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蝎毒液腺中的双重 α-酰胺化系统。

The Dual α-Amidation System in Scorpion Venom Glands.

机构信息

Departamento de Medicina Molecular y Bioprocesos, Instituto de Biotecnología, Universidad Nacional Autónoma de México, Avenida Universidad 2001, Colonia Chamilpa, Cuernavaca, Morelos 62210, Mexico.

出版信息

Toxins (Basel). 2019 Jul 20;11(7):425. doi: 10.3390/toxins11070425.

Abstract

Many peptides in scorpion venoms are amidated at their C-termini. This post-translational modification is paramount for the correct biological function of ion channel toxins and antimicrobial peptides, among others. The discovery of canonical amidation sequences in transcriptome-derived scorpion proproteins suggests that a conserved enzymatic α-amidation system must be responsible for this modification of scorpion peptides. A transcriptomic approach was employed to identify sequences putatively encoding enzymes of the α-amidation pathway. A dual enzymatic α-amidation system was found, consisting of the membrane-anchored, bifunctional, peptidylglycine α-amidating monooxygenase (PAM) and its paralogs, soluble monofunctional peptidylglycine α-hydroxylating monooxygenase (PHM) and peptidyl-α-hydroxyglycine α-amidating lyase (PAL). Independent genes encode these three enzymes. Amino acid residues responsible for ion coordination and enzymatic activity are conserved in these sequences, suggesting that the enzymes are functional. Potential endoproteolytic recognition sites for proprotein convertases in the PAM sequence indicate that PAM-derived soluble isoforms may also be expressed. Sequences potentially encoding proprotein convertases (PC1 and PC2), carboxypeptidase E (CPE), and other enzymes of the α-amidation pathway, were also found, confirming the presence of this pathway in scorpions.

摘要

许多蝎毒液中的肽在其 C 末端酰胺化。这种翻译后修饰对于离子通道毒素和抗菌肽等的正确生物学功能至关重要。在转录组衍生的蝎原蛋白中发现典型的酰胺化序列表明,必须存在保守的酶α-酰胺化系统来负责这种蝎肽的修饰。采用转录组学方法来鉴定可能编码α-酰胺化途径的酶的序列。发现了一个双酶α-酰胺化系统,由膜锚定的双功能肽基甘氨酸α-酰胺化单加氧酶 (PAM) 及其同工酶、可溶性单功能肽基甘氨酸α-羟化单加氧酶 (PHM) 和肽基-α-羟基甘氨酸α-酰胺化裂解酶 (PAL) 组成。这三个酶由独立的基因编码。这些序列中保守了负责离子配位和酶活性的氨基酸残基,表明这些酶是有功能的。PAM 序列中可能存在针对蛋白原转化酶的内切酶识别位点,表明也可能表达 PAM 衍生的可溶性同工酶。还发现了可能编码蛋白原转化酶 (PC1 和 PC2)、羧肽酶 E (CPE) 和 α-酰胺化途径的其他酶的序列,证实了该途径在蝎子中的存在。

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