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首页> 外文期刊>Immunologic Research: A Selective Reference to Current Research and Practice >Killing machines: three pore-forming proteins of the immune system
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Killing machines: three pore-forming proteins of the immune system

机译:杀死机器:三种免疫系统的孔形成蛋白

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摘要

The evolution of early multicellular eukaryotes 400-500 million years ago required a defensive strategy against microbial invasion. Pore-forming proteins containing the membrane-attack-complex-perforin (MACPF) domain were selected as the most efficient means to destroy bacteria or virally infected cells. The mechanism of pore formation by the MACPF domain is distinctive in that pore formation is purely physical and unspecific. The MACPF domain polymerizes, refolds, and inserts itself into bilayer membranes or bacterial outer cell walls. The displacement of surface lipid/carbohy-drate molecules by the polymerizing MACPF domain creates clusters of large, water-filled holes that destabilize the barrier function and provide access for additional anti-bacterial or anti-viral effectors to sensitive sites that complete the destruction of the invader via enzymatic or chemical attack. The highly efficient mechanism of anti-microbial defense by a combined physical and chemical strategy using pore-forming MACPF-proteins has been retargeted during evolution of vertebrates and mammals for three purposes: (1) to kill extracellular bacteria C9/polyC9 evolved in conjunction with complement, (2) to kill virus infected and cancer cells perform-l/polyperforin-l CTL evolved targeted by NK and CTL, and (3) to kill intracellular bacteria transmembrane perforin-2/putative polyperforin-2 evolved targeted by phagocytic and nonphagocytic cells. Our laboratory has been involved in the discovery and description of each of the three pore-formers that will be reviewed here.
机译:早期多细胞真核生物的演变400-500万年前需要一种免受微生物入侵的防御策略。选择含有膜 - 攻击 - 复合物 - 穿孔蛋白(MACPF)结构域的孔形成蛋白质作为破坏细菌或病毒感染细胞的最有效手段。 MACPF结构域的孔形成机制是独特的,因为孔形成纯度的物理和非特异性。 MACPF结构域聚合,重折叠并将其自身插入双层膜或细菌外部电池壁。通过聚合MACPF结构域的表面脂质/碳水化合物分子的位移产生了稳定屏障功能的大型水填充孔的簇,并提供额外的抗细菌或抗病毒效应对完成破坏的敏感位点来获得额外的抗细菌或抗病毒效应。通过酶或化学攻击的入侵者。在脊椎动物和哺乳动物的演变期间,在三种目的的演变期间,在脊椎动物和哺乳动物的演变期间重新出现了使用孔形成麦克皮蛋白的抗微生物防御的高效机制:(1)与补体,(2)杀死病毒感染和癌细胞的癌细胞表现为NK和CTL的靶向靶向的-L / Polyperforin-L CTL,(3)杀死细胞内细菌跨膜穿孔素-2 /推定的多肽-2通过吞噬和非甘露物靶向进化细胞。我们的实验室已经参与了将在此进行审查的三种孔隙机中的每一个的发现和描述。

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