all
matrix projection models, whether historical or not). As this package
has developed, we have broadened the scope of this package to include
age-classified, age-by-stage, and stage-classified MPMs and IPMs, with
function-based MPMs and IPMs capable of handling a large range of
possible response distributions. We have also added the ability to
project matrices and IPMs in customized, complex ways. Through it all,
we have prioritized the development of core algorithms and methods to
construct these models and projections quickly, efficiently, and at
least relatively painlessly. Finally, we have incorporated quality
control routines in the core functions of all steps of the workflow,
giving users the opportunity to assess where weaknesses and errors lie.
Package lefko3
introduces a complete suite of functions
covering the MPM/IPM workflow, from dataset management to model
construction to the analysis of population dynamics. Dataset management
functions standardize demographic datasets from the dominant formats
into a format that facilitates matrix parameterization while accounting
for individual identity and other parameters. Demographic vital rate
models may be estimated using demographic datasets with this
standardized format, and these models take the form of generalized
linear or mixed linear models using a variety of response distributions.
Matrix estimation functions produce all necessary matrices from a single
dataset, including all times, patches, and populations in a single
output object, and do so quickly through core binaries engineered for
speed and accuracy. Deterministic and stochastic analysis functions
allow sensitivity analysis, elasticity analysis, LTRE analysis, etc.
Projection functions allow density dependent and independent with or
without enforced substochasticity, as well as stochastic, cyclical, and
replicated projections for even quite complex situations.
This vignette was written as a basic introduction to the concepts and
methods underlying lefko3
. The target audience is everyone
from beginners with little knowledge of population ecology and even less
of R, to experienced ecologists with advanced working knowledge
of R and the analysis of population dynamics. In addition to
this vignette, which covers the concepts, background, and workflow
underlying the package, we have created an online book entitled
lefko3: a gentle introduction, and a series of
vignettes focused on specific practical examples using the package to
run suites of comprehensive analyses. The book covers all major uses of
the package and contains lots of basic information and examples, and the
vignettes show the development of raw and function-based MPMs, IPMs, and
age-by-stage MPMs using two datasets included in lefko3
: a
dataset from a Swedish population of the perennial herb Lathyrus
vernus, and a dataset from an American population of the
terrestrial orchid Cypripedium candidum. In addition, we have
created a number of long-format vignettes and video tutorials. All of
these materials are available on the
projects page of
the Shefferson lab
website.
Matrix projection models (MPMs) are representations of the dynamics of a population across all life history stages deemed relevant, across the most relevant time interval (typically one year, but sometimes different, and assumed to be consistent within each analysis). They require a complete model of the organism’s life history prior to construction, and this model must explicitly describe all life stages and all life history transitions to be modeled. Each stage is mutually exclusive, meaning that an individual can only be in a single stage at a given time. Each stage is represented in the matrix by a single column and a single row. Each transition takes exactly one full time step, which needs to be defined consistently and should be equivalent to the approximate amount of time between consecutive monitoring occasions. Matrix elements (\(a_{kj}\)) show either the probability of transition for an individual in stage \(j\) at occasion t (along the columns), to stage \(k\) at occasion t+1 (along the rows), or the mean rate of production of new recruits into stage \(k\) at occasion t+1 (along the rows) by individuals in reproductive stage \(j\) in occasion t (along the columns). Conceptually, each individual is in a particular stage in the instance of monitoring or observation, and then either dies or completes a transition in the interval between that occasion’s observation and the next occasion’s observation. Death is not an explicit life stage and so is not modeled as such, instead becoming a potential endpoint of each transition.
Stages are generally defined under the assumption that they are unique moments in an organism’s life. This uniqueness is assumed to extend to the demography of the organism during its time within that stage. In some cases, stages are defined as developmental stages, as happens with insect instars. In other cases, stages are defined almost purely on the basis of size, as occurs with perennial herbs that may exhibit a different number of stems, leaves, and flowers in each growing season. In still other cases, stages may be defined via other characteristics. For example, the vegetative dormancy stage of some perennial herbs is defined by a lack of aboveground size, and so is characteristically not observable (Shefferson et al. 2001). In still other cases, age may also fall into a stage’s definition, as may the maturity status, observability, etc.
The timing of monitoring relative to the reproductive season impacts the structure of life history models. Life history models are typically categorized as either pre-breeding or post-breeding. Here, “breeding” refers to the production of offspring, and so a pre-breeding model assumes that monitoring is conducted immediately before the new recruits are born, while a post-breeding model assumes that the monitoring is conducted just after new recruits are born (in both cases, breeding is assumed to be seasonal). In a pre-breeding model, fecundity equals the production of newborns multiplied by the survival of newborns to age 1, since fecundity must take place over a full time step and the timing of the census misses both the birth event itself and the time in which the organism is a newborn (Kendall et al. 2019). In a post-breeding model, fecundity equals the survival of the parent from the stage/age preceding reproduction to reproduction itself, multiplied by the number of newborns produced (Kendall et al. 2019).
In monitoring studies of plant populations, the typical life history model a pre-breeding model, in which fecundity is estimated as the production of seeds in a given year multiplied by their over-winter survival probability as seeds and their germination probability in the following year. If the life history includes seed dormancy, then it is modeled by multiplying seed production by seed survival (which is given as the probability of maintaining seed viability from one year to the next), in the first instance, and then as seed survival for seeds already produced and dormant (seed survival may be modeled to decrease with increasing age of dormant seed). Added complexity can arise if there are multiple fecundity pathways, for example when clonal reproduction is also possible, or if multiple propagule stages exist, or if recruitment can be to seeds that immediately germinate as well as to seeds that are dormant for one or more years. We urge users to be careful with this step, as properly defining the life history model has important implications for all analyses of population dynamics (Kendall et al. 2019).
Figure 1 is a simple example of a stage-based life history model (technically a life cycle graph) and its associated Lefkovitch matrix for a terrestrial orchid species, Cypripedium candidum (Shefferson et al. 2001). Here, we show each stage as a node, and each transition as a uni-directional arrow (a). The rates and probabilities are shown as mathematical symbols in (b), with \(S_{kj}\) denoting survival-transition probability from stage \(j\) in occasion t to stage \(k\) in occasion t+1, and \(F_{kj}\) denoting the fecundity of reproductive stage \(j\) into recruit stage \(k\) in this life history.
Figure 1.1. Simple life history model (a) and ahistorical MPM (b) for Cypripedium candidum, a North American herbaceous plant species. Here, S is the dormant seed stage, J is the seedling stage, D is adult vegetative dormancy, V is adult vegetative sprouting, and F is flowering.
Figure 1b is an example of an ahistorical MPM (ahMPM), which is a matrix projection model in which the future stage of an individual is dependent only on its current stage, and not on previous stages. In other words, individual history is not incorporated into ahMPMs. It may seem odd that individual history is not incorporated into the matrices given that demographic datasets are composed of records of individual histories spanning several or even many observation events. However, construction of a typical ahMPM breaks up these individual histories into pairs of consecutive stages across time, with each pair treated as independent of every other pair of consecutive stages. For example, if an individual is in stage A in occasion 1, stage B in occasion 2, stage E in occasion 3, and dead in occasion 4, then its individual history is broken up into A-B, B-E, and E-Dead, with each pair assumed to be independent. The resulting projection matrix would be the same if these transitions originated from different individuals or the same one - their order and relationships do not have any impacts in ahMPM construction.
The matrix shown in figure 1.1 can be used to project population dynamics by predicting the future numbers of individuals in each stage. For this example, we can project forward by multiplying the projection matrix by a column vector of the numbers of individuals in each stage, given in the same order as the order of stages corresponding to the rows and columns of the matrix, in a particular time, as in
\[\begin{equation} \tag{1} \left[\begin{array} {rrrrr} n _{2,S} \\ n _{2,J} \\ n _{2,V} \\ n _{2,D} \\ n _{2,F} \end{array}\right] = \left[\begin{array} {rrrrr} S _{SS} & 0 & 0 & 0 & F _{SF} \\ S _{JS} & S _{JJ} & 0 & 0 & F _{JF} \\ 0 & S _{VJ} & S _{VV} & S _{VD} & S _{VF} \\ 0 & S _{DJ} & S _{DV} & S _{DD} & S _{DF} \\ 0 & 0 & S _{FV} & S _{FD} & S _{FF} \end{array}\right] \left[\begin{array} {rrrrr} n _{1,S} \\ n _{1,J} \\ n _{1,V} \\ n _{1,D} \\ n _{1,F} \end{array}\right] \end{equation}\]
where \(n _{1,S}\) is the number of individuals in stage \(S\) in occasion 1. The total population size in any given occasion is the sum of the numbers of individuals in all stages in that occasion. The actual discrete population growth rate is calculated as the ratio of total population size in occasion 2 to the total population size in occasion 1, and the asymptotic growth rate \(\lambda\) can be estimated as the dominant eigenvalue of this matrix.
The independence of consecutive stage-pairs reflects a central assumption in ahMPM analysis: the stage of an individual in the next occasion is influenced only by its current stage. Conceptually, if an organism’s stage in the next occasion is entirely determined by its current stage, then its previous states do not influence these transitions. Thus, standard ahMPMs are two dimensional and reflect only the current and next immediate stage of individuals, given by the columns and rows, respectively. This is ultimately an extension of the iid assumption in statistics - that the states of individuals are independent and originate from identically-distributed random variables.
MPMs have been estimated since the 1940s (Caswell 2001). We have never done a meta-analysis of all of these studies, but nonetheless it is safe to say that studies considering individual history are rare. The typical MPM study uses ahMPMs, and so assumes independence of stage transitions across time even from the same individual. In fact, at the time of writing, we are aware of only five examples of studies breaking these assumptions and using a historical approach, meaning that they incorporated some degree of individual history into matrix estimation and analysis (Ehrlén 2000; Shefferson, Warren II, and Pulliam 2014; Shefferson, Mizuta, and Hutchings 2017; Shefferson et al. 2018; deVries and Caswell 2018).
