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Apidaecin-type peptides: biodiversity, structure-function relationships and mode of action.

机译:Apidaecin型肽:生物多样性,结构功能关系和作用方式。

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Apidaecins (apidaecin-type peptides) refer to a series of small, proline-rich (Pro-rich), 18- to 20-residue peptides produced by insects. They are the largest group of Pro-rich antimicrobial peptides (AMPs) known to date. Structurally, apidaecins consist of two regions, the conserved (constant) region, responsible for the general antibacterial capacity, and the variable region, responsible for the antibacterial spectrum. The small, gene-encoded and unmodified apidaecins are predominantly active against many gram-negative bacteria by special antibacterial mechanisms. The mechanism of action by which apidaecins kill bacteria involves an initial non-specific binding of the peptides to an outer membrane (OM) component. This binding is followed by invasion of the periplasmic space, and by a specific and essentially irreversible combination with a receptor/docking molecule that may be a component of a permease-type transporter system on inner membrane (IM). In the final step, the peptide is translocated intothe interior of the cell where it meets its ultimate target. Evidence that apidaecins are non-toxic for human and animal cells is a prerequisite for using them as novel antibiotic drugs. This review presents the biodiversity, structure-function relationships, and mechanism of action of apidaecins.
机译:Apidaecins(Apidaecin型肽)是指昆虫产生的一系列小的,富含脯氨酸(Pro-rich),18至20个残基的肽。它们是迄今为止已知的最大的富含Pro的抗菌肽(AMP)组。在结构上,阿德霉素由两个区域组成,一个是保守的(恒定)区域,负责一般的抗菌能力;另一个是可变区域,负责抗菌谱。通过特殊的抗菌机制,小的,基因编码的和未修饰的阿迪霉素主要对许多革兰氏阴性细菌具有活性。芹菜素杀死细菌的作用机制涉及肽与外膜(OM)成分的初始非特异性结合。这种结合之后是周质空间的侵袭,并且是与受体/对接分子的特定且基本不可逆的结合,该受体/对接分子可能是内膜(IM)上渗透酶型转运蛋白系统的组成部分。在最后的步骤中,将肽转移到细胞内部,使其达到其最终靶标。芹菜素对人和动物细胞无毒的证据是将其用作新型抗生素的先决条件。这篇综述介绍了阿霉素的生物多样性,结构-功能关系和作用机理。

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