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首页> 美国卫生研究院文献>Springer Open Choice >Diagnostic value of DNA alteration: loss of heterozygosity or allelic imbalance—promising for molecular staging of prostate cancers
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Diagnostic value of DNA alteration: loss of heterozygosity or allelic imbalance—promising for molecular staging of prostate cancers

机译:DNA改变的诊断价值:杂合性丧失或等位基因失衡-有望用于前列腺癌的分子分期

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The biological behavior of prostate cancer is uncertain, and therefore, search for molecular prognostic markers associated with disease progression seems to be essential. We performed microsatellite allelotyping of DNA isolated from primary prostate tumors biopsies (prostate adenocarcinoma, PCa). We evaluated the frequency of allelic imbalance (AI), including loss of heterozygosity and/or microsatellite imbalance (LOH/MSI) as well as the association of these DNA alterations with clinicopathological variables. We assessed the significance of LOH/MSI alterations in selected imprinted and non-imprinted chromosomal regions (IR and NIR) in PCa. A total of 50 biopsies of prostate tumor (containing >75 % tumor cells) were histologically examined confirming prostate carcinoma. Microsatellite allelotyping using 16 microsatellite markers linked to the following chromosomal regions: 1p31.2, 3p21.3–25.3, 7q32.2, 9p21.3, 11p15.5, 12q23.2, and 16q22.1 was performed. The incidence of LOH/MSI alterations in prostate tumor cells was the highest for chromosomal regions 7q32.2 and 16q22.1 (31.25 and 26.60 %, respectively), followed by 1p31.2 and 3p21.3–25.3 (26.50 and 17.40 %, respectively). Statistically significant increase in LOH/MSI alterations has been observed for markers: D1S2137 (1p region; p = 0.00032), D9S974 (9p region; p = 0.0017), and D16S3025 (16q region; p = 0.0017). Statistically significant differences in frequency of LOH/MSI alterations in particular chromosomal regions have been found for 1p31.2, 7q32.2 and 16q22.1 (p = 0.027, p = 0.012 and p = 0.031, respectively). We documented statistically significant association between Fractional Allele Loss (FAL) index and advanced tumor stage (p < 0.05). We suggest that genomic instability of LOH/MSI type is a frequent event in prostate carcinogenesis and assessed as FAL index has clinical value for the molecular staging of prostate cancer in (TRUS)-guided prostate biopsy material.
机译:前列腺癌的生物学行为尚不确定,因此寻找与疾病进展相关的分子预后标记似乎是必不可少的。我们对从原发性前列腺肿瘤活检组织(前列腺腺癌,PCa)中分离的DNA进行了微卫星异型分析。我们评估了等位基因失衡(AI)的频率,包括杂合性和/或微卫星失衡(LOH / MSI)的丧失,以及这些DNA改变与临床病理变量的关联。我们评估了PCa中选定的印迹和非印迹染色体区域(IR和NIR)中LOH / MSI改变的重要性。组织学检查了总共50例前列腺肿瘤活检(包含> 75%的肿瘤细胞),证实了前列腺癌。使用链接到以下染色体区域的16个微卫星标记进行微卫星异型分析:1p31.2、3p21.3-25.3、7q32.2、9p21.3、11p15.5、12q23.2和16q22.1。前列腺肿瘤细胞中LOH / MSI改变的发生率在染色体区域7q32.2和16q22.1最高(分别为31.25和26.60%),其次是1p31.2和3p21.3-25.3(26.50和17.40%,分别)。观察到标记的LOH / MSI改变具有统计学上的显着增加:D1S2137(1p区域; p = 0.00032),D9S974(9p区域; p = 0.0017)和D16S3025(16q区域; p = 0.0017)。在1p31.2、7q32.2和16q22.1的特定染色体区域中,LOH / MSI改变频率的统计差异显着(分别为p = 0.027,p = 0.012和p = 0.031)。我们记录了分数等位基因损失(FAL)指数与晚期肿瘤分期之间的统计学显着关联(p <0.05)。我们建议LOH / MSI类型的基因组不稳定性是前列腺癌发生中的常见事件,并且根据FAL指数对(TRUS)指导的前列腺活检材料中的前列腺癌分子分期具有临床价值。

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