The historical MPM (hMPM) is an extension of the matrix projection model that incorporates information on one previous occasion into the determination of vital rates. Thus, the expected survival-transition probability of an individual in stage \(j\) at occasion t to stage \(k\) at occasion t+1 depends not only on its stage in occasion t but also on its stage in occasion t-1. Population ecologists considering this problem analytically might be inclined to add an extra dimension to the matrix to deal with this, thus creating a 3d array or cube. However, this is mathematically intractable, with many analyses becoming impossible (deVries and Caswell 2018). Instead, we utilize the approach developed by Ehrlén (2000), in which rows and columns represent life history stages paired in consecutive occasions. Thus, columns now represent the From pair of stages (stage in occasions t and t-1), and rows now represent the To pair of stages (stage in occasions t and t+1), as in Figure 1.2. This model is equivalent to the second-order model proposed by deVries and Caswell (2018), although the latter incorporates more history into transitions involving individuals just born (we explain the difference further in this vignette).
Figure 1.2. Historical MPM for Cypripedium candidum, a North American herbaceous plant.
Here, we can refer to matrix elements as \(a_{kjl}\), where the element represents the rate at which individuals transition to stage \(k\) in occasion t+1 after having been stage \(j\) in occasion t and stage \(l\) in occasion t-1. If \(n_{kjl}\) is the number of individuals making this transition, \(n_{.jl}\) is the total number of individuals in stage \(j\) in occasion t and stage \(l\) in occasion t-1 regardless of stage or even status as alive or dead in occasion t+1, \(m\) is the number of stages in the life history model, and \(d\) is the number of stages plus death in the life history model (so \(d=m+1\)), then we have
\[\begin{equation} \tag{2} a _{kjl} = \frac{n _{kjl}}{n _{.jl}} = \frac{n _{kjl}}{\sum_{i=1}^{d} n _{ijl}} \end{equation}\]
These values can be used to determine the associated elements of matrices in ahistorical MPMs, as follows:
\[\begin{equation} \tag{3} a _{kj} = \frac{\sum_{l=1}^{m} n _{kjl}}{\sum_{l=1}^{m} \sum_{i=1}^{d} n _{ijl}} \end{equation}\]
Note that although one can use the actual numbers of individuals making historical transitions to estimate ahistorical MPMs, one cannot use the matrix elements in a historical MPM to calculate the associated ahistorical MPM elements (and vice versa). Historical transitions must be weighted by the numbers of individuals corresponding to each transition from occasion t to t+1 that were in each previous stage to produce the correct ahistorical matrix element. Historical matrix elements are equal only to the ratios of numbers of individuals in these categories, rather than to the numbers of individuals themselves, and contain no information allowing the inference of the latter.
Historical MPMs can be projected forward in the same way that ahMPMs can. Here we see an example of a projection going forward one time step, using the hMPM shown in figure 1.2.
\[\begin{equation} \tag{4} \tiny \left[\begin{array} {rrrrrrrrrrrrrrrrr} n _{2,SS} \\ n _{2,JS} \\ n _{2,JJ} \\ n _{2,VJ} \\ n _{2,DJ} \\ n _{2,FJ} \\ n _{2,VV} \\ n _{2,DV} \\ n _{2,FV} \\ n _{2,VD} \\ n _{2,DD} \\ n _{2,FD} \\ n _{2,VF} \\ n _{2,DF} \\ n _{2,FF} \\ n _{2,SF} \\ n _{2,JF} \end{array}\right] = \left[\begin{array} {rrrrrrrrrrrrrrrrr} S _{SSS} & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & F _{SSF} & 0 \\ S _{JSS} & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & F _{JSF} & 0 \\ 0 & S _{JJS} & S _{JJJ} & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & F _{JJF} \\ 0 & S _{VJS} & S _{VJJ} & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & F _{VJF} \\ 0 & S _{DJS} & S _{DJJ} & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & F _{DJF} \\ 0 & S _{FJS} & S _{FJJ} & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & F _{FJF} \\ 0 & 0 & 0 & S _{VVJ} & 0 & 0 & S _{VVV} & 0 & 0 & S _{VVD} & 0 & 0 & S _{VVF} & 0 & 0 & 0 & 0 \\ 0 & 0 & 0 & S _{DVJ} & 0 & 0 & S _{DVV} & 0 & 0 & S _{DVD} & 0 & 0 & S _{DVF} & 0 & 0 & 0 & 0 \\ 0 & 0 & 0 & S _{FVJ} & 0 & 0 & S _{FVV} & 0 & 0 & S _{FVD} & 0 & 0 & S _{FVF} & 0 & 0 & 0 & 0 \\ 0 & 0 & 0 & 0 & S _{VDJ} & 0 & 0 & S _{VDV} & 0 & 0 & S _{VDD} & 0 & 0 & S _{VDF} & 0 & 0 & 0 \\ 0 & 0 & 0 & 0 & S _{DDJ} & 0 & 0 & S _{DDV} & 0 & 0 & S _{DDD} & 0 & 0 & S _{DDF} & 0 & 0 & 0 \\ 0 & 0 & 0 & 0 & S _{FDJ} & 0 & 0 & S _{FDV} & 0 & 0 & S _{FDD} & 0 & 0 & S _{FDF} & 0 & 0 & 0 \\ 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & S _{VFV} & 0 & 0 & S _{VFD} & 0 & 0 & S _{VFF} & 0 & 0 \\ 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & S _{DFV} & 0 & 0 & S _{DFD} & 0 & 0 & S _{DFF} & 0 & 0 \\ 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & S _{FFV} & 0 & 0 & S _{FFD} & 0 & 0 & S _{FFF} & 0 & 0 \\ 0 & 0 & 0 & 0 & 0 & F _{SFJ} & 0 & 0 & F _{SFV} & 0 & 0 & F _{SFD} & 0 & 0 & F _{SFF} & 0 & 0 \\ 0 & 0 & 0 & 0 & 0 & F _{JFJ} & 0 & 0 & F _{JFV} & 0 & 0 & F _{JFD} & 0 & 0 & F _{JFF} & 0 & 0 \\ \end{array}\right] \left[\begin{array} {rrrrrrrrrrrrrrrrr} n _{1,SS} \\ n _{1,JS} \\ n _{1,JJ} \\ n _{1,VJ} \\ n _{1,DJ} \\ n _{1,FJ} \\ n _{1,VV} \\ n _{1,DV} \\ n _{1,FV} \\ n _{1,VD} \\ n _{1,DD} \\ n _{1,FD} \\ n _{1,VF} \\ n _{1,DF} \\ n _{1,FF} \\ n _{1,SF} \\ n _{1,JF} \end{array}\right] \end{equation}\]
Here, \(n _{1,SS}\) is the number of individuals that were in stage \(S\) in both occasions 0 and 1, and \(n _{2,DF}\) is the number of individuals that were in stage \(D\) in occasion 2 and stage \(F\) in occasion 1.
Historical MPMs normally require a much larger number of elements to be parameterized than ahMPMs do. Figure 1.2 illustrates this issue, but the function-based matrix analysis in our Cypripedium candidum vignette provides a more realistic example. In that case study, we use a life history with 54 life stages, of which the first is a dormant seed stage, the next four are immature stages, the sixth is adult vegetative dormancy, the next 24 stages are size-classified non-flowering adults, and the final 24 stages are size-classified flowering adults. A life history with 54 stages yields an ahistorical matrix with 54 columns and 54 rows, and so 2,916 elements. A full historical matrix should have \(54 \times 54 = 2,916\) columns and 2,916 rows, consisting of 8,503,056 elements, because the column and row stages represent pairs of stages.
In an ahistorical matrix, the only true zeros will be those elements corresponding to biologically impossible transitions, or, in the raw matrix case, those elements without any individuals taking the respective transition in a given time step. However, most elements in a historical MPM are structural zeros. This happens because transition elements in hMPMs are only estimable if stage at occasion t is equal in the column and row stage pairs. For example, the transition probability between stage A in occasion t-1 and stage B in occasion t (column stage), to stage C in occasion t and stage D in occasion t+1 (row stage) equals 0, because an organism cannot be in both stages B and C in occasion t. Increasing the number of stages in a life history model causes these structural zeros to increase at a faster rate than the rate at which the number of truly estimable elements increases. In fact, if there are \(m\) stages in a life history, yielding \(m^2\) elements in an ahistorical matrix, then although there will be \(m^4\) elements in the historical matrix, only \(m^3\) will be potentially estimable while \((m-1)m^3\) are structural zeros (we say potentially because some of the logically possible transitions may still be biologically impossible, or may have no data to yield values other than 0). Thus, in the Cypripedium candidum example, all 2,916 elements of the ahMPM are potentially estimable (although some are biologically impossible), while only 157,464 of the 8,503,056 elements of the associated hMPM are potentially estimable and the rest are structural zeros.
Matrix projection models, whether historical or ahistorical, can also be categorized as either raw or function-based. The oldest and most common in the literature is the raw MPM, in which transition probabilities in the matrix are estimated by counting all of the individuals alive in a particular stage at occasion t, and dividing that number into the number of individuals from that set that are still alive in each possible stage in occasion t+1 (equations 2 and 3). For example, if 100 individuals are alive in stage D in year 2010, and 20 of these are alive in stage D in year 2011, as are a further 40 in stage V and a further 25 in stage F, then the associated transition probabilities are 0.20, 0.40, and 0.25, respectively. The overall survival probability for stage D is the sum of these transitions, or 0.85.
Methods for estimating fecundity in raw matrices vary. In the Cypripedium candidum vignette, we used counts of the number of fruits produced by each individual in a given year, and multiplied by the mean number of seeds per fruit and the mean germination probability in the next year. This study was conducted as a pre-breeding census - fecundity was estimated using a count of the seeds or other propagules that the plant produces (or a proxy thereof, such as the number of fruits multiplied by the mean number of seeds per fruit) multiplied by the probability of that propagule surviving to the next year in order to make sure that fecundity reflects demographic processes across a full time step (Kendall et al. 2019). In other systems in which offspring may be observed and tracked, counts of actual recruits may be possible, such as in studies of nesting birds, and as in Lathyrus vernus, an herbaceous perennial plant that is the subject of some vignettes included in this package.
