首页> 外文OA文献 >Genetic linkage to the type VII collagen gene (COL7A1) in 26 families with generalised recessive dystrophic epidermolysis bullosa and anchoring fibril abnormalities.
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Genetic linkage to the type VII collagen gene (COL7A1) in 26 families with generalised recessive dystrophic epidermolysis bullosa and anchoring fibril abnormalities.

机译:在26例普遍性隐性营养不良性大疱性表皮松解症和锚定纤维异常的家族中,与VII型胶原蛋白基因(COL7A1)的遗传连锁。

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摘要

To strengthen the evidence for genetic linkage to COL7A1, we have studied 26 generalised recessive dystrophic epidermolysis bullosa (EB) families of British, Italian, Irish, and South African origin. We chose two linkage markers, a COL7A1 PvuII intragenic polymorphism and a highly informative anonymous microsatellite marker, D3S1100, which maps close to the COL7A1 locus at 3p21.1-3. Diagnosis was established by family history, clinical examination, immunofluorescence, and ultrastructural studies. The PvuII marker was informative in 16 families with a maximum lod score (Zmax) of 3.51 at recombination fraction (theta) = 0. The D3S1100 microsatellite was informative in 24 out of 25 families with Zmax = 6.8 at theta = 0.05 (Z = 4.94 at theta = 0) and no obligatory recombination events. These data strongly suggest that COL7A1 mutations cause EB in these families and, combined with previous studies, indicate locus homogeneity. The importance of anchoring fibrils for dermal-epidermal adhesion is further underlined. D3S1100 may later prove useful in prenatal diagnosis of this disease, if used in combination with other markers.
机译:为了加强与COL7A1遗传连锁的证据,我们研究了26个英国,意大利,爱尔兰和南非血统的隐性营养不良性大疱性表皮松解(EB)家族。我们选择了两个连锁标记,一个COL7A1 PvuII基因内多态性和一个高度有用的匿名微卫星标记D3S1100,其与3p21.1-3处的COL7A1基因座接近。通过家族史,临床检查,免疫荧光和超微结构研究确定诊断。在重组分数(θ)= 0时,PvuII标记在16个家族中具有较高的lod得分(Zmax)为3.51。在25个家族中,D3S1100微卫星在θ= 0.05时Zmax = 6.8的25个家族中具有丰富的信息(Z = 4.94在θ= 0),没有强制性重组事件。这些数据强烈表明,COL7A1突变会导致这些家族中的EB,并与先前的研究相结合,表明基因座的均一性。进一步强调了锚定原纤维对于真皮-表皮粘附的重要性。如果与其他标记物结合使用,D3S1100可能在后来证明对该疾病的产前诊断中很有用。

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