Targeting glutamate carboxypeptidase II in IBD.

Q1 Pharmacology, Toxicology and Pharmaceutics

Advances in pharmacology Pub Date : 2024-01-01 Epub Date: 2024-10-15 DOI:10.1016/bs.apha.2024.10.001

Diane E Peters

引用次数: 0

Abstract

Over the past decade, the zinc metalloenzyme glutamate carboxypeptidase (GCPII) has emerged as a novel therapeutic target for IBD. This enzyme is minimally expressed in healthy ileum or colon, but is profoundly upregulated in multiple IBD subtypes including: adult and pediatric Crohn's disease (CD), adult and pediatric ulcerative colitis (UC), and UC pouchitis. Encouragingly, small molecule GCPII inhibitors display promising efficacy in chemical and genetic preclinical colitis models. In this chapter we will: (1) review GCPII biology, (2) present the data confirming its upregulation in IBD patients at gene and protein levels, (3) discuss foundational pre-clinical studies that established the anti-colitis efficacy of small molecule GCPII inhibitors, and (4) introduce the rationale and development of a novel class of GCPII inhibitors, including lead compound (S)-IBD3540, which hold therapeutic promise for IBD.

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在 IBD 中靶向谷氨酸羧肽酶 II。

在过去十年中，锌金属酶谷氨酸羧肽酶（GCPII）已成为治疗 IBD 的新靶点。这种酶在健康回肠或结肠中表达极少，但在多种 IBD 亚型中却严重上调，包括：成人和儿童克罗恩病（CD）、成人和儿童溃疡性结肠炎（UC）以及 UC 肠袋炎。令人鼓舞的是，小分子 GCPII 抑制剂在化学和遗传临床前结肠炎模型中显示出良好的疗效。在本章中，我们将(1)回顾 GCPII 的生物学特性，(2)介绍证实其在 IBD 患者体内基因和蛋白水平上调的数据，(3)讨论确定小分子 GCPII 抑制剂抗结肠炎疗效的基础临床前研究，(4)介绍新型 GCPII 抑制剂（包括先导化合物 (S)-IBD3540）的原理和开发，这些抑制剂有望治疗 IBD。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Advances in pharmacology Pharmacology, Toxicology and Pharmaceutics-Pharmacology

CiteScore

9.10

自引率

0.00%

发文量