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首页> 外文期刊>Investigative ophthalmology & visual science >Fuchs' Endothelial Corneal Dystrophy in Patients With Myotonic Dystrophy, Type 1
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Fuchs' Endothelial Corneal Dystrophy in Patients With Myotonic Dystrophy, Type 1

机译:霉菌营养不良患者患者内皮角膜营养不良,1型

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Purpose : RNA toxicity from CTG trinucleotide repeat (TNR) expansion within noncoding DNA of the transcription factor 4 (TCF4) and DM1 protein kinase (DMPK) genes has been described in Fuchs' endothelial corneal dystrophy (FECD) and myotonic dystrophy, type 1 (DM1), respectively. We prospectively evaluated DM1 patients and their families for phenotypic FECD and report the analysis of CTG expansion in the TCF4 gene and DMPK expression in corneal endothelium. Methods : FECD grade was evaluated by slit lamp biomicroscopy in 26 participants from 14 families with DM1. CTG TNR length in TCF4 and DMPK was determined by a combination of Gene Scan and Southern blotting of peripheral blood leukocyte DNA. Results : FECD grade was 2 or higher in 5 (36%) of 14 probands, significantly greater than the general population (5%) (P TCF4 (TCF4 TNR expansion in FECD, the probability of four FECD probands lacking TNR expansion was 0.4%. Neither severity of DM1 nor DMPK TNR length predicted the presence of FECD in DM1 patients. Conclusions : FECD was common in DM1 families, and the diseases cosegregated. TCF4 TNR expansion was lacking in DM1 families. These findings support a hypothesis that DMPK TNR expansion contributes to clinical FECD.
机译:目的:在Fuchs的内皮角膜营养不良(FECD)和肌肌营养不良(FECD)和Myotonic缺营药中描述了来自CTG三核苷酸的RNA毒性重复(TNR)膨胀,在转录因子4(TCF4)和DM1蛋白激酶(DMPK)基因的非编码DNA中,1型( DM1)分别。我们预期评估了DM1患者及其家族的表型FECD,并报告了在角膜内皮中TCF4基因和DMPK表达中CTG扩张的分析。方法:从14个与DM1的14个家庭中的26名参与者中,通过狭缝灯生物显微镜评估FECD等级。 TCF4和DMPK中的CTG TNR长度通过基因扫描和外周血白细胞DNA的组合来确定。结果:FECD等级为5(36%)的14个证据,明显大于一般人群(5%)(PTCF4(FECD中的TCF4 TNR扩展,缺乏TNR扩展的四个FECD证据的可能性为0.4% 。DM1和DMPK TNR长度的严重程度都预测了DM1患者中的FECD。结论:FECD在DM1家族中常见,疾病COSEGREGated。DM1家族缺乏TCF4 TNR扩张。DMPK TNR扩展缺乏明暗的假设有助于临床FECD。

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