LaRocca Timothy J, Stivison Elizabeth A, Hod Eldad A, Spitalnik Steven L, Cowan Peter J, Randis Tara M, Ratner Adam J
Department of Pediatrics, Columbia University, New York, New York, USA.
Institute of Human Nutrition, Columbia University, New York, New York, USA.
mBio. 2014 Aug 26;5(5):e01251-14. doi: 10.1128/mBio.01251-14.
A subgroup of the cholesterol-dependent cytolysin (CDC) family of pore-forming toxins (PFTs) has an unusually narrow host range due to a requirement for binding to human CD59 (hCD59), a glycosylphosphatidylinositol (GPI)-linked complement regulatory molecule. hCD59-specific CDCs are produced by several organisms that inhabit human mucosal surfaces and can act as pathogens, including Gardnerella vaginalis and Streptococcus intermedius. The consequences and potential selective advantages of such PFT host limitation have remained unknown. Here, we demonstrate that, in addition to species restriction, PFT ligation of hCD59 triggers a previously unrecognized pathway for programmed necrosis in primary erythrocytes (red blood cells [RBCs]) from humans and transgenic mice expressing hCD59. Because they lack nuclei and mitochondria, RBCs have typically been thought to possess limited capacity to undergo programmed cell death. RBC programmed necrosis shares key molecular factors with nucleated cell necroptosis, including dependence on Fas/FasL signaling and RIP1 phosphorylation, necrosome assembly, and restriction by caspase-8. Death due to programmed necrosis in RBCs is executed by acid sphingomyelinase-dependent ceramide formation, NADPH oxidase- and iron-dependent reactive oxygen species formation, and glycolytic formation of advanced glycation end products. Bacterial PFTs that are hCD59 independent do not induce RBC programmed necrosis. RBC programmed necrosis is biochemically distinct from eryptosis, the only other known programmed cell death pathway in mature RBCs. Importantly, RBC programmed necrosis enhances the growth of PFT-producing pathogens during exposure to primary RBCs, consistent with a role for such signaling in microbial growth and pathogenesis.
In this work, we provide the first description of a new form of programmed cell death in erythrocytes (RBCs) that occurs as a consequence of cellular attack by human-specific bacterial toxins. By defining a new RBC death pathway that shares important components with necroptosis, a programmed necrosis module that occurs in nucleated cells, these findings expand our understanding of RBC biology and RBC-pathogen interactions. In addition, our work provides a link between cholesterol-dependent cytolysin (CDC) host restriction and promotion of bacterial growth in the presence of RBCs, which may provide a selective advantage to human-associated bacterial strains that elaborate such toxins and a potential explanation for the narrowing of host range observed in this toxin family.
成孔毒素(PFT)家族中的胆固醇依赖性细胞溶素(CDC)亚组具有异常狭窄的宿主范围,因为它们需要与人CD59(hCD59)结合,hCD59是一种糖基磷脂酰肌醇(GPI)连接的补体调节分子。几种栖息于人类粘膜表面且可作为病原体的生物会产生hCD59特异性CDC,包括阴道加德纳菌和中间链球菌。这种PFT宿主限制的后果和潜在的选择优势尚不清楚。在此,我们证明,除了物种限制外,hCD59的PFT连接还会触发人类和表达hCD59的转基因小鼠的原代红细胞(红细胞[RBC])中一种以前未被认识的程序性坏死途径。由于红细胞缺乏细胞核和线粒体,通常认为它们发生程序性细胞死亡的能力有限。红细胞程序性坏死与有核细胞坏死性凋亡有共同的关键分子因素,包括对Fas/FasL信号传导和RIP1磷酸化的依赖性、坏死小体组装以及受caspase-8限制。红细胞中程序性坏死导致的死亡是由酸性鞘磷脂酶依赖性神经酰胺形成、NADPH氧化酶和铁依赖性活性氧形成以及糖酵解形成晚期糖基化终产物所执行的。不依赖hCD59的细菌PFT不会诱导红细胞程序性坏死。红细胞程序性坏死在生化上与红细胞凋亡不同,红细胞凋亡是成熟红细胞中唯一已知的另一种程序性细胞死亡途径。重要的是,红细胞程序性坏死在暴露于原代红细胞期间会增强产生PFT的病原体的生长,这与这种信号传导在微生物生长和发病机制中的作用一致。
在这项工作中,我们首次描述了红细胞(RBC)中一种新的程序性细胞死亡形式,它是由人类特异性细菌毒素对细胞的攻击所导致的。通过定义一种与坏死性凋亡(一种发生在有核细胞中的程序性坏死模式)有重要共同成分的新的红细胞死亡途径,这些发现扩展了我们对红细胞生物学和红细胞 - 病原体相互作用的理解。此外,我们的工作在胆固醇依赖性细胞溶素(CDC)宿主限制与红细胞存在时细菌生长促进之间建立了联系,这可能为产生此类毒素的人类相关细菌菌株提供选择优势,并为该毒素家族中观察到的宿主范围变窄提供潜在解释。
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