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作 者:王嵘[1,2] 郁知非[1,2] 顾建人[1,2] 李岱宗[1,2] 汪明春[1,2] 曹宇清
机构地区:[1]暨南大学医学院 [2]上海市肿瘤研究所
出 处:《白血病》1997年第3期129-131,共3页
摘 要:用PCR-VNTR多态分析,以白血病缓解期患者的骨髓有核细胞作为胚系对照,对27例急性白血病患者进行p53基因杂合子性缺失进行检测,结果发现在27例中13例呈异质性,其胚系的多态性率为48.2%(3/27)。对13例胚系的VNTR呈多态性的白血病患者(ALL10例,AML3例),进一步进行白血病细胞与胚系的PCR-VNTR配对分析,结果发现1例ALL患者白血病细胞的VNTR异质性消失,而呈均一性。提示此例ALL患者p53基因缺失一条等位基因,呈LOH。结果提示p53基因功能失活在急性淋巴细胞白血病的发病中可能起一定的作用。Using the variable number repeat (VNTR) polymorphism analysis by PCR in intron 1 of the p53 gene, in bone marrow nucleate cell from 27 patients with acute leukemia during complete remission serving as germline control. We found NVTR heterozygosity being 13/27(48.2%). In 13 cases with germline VNTR heterozygosity, including 10 ALL and 3 AML, PCR VNTR was analysed from leukemic cell. In one patient with ALL, VNTR is heterozygositic in germline control but changed to homozygosity in leukemic cell. This suggested one allel of p53 gene deleted (loss of heterozygosity) in leukemic cell. This result provides evidence that the inactivation of the p53 gene is probably related to the leukemogenesis of ALL.
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