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Re: Primary hyperoxaluria type III gene HOGA1 (Formerly DHDPSL) as a possible risk factor for idiopathic calcium oxalate urolithiasis

机译:回复:原发性高草酸尿症III型基因HOGA1(以前为DHDPSL)可能是特发性草酸钙尿石症的危险因素

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Background and Objectives: Primary hyperoxaluria types I and II (PHI and PHII) are rare monogenic causes of hyperoxaluria and-calcium oxalate urolithiasis. Recently, we described type III, due to mutations in HOGA1 (formerly DHDPSL), hypothesized to cause a gain of mitochondrial 4-hydroxy-2-oxoglutarate aldolase activity, resulting in excess oxalate. Design, Setting, Participants, & Measurements: To further explore the pathophysiology of HOGA1, we screened additional non-PHI-PHII patients and performed reverse transcription PCR analysis. Postulating that HOGA1 may influence urine oxalate, we also screened 100 idiopathic calcium oxalate stone formers. Results: Of 28 unrelated hyperoxaluric patients with marked hyperoxaluria not due to PHI, PHII, or any identifiable secondary cause, we identified 10 (36%) with two HOGA1 mutations (four novel, including a nonsense variant). Reverse transcription PCR of the stop codon and two common mutations showed stable expression.
机译:背景与目的:原发性I和II型高草酸尿症(PHI和PHII)是高草酸尿症和草酸钙尿石症的罕见单基因病因。最近,我们描述了III型,这是由于HOGA1(以前称为DHDPSL)中的突变引起的,据推测会引起线粒体4-羟基-2-氧代戊二酸醛缩酶活性的增加,从而导致草酸盐过量。设计,设置,参与者和测量:为了进一步探讨HOGA1的病理生理,我们筛选了其他非PHI-PHII患者并进行了逆转录PCR分析。假设HOGA1可能会影响尿液草酸,我们还筛选了100位特发性草酸钙结石形成剂。结果:在28例因PH,PHII或任何可识别的继发原因而并非明显的高草酸尿症的高血尿症患者中,我们鉴定出10个(36%)具有两个HOGA1突变(四个新突变,包括一个无意义的变异)。终止密码子和两个常见突变的反转录PCR显示稳定的表达。

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    《The Journal of Urology》 |2012年第3期|共2页
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    AssimosD.;

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  • 入库时间 2022-08-19 15:17:16

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