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Dynamics of virus and immune response in multi-epitope network

机译:多表位网络中病毒和免疫应答的动态

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The host immune response can often efficiently suppress a virus infection, which may lead to selection for immune-resistant viral variants within the host. For example, during HIV infection, an array of CTL immune response populations recognize specific epitopes (viral proteins) presented on the surface of infected cells to effectively mediate their killing. However HIV can rapidly evolve resistance to CTL attack at different epitopes, inducing a dynamic network of interacting viral and immune response variants. We consider models for the network of virus and immune response populations, consisting of Lotka-Volterra-like systems of ordinary differential equations. Stability of feasible equilibria and corresponding uniform persistence of distinct variants are characterized via a Lyapunov function. We specialize the model to a binary sequence setting, where for n epitopes there can be distinct viral variants mapped on a hypercube graph. The dynamics in several cases are analyzed and sharp polychotomies are derived characterizing persistent variants. In particular, we prove that if the viral fitness costs for gaining resistance to each epitope are equal, then the system of n+1 persistent virus strains. Overall, our results suggest that immunodominance, i.e. relative strength of immune response to an epitope, is the most important factor determining the persistent network structure.
机译:宿主免疫应答通常可以有效地抑制病毒感染,这可能导致宿主内的免疫病毒变体的选择。例如,在HIV感染期间,CTL免疫反应群体阵列识别出在感染细胞表面上呈现的特定表位(病毒蛋白),以有效地介导它们的杀戮。然而,HIV可以在不同表位迅速发展对CTL攻击的抗性,诱导相互作用的病毒和免疫反应变体的动态网络。我们考虑普通微分方程的Lotka-Volterra样本的病毒和免疫反应群体的模型。通过Lyapunov函数的特征在特征,可行平衡和不同变体的相应均匀持久性的稳定性。我们专业为模型到二进制序列设置,其中对于N个熵,可以存在映射在超立方体图表上的不同病毒变体。分析了几种情况下的动态,锐尖的聚焦衍生特征持久变体。特别地,我们证明,如果对每个表位的抗性的病毒性能成本相等,则N + 1持续病毒株的系统。总体而言,我们的结果表明免疫致常规,即对表位的免疫应答的相对强度,是确定持久网络结构的最重要因素。

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