Primary hyperoxaluria I, II, III types in children (review of literature)

Nephrology (Saint-Petersburg) Pub Date : 2023-03-06 DOI:10.36485/1561-6274-2023-27-1-18-30

M. Amiryan, Zh. G. Leviashvili, N. Savenkova

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Abstract

This review presents the latest data on the classification, pathogenesis, clinical and genetic features, and therapy of primary hyperoxaluria types I, II, and III in children with autosomal recessive inheritance. ORPHA portal of orphan diseases presents genes responsible for primary hyperoxaluria type I AGXT (93598); type II and type II GRHPR (93599), type III HOGA1 (93600). Worldwide genetic studies have established the pathogenesis, clinical phenotype and genotype features of primary hyperoxaluria. The pathogenesis of primary hyperoxaluria in children is based on impaired hepatic glyoxylate metabolism. The enzyme AGT catalyzes the conversion of L-alanine and glyoxylate to pyruvate and glycine, with vitamin B6 (pyridoxine) serving as a coenzyme for this reaction. Increased production of endogenous oxalate leads to increased blood oxalate concentrations and urinary oxalate excretion with the formation of renal calcium oxalate crystals and radiopaque concrements (calcium oxalate monohydrate – vevelite, calcium oxalate dihydrate – vedellite). High risk of progression to chronic kidney disease in primary hyperoxaluria in children of types I and II. Systemic oxalosis develops with increasing serum oxalate levels and the formation of calcium oxalate crystals with deposition in many organs and tissues. Therapy for primary hyperoxaluria in children includes: hydration (3l/m2/day) and citrates 100–150 mg/kg/day (potassium citrate 0.3–0.5 mmol/kg/day), pyridoxine at a dose of 5 to 20 mg/kg/day for vitamin B6 sensitive type I primary hyperoxaluria. Administration of oxalobacter formigenes and diet is effective. Combined liver and then kidney transplantation or simultaneous liver and kidney transplantation in patients with type I PH in B6-insensitive and isolated liver transplantation in B6-sensitive variants are performed. Timely molecular genetic testing in children with nephrocalcinosis makes it possible to establish a clinical and genetic diagnosis of type I, II, III PH, to carry out a personalised approach to treatment and to predict future health status.

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儿童原发性高草酸尿I、II、III型(文献回顾)

本文综述了常染色体隐性遗传儿童原发性高血氧症I型、II型和III型的分类、发病机制、临床和遗传特征以及治疗方面的最新资料。孤儿病的ORPHA门户显示了负责原发性高草酸尿I型AGXT的基因(93598);II型和II型GRHPR (93599)， III型HOGA1(93600)。世界范围内的遗传学研究已经确立了原发性高血氧症的发病机制、临床表型和基因型特征。儿童原发性高草酸尿的发病机制是基于肝脏乙醛酸代谢受损。AGT酶催化l -丙氨酸和乙醛酸盐转化为丙酮酸和甘氨酸，维生素B6(吡哆醇)作为该反应的辅酶。内源性草酸产生的增加导致血液草酸浓度和尿液草酸排泄增加，形成肾脏草酸钙晶体和不透射线的水泥(一水草酸钙-维维特，二水草酸钙-维维特)。I型和II型儿童原发性高草酸尿进展为慢性肾病的高风险随着血清草酸水平的升高和草酸钙晶体的形成并在许多器官和组织中沉积，全身性草酸病发展。儿童原发性高草酸尿的治疗包括:水合(3l/m2/天)和柠檬酸100 - 150mg /kg/天(柠檬酸钾0.3-0.5 mmol/kg/天)，吡哆醇5 - 20mg /kg/天治疗维生素B6敏感型I型原发性高草酸尿。给予草酸杆菌和饮食是有效的。对b6不敏感的I型PH患者进行联合肝肾移植或同时进行肝肾移植，对b6敏感变异患者进行分离肝移植。及时对肾钙化症患儿进行分子基因检测，可以建立I型、II型、III型PH的临床和遗传诊断，开展个性化的治疗方法，并预测未来的健康状况。

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

Nephrology (Saint-Petersburg)

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0.50

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