首页> 外文期刊>Breast cancer research and treatment. >Allelic loss of the PTEN region (10q23) in breast carcinomas of poor pathophenotype.
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Allelic loss of the PTEN region (10q23) in breast carcinomas of poor pathophenotype.

机译:不良表型的乳腺癌中PTEN区的等位基因缺失(10q23)。

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摘要

Loss of heterozygosity (LOH) in loci of the 10q23 region that harbor the PTEN gene and mutations in the sequence of this gene have been found in several primary human tumors including breast carcinomas, suggesting that this gene could be implicated in their pathogenesis. We investigated allelic losses in microsatellites of the 10q23 region, and their correlations with nine pathologic parameters in 105 breast carcinomas. The LOH analysis was performed by amplifying DNA by PCR, using five markers of the 10q23 region (D10S1687, D10S541, D10S2491, D10S583 and D10S571). LOH in at least one marker of the PTEN region was found in 29.5% of tumors. The statistical comparison between carcinomas with and without LOH in terms of the pathologic parameters showed significant differences in age (p = 0.03), lymph node metastases (p = 0.02), and higher histological grade (p = 0.02); a trend toward significance was found for progesterone receptors (p = 0.05). LOH in an individual marker and statistically significant relationships to tumor characteristics were observed at locus D10S541 for lymph node metastases (p = 0.04), at D10S2491 (intragenic to the PTEN gene) for lymph node metastases (p = 0.02), and at D10S583 for progesterone receptors (p = 0.01) and for high grade (p = 0.03). These results suggest the PTEN gene, or other genes of the 10q23 region, could be functionally related to breast cancer, probably influencing the development of histological features associated with poor prognosis.
机译:在包含乳腺癌的几种原发性人类肿瘤中发现了带有PTEN基因的10q23区基因座中的杂合子(LOH)丢失,并且该基因序列中的突变已被发现,这表明该基因可能与它们的发病机制有关。我们调查了10q23地区的微卫星中的等位基因缺失,以及它们与105例乳腺癌中9种病理参数的相关性。通过使用10q23区域的五个标记(D10S1687,D10S541,D10S2491,D10S583和D10S571)通过PCR扩增DNA进行LOH分析。在29.5%的肿瘤中发现了PTEN区至少一种标记物中的LOH。有和没有LOH的癌在病理参数方面的统计学比较显示,年龄(p = 0.03),淋巴结转移(p = 0.02)和更高的组织学等级(p = 0.02)存在显着差异。发现孕激素受体有显着趋势(p = 0.05)。在淋巴结转移的D10S541位点(p = 0.04),在淋巴结转移的D10S2491(PTEN基因内源),在D10S2491(P = 0.02)和在D10S583的D10S583处观察到了单个标志物的LOH及其与肿瘤特征的统计显着相关性。孕激素受体(p = 0.01)和高等级(p = 0.03)。这些结果表明,PTEN基因或10q23区域的其他基因可能与乳腺癌在功能上相关,可能影响与不良预后相关的组织学特征的发展。

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