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首页> 外文期刊>Journal of bacteriology >A Stochastic Mechanism for Biofilm Formation by Mycoplasma pulmonis
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A Stochastic Mechanism for Biofilm Formation by Mycoplasma pulmonis

机译:肺炎支原体形成生物膜的随机机制。

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Bacterial biofilms are communities of bacteria that are enclosed in an extracellular matrix. Within a biofilm the bacteria are protected from antimicrobials, environmental stresses, and immune responses from the host. Biofilms are often believed to have a highly developed organization that is derived from differential regulation of the genes that direct the synthesis of the extracellular matrix and the attachment to surfaces. The mycoplasmas have the smallest of the prokaryotic genomes and apparently lack complex gene-regulatory systems. We examined biofilm formation by Mycoplasma pulmonis and found it to be dependent on the length of the tandem repeat region of the variable surface antigen (Vsa) protein. Mycoplasmas that produced a short Vsa protein with few tandem repeats formed biofilms that attached to polystyrene and glass. Mycoplasmas that produced a long Vsa protein with many tandem repeats formed microcolonies that floated freely in the medium. The biofilms and the microcolonies contained an extracellular matrix which contained Vsa protein, lipid, DNA, and saccharide. As variation in the number of Vsa tandem repeats occurs by slipped-strand mispairing, the ability of the mycoplasmas to form a biofilm switches stochastically.
机译:细菌生物膜是封闭在细胞外基质中的细菌群落。在生物膜内,细菌受到保护,免受抗菌剂,环境压力和宿主的免疫反应。人们通常认为生物膜具有高度发达的组织,该组织源于指导细胞外基质合成和附着于表面的基因的差异调节。支原体具有最小的原核基因组,并且显然缺乏复杂的基因调控系统。我们检查了肺炎支原体的生物膜形成,发现它取决于可变表面抗原(Vsa)蛋白串联重复序列区域的长度。产生短串联序列重复的短Vsa蛋白的支原体形成附着在聚苯乙烯和玻璃上的生物膜。产生具有许多串联重复序列的长Vsa蛋白的支原体形成了微菌落,可在培养基中自由漂浮。生物膜和微菌落包含细胞外基质,其中包含Vsa蛋白,脂质,DNA和糖。由于滑链错配导致Vsa串联重复数目发生变化,支原体形成生物膜的能力随机切换。

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