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最佳卵黄样黄斑营养不良(VMD2)基因座至11号染色体着丝粒周围区域的高分辨率减数分裂和物理图谱绘制。

High-resolution meiotic and physical mapping of the best vitelliform macular dystrophy (VMD2) locus to pericentromeric chromosome 11.

作者信息

Weber B H, Vogt G, Stöhr H, Sander S, Walker D, Jones C

机构信息

Institut für Humangenetik, Biozentrum, Würzburg, Germany.

出版信息

Am J Hum Genet. 1994 Dec;55(6):1182-7.

Abstract

Best vitelliform macular dystrophy (VMD2) has previously been linked to several microsatellite markers from chromosome 11. Subsequently, additional genetic studies have refined the Best disease region to a 3.7-cM interval flanked by markers at D11S903 and PYGM. To further narrow the interval containing the Best disease gene and to obtain an estimate of the physical size of the minimal candidate region, we used a combination of high-resolution PCR hybrid mapping and analysis of recombinant Best disease chromosomes. We identified six markers from within the D11S903-PYGM interval that show no recombination with the defective gene in three multigeneration Best disease pedigrees. Our hybrid panel localizes these markers on either side of the centromere on chromosome 11. The closest markers flanking the disease gene are at D11S986 in band p12-11.22 on the short arm and at D11S480 in band q13.2-13.3 on the proximal long arm. This study demonstrates that the physical size of the Best disease region is exceedingly larger than previously estimated from the genetic data, because of the proximity of the defective gene to the centromere of chromosome 11.

摘要

最佳卵黄样黄斑营养不良(VMD2)此前已与11号染色体上的几个微卫星标记相关联。随后,更多的遗传学研究将最佳疾病区域细化到了一个3.7厘摩的区间,该区间两侧分别是标记D11S903和PYGM。为了进一步缩小包含最佳疾病基因的区间,并估算最小候选区域的物理大小,我们结合使用了高分辨率PCR杂交定位和重组最佳疾病染色体分析。我们在D11S903 - PYGM区间内鉴定出六个标记,在三个多代最佳疾病家系中,这些标记与缺陷基因无重组现象。我们的杂交面板将这些标记定位在11号染色体着丝粒两侧。位于疾病基因两侧最近的标记分别是位于短臂p12 - 11.22带的D11S986和位于近端长臂q13.2 - 13.3带的D11S480。这项研究表明,由于缺陷基因靠近11号染色体的着丝粒,最佳疾病区域的物理大小比先前从遗传数据估算的要大得多。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a129/1918450/27ed556e1c25/ajhg00045-0117-a.jpg

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