首页> 美国卫生研究院文献>The Journal of Molecular Diagnostics : JMD >Comparison of the Microsatellite Instability Analysis System and the Bethesda Panel for the Determination of Microsatellite Instability in Colorectal Cancers
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Comparison of the Microsatellite Instability Analysis System and the Bethesda Panel for the Determination of Microsatellite Instability in Colorectal Cancers

机译:微卫星不稳定性分析系统与Bethesda面板用于确定结直肠癌微卫星不稳定性的比较

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摘要

Microsatellite instability (MSI) analysis of colorectal cancers is clinically useful to identify patients with hereditary nonpolyposis colorectal cancer (HNPCC) caused by germline mutations of mismatch repair genes. MSI status may also predict cancer response/resistance to certain chemotherapies. We evaluated the MSI Analysis System (Promega Corp.; five mononucleotide and two pentanucleotide repeats) and compared the results to the Bethesda panel, which interrogates five microsatellite loci recommended by the 1997 National Cancer Institute-sponsored MSI workshop (three dinucleotide and two mononucleotide repeats). Thirty-four colorectal cancers were analyzed by both assays. The overall concordance between the two assays was 85% (29 of 34). There was complete concordance between the two assays for all of the MSI-high (11 of 11) and microsatellite stable (MSS; 18 of 18) cases. In the 11 MSI-high cases, all 5 of the mononucleotide loci in the MSI Analysis System demonstrated shifted alleles (100% sensitivity), and each shift resulted in products that were smaller in size than the germline alleles. All (5 of 5) of the cases interpreted as MSI-low by the Bethesda assay were interpreted as MSS by the MSI Analysis System. Our results suggest that the MSI Analysis System is generally superior and may help resolve cases of MSI-low into either MSI-high or MSS.
机译:大肠癌的微卫星不稳定性(MSI)分析在临床上可用于鉴定患有由不匹配修复基因的种系突变引起的遗传性非息肉病性大肠癌(HNPCC)的患者。 MSI状态还可以预测癌症对某些化学疗法的反应/耐药性。我们评估了MSI分析系统(Promega Corp .;五个单核苷酸和两个五核苷酸重复序列),并将结果与​​Bethesda小组进行了比较,该小组询问了1997年美国国家癌症研究所资助的MSI研讨会推荐的五个微卫星基因座(三个二核苷酸和两个单核苷酸重复序列) )。通过两种测定法分析了34种结肠直肠癌。两种测定之间的总体一致性为85%(34中的29)。对于所有MSI高(11个中的11个)和微卫星稳定(MSS; 18个中的18个)病例,两种检测方法之间完全一致。在11个MSI高的病例中,MSI分析系统中的所有5个单核苷酸基因座均显示了等位基因移位(100%敏感性),并且每次移位导致产物的大小均小于种系等位基因。贝塞斯达(Bethesda)分析将所有案例(5个中的5个)解释为MSI低,MSI分析系统将其解释为MSS。我们的结果表明,MSI分析系统通常比较优越,可以帮助将MSI低的情况解析为MSI高或MSS的情况。

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