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黄色粘球菌发育细胞命运产生:发育调节蛋白的异质积累和 MazF 在发育裂解中的作用的再检验。

Myxococcus xanthus developmental cell fate production: heterogeneous accumulation of developmental regulatory proteins and reexamination of the role of MazF in developmental lysis.

机构信息

Department of Ecophysiology, Max Planck Institute for Terrestrial Microbiology, Marburg, Germany.

出版信息

J Bacteriol. 2012 Jun;194(12):3058-68. doi: 10.1128/JB.06756-11. Epub 2012 Apr 6.

Abstract

Myxococcus xanthus undergoes a starvation-induced multicellular developmental program during which cells partition into three known fates: (i) aggregation into fruiting bodies followed by differentiation into spores, (ii) lysis, or (iii) differentiation into nonaggregating persister-like cells, termed peripheral rods. As a first step to characterize cell fate segregation, we enumerated total, aggregating, and nonaggregating cells throughout the developmental program. We demonstrate that both cell lysis and cell aggregation begin with similar timing at approximately 24 h after induction of development. Examination of several known regulatory proteins in the separated aggregated and nonaggregated cell fractions revealed previously unknown heterogeneity in the accumulation patterns of proteins involved in type IV pilus (T4P)-mediated motility (PilC and PilA) and regulation of development (MrpC, FruA, and C-signal). As part of our characterization of the cell lysis fate, we set out to investigate the unorthodox MazF-MrpC toxin-antitoxin system which was previously proposed to induce programmed cell death (PCD). We demonstrate that deletion of mazF in two different wild-type M. xanthus laboratory strains does not significantly reduce developmental cell lysis, suggesting that MazF's role in promoting PCD is an adaption to the mutant background strain used previously.

摘要

黄色粘球菌在饥饿诱导的多细胞发育过程中会发生分化,细胞会分为三种已知的命运:(i)聚集形成子实体,然后分化为孢子;(ii)裂解;或(iii)分化为非聚集的持久细胞,称为外周杆状细胞。作为对细胞命运分离进行特征描述的第一步,我们在整个发育过程中对总细胞、聚集细胞和非聚集细胞进行了计数。我们证明,细胞裂解和细胞聚集几乎同时开始,大约在诱导发育后 24 小时。对分离的聚集和非聚集细胞部分中的几种已知调节蛋白的检查揭示了参与 IV 型菌毛(T4P)介导的运动(PilC 和 PilA)和发育调节(MrpC、FruA 和 C 信号)的蛋白积累模式以前未知的异质性。作为我们对细胞裂解命运的特征描述的一部分,我们着手研究了以前提出的诱导程序性细胞死亡(PCD)的非正统 MazF-MrpC 毒素-抗毒素系统。我们证明,在两个不同的野生型 M. xanthus 实验室菌株中删除 mazF 不会显著减少发育细胞的裂解,这表明 MazF 在促进 PCD 中的作用是对以前使用的突变背景菌株的适应。

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