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正常骨髓细胞中多药耐药基因1(MDR1)的表达及其对白血病造血的影响。

Expression of MDR1 by normal bone marrow cells and its implication for leukemic hematopoiesis.

作者信息

Drach J, Zhao S, Drach D, Körbling M, Engel H, Andreeff M

机构信息

Department of Hematology, University of Texas M.D. Anderson Cancer Center, Houston, USA.

出版信息

Leuk Lymphoma. 1995 Feb;16(5-6):419-24. doi: 10.3109/10428199509054428.

Abstract

Expression of MDR1 is a well-characterized mechanism leading to resistance of tumor cells to drugs like vinca-alkaloids, anthracyclines, and epipodophyllotoxins. In hematopoiesis, recent data indicate that not only leukemic cells, but also some populations of normal hematopoietic cells, particularly CD34+ progenitor cells as well as peripheral blood lymphocytes, express a functional multidrug-resistant phenotype. Among CD34+ cells, we found evidence that myeloid committed precursor cells (CD34+/CD33+) have lower levels of MDR1 expression than earlier CD34+ cell populations, but there was no difference in MDR1 expression between CD34+/HLA-DR- and CD34+/HLA-DR+ subpopulations. During normal myeloid differentiation, MDR1 expression is down-regulated, which is similar to our observations in acute myelogenous leukemia (AML): MDR1 expression was only rarely detected in acute promyelocytic leukemia, which was in contrast to other subtypes of AML; also, within leukemic subpopulations of the same patient, higher MDR1 levels were correlated with a more immature immunophenotype. Regarding regulation of MDR1 expression, we did not observe changes of MDR1 expression in normal CD34+ cells in response to various cytokines. However, in 2 patients with AML treated with interleukin-3 and granulocyte-colony stimulating factor, respectively, a significant down-regulation of MDR1 expression was found after 24 hours. In conclusion, there is evidence that the pattern of MDR1 expression observed in leukemias reflects the distribution of MDR1 in normal hematopoiesis. In contrast to normal CD34+ cells, leukemic cells from some AML patients can respond to cytokines with a down-regulation of MDR1, which may contribute to response to cytokine/chemotherapy combinations.

摘要

MDR1的表达是一种已被充分表征的机制,可导致肿瘤细胞对长春花生物碱、蒽环类药物和表鬼臼毒素等药物产生耐药性。在造血过程中,最近的数据表明,不仅白血病细胞,而且一些正常造血细胞群体,特别是CD34+祖细胞以及外周血淋巴细胞,都表达功能性多药耐药表型。在CD34+细胞中,我们发现有证据表明,髓系定向前体细胞(CD34+/CD33+)的MDR1表达水平低于早期CD34+细胞群体,但CD34+/HLA-DR-和CD34+/HLA-DR+亚群之间的MDR1表达没有差异。在正常髓系分化过程中,MDR1表达下调,这与我们在急性髓性白血病(AML)中的观察结果相似:在急性早幼粒细胞白血病中很少检测到MDR1表达,这与AML的其他亚型形成对比;此外,在同一患者的白血病亚群中,较高的MDR1水平与更不成熟的免疫表型相关。关于MDR1表达的调节,我们没有观察到正常CD34+细胞中MDR1表达因各种细胞因子而发生变化。然而,在分别接受白细胞介素-3和粒细胞集落刺激因子治疗的2例AML患者中,24小时后发现MDR1表达明显下调。总之,有证据表明,白血病中观察到的MDR1表达模式反映了MDR1在正常造血中的分布。与正常CD34+细胞不同,一些AML患者的白血病细胞可对细胞因子产生反应,导致MDR1下调,这可能有助于对细胞因子/化疗联合治疗的反应。

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