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BAT-26 and BAT-40 Instability in Colorectal Adenomas and Carcinomas and Germline Polymorphisms

机译:大肠腺瘤,癌和生殖细胞多态性中的BAT-26和BAT-40不稳定性

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摘要

Analysis of the mononucleotide repeats BAT-26 and BAT-40 has reportedly revealed significant microsatellite instability in sporadic colorectal adenomas, whereas studies with dinucleotide and tetranucleotide repeats have not. In addition, BAT-26 has been reported to be "quasimonomorphic" in the germline. We evaluated BAT-26 and BAT-40 in a series of colorectal tumors previously analyzed with a panel of tetranucleotide repeats. Instability in BAT-26 or BAT-40 was significantly associated with tetranucleotide repeat instability in sporadic adenomas and carcinomas (P < 0.0001) and was similarly much less common in adenomas than in carcinomas. Germline polymorphisms in both BAT-40 and BAT-26 were identified, and the frequency of BAT-26 polymorphisms was significantly higher in African Americans than in Caucasians (7.7% versus 0.08%, P < 0.001). BAT-26 and BAT-40 may be very useful in evaluating instability in small tumors, as sufficient DNA to be amplified by large panels of microsatellites is not always available from such lesions. Polymorphisms in these microsatellites, however, limit their utility in determinations of microsatellite instability without corresponding normal DNA.
机译:据报道,对单核苷酸重复序列BAT-26和BAT-40的分析揭示了散发性结直肠腺瘤中显着的微卫星不稳定性,而对二核苷酸和四核苷酸 的研究重复没有。另外,据报道,BAT-26在种系中是 “准单态的”。我们评估了先前用 一组四核苷酸重复序列分析的一系列结直肠肿瘤中的BAT-26和 BAT-40。在散发性腺瘤和癌中,BAT-26或BAT-40 的不稳定性与四核苷酸重复不稳定性 显着相关(P <0.0001),并且 相似在腺瘤中比在癌症中少得多。 BAT-40和BAT-26的胚芽 多态性都得到了鉴定,并且BAT-26多态性的发生频率在非洲裔美国人中明显高于 在白种人中(7.7%对0.08%, P <0.001)。 BAT-26和BAT-40在评估小肿瘤中的 不稳定性方面可能非常有用,因为并非总是可以从 此类病变。但是,这些微卫星中的多态性 限制了它们在确定微卫星不稳定性 而没有相应正常DNA的情况下的效用。

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  • 来源
    《American Journal of Pathology》 |1999年第6期|00001637-00001641|共5页
  • 作者单位

    From the Departments of Pathology,University of Utah Health Sciences Center, Salt Lake City, Utah;

    Oncological Sciences,University of Utah Health Sciences Center, Salt Lake City, Utah;

    and The Fred Hutchinson Cancer Research Center,Seattle, Washington;

    and Human Genetics,University of Utah Health Sciences Center, Salt Lake City, Utah;

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  • 入库时间 2022-08-17 14:17:20

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