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A Metabolic Enzyme as a Primary Virulence Factor of Mycoplasma mycoides subsp. mycoides Small Colony

机译:代谢酶作为支原体支原体亚种的主要毒力因子。霉菌小菌落

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During evolution, pathogenic bacteria have developed complex interactions with their hosts. This has frequently involved the acquisition of virulence factors on pathogenicity islands, plasmids, transposons, or prophages, allowing them to colonize, survive, and replicate within the host. In contrast, Mycoplasma species, the smallest self-replicating organisms, have regressively evolved from gram-positive bacteria by reduction of the genome to a minimal size, with the consequence that they have economized their genetic resources. Hence, pathogenic Mycoplasma species lack typical primary virulence factors such as toxins, cytolysins, and invasins. Consequently, little is known how pathogenic Mycoplasma species cause host cell damage, inflammation, and disease. Here we identify a novel primary virulence determinant in Mycoplasma mycoides subsp. mycoides Small Colony (SC), which causes host cell injury. This virulence factor, released in significant amounts in the presence of glycerol in the growth medium, consists of toxic by-products such as H2O2 formed by l-α-glycerophosphate oxidase (GlpO), a membrane-located enzyme that is involved in the metabolism of glycerol. When embryonic calf nasal epithelial cells are infected with M. mycoides subsp. mycoides SC in the presence of physiological amounts of glycerol, H2O2 is released inside the cells prior to cell death. This process can be inhibited with monospecific anti-GlpO antibodies.
机译:在进化过程中,病原细菌与其宿主之间形成了复杂的相互作用。这通常涉及在致病岛,质粒,转座子或原噬菌体上获取毒力因子,从而使其在宿主内定植,存活和复制。相反,最小的自我复制生物 Mycoplasma 物种通过将基因组减少到最小大小而从革兰氏阳性细菌中逐渐退步,从而节省了遗传资源。因此,致病性支原体物种缺乏典型的主要毒力因子,例如毒素,溶细胞素和侵袭素。因此,鲜为人知的致病性<支原体>支原体种类如何导致宿主细胞损伤,炎症和疾病。在这里,我们确定了 Mycoplasma mycoides 亚种中的新型主要毒力决定因素。 mycoides 小菌落(SC),会导致宿主细胞受伤。这种毒性因子在生长介质中存在甘油时会大量释放,由有毒的副产物组成,例如由L-α-形成的H 2 O 2 甘油磷酸氧化酶(GlpO),一种膜定位的酶,参与甘油的代谢。当胚胎小牛的鼻上皮细胞被 M感染时。杀菌剂子空间在存在一定量甘油的情况下, mycoides SC会在细胞死亡前在细胞内释放出来。可以用单特异性抗GlpO抗体抑制该过程。

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