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首页> 外文期刊>Breast cancer research and treatment. >Allelic loss of chromosome 3p24 correlates with tumor progression rather than with retinoic acid receptor beta2 expression in breast carcinoma.
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Allelic loss of chromosome 3p24 correlates with tumor progression rather than with retinoic acid receptor beta2 expression in breast carcinoma.

机译:染色体3p24的等位基因缺失与肿瘤的进展有关,而不是与视黄酸受体β2在乳腺癌中的表达有关。

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摘要

A tumor suppressor gene. retinoic acid receptor (RAR) beta2, has been mapped to chromosome 3p24, a region where loss of heterozygosity (LOH) has been observed commonly in carcinomas of various tumor tissues. RAR beta2 expression is reduced or lost in many malignant tumors including breast cancer, however, whether LOH accounts for the loss of expression of RAR beta2 in breast cancer is unknown. We, therefore, assessed LOH on chromosome band 3p24 to correlate it with RAR beta2 expression and other established prognostic parameters in 52 breast carcinomas. Based on three microsatellites, D3S 1283, D3S 1293 and D3S 1286. all of the tumors were informative, of these, 12 (23%) exhibited LOH. RAR beta2 expression was lost in 42% (19/45) of these samples. We found that LOH on chromosome band 3p24 was not correlated with loss of RAR beta2, but correlated with higher histological grade, p53-positivity, and loss of estrogen and progesterone receptors. Our findings suggest that LOH of the RAR beta2 gene does not account for the frequent loss of RAR beta2 expression in breast cancer but the genomic structural alteration at or close to the RAR beta2 gene locus are likely to be associated with tumor progression and/or loss of hormonal dependency.
机译:肿瘤抑制基因。维甲酸受体(RAR)beta2已定位到3p24号染色体,该区域通常在各种肿瘤组织的癌症中均观察到杂合性(LOH)丢失。在包括乳腺癌在内的许多恶性肿瘤中,RAR beta2的表达都会降低或丢失,但是,LOH是否会导致乳腺癌中RAR beta2的表达丢失尚不清楚。因此,我们评估了3p24染色体带上的LOH,以使其与RAR beta2表达和52个乳腺癌中其他已建立的预后参数相关。基于三个微卫星D3S 1283,D3S 1293和D3S1286。所有肿瘤均具有信息性,其中12个(23%)表现出LOH。这些样品中有42%(19/45)丢失了RAR beta2表达。我们发现染色体3p24上的LOH与RAR beta2的丢失无关,但与更高的组织学等级,p53阳性以及雌激素和孕激素受体的丢失有关。我们的发现表明,RAR beta2基因的LOH不能解释乳腺癌中RAR beta2表达的频繁丧失,但RAR beta2基因位点或附近的基因组结构改变可能与肿瘤的进展和/或丧失有关。激素依赖性

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