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Novel dermaseptin, adenoregulin and caerin homologs from the Central American red-eyed leaf frog, Agalychnis callidryas, revealed by functional peptidomics of defensive skin secretion

机译:来自中美洲红眼蛙Agalychnis callidryas的新型dermaseptin,腺苷调节蛋白和caerin同源物,通过防御性皮肤分泌功能性肽组学揭示

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By integrating systematic peptidome and transcriptome studies of the defensive skin secretion of the Central American red-eyed leaf frog, Agalychnis callidryas, we have identified novel members of three previously described antimicrobial peptide families, a 27-mer dermaseptin-related peptide (designated DRP-AC4), a 33-mer adenoregulin-related peptide (designated ARP-ACl) and most unusually, a 27-mer caerin-re-lated peptide (designated CRP-ACl). While dermaseptin and adenoregulin were originally isolated from phyllomedusine leaf frogs, the caerins, until now, had only been described in Australian frogs of the genus, Litoria. Both the dermaseptin and adenoregulin were C-terminally amidated and lacked the C-terminal tripeptide of the biosynthetic precursor sequence. In contrast, the caerin-related peptide, unlike the majority of Litoria analogs, was not C-terminally amidated. The present data emphasize the need for structural characterization of mature peptides to ensure that unexpected precursor cleavages and/or post-translational modifications do not produce mature peptides that differ in structure to those predicted from cloned biosynthetic precursor cDNA. Additionally, systematic study of the secretory peptidome can produce unexpected results such as the CRP described here that may have phylogenetic implications. It is thus of the utmost importance in the functional evaluation of novel peptides that the primary structure of the mature peptide is unequivocally established - something that is often facilitated by cloning biosynthetic precursor cDNAs but obviously not reliable using such data alone.
机译:通过整合中美洲红眼蛙Agalychnis callidryas的防御性皮肤分泌的系统化肽组和转录组研究,我们确定了先前描述的三个抗菌肽家族的新成员,这是一种27-mer肽酶相关肽(称为DRP- AC4),一种33聚体腺调节蛋白相关肽(称为ARP-ACl),最不常见的是27聚体caerin相关肽(称为CRP-ACl)。虽然最初是从phyllomedusine叶蛙中分离出皮肤抑素和腺苷调节蛋白,但迄今为止,caerins仅在澳大利亚Litoria蛙中有描述。皮肤肽素和腺调节蛋白都被C-末端酰胺化并且缺乏生物合成前体序列的C-末端三肽。相反,与大多数Litoria类似物不同,与caerin相关的肽不是C端酰胺化的。本数据强调了对成熟肽进行结构表征的需要,以确保意想不到的前体裂解和/或翻译后修饰不会产生结构上与从克隆的生物合成前体cDNA预测的结构不同的成熟肽。此外,对分泌型肽组的系统研究可能会产生意想不到的结果,例如此处描述的CRP,可能会对系统发育产生影响。因此,在新型肽的功能评估中,至关重要的是要明确地确定成熟肽的一级结构-通常通过克隆生物合成前体cDNA来促进这种结构,但仅使用此类数据显然不可靠。

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