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Chemical synthesis and biological activity of a novel antibacterial peptide deduced from a pig myeloid cDNA

机译:从猪髓系cDNA推断出的新型抗菌肽的化学合成和生物学活性

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>Several myeloid precursors of antibacterial peptides have recently been shown to share homologous pre- and pro-regions. Taking advantage of this homology, a novel cDNA was cloned from pig bone marrow RNA. This encodes a 166-residue polypeptide with highly conserved pre- (29 residues) and pro- (101 residues) sequences, followed by a unique, 36-residue C-terminal sequence. Structure analyses of this C-terminal region have identified a highly cationic sequence predicted to adopt an amphipathic α-helical conformation. A peptide corresponding to this sequence was chemically synthesized and shown to arrest the growth of both Gram-positive and Gram-negative bacteria. At least for Escherichia coli, the activity of this peptide appears to be mediated by its ability to permeabilize the bacterial membranes.
机译:>最近已显示出抗菌肽的几种髓样前体共享同源的前区和前区。利用这种同源性,从猪骨髓RNA中克隆了新的cDNA。这编码具有高保守的前(29个残基)和前(101个残基)序列的166个残基多肽,然后是独特的36个残基的C末端序列。此C末端区域的结构分析已确定了预计将采用两亲性α-螺旋构象的高度阳离子序列。化学合成对应于该序列的肽,并显示其阻止革兰氏阳性细菌和革兰氏阴性细菌的生长。至少对于大肠杆菌而言,该肽的活性似乎是由其渗透细菌膜的能力介导的。

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