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Abstract In the secondary lymphoid tissues, human immunodeficiency virus (HIV) can replicate both in the follicular and the extrafollicular compartments. Yet, virus is concentrated in the follicular compartment in the absence of antiretroviral therapy, in part due to the lack of cytotoxic T lymphocyte (CTL)-mediated activity there. CTL home to the extrafollicular compartment, where they can suppress virus load to relatively low levels. We use mathematical models to show that this compartmentalization can explain seemingly counterintuitive observations. First, it can explain the observed constancy of the viral decline slope during antiviral therapy in the peripheral blood, irrespective of the presence of CTL in SIV-infected macaques, under the assumption that CTL-mediated lysis significantly contributes to virus suppression. Second, it can account for the relatively long times it takes for CTL escape mutants to emerge during chronic infection even if CTL-mediated lysis is responsible for virus suppression. The reason is the heterogeneity in CTL activity, and the consequent heterogeneity in selection pressure between the follicular and extrafollicular compartments. Hence, to understand HIV dynamics more thoroughly, this analysis highlights the importance of measuring virus populations separately in the extrafollicular and follicular compartments rather than using virus load in peripheral blood as an observable; this hides the heterogeneity between compartments that might be responsible for the particular patterns seen in the dynamics and evolution of the HIV in vivo. 

We consider spatial population dynamics on a lattice, following a type of a contact (birth–death) stochastic process. We show that simple mathematical approximations for the density of cells can be obtained in a variety of scenarios. In the case of a homogeneous cell population, we derive the cellular density for a two-dimensional (2D) spatial lattice with an arbitrary number of neighbors, including the von Neumann, Moore, and hexagonal lattice. We then turn our attention to evolutionary dynamics, where mutant cells of different properties can be generated. For disadvantageous mutants, we derive an approximation for the equilibrium density representing the selection–mutation balance. For neutral and advantageous mutants, we show that simple scaling (power) laws for the numbers of mutants in expanding populations hold in 2D and 3D, under both flat (planar) and range population expansion. These models have relevance for studies in ecology and evolutionary biology, as well as biomedical applications including the dynamics of drug-resistant mutants in cancer and bacterial biofilms.