Restoring function to inactivating G protein-coupled receptor variants in the hypothalamic–pituitary–gonadal axis†

IF 3.3 4区医学 Q2 ENDOCRINOLOGY & METABOLISM

Journal of Neuroendocrinology Pub Date : 2024-06-09 DOI:10.1111/jne.13418

Tarryn Radomsky, Ross C. Anderson, Robert P. Millar, Claire L. Newton

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Abstract

G protein-coupled receptors (GPCRs) are central to the functioning of the hypothalamic–pituitary–gonadal axis (HPG axis) and include the rhodopsin-like GPCR family members, neurokinin 3 receptor, kappa-opioid receptor, kisspeptin 1 receptor, gonadotropin-releasing hormone receptor, and the gonadotropin receptors, luteinizing hormone/choriogonadotropin receptor and follicle-stimulating hormone receptor. Unsurprisingly, inactivating variants of these receptors have been implicated in a spectrum of reproductive phenotypes, including failure to undergo puberty, and infertility. Clinical induction of puberty in patients harbouring such variants is possible, but restoration of fertility is not always a realisable outcome, particularly for those patients suffering from primary hypogonadism. Thus, novel pharmaceuticals and/or a fundamental change in approach to treating these patients are required. The increasing wealth of data describing the effects of coding-region genetic variants on GPCR function has highlighted that the majority appear to be dysfunctional as a result of misfolding of the encoded receptor protein, which, in turn, results in impaired receptor trafficking through the secretory pathway to the cell surface. As such, these intracellularly retained receptors may be amenable to ‘rescue’ using a pharmacological chaperone (PC)-based approach. PCs are small, cell permeant molecules hypothesised to interact with misfolded intracellularly retained proteins, stabilising their folding and promoting their trafficking through the secretory pathway. In support of the use of this approach as a viable therapeutic option, it has been observed that many rescued variant GPCRs retain at least a degree of functionality when ‘rescued’ to the cell surface. In this review, we examine the GPCR PC research landscape, focussing on the rescue of inactivating variant GPCRs with important roles in the HPG axis, and describe what is known regarding the mechanisms by which PCs restore trafficking and function. We also discuss some of the merits and obstacles associated with taking this approach forward into a clinical setting.

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恢复下丘脑-垂体-性腺轴中失活 G 蛋白偶联受体变体的功能1。

G 蛋白偶联受体（GPCRs）是下丘脑-垂体-性腺轴（HPG 轴）功能的核心，包括类罗丹明 GPCR 家族成员、神经激肽 3 受体、卡帕类阿片受体、kisspeptin 1 受体、促性腺激素释放激素受体，以及促性腺激素受体、黄体生成素/绒毛促性腺激素受体和卵泡刺激素受体。毫不奇怪，这些受体的失活变体与一系列生殖表型有关，包括无法进入青春期和不育症。临床上可以诱导携带此类变异体的患者进入青春期，但恢复生育能力并非总能实现，尤其是对那些患有原发性性腺功能减退症的患者而言。因此，需要新型药物和/或从根本上改变治疗这些患者的方法。描述编码区基因变异对 GPCR 功能影响的数据越来越丰富，这些数据突出表明，大多数基因变异似乎是由于编码的受体蛋白折叠错误而导致功能障碍，这反过来又会导致受体通过分泌途径向细胞表面的转运功能受损。因此，这些滞留在细胞内的受体可能可以通过基于药理学伴侣（PC）的方法进行 "拯救"。PC 是一种具有细胞渗透性的小分子，据推测能与折叠错误的细胞内滞留蛋白相互作用，稳定它们的折叠并促进它们通过分泌途径进行运输。为了支持将这种方法作为一种可行的治疗方案，我们观察到许多被拯救的变体 GPCR 在被 "拯救 "到细胞表面时至少保留了一定程度的功能。在本综述中，我们审视了 GPCR PC 的研究现状，重点关注在 HPG 轴中发挥重要作用的失活变异 GPCR 的拯救，并介绍了 PC 恢复贩运和功能的已知机制。我们还讨论了将这种方法应用于临床的一些优点和障碍。

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

Journal of Neuroendocrinology 医学-内分泌学与代谢

CiteScore

6.40

自引率

6.20%

发文量

137

审稿时长

4-8 weeks

期刊介绍： Journal of Neuroendocrinology provides the principal international focus for the newest ideas in classical neuroendocrinology and its expanding interface with the regulation of behavioural, cognitive, developmental, degenerative and metabolic processes. Through the rapid publication of original manuscripts and provocative review articles, it provides essential reading for basic scientists and clinicians researching in this rapidly expanding field. In determining content, the primary considerations are excellence, relevance and novelty. While Journal of Neuroendocrinology reflects the broad scientific and clinical interests of the BSN membership, the editorial team, led by Professor Julian Mercer, ensures that the journal’s ethos, authorship, content and purpose are those expected of a leading international publication.