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作 者:缪为民[1] 魏勇[1] 邓炜[1] 周炜[1] 李恒俊 柴建华[1] 谈家桢[1]
机构地区:[1]复旦大学遗传学研究所
出 处:《高技术通讯》1996年第8期41-45,共5页Chinese High Technology Letters
基 金:863计划资助;国家自然科学基金
摘 要:人类X染色体短臂21.3—11.3区是含有视网膜色素变性等数种遗传病基因位点的区域。我们对这个具有重要医学生物学意义的区段进行了YAC重叠群构建。用这一区域已知的探针(OTC、DXS166、DMDcDNA)及STS位标,以YAC菌落原位杂交法及PCR法进行了YAC的筛选;也采用了法国CEPH和英国ICRF的部分YAC;总共得到了55个阳性YAC。对上述YAC进行了长度测定,26对微卫星STS图谱分析,单拷贝探针的杂交定位,Alu-PCR指纹图谱分析。综合上述信息,对这些YAC进行了排序,在Xp21.3-11.3区得到了6个0YAC重叠群,覆盖了约15Mb的范围。这些YAC重叠群的构建为开展该区域疾病基因的定位克隆(Positionalcloning)及DNA顺序测定奠定了基础。Human X chromosome short arm Xp21. 3-p11. 3 is an area which contains several genetic disease gene lo'ci. In this work, the YAC contig construction was done for this region. Some DNA probes and STS markers was used for YAC screening. Totally 55 YACs were obtained from the YAC libraries of CEPH,ICRF and ours.The size determination, 26 pairs of microsatelite STS analysis, single copy probe hybridization and Alu-PCR fingerprinting were Performed with these YACs. These results allowed us to map these YACs, and finally 6 YAC contigs were obtained in Xp21. 3-11.3,covering about 15 Mb.This work will greatly facilitate the positional cloning of disease genes or the genome sequencins in this important region.
分 类 号:R394[医药卫生—医学遗传学]
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