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海洋无脊椎动物:生物医学相关金属氨基肽酶 M1 和 M17 家族抑制剂的极有前景但尚未开发的来源。

Marine Invertebrates: A Promissory Still Unexplored Source of Inhibitors of Biomedically Relevant Metallo Aminopeptidases Belonging to the M1 and M17 Families.

机构信息

Center for Protein Studies, Faculty of Biology, University of Havana, Havana 10400, Cuba.

Department of Biological Sciences, University of Calgary, Calgary, AB T2N 1N4, Canada.

出版信息

Mar Drugs. 2023 Apr 28;21(5):279. doi: 10.3390/md21050279.

Abstract

Proteolytic enzymes, also known as peptidases, are critical in all living organisms. Peptidases control the cleavage, activation, turnover, and synthesis of proteins and regulate many biochemical and physiological processes. They are also involved in several pathophysiological processes. Among peptidases, aminopeptidases catalyze the cleavage of the N-terminal amino acids of proteins or peptide substrates. They are distributed in many phyla and play critical roles in physiology and pathophysiology. Many of them are metallopeptidases belonging to the M1 and M17 families, among others. Some, such as M1 aminopeptidases N and A, thyrotropin-releasing hormone-degrading ectoenzyme, and M17 leucyl aminopeptidase, are targets for the development of therapeutic agents for human diseases, including cancer, hypertension, central nervous system disorders, inflammation, immune system disorders, skin pathologies, and infectious diseases, such as malaria. The relevance of aminopeptidases has driven the search and identification of potent and selective inhibitors as major tools to control proteolysis with an impact in biochemistry, biotechnology, and biomedicine. The present contribution focuses on marine invertebrate biodiversity as an important and promising source of inhibitors of metalloaminopeptidases from M1 and M17 families, with foreseen biomedical applications in human diseases. The results reviewed in the present contribution support and encourage further studies with inhibitors isolated from marine invertebrates in different biomedical models associated with the activity of these families of exopeptidases.

摘要

蛋白水解酶,也被称为肽酶,在所有生物体中都至关重要。肽酶控制蛋白质和肽底物的切割、激活、转化和合成,并调节许多生化和生理过程。它们还参与几种病理生理过程。在肽酶中,氨肽酶催化蛋白质或肽底物的 N 端氨基酸的裂解。它们分布在许多门中,在生理学和病理生理学中发挥关键作用。其中许多是属于 M1 和 M17 家族的金属肽酶等。有些,如 M1 氨肽酶 N 和 A、促甲状腺素释放激素降解酶、M17 亮氨酰氨肽酶,是为人类疾病,包括癌症、高血压、中枢神经系统疾病、炎症、免疫系统疾病、皮肤病理学和传染病,如疟疾,开发治疗药物的靶点。氨肽酶的相关性促使人们寻找和鉴定强效和选择性抑制剂,作为控制蛋白水解的主要工具,对生物化学、生物技术和生物医学有影响。本研究重点介绍海洋无脊椎动物生物多样性,作为 M1 和 M17 家族金属氨肽酶抑制剂的重要且有前途的来源,预计在人类疾病的生物医学应用中有前景。本研究综述的结果支持并鼓励在与这些外肽酶家族活性相关的不同生物医学模型中,对从海洋无脊椎动物中分离的抑制剂进行进一步研究。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b9ee/10221039/744c68ae333d/marinedrugs-21-00279-g001.jpg

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