In function-based MPMs, matrix elements are populated by kernels that link together functions representing key demographic processes governing each transition. Typically, demographic datasets are analyzed via linear models to estimate demographic parameters such as survival probability, the probability of becoming a certain size assuming survival, and fecundity. These linear models are developed using nested subsets of the demographic data used in a study in order to estimate conditional probabilities reflecting all of the demographic processes that must occur over the span of a single time step. Matrix elements are then estimated as products of responses from these linear models set to particular inputs corresponding to stage at occasion t and occasion t+1, as well as any other parameters governing the construction of the matrix. Function-based MPMs are more recent inventions than raw MPMs, and their strengths are making them increasingly common in the literature.
Easterling, Ellner, and Dixon (2000)
proposed a method of analyzing population dynamics called the
integral projection model (IPM), which modeled the life
history of an organism using a continuous size metric modeled on a
Gaussian distribution. At least theoretically, the aim was to produce a
model that was not contingent on a stage classification together with a
function-based kernel to model population dynamics. In practice,
however, size was and is discretized into many fine-scale size classes.
The result is that, in practice, IPMs are actually high resolution
function-based MPMs, breaking up a life history into many fine-scale
size classes using a continuous measure of size and then estimating
survival-transitions and fecundity according to these fine-scale size
classes (Ellner and Rees 2006). Package
lefko3 easily handles the creation and analysis of IPMs. We
include a vignette in lefko3
showing an example, and also
devote a chapter of the free e-book lefko3: a gentle
introduction to the topic.
The example from Figures 1.1 and 1.2 may help to illustrate the procedure of creating a function-based MPM. In Cypripedium candidum, the simple life history model shown in Figure 1 includes one adult stage that is not observable (D - vegetative dormancy), one adult stage that is observable but not reproductive (V - vegetative sprouting), and one adult stage that is both observable and reproductive (F - flowering). If \(\sigma _{.jl}\) is the probability of survival from stage \(j\) in occasion t and stage \(l\) in occasion t-1 to any stage in occasion t+1, \(\rho _{.jl}\) is the probability of sprouting in occasion t+1 after being stage \(j\) in occasion t and stage \(l\) in occasion t-1 and surviving to occasion t+1, and \(\gamma _{.jl}\) is the probability of flowering in occasion t+1 after being stage \(j\) in occasion t and stage \(l\) in occasion t-1 and surviving to and sprouting in occasion t+1, then
\[\begin{equation} \tag{5} a _{DDD} = \sigma _{.DD} (1 - \rho _{.DD}) \end{equation}\]
\[\begin{equation} \tag{6} a _{VDD} = \sigma _{.DD} \rho _{.DD} (1 - \gamma _{.DD}) \end{equation}\]
\[\begin{equation} \tag{7} a _{FDD} = \sigma _{.DD} \rho _{.DD} \gamma _{.DD} \end{equation}\]
In both raw and function-based MPMs, most estimated elements are survival-transition probabilities. In ahMPMs, these give the probability of an individual in stage \(j\) at occasion t surviving and transitioning to stage \(k\) at occasion t+1. Fewer elements are devoted to fecundity, although life history models with more reproductive stages and more recruit stages will have more fecundity elements. In Figure 1.1, fecundity is shown in the top-right of the matrix, as the mean production of seeds either dormant or germinating in the next occasion. Ignoring the fecundity elements, we have a survival-transition matrix (symbolized as either U or T), in which the column sums correspond to the expected survival probabilities of individuals in each stage from occasion t to occasion t+1. Ignoring the survival-transition terms, we have the fecundity matrix (symbolized as F), in which the column sums correspond to the expected overall time-specific fecundity of individuals in these respective stages. The full MPM (symbolized as A) is the matrix sum of the survival-transition matrix and the fecundity matrix.
In principle, everything just noted about function-based ahMPMs also applies to function-based hMPMs. However, there is a key difference in terms of the distribution of elements within the matrix. The inclusion of stage or condition in occasion t-1 increases both the number of survival-transition elements and the number of fecundity elements, and also has the effect of dispersing the locations of these elements across the matrix. Whereas estimated transitions in ahMPMs will generally occur in dense patches of estimated elements, in hMPMs, most elements are structural zeros, with elements occurring either individually surrounded by zeros, or in small patches of estimated elements surrounded by zeros. This makes error-checking more challenging, because the user needs to be aware of where elements are supposed to occur in order to check their values properly.
deVries and Caswell (2018) detail different approaches to the development of hMPMs, differing in how state or stage in occasion t-1 is incorporated into the matrix. Full prior stage dependence models deal with history by incorporating prior condition as the exact stage of an organism in occasion t-1, yielding a matrix showing stage pairs in occasion t-1 and t along the columns of the matrix, and stage pairs in occasion t and t+1 along the rows of the matrix. Prior condition models deal with history by making the transition from stage t to stage t+1 a function of stage at occasion t and condition in occasion t-1. Prior condition can be determined in the same way that current stage is determined (e.g. size classification), or a different measure of condition can be used, such as growth (i.e. the change in size between occasions t-1 and t).
One key feature proposed by deVries and Caswell (2018) is the addition of a new stage to account for the prior status of newborn individuals. This reflects a slightly different interpretation from Ehrlén (2000) of the historical transition. In Ehrlén (2000), all matrix elements simply reflect the order of the events in a single transition, including both fecundity and survival-transition events. However, in deVries and Caswell (2018), these matrix elements must also reflect the history of specific individuals. In the latter case, the fact that a newborn in occasion t did not exist in occasion t-1 leads to the creation of a new prior stage to account for the time immediately prior to birth. This new stage only exists in the immediate prior occasion, and is only used for newborns in the first survival transition from birth. So, for example, in a three stage MPM where the 1st stage is the newborn stage and only the 3rd stage is reproductive, we add a 4th stage to the prior portion of the row and column. Thus, we may start with the following hMPM in Ehrlén (2000) format:
\[\begin{equation} \tag{8} \tiny \left[\begin{array} {rrrrrrrrr} n _{2,AA} \\ n _{2,BA} \\ n _{2,CA} \\ n _{2,AB} \\ n _{2,BB} \\ n _{2,CB} \\ n _{2,AC} \\ n _{2,BC} \\ n _{2,CC} \end{array}\right] = \left[\begin{array} {rrrrrrrrr} S _{AAA} & 0 & 0 & S _{AAB} & 0 & 0 & S _{AAC} & 0 & 0 \\ S _{BAA} & 0 & 0 & S _{BAB} & 0 & 0 & S _{BAC} & 0 & 0 \\ S _{CAA} & 0 & 0 & S _{CAB} & 0 & 0 & S _{CAC} & 0 & 0 \\ 0 & S _{ABA} & 0 & 0 & S _{ABB} & 0 & 0 & S _{ABC} & 0 \\ 0 & S _{BBA} & 0 & 0 & S _{BBB} & 0 & 0 & S _{BBC} & 0 \\ 0 & S _{CBA} & 0 & 0 & S _{CBB} & 0 & 0 & S _{CBC} & 0 \\ 0 & 0 & S _{ACA} + F _{ACA} & 0 & 0 & S _{ACB} + F _{ACB} & 0 & 0 & S _{ACC} + F _{ACC} \\ 0 & 0 & S _{BCA} & 0 & 0 & S _{BCB} & 0 & 0 & S _{BCC} \\ 0 & 0 & S _{CCA} & 0 & 0 & S _{CCB} & 0 & 0 & S _{CCC} \\ \end{array}\right] \left[\begin{array} {rrrrrrrrr} n _{1,AA} \\ n _{1,BA} \\ n _{1,CA} \\ n _{1,AB} \\ n _{1,BB} \\ n _{1,CB} \\ n _{1,AC} \\ n _{1,BC} \\ n _{1,CC} \end{array}\right] \end{equation}\]
This hMPM becomes as follows in deVries and Caswell (2018) format:
\[\begin{equation} \tag{9} \tiny \left[\begin{array} {rrrrrrrrrrrr} n _{2,AA} \\ n _{2,BA} \\ n _{2,CA} \\ n _{2,AB} \\ n _{2,BB} \\ n _{2,CB} \\ n _{2,AC} \\ n _{2,BC} \\ n _{2,CC} \\ n _{2,AP} \\ n _{2,BP} \\ n _{2,CP} \end{array}\right] = \left[\begin{array} {rrrrrrrrrrrr} S _{AAA} & 0 & 0 & S _{AAB} & 0 & 0 & S _{AAC} & 0 & 0 & S _{AA,AP} & 0 & 0 \\ S _{BAA} & 0 & 0 & S _{BAB} & 0 & 0 & S _{BAC} & 0 & 0 & S _{BA,AP} & 0 & 0 \\ S _{CAA} & 0 & 0 & S _{CAB} & 0 & 0 & S _{CAC} & 0 & 0 & S _{CA,AP} & 0 & 0 \\ 0 & S _{ABA} & 0 & 0 & S _{ABB} & 0 & 0 & S _{ABC} & 0 & 0 & 0 & 0 \\ 0 & S _{BBA} & 0 & 0 & S _{BBB} & 0 & 0 & S _{BBC} & 0 & 0 & 0 & 0 \\ 0 & S _{CBA} & 0 & 0 & S _{CBB} & 0 & 0 & S _{CBC} & 0 & 0 & 0 & 0 \\ 0 & 0 & S _{ACA} & 0 & 0 & S _{ACB} & 0 & 0 & S _{ACC} & 0 & 0 & 0 \\ 0 & 0 & S _{BCA} & 0 & 0 & S _{BCB} & 0 & 0 & S _{BCC} & 0 & 0 & 0 \\ 0 & 0 & S _{CCA} & 0 & 0 & S _{CCB} & 0 & 0 & S _{CCC} & 0 & 0 & 0 \\ 0 & 0 & F _{AP,CA} & 0 & 0 & F _{AP,CB} & 0 & 0 & F _{AP,CC} & 0 & 0 & 0\\ 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 \\ 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 & 0 \\ \end{array}\right] \left[\begin{array} {rrrrrrrrrrrr} n _{1,AA} \\ n _{1,BA} \\ n _{1,CA} \\ n _{1,AB} \\ n _{1,BB} \\ n _{1,CB} \\ n _{1,AC} \\ n _{1,BC} \\ n _{1,CC} \\ n _{1,AP} \\ n _{1,BP} \\ n _{1,CP} \end{array}\right] \end{equation}\]
Note that matrix 9 above can be reduced by two rows and two columns, since transitions from the newborn prior stage (P) can only be to the newborn stage (A).
