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Expression of a 95 kDa membrane protein is associated with low daunorubicin accumulation in leukaemic blast cells.

机译:95 kDa膜蛋白的表达与白血病母细胞中柔红霉素的低积累有关。

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摘要

A 95 kDa membrane protein (P-95) has been previously noted to be overexpressed in a doxorubicin-resistant subline of the MCF-7 breast cancer line and in clinical samples obtained from patients with solid tumours refractory to doxorubicin. We performed Western blotting on blast cell lysates from adults with acute myeloid leukaemia, using antisera to P-95. Concomitant flow cytometric assays measured daunorubicin accumulation and retention. Blasts from 16/46 patient samples had detectable P-95 and had reduced accumulation of daunorubicin compared with the negative marrows. Experiments with the P-95 positive MCF-7 multidrug-resistant subline demonstrated decreased daunorubicin accumulation and retention relative to the sensitive parent line. AML blast cells positive for P-95 also demonstrated greater overall in vitro survival in the presence of daunorubicin relative to the P-95-negative samples. The expression of P-95 did not correlate with failure to achieve an initial complete remission with daunorubicin and cytarabine induction chemotherapy. We conclude that the P-95 protein may possess an efflux transporter function, and may represent another mechanism responsible for anthracycline resistance in acute myeloid leukaemia.
机译:先前已经注意到,在MCF-7乳腺癌细胞系对阿霉素耐药的亚系中以及从对阿霉素难治的实体瘤患者获得的临床样品中,一种95 kDa的膜蛋白(P-95)过表达。我们使用P-95抗血清,对来自患有急性髓性白血病的成人的原始细胞裂解物进行了蛋白质印迹分析。伴随的流式细胞术测定了柔红霉素的积累和保留。与阴性骨髓相比,来自16/46患者样品的冲击波可检测到P-95,柔红霉素的积聚减少。使用P-95阳性MCF-7多药耐药的亚系进行的实验表明,柔红霉素的积累和保留相对于敏感的亲本系而言有所降低。相对于P-95阴性样品,在存在柔红霉素的情况下,P-95阳性的AML原始细胞在体外的总体存活率更高。 P-95的表达与柔红霉素和阿糖胞苷诱导化疗未能实现初始完全缓解的失败无关。我们得出的结论是,P-95蛋白可能具有外排转运蛋白功能,并且可能代表了急性髓性白血病中对蒽环类药物耐药的另一种机制。

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