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首页> 外文期刊>mSphere >Architecture and Self-Assembly of Clostridium sporogenes and Clostridium botulinum Spore Surfaces Illustrate a General Protective Strategy across Spore Formers
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Architecture and Self-Assembly of Clostridium sporogenes and Clostridium botulinum Spore Surfaces Illustrate a General Protective Strategy across Spore Formers

机译:Clostridium Sporogenes和Clostridium Botulinum孢子表面的建筑和自组装说明了孢子成型器的一般保护策略

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Spores, the infectious agents of many Firmicutes , are remarkably resilient cell forms. Even distant relatives can have similar spore architectures although some display unique features; they all incorporate protective proteinaceous envelopes. We previously found that Bacillus spores can achieve these protective properties through extensive disulfide cross-linking of self-assembled arrays of cysteine-rich proteins. We predicted that this could be a mechanism employed by spore formers in general, even those from other genera. Here, we tested this by revealing in nanometer detail how the outer envelope (exosporium) in Clostridium sporogenes (surrogate for C. botulinum group I), and in other clostridial relatives, forms a hexagonally symmetric semipermeable array. A cysteine-rich protein, CsxA, when expressed in Escherichia coli , self-assembles into a highly thermally stable structure identical to that of the native exosporium. Like the exosporium, CsxA arrays require harsh “reducing” conditions for disassembly. We conclude that in vivo , CsxA self-organizes into a highly resilient, disulfide cross-linked array decorated with additional protein appendages enveloping the forespore. This pattern is remarkably similar to that in Bacillus spores, despite a lack of protein homology. In both cases, intracellular disulfide formation is favored by the high lattice symmetry. We have identified cysteine-rich proteins in many distantly related spore formers and propose that they may adopt a similar strategy for intracellular assembly of robust protective structures. IMPORTANCE Bacteria such as those causing botulism and anthrax survive harsh conditions and spread disease as spores. Distantly related species have similar spore architectures with protective proteinaceous layers aiding adhesion and targeting. The structures that confer these common properties are largely unstudied, and the proteins involved can be very dissimilar in sequence. We identify CsxA as a cysteine-rich protein that self-assembles in a two-dimensional lattice enveloping the spores of several Clostridium species. We show that apparently unrelated cysteine-rich proteins from very different species can self-assemble to form remarkably similar and robust structures. We propose that diverse cysteine-rich proteins identified in the genomes of a broad range of spore formers may adopt a similar strategy for assembly.
机译:孢子,许多压缩的传染病,是显着的弹性细胞形式。即使是遥远的亲戚也可以具有相似的孢子架构,尽管有些展示独特的功能;它们都包含保护性蛋白质包膜。我们以前发现芽孢杆菌孢子可以通过广泛的二硫化物交联,通过广泛的富含半胱氨酸阵列的半胱氨酸阵列进行广泛的二硫化物交联来实现这些保护性能。我们预测,这可能是孢子成型器一般雇用的机制,即使是来自其他属的人。这里,通过纳米详细揭示外壳(外孢子虫)在梭菌孢子引发(C.肉毒杆菌基团I)中的外壳(exosporium)以及其他梭菌亲属中的外壳(exosporium)形成这一点,形成六角对称的半透性阵列。富含半胱氨酸的蛋白质,CSXA,当在大肠杆菌中表达时,自组装成高度热稳定的结构,与天然群岛的高度热稳定的结构相同。与exosporium一样,CSXA阵列需要苛刻的“减少”条件来拆卸。我们得出结论,在体内,CSXA自组织成高度弹性的,二硫化的交联阵列装饰着包裹额外额外的额外的蛋白质阑尾。尽管缺乏蛋白质同源性,但这种模式非常类似于芽孢杆菌孢子中的模式。在这两种情况下,细胞内二硫化物形成由高晶格对称性青少细胞。我们已经在许多远端相关的孢子成型器中鉴定了富含半胱氨酸的蛋白质,并提出了它们可以采用类似的鲁棒保护结构的细胞内组装策略。诸如导致肉毒杆菌和炭疽病的重要细菌生存恶劣的条件并作为孢子传播疾病。远处相关的物种具有类似的孢子架构,具有保护性蛋白质层,防止粘附和靶向。赋予这些常见特性的结构大大沉积,并且所涉及的蛋白质依次非常异常。我们将CSXA鉴定为富含半胱氨酸的蛋白质,其在包围几种梭菌种类的孢子的二维格子中自组装。我们表明,从非常不同的物种中显然无关的富含半胱氨酸的蛋白质可以自组装以形成显着相似和稳健的结构。我们提出在广泛的孢子成形剂的基因组中鉴定的多样化富含半胱氨酸的蛋白质可以采用类似的组装策略。

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