Package lefko3
generally implements the full prior
stage dependence model approach, particularly in the
development of raw matrices. However, in principle, function-based
matrices developed with lefko3
can be seen as falling
within the prior condition model approach where prior
condition is determined in the same way as current stage. We also
implement both the Ehrlén (2000) format
and the deVries and Caswell (2018) format,
and use the former as the default. We leave it to the user to decide
which approach to use.
deVries and Caswell (2018) also suggest
that hMPMs can be organized differently to yield more intuitive models.
In particular, matrices may be as organized as block matrices where the
component blocks are essentially matrices showing the transitions from
all stages in occasion t to stages in occasion t+1
conditioned on individuals having been in the same stage in occasion
t-1. We refer to these block component matrices as
conditional matrices, since they show transitions from
occasion t to occasion t+1 conditional on the same
previous stage in occasion t-1. We have developed function
cond_hmpm()
to take full hMPMs and decompose them into
their associated conditional matrices.
Some population biologists working with lefko3
may wish to
produce Leslie matrices, which classify an organism only by age. A
Leslie matrix has the following general form
\[\begin{equation} \tag{10} \tiny \left[\begin{array} {rrrrrrr} n _{2, 0} \\ n _{2, 1} \\ n _{2, 2} \\ n _{2, 3} \\ \vdots \\ n _{2, a-1} \\ n _{2, a} \end{array}\right] = \left[\begin{array} {rrrrrrr} 0 & F _1 & F _2 & F _3 & \cdots & F _{a-1} & F _a \\ S _{1,0} & 0 & 0 & 0 & \cdots & 0 & 0 \\ 0 & S _{2,1} & 0 & 0 & \cdots & 0 & 0 \\ 0 & 0 & S _{3,2} & 0 & \cdots & 0 & 0 \\ \vdots & & & & & & \vdots \\ 0 & 0 & 0 & 0 & \cdots & 0 & S _{5+B,4C} \\ 0 & 0 & 0 & 0 & \cdots & S _{a,a-1} & S _{>a,a} \\ \end{array}\right] \left[\begin{array} {rrrrrrr} n _{1, 0} \\ n _{1, 1} \\ n _{1, 2} \\ n _{1, 3} \\ \vdots \\ n _{1, a-1} \\ n _{1, a} \end{array}\right] \end{equation}\]
Here, \(n _{2, 0}\) refers to the
number of newborn (age = 0) individuals in time 2, \(a\) is the final age in the model, \(S _{1, 0}\) is the survival probability of
a newborn individual (age = 0) to the next age, \(F _1\) is the fecundity of an individual in
age 1, and \(S _{>a, a}\) is the
survival of individuals in the final modeled age to the next age (and
later). Note that in Leslie models, survival transitions are always just
below the diagonal or in the final lower-right element of the diagonal,
and fecundity transitions are always in the top row. Note also that
age-classified models are inherently ahistorical, and so no historical
models are possible. Package lefko3
estimates both raw and
function-based forms of these.
Package lefko3
can also handle the estimation and analysis
of age-by-stage MPMs. These matrices incorporate both stages (whether
size-classified or not), as well as the ages in which they occur. For
example, in a three stage life history with a single newborn stage and
two adult stages, only one of which is reproductive (as in equations 1,
4, 8, and 9), and in which age impacts survival and fecundity only for
the first 4 years, beyond which survival and fecundity transitions
remain the same, we have the following ahistorical age-by-stage matrix.
\[\begin{equation} \tag{11} \tiny \left[\begin{array} {rrrrrrr} n _{2,1A} \\ n _{2,2B} \\ n _{2,2C} \\ n _{2,3B} \\ n _{2,3C} \\ n _{2,4B} \\ n _{2,4C} \end{array}\right] = \left[\begin{array} {rrrrrrr} 0 & 0 & F _{1A,2C} & 0 & F _{1A,3C} & 0 & F _{1A,4+C} \\ S _{2B,1A} & 0 & 0 & 0 & 0 & 0 & 0 \\ S _{2C,1A} & 0 & 0 & 0 & 0 & 0 & 0 \\ 0 & S _{3B,2B} & S _{3B,2C} & 0 & 0 & 0 & 0 \\ 0 & S _{3C,2B} & S _{3C,2C} & 0 & 0 & 0 & 0 \\ 0 & 0 & 0 & S _{4B,3B} & S _{4B,3C} & S _{5+B,4B} & S _{5+B,4C} \\ 0 & 0 & 0 & S _{4C,3B} & S _{4C,3C} & S _{5+C,4B} & S _{5+C,4C} \\ \end{array}\right] \left[\begin{array} {rrrrrrr} n _{1,1A} \\ n _{1,2B} \\ n _{1,2C} \\ n _{1,3B} \\ n _{1,3C} \\ n _{1,4B} \\ n _{1,4C} \end{array}\right] \end{equation}\]
The above matrix is ahistorical. Package lefko3
does not
currently support historical age-by-stage matrices, although they are
certainly possible.
The basic workflow to analysis with package lefko3
starts
with the development of a life history model that encapsulates all of
the appropriate life stages relevant to population dynamics. We do not
present a complete discussion on this step, instead focusing on a sketch
of the process focused on the life cycle graph and noting key issues
related to this package. We encourage users to explore the literature on
this subject, but particularly note chapters 3 and 4 in Caswell (2001) for a good treatment useful for
beginners. Stages need to be defined carefully, and should strongly
account for variability in vital rates. Statistical approaches such as
Jenks natural breaks optimization can help determine ideal
“natural” breaks in the distribution of size data to act as borders
between size-classified stages in raw MPMs (Jenks
1967). In contrast, stages within function-based MPMs are more
straightforward to define, with regular breaks across the size spectrum.
We also note Kendall et al. (2019) as a
good reference detailing common problems in MPM construction and how to
avoid them through proper development and operationalization of life
history models. Beissinger and Westphal
(1998), Wardle (1998), and Salguero-Gómez and Casper (2010) provide good
discussions of the proper application of life history models to
understand population dynamics through the MPM approach.
Here we utilize a life cycle graph approach to build a life history model. A life cycle graph shows the life history of an organism as a series of nodes and arrows. The nodes represent unique stages that the individual may go through during development, and individuals are noted as occurring in these stages during monitoring sessions conducted over a roughly or strictly regular frequency, such as at the start of the growing season every year, or over specific dates each year. Arrows represent transitions between stages across consecutive occasions. These may be interpreted either as probabilities of survival when reflecting the individual’s stage across time, or as rates when reflecting the production of offspring. A good life cycle graph, and in general a good life history model, must explicitly include representations of all stages possible for the organism to enter, and all biologically plausible transitions between these transitions. Figure 1a shows an example of a life cycle graph.
The construction of a good life history model is not as easy as it might appear, particularly because it can be influenced by factors seemingly external to the life history of the organism. Some of the most important considerations outside of the species’ biology include the size of the dataset, and the decision of whether to create a raw MPM or a function-based MPM. All else being equal, a larger dataset and a function-based MPM will allow more stages to be used in the life history. Assuming a dataset of fixed size, raw MPMs will include more and more zeros as the number of stages in the life history model increases. This happens because the chance of having any individuals actually move through a specific transition decreases as the number of possible transitions increases. These functional zeros that become increasingly common with increasing stages can cause problems in analysis, because they suggest that some transitions are impossible when, in fact, individuals moving through them were missing just by chance. Even a transition with extremely high probability may be missing in some years just by chance. One impact of this would be the reduction of the mean transition within an element-wise mean matrix to an unrealistic level, causing the predicted population growth rate to be artificially low.
Function-based MPMs are better able to handle large numbers of matrix elements because the risk of overparameterization is reduced by parsimonious model selection when vital rate models are determined. However, the size of the dataset influences the statistical power of these vital rate models, with smaller datasets yielding larger error associated with matrix elements and hence a loss of variability with potentially important factors. Loss of statistical power in vital rate models can lead to the loss of important process variance, and can make the population appear more static than it really is. Further, developing function-based MPMs for life history models that include stages rarely or never actually observed can yield problematic inferences, such as matrices suggesting that some stages have survival probabilities greater than 1.0. Chapter 6 in Morris and Doak (2002) provides a good description of techniques that may be used to define stages and to determine the exact number to use given the context imposed by a given dataset of a given size. Ellner and Rees (2006) and Doak et al. (2021) provide some discussion of this issue within the context of integral projection model development.
Once a life history model is developed, we need to characterize the main
life stages in a way that is relevant to the dataset. We do this with
the sf_create()
function, which creates a
stageframe object. This term is a combination of the
terms life history stage and data frame, and the
object itself is a data frame that describes all of the life history
stages. This object is created in a way that shows how stage relates to
size, reproductive status, observation status, propagule status,
maturity status, entry status (i.e. a stage’s ability to serve as the
first stage of an individual’s life), and presence in the dataset, and
in which the description of each life stage is unique. A good stageframe
describes stages in ways that matrix-estimating functions utilize to
compute elements accurately, and also allows the user to stipulate extra
descriptive information on each stage as text. If the user wishes to
create an IPM or a function-based MPM with many stages, then this
function also allows stage definition to be automated.
