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Genome-wide linkage scan of prostate cancer Gleason score and confirmation of chromosome 19q.

机译:前列腺癌Gleason评分的全基因组连锁扫描和19q染色体的确认。

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Despite evidence that prostate cancer has a genetic etiology, it has been extremely difficult to confirm genetic linkage results across studies, emphasizing the large extent of genetic heterogeneity associated with this disease. Because prostate cancer is common-approximately one in six men will be diagnosed with prostate cancer in their life-genetic linkage studies are likely plagued by phenocopies (i.e., men with prostate cancer due to environmental or lifestyle factors), weakly penetrant alleles, or a combination of both, making it difficult to replicate linkage findings. One way to account for heterogeneous causes is to use clinical information that is related to the aggressiveness of disease as an endpoint for linkage analyses. Gleason grade is a measure of prostate tumor differentiation, with higher grades associated with more aggressive disease. This semi-quantitative score has been used as a quantitative trait for linkage analysis in several prior studies. Our aim was to determine if prior linkage reports of Gleason grade to specific loci could be replicated, and to ascertain if new regions of linkage could be found. Gleason scores were available for 391 affected sib pairs from 183 hereditary prostate cancer pedigrees as part of the PROGRESS study. Analyzing Gleason score as a quantitative trait, and using microsatellite markers, suggestive evidence for linkage (P-value
机译:尽管有证据表明前列腺癌具有遗传病因,但要在整个研究中确认遗传连锁结果非常困难,强调了与此疾病相关的广泛遗传异质性。由于前列腺癌是常见病,因此大约有六分之一的男性将在其生命遗传联系研究中被诊断出患有前列腺癌。表型(即,由于环境或生活方式因素而患有前列腺癌的男性),渗透力弱的等位基因或两者的结合,使得很难复制连锁发现。解决异类原因的一种方法是使用与疾病的侵袭性相关的临床信息作为连锁分析的终点。格里森分级是对前列腺肿瘤分化程度的一种度量,较高的等级与更具侵略性的疾病有关。在一些先前的研究中,该半定量得分已用作连锁分析的定量特征。我们的目的是确定是否可以复制以前与特定基因座有关的格里森级连锁报告,并确定是否可以找到新的连锁区域。作为PROGRESS研究的一部分,格里森评分可用于183个遗传性前列腺癌谱系中的391个受影响同胞对。分析格里森分数作为定量特征,并使用微卫星标记,在染色体19q和5q上发现了连锁的暗示证据(P值

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