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Protein cross-linking by chlorinated polyamines and transglutamylation stabilizes neutrophil extracellular traps

机译:通过氯化多胺交联蛋白质和转膜淀粉化稳定中性粒细胞细胞外陷阱

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摘要

Neutrophil extracellular trap (NET) ejected from activated dying neutrophils is a highly ordered structure of DNA and selected proteins capable to eliminate pathogenic microorganisms. Biochemical determinants of the non-randomly formed stable NETs have not been revealed so far. Studying the formation of human NETs we have observed that polyamines were incorporated into the NET. Inhibition of myeloperoxidase, which is essential for NET formation and can generate reactive chlorinated polyamines through hypochlorous acid, decreased polyamine incorporation. Addition of exogenous primary amines that similarly to polyamines inhibit reactions catalyzed by the protein cross-linker transglutaminases (TGases) has similar effect. Proteomic analysis of the highly reproducible pattern of NET components revealed cross-linking of NET proteins through chlorinated polyamines and ? ( γ -glutamyl)lysine as well as bis- γ -glutamyl polyamine bonds catalyzed by the TGases detected in neutrophils. Competitive inhibition of protein cross-linking by monoamines disturbed the cross-linking pattern of NET proteins, which resulted in the loss of the ordered structure of the NET and significantly reduced capacity to trap bacteria. Our findings provide explanation of how NETs are formed in a reproducible and ordered manner to efficiently neutralize microorganisms at the first defense line of the innate immune system.
机译:从活性染色中性粒细胞排出的嗜中性粒细胞外阱(网)是一种高度有序的DNA结构,以及能够消除致病微生物的选定蛋白质。到目前为止,尚未揭示非随机形成的稳定网的生化决定簇。研究人体网的形成,我们观察到多胺掺入网中。抑制髓过氧化物酶,这对于净形成至关重要,可以通过次氯酸产生反应性氯化多胺,降低多胺掺入。添加与多胺抑制因蛋白质交联剂转谷氨酰胺酶(TGase)催化的多胺的反应的外源伯胺具有类似的效果。高度可重复的净组分模式的蛋白质组学分析显示净蛋白通过氯化多胺的交联和β (γ-戊酰基)赖氨酸以及通过中性粒细胞中检测到的TGase催化的双-γ-戊酰基多胺键。通过单胺对蛋白质交联的竞争性抑制干扰了净蛋白的交联模式,导致净有序结构的损失,并显着降低了捕获细菌的能力。我们的研究结果提供了对净的方式以可再生和有序的方式形成的说明,以便在先天免疫系统的第一防线线上有效地中和微生物。

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