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一种“内向外”整合素激活和选择性 T 淋巴细胞募集的集成随机模型。

An integrated stochastic model of "inside-out" integrin activation and selective T-lymphocyte recruitment.

机构信息

Department of Chemical and Biomolecular Engineering, University of Pennsylvania, Philadelphia, Pennsylvania 19104, USA.

出版信息

Langmuir. 2012 Jan 31;28(4):2225-37. doi: 10.1021/la203803e. Epub 2012 Jan 4.

Abstract

The pattern of T-lymphocyte homing is hypothesized to be controlled by combinations of chemokine receptors and complementary chemokines. Here, we use numerical simulation to explore the relationship among chemokine potency and concentration, signal transduction, and adhesion. We have developed a form of adhesive dynamics-a mechanically accurate stochastic simulation of adhesion-that incorporates stochastic signal transduction using the next subvolume method. We show that using measurable parameter estimates derived from a variety of sources, including signaling measurements that allow us to test parameter values, we can readily simulate approximate time scales for T-lymphocyte arrest. We find that adhesion correlates with total chemokine receptor occupancy, not the frequency of occupation, when multiple chemokine receptors feed through a single G-protein. A general strategy for selective T-lymphocyte recruitment appears to require low affinity chemokine receptors. For a single chemokine receptor, increases in multiple cross-reactive chemokines can lead to an overwhelming increase in adhesion. Overall, the methods presented here provide a predictive framework for understanding chemokine control of T-lymphocyte recruitment.

摘要

T 淋巴细胞归巢的模式被假设是由趋化因子受体和互补趋化因子的组合控制的。在这里,我们使用数值模拟来探索趋化因子效力和浓度、信号转导和黏附之间的关系。我们已经开发了一种黏附动力学形式——一种使用下一个子体积方法进行的机械准确的随机黏附模拟。我们表明,使用从各种来源得出的可测量参数估计值,包括允许我们测试参数值的信号测量,我们可以轻松模拟 T 淋巴细胞阻滞的近似时间尺度。我们发现,当多个趋化因子受体通过单个 G 蛋白传递时,黏附与总趋化因子受体占有率相关,而不是占有率的频率。选择性 T 淋巴细胞募集的一般策略似乎需要低亲和力的趋化因子受体。对于单个趋化因子受体,多种交叉反应性趋化因子的增加会导致黏附的压倒性增加。总的来说,这里提出的方法为理解趋化因子对 T 淋巴细胞募集的控制提供了一个预测框架。

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