Once the stageframe has been created, the demographic data needs to be
organized into a format that lefko3
can use. The proper
format is one that we term historically-formatted vertical
format, or hfv format for short. We have
developed two functions for this purpose, depending on the original
format of the data. If the data is arranged horizontally,
meaning that individual life histories are recorded in a spreadsheet in
which each unique individual’s data is organized within a single row,
where columns correspond to descriptor variables and to condition at
different times, then the verticalize3()
function can
standardize this dataset into the proper format. If the dataset is in
vertical, ahistorical format, in which an individual’s
condition across time is recorded across rows in a spreadsheet, with a
single row corresponding to either a single observation or to a pair of
consecutive observations, then the historicalize3()
function can standardize the dataset properly. These functions both can
also add some new variables that might be of use. For example, both
functions can estimate radial density if Cartesian coordinates for each
datum and a radius are provided. Both functions are powered by binaries
built in C++ using single control loops to propagate each data frame
properly and efficiently, and so run very quickly (typically under 1s on
a 2019 MacBook Pro). The case studies included in lefko3
illustrate the usage of these functions on real data. The function
summary_hfv()
can be used to provide quick details about
the resulting standardized datasets.
MPMs are often estimated only partially from available demographic
datasets. Some transitions are parameterized using information gathered
from other studies, whether through direct input in the matrix or
through the development of kernels contingent on external information.
Other transitions might also be estimated via proxy transitions
elsewhere in the matrix. In lefko3
, this information can be
provided in one of two ways. The preferred, and most recently developed,
method is through the supplement table, which can be
developed using the supplemental()
function. This function
allows users to create a data frame detailing:
Examples might illustrate where this approach is useful. If I lack my own data on subterranean juvenile stages in a plant species, but I have estimates of survival for those stages form another study, then I might use those estimates as constants in the MPM. I can also set some transitions explicitly to 0 if I believe that there is a biological need for such an override. Further, if I lack demographic data on the development of germinated seeds to the seedling or earliest adult stage, but I have reason to believe that the survival probabilities should be similar to the survival within an observed stage of seedlings or small adults, then I can use the latter survival-transitions as proxies (or even decrease them via a multiplier). Finally, if fecundity is a function of seed production, survival to the next year, and germination probability, then germination probability might be estimated via a separate field germination study. I might wish to incorporate this germination probability both as a constant transition, and as a multiplier on estimated fecundity. Supplement tables provide the means to include all of this information.
Historical MPMs are not necessarily justified in all cases. We urge the
reader to use the principle of parsimony in deciding this. For example,
users may analyze whether lagged effects of previous stage appear to
influence vital rates. Package lefko3
includes one method
to do this based on linear modeling. A number of other methods exist,
mostly focused on what are known as memory models (Brownie et al. 1993; Pradel, Wintrebert, and Gimenez
2003; Cole et al. 2014). Here, we focus only on the main
lefko3
method, and leave it to the reader to explore other
options.
In lefko3
, function modelsearch()
allows users
to explore whether history influences component vital rates, and to
develop linear models of these vital rates. The results can be used to
decide not only whether a historical MPM is justified, but also to
develop function-based hMPMs and ahMPMs themselves. Package
lefko3
can estimate linear models to estimate up to
fourteen different vital rates:
Survival probability - This is the probability
of surviving from occasion t to occasion t+1, given
that the individual is in stage \(j\)
in occasion t (and, if historical, in stage \(l\) in occasion t-1). In
lefko3
, this parameter may be modeled as a function of up
to three size metrics, reproductive status, patch, year, age, and a
number of individual or environmental covariates in occasions t
and t-1, and individual identity. This parameter is required in
all function-based matrices.
Observation probability - This is an optional
parameter denoting the probability of observation in occasion
t+1 of an individual in stage \(k\) given survival from occasion t
to occasion t+1. This parameter is only used when at least one
stage is not observable. For example, some plants are capable of
vegetative dormancy, in which case they are alive but do not necessarily
sprout in all years in which they are in this stage. In these cases, the
probability of sprouting may be estimated as the observation
probability, and its complement is the probability of becoming dormant
assuming survival. Note that this probability does not refer to observer
effort, and so should only be used to differentiate completely
unobservable stages where the observation status refers to an important
biological phenomenon, such as when individuals may be alive but have a
size of 0. In lefko3
, this parameter may be modeled as a
function of up to three size metrics, reproductive status, patch, year,
age, and a number of individual or environmental covariates in occasions
t and t-1, and individual identity.
Primary size transition probability - This is
the probability of becoming size \(k\)
in occasion t+1 assuming survival from occasion t to
occasion t+1 and observation in that time. In
lefko3
, this parameter may be modeled as a function of up
to three size metrics, reproductive status, patch, year, age, and a
number of individual or environmental covariates in occasions t
and t-1, and individual identity.
Secondary size transition probability - This is
the probability of becoming size \(k\)
in occasion t+1 assuming survival from occasion t to
occasion t+1 and observation in that time, within a second size
metric used for classification in addition to the primary metric. In
lefko3
, this parameter may be modeled as a function of up
to three size metrics, reproductive status, patch, year, age, and a
number of individual or environmental covariates in occasions t
and t-1, and individual identity.
Tertiary size transition probability - This is
the probability of becoming size \(k\)
in occasion t+1 assuming survival from occasion t to
occasion t+1 and observation in that time, within a third size
metric used for classification in addition to the primary and secondary
metrics. In lefko3
, this parameter may be modeled as a
function of up to three size metrics, reproductive status, patch, year,
age, and a number of individual or environmental covariates in occasions
t and t-1, and individual identity.
Reproduction probability - This is an optional
parameter denoting the probability of reproducing in occasion
t+1 given survival from occasion t to occasion
t+1, and observation in that time. Note that this should be
used only if the researcher wishes to separate breeding from
non-breeding mature stages. If all adult stages are potentially
reproductive and no separation of reproducing from non-reproducing
adults is desired, then this parameter should not be estimated. In
lefko3
, this parameter may be modeled as a function of up
to three size metrics, reproductive status, patch, year, age, and a
number of individual or environmental covariates in occasions t
and t-1, and individual identity.
Fecundity rate - Under the default setting, this
is the rate of successful production of offspring in occasion t
by individuals alive, observable, and reproductive in that time, and, if
desired and sufficient information is provided in the dataset, the
survival of those offspring into occasion t+1 in whatever
juvenile class is possible. Thus, the fecundity rate of seed-producing
plants might be split into seedlings, which are plants that germinated
within a year of seed production, and dormant seeds. Alternatively, it
may be given only as produced fruits or seeds, with the survival and
germination of seeds provided elsewhere in the MPM development process,
such as within a supplement table. An additional setting allows
fecundity rate to be estimated using data provided for occasion
t+1 instead of occasion t. In lefko3
,
this parameter may be modeled as a function of up to three size metrics,
reproductive status, patch, year, age, and a number of individual or
environmental covariates in occasions t and t-1, and
individual identity.
Juvenile survival probability - This is an
optional parameter that is used to model the probability of surviving
from juvenile stage \(j\) in occasion
t to occasion t+1. It is used only when the user
wishes to model juvenile vital rates separately from adults, assuming
different relationships with explanatory variables than those used to
classify adults. In lefko3
, this parameter may be modeled
as a function of up to three size metrics, patch, year, and a number of
individual or environmental covariates in occasions t and
t-1, and individual identity.
Juvenile observation probability - This is an
optional parameter denoting the probability of observation in occasion
t+1 of an individual in mature stage \(k\) given survival from a juvenile stage in
occasion t to occasion t+1. It is used only when the
user wishes to model juvenile vital rates separately from adults,
assuming different relationships with explanatory variables than those
used to classify adults. In lefko3
, this parameter may be
modeled as a function of up to three size metrics, patch, year, and a
number of individual or environmental covariates in occasions t
and t-1, and individual identity, and all other caveats noted
in (2) above apply.
Juvenile primary size transition probability -
This is an optional parameter denoting the probability of becoming
mature size \(k\) in occasion
t+1 assuming survival from juvenile stage \(j\) in occasion t to occasion
t+1 and observation in that time. It is used only when the user
wishes to model juvenile vital rates separately from adults, assuming
different relationships with explanatory variables than those used to
classify adults. In lefko3
, this parameter may be modeled
as a function of up to three size metrics, patch, year, and a number of
individual or environmental covariates in occasions t and
t-1, and individual identity.
Juvenile secondary size transition probability -
This is an optional parameter denoting the probability of becoming
mature size \(k\) in occasion
t+1 assuming survival from juvenile stage \(j\) in occasion t to occasion
t+1 and observation in that time, in a secondary size metric in
addition to the primary size metric. It is used only when the user
wishes to model juvenile vital rates separately from adults, assuming
different relationships with explanatory variables than those used to
classify adults. In lefko3
, this parameter may be modeled
as a function of up to three size metrics, patch, year, and a number of
individual or environmental covariates in occasions t and
t-1, and individual identity.
Juvenile tertiary size transition probability -
This is an optional parameter denoting the probability of becoming
mature size \(k\) in occasion
t+1 assuming survival from juvenile stage \(j\) in occasion t to occasion
t+1 and observation in that time, in a tertiary size metric in
addition to the primary and secondary size metrics. It is used only when
the user wishes to model juvenile vital rates separately from adults,
assuming different relationships with explanatory variables than those
used to classify adults. In lefko3
, this parameter may be
modeled as a function of up to three size metrics, patch, year, and a
number of individual or environmental covariates in occasions t
and t-1, and individual identity.
Juvenile reproduction probability - This is an
optional parameter denoting the probability of reproducing in mature
stage \(k\) in occasion t+1
given survival from juvenile stage j in occasion t to
occasion t+1, and observation in that time. It is used only
when the user wishes to model juvenile vital rates separately from
adults, assuming different relationships with explanatory variables than
those used to classify adults. In lefko3
, this parameter
may be modeled as a function of up to three size metrics, patch, year,
and a number of individual or environmental covariates in occasions
t and t-1, and individual identity, and all other
caveats in (4) apply.
Juvenile maturity probability - This is an
optional parameter denoting the probability of becoming mature in
occasion t+1 given survival from juvenile stage j in
occasion t to occasion t+1. This is a different
parameter than (13) above and is particularly used to weight transition
probabilities to juvenile vs. mature stages properly in matrices with
defined juvenile stages. It is used only when the user wishes to model
juvenile vital rates separately from adults, assuming different
relationships with explanatory variables than those used to classify
adults. In lefko3
, this parameter may be modeled as a
function of up to three size metrics, patch, year, and a number of
individual or environmental covariates in occasions t and
t-1, and individual identity, and all other caveats in (1)
apply.
