Nyström-Lahti M, Parsons R, Sistonen P, Pylkkänen L, Aaltonen L A, Leach F S, Hamilton S R, Watson P, Bronson E, Fusaro R
Department of Medical Genetics, University of Helsinki, Finland.
Am J Hum Genet. 1994 Oct;55(4):659-65.
Two susceptibility loci for hereditary nonpolyposis colorectal cancer (HNPCC) have been identified, and each contains a mismatch repair gene: MSH2 on chromosome 2p and MLH1 on chromosome 3p. We studied the involvement of these loci in 13 large HNPCC kindreds originating from three different continents. Six families showed close linkage to the 2p locus, and a heritable mutation of the MSH2 gene was subsequently found in four. The 2p-linked kindreds included a family characterized by the lack of extracolonic manifestations (Lynch I syndrome), as well as two families with cutaneous manifestations typical of the Muir-Torre syndrome. Four families showed evidence for linkage to the 3p locus, and a heritable mutation of the MLH1 gene was later detected in three. One 3p-linked kindred was of Amerindian origin. Of the remaining three families studied for linkage, one showed lod scores compatible with exclusion of both MSH2 and MLH1, while lod scores obtained in the other two families suggested exclusion of one HNPCC locus (MSH2 or MLH1) but were uninformative for markers flanking the other locus. Our results suggest that mismatch repair genes on 2p and 3p account for a major share of HNPCC in kindreds that can be evaluated by linkage analysis.
遗传性非息肉病性结直肠癌(HNPCC)的两个易感基因座已被确定,每个基因座都包含一个错配修复基因:位于2号染色体短臂上的MSH2和位于3号染色体短臂上的MLH1。我们研究了来自三大洲的13个大型HNPCC家系中这些基因座的情况。六个家系显示与2p基因座紧密连锁,随后在其中四个家系中发现了MSH2基因的遗传性突变。与2p连锁的家系包括一个以缺乏结肠外表现为特征的家系(林奇I综合征),以及两个具有穆尔-托综合征典型皮肤表现的家系。四个家系显示与3p基因座连锁的证据,后来在其中三个家系中检测到了MLH1基因的遗传性突变。一个与3p连锁的家系起源于美洲印第安人。在其余三个进行连锁研究的家系中,一个家系的对数优势分数与排除MSH2和MLH1均相符,而另外两个家系获得的对数优势分数表明排除了一个HNPCC基因座(MSH2或MLH1),但对于另一个基因座侧翼的标记无信息价值。我们的结果表明,2p和3p上的错配修复基因在可通过连锁分析评估的家系中占HNPCC的很大一部分。
