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肽基甘氨酸α-酰胺化单加氧酶作为人类疾病的治疗靶点或生物标志物。

Peptidylglycine α-amidating monooxygenase as a therapeutic target or biomarker for human diseases.

作者信息

Merkler David J, Hawley Aidan J, Eipper Betty A, Mains Richard E

机构信息

Department of Chemistry, University of South Florida, Tampa, Florida, USA.

Department of Molecular Biology & Biophysics, University of Connecticut Health Center, Farmington, Connecticut, USA.

出版信息

Br J Pharmacol. 2022 Jul;179(13):3306-3324. doi: 10.1111/bph.15815. Epub 2022 Feb 28.

Abstract

Peptides play a key role in controlling many physiological and neurobiological pathways. Many bioactive peptides require a C-terminal α-amide for full activity. The bifunctional enzyme catalysing α-amidation, peptidylglycine α-amidating monooxygenase (PAM), is the sole enzyme responsible for amidated peptide biosynthesis, from Chlamydomonas reinhardtii to Homo sapiens. Many neuronal and endocrine functions are dependent upon amidated peptides; additional amidated peptides are growth promoters in tumours. The amidation reaction occurs in two steps, glycine α-hydroxylation followed by dealkylation to generate the α-amide product. Currently, most potentially useful inhibitors target the first reaction, which is rate-limiting. PAM is a membrane-bound enzyme that visits the cell surface during peptide secretion. PAM is then used again in the biosynthetic pathway, meaning that cell-impermeable inhibitors or inactivators could have therapeutic value for the treatment of cancer or psychiatric abnormalities. To date, inhibitor design has not fully exploited the structures and mechanistic details of PAM.

摘要

肽在控制许多生理和神经生物学途径中起关键作用。许多生物活性肽需要C末端α-酰胺才能具有完全活性。催化α-酰胺化的双功能酶——肽基甘氨酸α-酰胺化单加氧酶(PAM),是从莱茵衣藻到智人负责酰胺化肽生物合成的唯一酶。许多神经元和内分泌功能依赖于酰胺化肽;另外,酰胺化肽是肿瘤中的生长促进剂。酰胺化反应分两步进行,先是甘氨酸α-羟基化,然后脱烷基生成α-酰胺产物。目前,大多数潜在有用的抑制剂靶向第一步反应,这是限速步骤。PAM是一种膜结合酶,在肽分泌过程中会到达细胞表面。然后PAM会在生物合成途径中再次使用,这意味着细胞不可渗透的抑制剂或失活剂可能对癌症或精神异常的治疗具有治疗价值。迄今为止,抑制剂设计尚未充分利用PAM的结构和作用机制细节。

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