Of these fourteen vital rates, most users will estimate at least
parameters (1) survival probability, (3) size transition probability,
and (7) fecundity. These three are the default set for function
modelsearch()
. Parameters (2) observation probability and
(6) reproduction probability may be used when some stages are included
that are completely unobservable (and so do not have any size), or that
are mature but non-reproductive, respectively. Parameters (8) through
(14) should only be added if the dataset contains juvenile individuals
transitioning to maturity, and these juveniles live essentially as a
single stage before transitioning to maturity, or before transitioning
to a stage that is size-classified in the same manner as adult stages
are.
Function modelsearch()
handles the entire modeling process
using an exhaustive model building process combined with information
theoretical model selection using model AICc and the number of estimated
parameters in each model. It handles the development of global models,
exhaustive model building, and the selection of best-fit models. Users
should provide this function with information about the following:
Individual history - Are the matrices to be built historical or ahistorical? If the former, then the state of the individual in occasion t-1 will be included in modeling.
Modeling approach - Should the models be estimated as generalized linear models (GLMs) or mixed linear models? While most function-based matrix models are estimated as the former, the latter approach can account for repeated observations of the same individual by including individual identity as a random factor. Mixed models also allow time and patch to be treated as random variables, which allows for broader and more theoretically sound inference.
Suite of factors - Should both size and reproductive status be tested as causal factors? Should two-way interactions be included? Alternatively, should models be estimated as constants?
Suite of vital rates - Which adult demographic parameters should be estimated? The defaults are (1) survival, (3) primary size, and (7) fecundity. Should (2) observation status, (6) reproductive status, or (4) secondary size or (5) tertiary size also be modeled?
Juvenile vital rate estimation - Should juvenile parameters (8) through (14) also be modeled separately from adult parameters?
Best-fit criterion - If a model with fewer parameters exists within 2.0 AICc units of the model with the lowest AICc, then should this model be used as the best-fit model (the default), or should the model with the lowest AICc always be chosen?
Size distribution - Should size be modeled as a continuous variable under a Gaussian or Gamma distribution, or as a count variable under either a Poisson or negative binomial distribution? If a count variable, then should the distribution be zero-inflated to account for excess zeros, zero-truncated to account for a lack of zeros, or left unaltered?
Fecundity distribution - Should fecundity be modeled as a continuous variable under a Gaussian or Gamma distribution, or as a count variable under either a Poisson or negative binomial distribution? If a count variable, then should the distribution be zero-inflated to account for excess zeros, zero-truncated to account for a lack of zeros, or left unaltered?
Continuous distribution estimation method - If using a Gaussian or Gamma distribution for size, then should the probability of transition be estimated via the cumulative density function (CDF) method (the default), or the midpoint method? See Doak et al. (2021) for a discussion of the relative merits of both.
Timing of fecundity - Function
modelsearch()
assumes that linear models of fecundity use a
metric counted or measured in occasion t as the response. This
applies well with most herbaceous plant datasets, where flowers or seeds
produced in one year might be the fecundity response measured. However,
users not wishing to follow this default behavior can use the
fectime
option to stipulate a fecundity metric measured in
occasion t+1.
Age - Is an age or age x stage MPM the main
goal? Currently only age MPMs and ahistorical age x stage MPMs are
offered in lefko3
.
Individual covariates and environmental state variables - Should individual or environmental covariates be tested as causal factors on vital rates? If so, then should they be included as fixed, quantitative terms or as random, categorical terms?
Stage groups - If stage groups are noted in the stageframe, then should they also be used as fixed, independent categorical predictors in modeling?
Missing values for occasions and patches - Should occasions or patches with coefficients that drop to 0 in modeling be estimated as random draws from the corresponding distributions of occasion or patch coefficients?
Censoring - Should data points marked as questionable be used or eliminated?
Variable names - The names of all relevant
variables in the dataset need to be specified. Note that the default
behavior assumes variable names output via the
historicalize3()
or verticalize3()
functions,
which produce standardized historically-formatted vertical (hfv
format) datasets.
Once all decisions are made and associated input terms are provided,
modelsearch()
goes to work. The result is a
lefkoMod
object, which is a list in which the first 14
elements are the best-fit models developed for each vital rate. These
are followed by an equivalent number of elements showing the full model
tables developed and tested, followed by a table detailing the names and
definitions of terms used in modeling, an element detailing the best-fit
criterion used, and ending on quality control data showing the number of
individuals and the number of unique transitions used in the estimation
of each model, as well as the overall accuracy of the models. Depending
on user choices, linear modeling is handled through the
lm()
and glm()
functions in the
stats
package, the glm.nb()
function in the
MASS
package, the lmer()
and
glmer()
functions in lme4
(Bates et al. 2015), the glmmTMB()
function in glmmTMB
(Brooks et al.
2017), the glm.nb()
function in package
MASS
, the vglm()
function in package
VGAM
(Yee and Wild 1996; Yee
2015), or the zeroinfl()
function in package
pscl
(Zeileis, Kleiber, and Jackman
2008). Exhaustive model building proceeds through the
dredge()
function in package MuMIn
(Bartoń 2014). Model selection is handled
through assessment of AICc and the number of parameters estimated per
model (see 6. Best-fit criterion above).
If modelsearch()
is set for historical analysis
(historical = TRUE
, the default), then the decision of
whether to develop a historical MPM can be made on the basis of whether
any best-fit vital rate model includes size or reproductive status in
occasion t-1. If at least one vital rate does, then a
historical MPM is justified. Otherwise, it is not. Regardless, the
output can be used to create a function-based MPM in the next step.
Advanced users of lefko3
may wish to create their own
models without the package’s automated model selection function. In that
case, lefko3
’s matrix functions can accommodate single
models developed using the functions and packages mentioned before.
MPM creation can be accomplished with eight different functions:
rlefko2()
- Creates raw ahistorical stage-classified
MPMs given a dataset, a stageframe, and a supplement table.
rlefko3()
- Creates raw historical stage-classified
MPMs given a dataset, a stageframe, and a supplement table.
arlefko2()
- Creates raw ahistorical age-by-stage
MPMs given a dataset, a stageframe, and a supplement table.
rleslie()
- Creates raw age-classified MPMs given a
dataset, a stageframe, and a supplement table
flefko2()
- Creates function-based ahistorical MPMs
and IPMs given a dataset, a set of models, a stageframe, and a
supplement table.
flefko3()
- Creates function-based historical MPMs
and IPMs given a dataset, a set of models, a stageframe, and a
supplement table.
aflefko2()
- Creates function-based ahistorical
age-by-stage MPMs given a dataset, a set of models, a stageframe, and a
supplement table.
fleslie()
- Creates function-based age-classified
MPMs given a dataset, a set of models, a stageframe, and a supplement
table.
These functions incorporate binary kernels developed to handle the
estimation of matrix elements quickly and efficiently. A single run of
flefko3()
, for example, should be able to yield all annual
matrices for all patches for the Cypripedium candidum dataset
provided with lefko3
in under a half-minute on most
machines (14s or so on RPS’ 2019 MacBook Pro with 2.3 GHz 8-Core Intel
Core i9). Parallel computing should not be necessary even with the
slowest of current machines, provided that the machine is current enough
to handle at least R 3.6.3.
The output for each of these functions is a lefkoMat
object, which is an S3 object (i.e. a list with pre-defined elements).
These lists include elements A
, U
, and
F
, which are themselves lists of complete projection
matrices, survival-transition matrices, and fecundity matrices,
respectively. For example, code such as matobject$A[[1]]
would access the first complete projection matrix in a
lefkoMat
object named matobject
. They are
followed by elements referred to as ahstages
,
hstages
, and agestages
, which provide data
frames describing the stages (technically showing the stageframe, though
edited by the function for consistency), the historical stage-pairs, and
the age-stage pairs shown in the order in which they occur within the
matrices. The labels
element is a data frame giving a
description of each matrix in the order in which it occurs within the
A
, U
, and F
elements, including
the population, patch, and monitoring time designations. The final
elements are quality control outputs that vary in content depending on
whether the output matrices are raw or function-based, but nonetheless
always include at least the numbers of individuals and
individual-transitions used for estimation.
Users wishing to check the output MPMs for errors or simply understand
more about them may utilize functions summary()
and
cond_hmpm()
. Function summary()
summarizes
each lefkoMat
object used as input, and also checks the
survival of stages, stage-pairs, or age-stages by assessing the column
sums for each U
matrix and providing warnings if any
survival probabilities fall below 0 or are greater than 1. Function
cond_hmpm()
decomposes hMPMs into MPMs showing transitions
from occasion t to occasion t+1, but conditioned on
the same stage at occasion t-1. Thus, a single hMPM with five
stages and 25 stage pairs would be broken down into five conditional
MPMs, one for each stage at occasion t-1, with five columns and
five rows denoting stage at occasions t and t+1,
respectively. These can be examined individually, and the survival of
stages from occasion t to occasion t+1 can be assessed
as a function of stage in occasion t-1 by taking the associated
column sums of these conditional matrices.
Some population ecologists will wish to utilize the power and
functionality of lefko3
on already existing matrices.
Although many analytical functions work with simple lists of matrices,
users may import sets of matrices as lefkoMat
objects in
order to utilize the most powerful analyses. The
create_lM()
function allows users to take a list of square
matrices of equal dimensions, and import them into a
lefkoMat
object. Users wishing to do this will also need to
develop a stageframe, and to input the order of populations, patches,
and years associated with the order of matrices in the input list.
Function create_lM()
runs several quality checks on the
input data, and assuming that there are no obvious inconsistencies,
yields the final lefkoMat
object for further use in
analysis.
Users may also import IPMs. If the characteristics of the kernels
propagating an IPM are properly described in a publication, and the
kernel is composed of generalized linear models or generalized linear
mixed models, then function vrm_import()
allows this
information to be input into lefko3
and used to recreate
the IPMs in discretized form. Please see lefko3: a gentle
introduction for more information, or see the function example.
