Kastrinos Fay, Stoffel Elena M, Balmaña Judith, Steyerberg Ewout W, Mercado Rowena, Syngal Sapna
Division of Gastroenterology, Brigham and Women's Hospital, Boston, Massachusetts, Boston, MA 02115, USA.
Cancer Epidemiol Biomarkers Prev. 2008 Aug;17(8):2044-51. doi: 10.1158/1055-9965.EPI-08-0301.
Lynch syndrome is caused by germ-line mismatch repair gene mutations. We examined the phenotypic differences between MLH1 and MSH2 gene mutation carriers and whether mutation type (point versus large rearrangement) affected phenotypic expression.
This is a cross-sectional prevalence study of 1,914 unrelated probands undergoing clinical genetic testing for MLH1 and MSH2 mutations at a commercial laboratory.
Fifteen percent (285 of 1,914) of subjects had pathogenic mutations (112 MLH1, 173 MSH2). MLH1 carriers had a higher prevalence of colorectal cancer (79% versus 69%, P = 0.08) and younger mean age at diagnosis (42.2 versus 44.8 years, P = 0.03) than MSH2 carriers. Forty-one percent of female carriers had endometrial cancer and prevalence was similar in both groups. Other cancers were more frequent in MSH2 carriers (24% versus 9%, P = 0.001) and their families (P < 0.001). Multivariable analyses confirmed these associations. Of the 1,016 subjects who underwent Southern blot analysis, 42 had large rearrangements (7 MLH1, 35 MSH2). There were no phenotypic differences between carriers with large rearrangements and point mutations.
In this large study of mismatch repair gene mutation carriers from the United States, MLH1 carriers had more colorectal cancer than MSH2 carriers whereas endometrial cancer prevalence was similar. Large genomic rearrangements were more frequent in the MSH2 gene. MSH2 carriers and their relatives have more extracolonic nonendometrial Lynch syndrome-associated cancers and may benefit from additional screening.
林奇综合征由种系错配修复基因突变引起。我们研究了MLH1和MSH2基因突变携带者之间的表型差异,以及突变类型(点突变与大片段重排)是否影响表型表达。
这是一项横断面患病率研究,对1914名在商业实验室接受MLH1和MSH2突变临床基因检测的无亲缘关系的先证者进行了研究。
15%(1914名中的285名)受试者存在致病突变(112名MLH1突变,173名MSH2突变)。与MSH2突变携带者相比,MLH1突变携带者患结直肠癌的患病率更高(79%对69%,P = 0.08),诊断时的平均年龄更小(42.2岁对44.8岁,P = 0.03)。41%的女性携带者患有子宫内膜癌,两组患病率相似。其他癌症在MSH2突变携带者(24%对9%,P = 0.001)及其家族中更常见(P < 0.001)。多变量分析证实了这些关联。在1016名接受Southern印迹分析的受试者中,42名存在大片段重排(7名MLH1突变,35名MSH2突变)。大片段重排携带者与点突变携带者之间没有表型差异。
在这项对来自美国的错配修复基因突变携带者的大型研究中,MLH1突变携带者患结直肠癌的比例高于MSH2突变携带者,而子宫内膜癌患病率相似。MSH2基因中大片段基因组重排更常见。MSH2突变携带者及其亲属有更多的结肠外非子宫内膜林奇综合征相关癌症,可能从额外的筛查中获益。
