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首页> 外文期刊>Pathology oncology research: POR >Investigation of microsatellite instability in Turkish breast cancer patients
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Investigation of microsatellite instability in Turkish breast cancer patients

机译:土耳其乳腺癌患者微卫星不稳定性的调查

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Multiple somatic and inherited genetic changes that lead to loss of growth control may contribute to the development of breast cancer. Microsatellites are tandem repeats of simple sequences that occur abundantly and at random throughout most eucaryotic genomes. Microsatellite instability (MI), characterized by the presence of random contractions or expansions in the length of simple sequence repeats or microsatellites, is observed in a variety of tumors. The aim of this study was to compare tumor DNA fingerprints with constitutional DNA fingerprints to investigate changes specific to breast cancer and evaluate its correlation with clinical characteristics. Tumor and normal tissue samples of 38 patients with breast cancer were investigated by comparing PCR-amplified microsatellite sequences D2S443 and D21S1436. Microsatellite instability at D21S1436 and D2S443 was found in 5 (13%) and 7 (18%) patients, respectively. Two patients displayed instability at both marker loci. No association was found between MI and age, family history, lymph node involvement and other clinical parameters.
机译:导致无法控制生长的多种体细胞遗传病和遗传遗传病可能有助于乳腺癌的发展。微卫星是简单序列的串联重复,在大多数真核基因组中大量随机发生。在多种肿瘤中都观察到微卫星不稳定性(MI),其特征是在简单序列重复序列或微卫星的长度上存在随机收缩或扩展。这项研究的目的是比较肿瘤DNA指纹与体质DNA指纹,以调查特定于乳腺癌的变化并评估其与临床特征的相关性。通过比较PCR扩增的微卫星序列D2S443和D21S1436,研究了38例乳腺癌患者的肿瘤和正常组织样本。 D21S1436和D2S443的微卫星不稳定性分别在5位(13%)和7位(18%)患者中发现。两名患者在两个标记位点均显示不稳定。在MI与年龄,家族史,淋巴结受累及其他临床参数之间未发现关联。

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