Package lefko3
includes a number of functions to aid
analysis once matrices are created. These may be of greater utility in
some circumstances than established functions such as
eigen()
, because our functions are made to handle even
extremely large, sparse matrices. Currently, we include functions to
estimate element-wise arithmetic mean matrices, discrete and stochastic
population growth rate, stable and long-run stage structure,
reproductive value, deterministic and stochastic sensitivity and
elasticity, and deterministic and stochastic life table response
experiments (LTRE and sLTRE). We also include a basic projection
function that can work under deterministic, stochastic, and density
dependent assumptions. Plans are in the works for further analysis
functions in the future.
Population ecologists most typically run deterministic projection analyses. These analyses take single matrices, and project them a theoretically infinite numbers of times. In most cases, such an infinite projection yields a set of asymptotic properties that are measurable using eigen analysis. For example, the long-run population growth rate should asymptotically approach the largest real part of the dominant eigenvalue.
Ecologists wishing to assess the influence of environmental variability may instead wish to assume temporal environmental stochasticity. Under this assumption, the population is projected into the future by randomly shuffling with resampling all matrices associated with that specific population. Several theorems predict that such a long-run projection will typically yield roughly stable characteristics, including the long-run mean population growth rate and the long-run average stage structure, and that these characteristics may differ strongly from those predicted under deterministic analysis.
Package lefko3
contains functions that quickly assess
deterministic and stochastic properties. In addition, users may use the
projection3()
function to conduct user-defined projections
of various sorts, including even cyclical and unequally weighted
stochastic projections.
Package lefko3
also provides the ability to conduct density
dependent projections. Readers of the density dependence literature will
know that there are many forms of density dependent functions that can
be applied to matrix projection. The oldest forms typically applied a
function such as the logistic function to all matrix elements, generally
by multiplying each matrix element by some function of density (e.g., Leslie 1959). More recent forms
incorporate complex approaches, often separating density dependent
functions by vital rate (e.g., Jensen
1995).
To provide the greatest flexibility, lefko3
currently
implements density dependence in three different ways. First, density
dependence may be set on matrix elements themselves using the
density_input()
function in conjunction with the two
projection functions, projection3()
and
f_projection3()
. This function allows users to list all
matrix elements that should be subject to density dependence with a time
lag, and to stipulate the characteristics of the density dependence.
Shorthand abbreviations can be used in function
density_input()
to describe where density, such as
all
for all stages, rep
for reproductive
stages, nrep
for mature but non-reproductive stages, etc. A
default time delay of 1 time step is applied, and this can be set to any
positive integer.Most users will be interested in this form.
The second form of density dependence is vital rate density dependence,
assuming a time lag. This form modifies vital rates developed for
function-based MPMs by density, and so is less general than the previous
approach. This can be operationalized using the
density_vr()
function in conjunction with function
f_projection3()
.
The third form is spatial density dependence in vital rate models. This form of density dependence models spatial density rather population size, and is incorporated into vital rate model development in function-based MPMs.
Currently, lefko3
includes four density dependence
functions that can be chosen, with projections capable of including
multiple functions and time delays. The first is the Ricker function,
which is given as
\[\begin{equation} \tag{12} \phi_{t+1} = \phi_t \times \alpha e^{-\beta n_t} \end{equation}\]
where \(\alpha\) and \(\beta\) are the density dependence parameters, and \(\beta\) in particular gives the strength of density dependence. This equation is among the most interesting in the density dependence literature, because it is capable of producing oscillations, even multi-period oscillations, and chaos.
The second density dependence function applied in lefko3
is
the Beverton-Holt equation, which is given as
\[\begin{equation} \tag{13} \phi_{t+1} = \phi_t \times \frac{\alpha}{1 + \beta n_t} \end{equation}\]
where \(\alpha\) and \(\beta\) are, once again, the density dependence parameters, and \(\beta\) in particular gives the strength of density dependence. This function generally asymptotes at an equilibrium density, and so is not capable of producing the complex patterns that the Ricker model is capable of.
The third function implemented in lefko3
is the Usher
function, given as
\[\begin{equation} \tag{14} \phi_{t+1} = \phi_t \times \frac{1}{1 + e^{\alpha n_t + \beta}} \end{equation}\]
where both \(\alpha\) and \(\beta\) give the strength of density dependence, though the former via an interaction with density and the latter via an addition to the exponential effect.
Finally, lefko3
also implements a form of the logistic
equation, given as
\[\begin{equation} \tag{15} \phi_{t+1} = \phi_t \times (1 - \frac{n_t}{K}) \end{equation}\]
where only one parameter, \(K\), is needed.
Package lefko3
currently implements these analyses via the
projection3()
and f_projection3()
functions.
Settings for this function also allow the user to stipulate whether the
projection should force matrices to remain substochastic. Two forms of
substochasticity are allowed: 1) a simple form in which
survival-transition probabilities can be prevented from moving outside
of the interval [0, 1] and fecundity can be prevented from becoming
negative, and 2) a more complicated form that keeps the column sums in
survival-transitions matrices (equivalent to the survival probabilities
of stages, stage-pairs, or age-stages) within the interval [0, 1] and
prevents fecundity from becoming negative. We are currently developing
functions to analyze density-dependent projection results, including
sensitivity and elasticity analyses.
Package lefko3
allows the estimation of both the
deterministic and stochastic population growth rates. The deterministic
population growth rate is estimated with function
lambda3()
, and estimates the population growth rate (\(\lambda\)) as the dominant eigenvalue of
each matrix provided (technically, the largest real part of the
estimated eigenvalues). Where matrices are large and sparse, as in most
historical or age-by-stage cases, lambda3()
first converts
matrices to sparse format in order to speed up estimation.
The function slambda3()
estimates the log stochastic
population growth rate in its instantaneous form (\(a = \text{log} \lambda _{S}\)). This is
estimated as the mean log discrete population growth rate across a
user-specified number of random draws of the supplied annual matrices:
\[\begin{equation} \tag{16} a = \text{log} \lambda _{S} = \frac{1}{T} \sum _{t=1}^{T} \text{log} \frac{N _{t}}{N _{t-1}} \end{equation}\]
where \(N _t\) is the population
size in occasion \(t\), and \(T\) is the number of occasions projected
forward, set to 10,000 by default. Function slambda3()
does
not shuffle across patches or populations, instead shuffling within
patches, or shuffling annual matrices calculated as element-wise means
of patch matrices within the same population and the same time. The
methodology is based on Morris and Doak
(2002), though accounts for spatial averaging of patches and can
easily handle large and sparse matrices.
In ahistorical analysis, the stable stage distribution and the reproductive value of stages are estimated as the standardized right and left eigenvectors, respectively, associated with the dominant eigenvalue of the matrix. Standardization of the stable stage distribution is handled by dividing each respective element of the right eigenvector by the sum of the elements in that eigenvector. Standardization of the reproductive value vector is handled by dividing each element in the left eigenvector by the value of the first non-zero element in that eigenvector.
The methods mentioned above apply to historical matrices as well.
However, as described, they only provide the stable stage distribution
and reproductive values of stage pairs. We provide two functions,
stablestage3()
and repvalue3()
, to allow the
estimation of these vectors for both ahistorical and historical MPMs.
When provided with a historical MPM, these functions also estimate
historically-corrected stable stage distributions and
reproductive value vectors, which correspond to the original stages in
the associated life history model rather than the stage pairs, and so
are comparable against the ahistorical stable stage distributions and
reproductive value vectors. The historically-corrected stable stage
proportion for stage \(j\) is estimated
as the sum of all stable stage proportions for stage \(j\) in occasion t across all
stages in occasion t-1, as in:
\[\begin{equation} \tag{17} SS _j = \sum _{l=1}^{m} w _{jl} \end{equation}\]
where \(l\) is stage in occasion t-1, \(m\) is the number of stages, \(SS_j\) is the stable stage proportion of stage \(j\), and \(w _{jl}\) is the stable stage proportion of stage pair \(jl\) given as the standardized right eigenvector corresponding to the dominant eigenvalue of the hMPM. The historically-corrected reproductive value of stage \(j\) is calculated as the sum of all reproductive values for stage \(j\) in occasion t across all stages in occasion t-1, weighted by the stable stage proportion of the respective stage pair divided by the stable stage proportion of stage \(j\) at occasion t (Ehrlén 2000), as in:
\[\begin{equation} \tag{18} RV _j = \sum _{l=1}^{m} v _{jl} (w _{jl} / SS _{j}) \end{equation}\]
where \(RV _j\) refers to reproductive value of stage \(j\), and \(v _{jl}\) refers to the reproductive value of the stage pair as given by the standardized left eigenvector of the dominant eigenvalue of the historical MPM. The influence of history can make these numbers differ quite dramatically from those produced by ahistorical matrices.
Package lefko3
also handles the estimation of stochastic
stable stage distribution and reproductive value vectors. It handles
this through projection of shuffled temporal matrices, typically 10,000
occasions forward though the exact number can be set as needed.
According to the stochastic strong and weak ergodic theorems, this
random shuffling should eventually yield a roughly stationary
distribution of stage proportions and stage reproductive values. Thus,
the stochastic stable structure is estimated as the arithmetic mean
vector of the final set of typically one or two thousand predicted stage
proportion vectors in such a projection.
The stochastic reproductive value is more complicated. Imagine a vector, \(\mathbf{x}(t)\), which includes the expected number of offspring produced by each stage in occasion t+1. This is referred to as the undiscounted reproductive value vector because it is not standardized, and so is likely to eventually move to an extreme value such as infinity. It turns out that \(\mathbf{x}(t)\) is related to other occasions in this projection via:
\[\begin{equation} \tag{19} \mathbf{x}^\top(t) = \mathbf{x}^\top(t+1)\mathbf{A}_t \end{equation}\]
Standardizing leads to the discounted reproductive value vector, as below:
\[\begin{equation} \tag{20} \mathbf{v}(t) = \frac{\mathbf{x}(t)}{\lVert \mathbf{x}(t) \rVert} \end{equation}\]
The reproductive value vector can then be projected as well, as in
\[\begin{equation} \tag{21} \mathbf{v}(t) = \frac{\mathbf{v}^\top(t+1)\mathbf{A}_t}{\lVert \mathbf{v}^\top(t+1)\mathbf{A}_t \rVert} \end{equation}\]
The reproductive value is projected backwards in time, and package
lefko3
takes its average in the final one or two thousand
portions of the backward projection.
