Human glyoxylate metabolism revisited: New insights pointing to multi-organ involvement with implications for siRNA-based therapies in primary hyperoxaluria.

IF 4.2 2区医学 Q1 ENDOCRINOLOGY & METABOLISM Journal of Inherited Metabolic Disease Pub Date : 2024-11-24 DOI:10.1002/jimd.12817

Ronald J A Wanders, Jaap W Groothoff, Lisa J Deesker, Eduardo Salido, Sander F Garrelfs

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Abstract

Glyoxylate is a toxic metabolite because of its rapid conversion into oxalate, as catalyzed by the ubiquitous enzyme lactate dehydrogenase. This requires the presence of efficient glyoxylate detoxification systems in multiple subcellular compartments, as glyoxylate is produced in peroxisomes, mitochondria, and the cytosol. Alanine glyoxylate aminotransferase (AGT) and glyoxylate reductase/hydroxypyruvate reductase (GRHPR) are the key enzymes involved in glyoxylate detoxification. Bi-allelic mutations in the genes coding for these enzymes cause primary hyperoxaluria type 1 (PH1) and 2 (PH2), respectively. Glyoxylate is derived from various sources, including 4-hydroxyproline, which is degraded in mitochondria, generating pyruvate and glyoxylate, as catalyzed by the mitochondrial enzyme 4-hydroxy-2-oxoglutarate aldolase (HOGA); however, counterintuitively, a defect in HOGA1 is the molecular basis of primary hyperoxaluria type 3 (PH3). Irrespective of its underlying cause, hyperoxaluria in humans leads to nephrocalcinosis, recurrent urolithiasis, and kidney damage, which may culminate in kidney failure requiring combined liver-kidney transplantation in severely affected patients. In the past few years, therapeutic options, especially for primary hyperoxaluria type 1 (PH1), have greatly been improved thanks to the introduction of two RNAi-based therapies that inhibit either the production of glycolate oxidase (lumasiran) or lactate dehydrogenase (nedosiran). While lumasiran only targets PH1 patients, nedosiran was specifically developed to target all three subtypes of PH. Inspired by the findings reported in the literature that nedosiran effectively reduced urinary oxalate excretion in PH1 patients but not in PH2 or PH3 patients, we have now revisited glyoxylate metabolism in humans and performed a thorough literature study which revealed that glyoxylate/oxalate metabolism is not confined to the liver but instead involves multiple different organs. This new view on glyoxylate/oxalate metabolism in humans may well explain the disappointing results of nedosiran in PH2 and PH3, and provides new clues for the future generation of new therapeutic strategies for PH2 and PH3.

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人类乙醛酸代谢再探：多器官参与的新发现，对基于 siRNA 的原发性高草酸尿症疗法的影响。

在无处不在的乳酸脱氢酶催化下，乙醛酸会迅速转化为草酸盐，因此乙醛酸是一种有毒的代谢物。这就要求在多个亚细胞区存在高效的乙醛酸解毒系统，因为乙醛酸是在过氧物酶体、线粒体和细胞质中产生的。乙醛酸丙氨酸氨基转移酶（AGT）和乙醛酸还原酶/羟基丙酮酸还原酶（GRHPR）是参与乙醛酸解毒的关键酶。这些酶编码基因的双等位基因突变分别导致原发性高草酸尿症 1 型（PH1）和 2 型（PH2）。在线粒体酶 4-hydroxy-2-oxoglutarate aldolase（HOGA）的催化下，4-羟基脯氨酸在线粒体中降解，生成丙酮酸和乙醛酸；然而，与直觉相反的是，HOGA1 的缺陷是原发性高草酸尿症 3 型（PH3）的分子基础。无论其根本原因如何，人类高草酸尿症都会导致肾钙化、复发性尿路结石和肾损伤，严重患者可能最终导致肾衰竭，需要进行肝肾联合移植。在过去几年中，由于引入了两种基于 RNAi 的疗法，抑制乙醛酸氧化酶（lumasiran）或乳酸脱氢酶（nedosiran）的产生，治疗方案，尤其是原发性高草酸尿症 1 型（PH1）的治疗方案得到了极大的改善。鲁马西兰只针对 PH1 患者，而奈多西兰则是专门针对 PH 的所有三种亚型开发的。有文献报道，奈多西兰能有效减少 PH1 患者的尿草酸盐排泄，但不能减少 PH2 或 PH3 患者的尿草酸盐排泄，受此启发，我们现在重新审视了人类的乙醛酸代谢，并进行了全面的文献研究，结果发现乙醛酸/草酸盐代谢并不局限于肝脏，而是涉及多个不同的器官。这一关于人体乙醛酸盐/草酸盐代谢的新观点很好地解释了奈多西兰在 PH2 和 PH3 中令人失望的结果，并为未来针对 PH2 和 PH3 的新治疗策略提供了新的线索。

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来源期刊

Journal of Inherited Metabolic Disease 医学-内分泌学与代谢

CiteScore

9.50

自引率

7.10%

发文量

117

审稿时长

4-8 weeks

期刊介绍： The Journal of Inherited Metabolic Disease (JIMD) is the official journal of the Society for the Study of Inborn Errors of Metabolism (SSIEM). By enhancing communication between workers in the field throughout the world, the JIMD aims to improve the management and understanding of inherited metabolic disorders. It publishes results of original research and new or important observations pertaining to any aspect of inherited metabolic disease in humans and higher animals. This includes clinical (medical, dental and veterinary), biochemical, genetic (including cytogenetic, molecular and population genetic), experimental (including cell biological), methodological, theoretical, epidemiological, ethical and counselling aspects. The JIMD also reviews important new developments or controversial issues relating to metabolic disorders and publishes reviews and short reports arising from the Society''s annual symposia. A distinction is made between peer-reviewed scientific material that is selected because of its significance for other professionals in the field and non-peer- reviewed material that aims to be important, controversial, interesting or entertaining (“Extras”).