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Designing lymphocyte functional structure for optimal signal detection: Viola, T cells

机译:设计用于最佳信号检测的淋巴细胞功能结构:中提琴,T细胞

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One basic task of immune systems is to detect signals from unknown "intruders" amidst a noisy background of harmless signals. To clarify the functional importance of many observed lymphocyte properties, I ask: What properties would a cell have if one designed it according to the theory of optimal detection, with minimal regard for biological constraints? Sparse and reasonable assumptions about the statistics of available signals prove sufficient for deriving many features of the optimal functional structure, in an incremental and modular design. The use of one common formalism guarantees that all parts of the design collaborate to solve the detection task. Detection performance is computed at several stages of the design. Comparison between design variants reveals e.g, the importance of controlling the signal integration time. This predicts that an appropriate control mechanism should exist. Comparing the design to reality, I find a striking similarity with many features of T cells. For example, the formalism dictates clonal specificity, serial receptor triggering, (grades of) anergy, negative and positive selection, co-stimulation, high-zone tolerance, and clonal production of cytokines. Serious mismatches should be found if T cells were hindered by mechanistic constraints or vestiges of their (co-)evolutionary history, but I have not found clear examples. By contrast, fundamental mismatches abound when comparing the design to immune systems of e.g. invertebrates. The wide-ranging differences seem to hinge on the (in)ability to generate a large diversity of receptors. (C) 2000 Academic Press. [References: 30]
机译:免疫系统的一项基本任务是在嘈杂的无害信号背景中检测来自未知“入侵者”的信号。为了阐明许多观察到的淋巴细胞特性的功能重要性,我问:如果一个细胞根据最佳检测理论在不考虑生物学限制的情况下对其进行设计,它将具有哪些特性?事实证明,对可用信号统计的稀疏合理假设足以在增量和模块化设计中推导最佳功能结构的许多特征。一种通用形式主义的使用保证了设计的所有部分都可以协作来解决检测任务。检测性能是在设计的几个阶段进行计算的。设计变体之间的比较揭示了例如控制信号积分时间的重要性。这预示应该存在适当的控制机制。将设计与现实进行比较,我发现T细胞的许多功能具有惊人的相似性。例如,形式主义决定了克隆特异性,系列受体触发,无反应性((等级)),阴性和阳性选择,共同刺激,高区耐受性以及细胞因子的克隆产生。如果T细胞受到机械限制或它们的(共同)进化历史的遗迹阻碍,则应该发现严重的错配,但我还没有找到明确的例子。相比之下,当将设计与例如免疫系统的免疫系统进行比较时,基本错配比比皆是。无脊椎动物。广泛的差异似乎取决于产生多种受体的(不)能力。 (C)2000学术出版社。 [参考:30]

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