From orphan to oncogene: The role of GPR35 in cancer and immune modulation

IF 9.3 2区医学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY

Cytokine & Growth Factor Reviews Pub Date : 2024-06-01 DOI:10.1016/j.cytogfr.2024.03.004

Simran Takkar , Gunjan Sharma , Jyoti B. Kaushal , K.M. Abdullah , Surinder K. Batra , Jawed A. Siddiqui

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引用次数: 0

Abstract

G protein-coupled receptors (GPCRs) are well-studied and the most traceable cell surface receptors for drug discovery. One of the intriguing members of this family is G protein-coupled receptors 35 (GPR35), which belongs to the class A rhodopsin-like family of GPCRs identified over two decades ago. GPR35 presents interesting features such as ubiquitous expression and distinct isoforms. Moreover, functional and genome-wide association studies on its widespread expression have linked GPR35 with pathophysiological disease progression. Various pieces of evidence have been accumulated regarding the independent or endogenous ligand-dependent role of GPR35 in cancer progression and metastasis. In the current scenario, the relationship of this versatile receptor and its putative endogenous ligands for the activation of oncogenic signal transduction pathways at the cellular level is an active area of research. These intriguing features offered by GPR35 make it an oncological target, justifying its uniqueness at the physiological and pathophysiological levels concerning other GPCRs. For pharmacologically targeting receptor-induced signaling, few potential competitive antagonists have been discovered that offer high selectivity at a human level. In addition to its fascinating features, targeting GPR35 at rodent and human orthologue levels is distinct, thus contributing to the sub-species selectivity. Strategies to modulate these issues will help us understand and truly target GPR35 at the therapeutic level. In this article, we have provided prospects on each topic mentioned above and suggestions to overcome the challenges. This review discusses the molecular mechanism and signal transduction pathways activated by endogenous ligands or spontaneous auto-activation of GPR35 that contributes towards disease progression. Furthermore, we have highlighted the GPR35 structure, ubiquitous expression, its role in immunomodulation, and at the pathophysiological level, especially in cancer, indicating its status as a versatile receptor. Subsequently, we discussed the various proposed ligands and their mechanism of interaction with GPR35. Additionally, we have summarized the GPR35 antagonist that provides insights into the opportunities for therapeutically targeting this receptor.

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从孤儿到癌基因：GPR35 在癌症和免疫调节中的作用。

G 蛋白偶联受体（GPCR）是研究得最透彻的细胞表面受体，也是药物发现中最容易追踪的细胞表面受体。二十多年前发现的 G 蛋白偶联受体 35（GPR35）属于 GPCR 的 A 类视黄醛样家族，是这一家族中引人入胜的成员之一。GPR35 具有无处不在的表达和不同的同工型等有趣特征。此外，对其广泛表达的功能性和全基因组关联研究表明，GPR35 与病理生理疾病的进展有关。关于 GPR35 在癌症进展和转移中的独立或内源性配体依赖性作用，已经积累了各种证据。在目前的情况下，这种多用途受体及其假定的内源性配体在细胞水平激活致癌信号转导通路的关系是一个活跃的研究领域。GPR35 所具有的这些引人入胜的特点使其成为肿瘤靶点，并证明了它在生理和病理生理学水平上相对于其他 GPCR 的独特性。在以受体诱导信号为药物靶点方面，已发现的潜在竞争性拮抗剂中，只有少数能在人体水平上提供高选择性。除了其引人入胜的特点外，靶向啮齿动物和人类同源物水平的 GPR35 也各不相同，因此造成了亚种选择性。调节这些问题的策略将有助于我们了解并真正在治疗层面上靶向 GPR35。在本文中，我们对上述每个主题进行了展望，并提出了克服挑战的建议。本综述讨论了由内源性配体激活或 GPR35 自发自动激活导致疾病进展的分子机制和信号转导途径。此外，我们还强调了 GPR35 的结构、泛在表达、在免疫调节中的作用以及在病理生理学水平上的作用，尤其是在癌症中的作用，这表明它是一种多功能受体。随后，我们讨论了各种拟议配体及其与 GPR35 的相互作用机制。此外，我们还总结了 GPR35 拮抗剂，为针对该受体的治疗提供了机会。

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

Cytokine & Growth Factor Reviews 生物-生化与分子生物学

CiteScore

21.10

自引率

1.50%

发文量

审稿时长

22 days

期刊介绍： Cytokine & Growth Factor Reviews is a leading publication that focuses on the dynamic fields of growth factor and cytokine research. Our journal offers a platform for authors to disseminate thought-provoking articles such as critical reviews, state-of-the-art reviews, letters to the editor, and meeting reviews. We aim to cover important breakthroughs in these rapidly evolving areas, providing valuable insights into the multidisciplinary significance of cytokines and growth factors. Our journal spans various domains including signal transduction, cell growth and differentiation, embryonic development, immunology, tumorigenesis, and clinical medicine. By publishing cutting-edge research and analysis, we aim to influence the way researchers and experts perceive and understand growth factors and cytokines. We encourage novel expressions of ideas and innovative approaches to organizing content, fostering a stimulating environment for knowledge exchange and scientific advancement.