Package lefko3
contains functions allowing users to conduct
deterministic and stochastic sensitivity and elasticity analyses.
Sensitivity and elasticity analysis are forms of perturbation analysis,
and we urge readers to consult Caswell
(2001) and Caswell (2019) to become
fully acquainted with the topic. Here, we discuss just the most
important aspects to understand these analyses as conducted using
lefko3
.
The sensitivity of \(\lambda\), the deterministic population growth rate, to a specific element in a projection matrix can be calculated using eigen analysis as
\[\begin{equation} \tag{22} \frac{\partial \lambda}{\partial a _{kj}} = \frac{\bar{v} _{k} w _{j}}{<\mathbf{w}, \mathbf{v}>} \end{equation}\]
Here, \(\mathbf{w}\) is the stable stage distribution vector calculated as the right eigenvector of the dominant eigenvalue of the matrix (standardized to sum to 1), \(\mathbf{v}\) is the reproductive value vector calculated as the associated left eigenvector (standardized by dividing by the value of the first non-zero value), and \(\bar{v} _{k}\) is the complex conjugate of element \(k\) of \(\mathbf{v}\). \(k\) is the stage in occasion t+1 and in the ahMPM refers to the corresponding row, while \(j\) refers to stage in occasion t and in an ahMPM refers to the corresponding column. The term \(<\mathbf{w}, \mathbf{v}>\) refers to the scalar product of these vectors.
In the hMPM case, the basic method is essentially the same as in equation 22, although the equation itself changes somewhat, with the sensitivity of \(\lambda\) to each matrix element given as
\[\begin{equation} \tag{23} \frac{\partial \lambda}{\partial a _{kjl}} = \frac{\bar{v} _{kj} w _{jl}}{<\mathbf{w}, \mathbf{v}>} \end{equation}\]
Here, \(k\) is stage in occasion t+1, \(j\) is stage in occasion t, \(l\) is stage in occasion t-1, \(kj\) refers both to the stage pair in occasions t+1 and t as well as the corresponding row in the historical matrix, and \(jl\) refers both to the stage pair in occasions t and t-1 as well as the corresponding column in the historical matrix. Historically-corrected sensitivities may also be estimated for the basic stages of the life history model using the historically-corrected stable stage distributions and reproductive values given in equations 17 and 18 as input in equation 22.
Sensitivities show how much a small, additive change in a matrix element can alter \(\lambda\), but do so by estimating the local slope of \(\lambda\) given in terms of the matrix element (Caswell 2001). Sensitivities are also typically non-zero even for impossible transitions represented by zeros in the matrix. Elasticities, in contrast, show the influence of small, proportional changes in matrix elements on \(\lambda\), essentially given as local slopes of \(log \lambda\) given in terms of the logarithms of matrix elements. This results in impossible transitions yielding elasticities equal to 0. In the ahistorical case, the elasticity, \(e _{kj}\), of \(\lambda\) to change in a matrix element \(a _{kj}\) is given as
\[\begin{equation} \tag{24} e _{kj} = \frac{a _{kj}}{\lambda} \frac{\partial \lambda}{\partial a _{kj}} \end{equation}\]
The historical case is just an extension of the above.
\[\begin{equation} \tag{25} e _{kjl} = \frac{a _{kjl}}{\lambda} \frac{\partial \lambda}{\partial a _{kjl}} \end{equation}\]
Here, we use row and column definitions equivalent to those used in the historical sensitivity case. This makes the elasticity a function of the sensitivity of \(\lambda\) to the matrix element, as well as of the value of the matrix element itself. Thus, structural zeros in the hMPM must have elasticity equal to 0, although it is entirely possible that they have non-zero sensitivities.
Elasticities calculated for hMPMs can be compared to those calculated in ahMPMs easily because elasticities may be added by stage or transition type, with all elasticities corresponding to a specific matrix necessarily summing to 1.0. Thus, we can calculate the stage pair elasticities resulting from a historical MPM analysis as
\[\begin{equation} \tag{26} e _{kj} = \sum_{i=1}^{m} e _{kji} \end{equation}\]
with all symbol definitions as before. We have provided a
summary()
function for elasticity output in
lefko3
that automatically groups the resulting elasticities
by the kind of ahistorical or historical transition.
Stochastic sensitivity and elasticity analysis are also available. Per Caswell (2001), the sensitivity of \(a = \text{log} \lambda _{S}\) to changes in a specific element is given as:
\[\begin{equation} \tag{27} \frac{\partial \text{log} \lambda _S}{\partial a _{kj}} = \lim_{T \to \infty} \frac{1}{T} \sum_{t=0}^{T-1} \frac{\mathbf{v}(t+1) \mathbf{w}^\top(t)}{\mathbf{v}^\top(t+1) \mathbf{w}(t+1)} \end{equation}\]
where \(t\) refers to a specific monitoring occasion and \(T\) refers to the number of occasions projected forward. Similarly, the stochastic elasticity of \(a = \text{log} \lambda _{S}\) to changes in a specific element is given as:
\[\begin{equation} \tag{28} \frac{\partial \text{log} \lambda _S}{\partial \text{log} a _{kj}} = \lim_{T \to \infty} \frac{1}{T} \sum_{t=0}^{T-1} \frac{\bigl(\mathbf{v}(t+1) \mathbf{w}^\top(t) \bigr) \circ \mathbf{A_t}}{\mathbf{v}^\top(t+1) \mathbf{w}(t+1)} \end{equation}\]
where \(\mathbf{A_t}\) refers to the A matrix corresponding to occasion t. Stochastic sensitivities for hMPMs may be converted to historically-corrected format as in the deterministic case, and stochastic elasticities may be summed as before.
Users working with elasticities, whether deterministic or stochastic,
may find the summary.lefkoElas()
function useful. If an
elasticity analysis is conducted on a lefkoMat
object, then
the information in that object can be used to summarize summed
elasticity according to different sorts of transitions. In the
ahistorical case, elasticities are sorted by growth, stasis, shrinkage,
and fecundity. In the historical case, they are sorted by transition
pairs across three consecutive occasions (e.g. stasis followed growth
vs. shrinkage followed by stasis vs. growth followed by reproduction).
MPMs are very useful tools to describe and explore population dynamics. However, sometimes we may wish to know how specific factors or treatments impact the population growth rate, and through what elements and vital rates those impacts are achieved. Life table response experiments (LTREs) provide the means to evaluate these impacts via methodologies that compare matrices for their impacts on the growth rate of some reference matrix or set of matrices.
Several forms of LTRE exist. The simplest and earliest developed is the fixed, one-way LTRE, which evaluates the impact of a single factor on the asymptotic population growth rate \(\lambda\). Imagine two matrices, the first a matrix derived from some treatment such as a particular management regime, \(\mathbf{A^{(m)}}\), and a reference matrix from a control regime, \(\mathbf{A^{(R)}}\). Per Caswell (2001), if we estimate a matrix \(\mathbf{A^{(m+R)/2}}\) that is the element-wise arithmetic mean matrix of \(\mathbf{A^{(m)}}\) and \(\mathbf{A^{(R)}}\), then:
\[\begin{equation} \tag{29} \Delta \lambda = \lambda^{(m)} - \lambda^{(R)} \approx \sum_{j,i} ((a_{ji}^{(m)} - a_{ji}^{(R)}) (\frac{\partial \lambda}{\partial a_{ji}})) | _\mathbf{A^{(m+R)/2}} \end{equation}\]
Since 2010, several stochastic life table response experiment (sLTREs)
methodologies have also been developed. sLTREs measure the impact of one
or more treatments on the log stochastic growth rate, \(a = \text{log} \lambda _{S}\). However, the
treatment and reference here are not single matrices, but sets of
matrices that vary randomly across time. Here, we assume that \(log\lambda^{(m)}\) and \(log\lambda^{(R)}\) are the log stochastic
growth rates of the treatment MPM and the reference MPM, respectively.
Package lefko3
currently implements the Davison et al. (2010) simulated sLTRE, where:
\[\begin{equation} \tag{30} \Delta \text{log} \lambda _{S} = log\lambda^{(m)} - log\lambda^{(R)} \approx \sum_{j,i} [log \mu_{ji}^{(m)} - log \mu_{ji}^{(R)}] E_{ji}^{\mu} + [log \sigma_{ji}^{(m)} - log \sigma_{ji}^{(R)}] E_{ji}^{\sigma} \end{equation}\]
In the above equation, \(E_{ji}^{\mu}\) and \(E_{ji}^{\sigma}\) are the stochastic
elasticities of the log stochastic growth rate to changes in the mean
and standard deviation, respectively, of the element at row \(j\) and column \(i\) in the reference matrix set. Function
ltre3()
handles all of these calculations.
Davison et al. (2013) presented an
analytical solution to the sLTRE, and we are currently working to
implement this version in lefko3
as well.
Users can take the MPMs produced by MPM creation functions in package
lefko3
and plug them into MPM or matrix analysis functions
in other packages. Matrices produced by lefko3
are stored
within lefkoMat
objects, and users wishing to work with
analysis functions in other packages need only extract the matrices from
them. This allows the use of all functions that work with matrices,
including functions in base R such as eigen()
, as well as
in packages such as popbio
(Stubben
and Milligan 2007) and popdemo
(Stott, Hodgson, and Townley 2012). We encourage
users to explore whether the packages and functions they wish to use can
handle sparse matrices, as well as large matrices - some were not
designed to and can fail or yield unpredictable behavior when applied
particularly to historical matrices produced by lefko3
.
We are grateful to two anonymous reviewers whose scrutiny improved the quality of this vignette. The project resulting in this package and this tutorial was funded by Grant-In-Aid 19H03298 from the Japan Society for the Promotion of Science.