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Mutation of Solute Carrier SLC16A12 Associates with a Syndrome Combining Juvenile Cataract with Microcornea and Renal Glucosuria

机译:溶质载体SLC16A12突变与青少年白内障与微角膜和肾糖尿合并症。

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摘要

Unobstructed vision requires a particular refractive index of the lens, a measure based on the organization of the structural proteins within the differentiated lens cells. To ensure an intact lens structure, homeostasis within the lens cells is indispensable. Alterations of the lens structure result in opacity and lead to cataract. Renal glucosuria is defined by elevated glucose level in the urine without hyperglycemia and without evidence of morphological renal anomalies. In a Swiss family with autosomal dominant juvenile cataract, microcornea, and renal glucosuria, we have identified a nonsense mutation in a member of the carboxylic acid transporter family SLC16. The underlying gene defect in SLC16A12 resides within a 3 cM region on chromosome 10q23.13 defined by linkage mapping of this phenotype. We found tissue-specific variability of SLC16A12 transcript levels in control samples, with high expression in the eye and kidney, the two organs affected by this syndrome. This report demonstrates biological relevance of this solute carrier. We hypothesize that SLC16A12 is important for lens and kidney homeostasis and discuss its potential role in age-related cataract.
机译:畅通无阻的视力需要晶状体的特定折射率,这是基于分化的晶状体细胞内结构蛋白的组织的一种度量。为了确保完整的晶状体结构,晶状体细胞内的动态平衡是必不可少的。晶状体结构的改变导致不透明并导致白内障。肾性糖尿症的定义是尿液中葡萄糖水平升高,没有高血糖症,也没有肾脏形态学异常的迹象。在一个具有常染色体显性遗传的青少年白内障,微角膜和肾糖尿症的瑞士家庭中,我们发现了一个羧酸转运蛋白家族SLC16的无意义突变。 SLC16A12中潜在的基因缺陷位于染色体10q23.13的3 cM区域内,该区域由该表型的连锁作图定义。我们在对照样品中发现了SLC16A12转录本水平的组织特异性变异性,在受此综合征影响的两个器官的眼睛和肾脏中高表达。该报告证明了这种溶质载体的生物学意义。我们假设SLC16A12对于晶状体和肾脏的动态平衡很重要,并讨论其在与年龄有关的白内障中的潜在作用。

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