Four novel variants identified in primary hyperoxaluria and genotypic and phenotypic analysis in 21 Chinese patients

Qing, Xin; Dong, Yameng; Guo, Wenbo; Zhao, Xiangzhong; Liu, Zhiying; Shi, Xiaomeng; Lang, Yanhua; Shao, Leping

doi:10.3389/fgene.2023.1124745

Cited by 3 publications

(1 citation statement)

References 60 publications

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“…The relation between the molecular and clinical aspects of PH1 can be exploited not only to explain or predict treatment responsiveness, but also to interpret the effects of newly-identified mutations. In the last years, a more rapid and comprehensive genetic characterization of hyperoxaluria patients has been performed, which in turn has increased the number of new mutations identified in the genes associated with the three forms of PH [ 52 – 54 , 55 ▪ , 56 ▪ ]. This situation has posed new challenges in the interpretation of missense variants, and has highlighted the use of functional studies to support pathogenicity assessment [ 57 ].…”

Section: Molecular Pathogenesis Of Primary Hyperoxaluria Type 1 (Ph1)mentioning

confidence: 99%

A molecular journey on the pathogenesis of primary hyperoxaluria

Cellini

2024

Current Opinion in Nephrology &Amp; Hypertension

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Purpose of review Primary hyperoxalurias (PHs) are rare disorders caused by the deficit of liver enzymes involved in glyoxylate metabolism. Their main hallmark is the increased excretion of oxalate leading to the deposition of calcium oxalate stones in the urinary tract. This review describes the molecular aspects of PHs and their relevance for the clinical management of patients. Recent findings Recently, the study of PHs pathogenesis has received great attention. The development of novel in vitro and in vivo models has allowed to elucidate how inherited mutations lead to enzyme deficit, as well as to confirm the pathogenicity of newly-identified mutations. In addition, a better knowledge of the metabolic consequences in disorders of liver glyoxylate detoxification has been crucial to identify the key players in liver oxalate production, thus leading to the identification and validation of new drug targets. Summary The research on PHs at basic, translational and clinical level has improved our knowledge on the critical factors that modulate disease severity and the response to the available treatments, leading to the development of new drugs, either in preclinical stage or, very recently, approved for patient treatment.

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Section: Molecular Pathogenesis Of Primary Hyperoxaluria Type 1 (Ph1)mentioning

confidence: 99%

A molecular journey on the pathogenesis of primary hyperoxaluria

Cellini

2024

Current Opinion in Nephrology &Amp; Hypertension

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Clinical characteristics, genetic profile and short-term outcomes of children with primary hyperoxaluria type 2: a nationwide experience

Krishnasamy,

Deepthi,

Kamath

et al. 2023

Pediatr Nephrol

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Mutation Characteristics of Primary Hyperoxaluria in the Chinese Population and Current International Diagnosis and Treatment Status

Zhu,

Cheung,

Zhang

et al. 2024

Kidney Dis

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Background: Primary hyperoxaluria (PH) is a rare autosomal recessive disorder, mainly due to the increase in endogenous oxalate production, causing a series of clinical features such as kidney stones, nephrocalcinosis, progressive impairment of renal function, and systemic oxalosis. There are three common genetic causes of glycolate metabolism anomalies. Among them, PH type 1 is the most prevalent and severe type, and early end-stage renal failure often occurs. Summary: This review summarizes primary hyperoxaluria through pathophysiology, genotype, clinical manifestation, diagnosis, and treatment options. And explore the characteristics of Chinese PH patients. Key Messages: Diagnosis of this rare disease is based on clinical symptoms, urinary or blood oxalate concentrations, liver biopsy, and genetic testing. Currently, the main treatment is massive hydration, citrate inhibition of crystallization, dialysis, liver and kidney transplantation, and pyridoxine. Recently, RNA interference drugs have also been used. In addition, technologies such as gene editing and autologous liver cell transplantation are also being developed. C.815_816insGA and c.33_34insC mutation in the AGXT gene could be a common variant in Chinese PH1 population. Mutations at the end of exon 6 account for approximately 50% of all Chinese HOGA1 mutations. Currently, the treatment of PH in China still relies mainly on symptomatic and high-throughput dialysis, with poor prognosis (especially for PH1 patients).

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Four novel variants identified in primary hyperoxaluria and genotypic and phenotypic analysis in 21 Chinese patients

Cited by 3 publications

References 60 publications

A molecular journey on the pathogenesis of primary hyperoxaluria

A molecular journey on the pathogenesis of primary hyperoxaluria

Clinical characteristics, genetic profile and short-term outcomes of children with primary hyperoxaluria type 2: a nationwide experience

Mutation Characteristics of Primary Hyperoxaluria in the Chinese Population and Current International Diagnosis and Treatment Status

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