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氯高铁血红素对蒽环类抗生素诱导的造血细胞细胞毒性的预防作用

Prevention of anthracycline-induced cytotoxicity in hemopoietic cells by hemin.

作者信息

Tsiftsoglou A S, Wong W, Wheeler C, Steinberg H N, Robinson S H

出版信息

Cancer Res. 1986 Jul;46(7):3436-40.

PMID:3708575
Abstract

Anthracyclines such as Adriamycin (ADR) and daunomycin markedly inhibit cell growth in vivo and in vitro. These studies demonstrate that 30 microM hemin, which induces hemoglobin synthesis in human and murine erythroleukemia cells in culture, markedly decreases the cytotoxicity of ADR in a variety of hemopoietic cell lines (K562, HEL-1, MEL-745, HL-60, and U937) and in erythroid burst-forming cells from normal human marrow. Hemin failed to protect four of the five nonhemopoietic cell lines tested, including MCF-, breast adenocarcinoma cells, C-205 colon carcinoma cells, mouse 3T3 fibroblasts, and mouse kidney VERO cells. Hemin did protect human neuroblastoma IMP-32 cells from ADR cytotoxicity; however, this nonhemopoietic cell line undergoes dendrite formation in response to hemin induction. Cytofluorographic analysis of cellular ADR content and labeling studies with [3H]daunomycin demonstrated that hemin decreases the intracellular accumulation of these anthracyclines by more than 50% in K562 erythroleukemia cells. These studies indicate that small doses of hemin prevent intracellular accumulation of anthracyclines and thereby markedly reduce anthracycline toxicity to cells. Since this protective effect is observed preferentially with hemopoietic cells, it is possible that this finding could be exploited to protect the bone marrow from the cytotoxic action of anthracyclines during therapy for nonhemopoietic tumors.

摘要

阿霉素(ADR)和柔红霉素等蒽环类药物在体内和体外均能显著抑制细胞生长。这些研究表明,30微摩尔的氯化血红素可诱导培养的人及小鼠红白血病细胞合成血红蛋白,它能显著降低阿霉素对多种造血细胞系(K562、HEL-1、MEL-745、HL-60和U937)以及正常人骨髓红系爆式集落形成细胞的细胞毒性。氯化血红素未能保护所测试的五种非造血细胞系中的四种,包括MCF-乳腺癌细胞、C-205结肠癌细胞、小鼠3T3成纤维细胞和小鼠肾VERO细胞。氯化血红素确实保护人神经母细胞瘤IMP-32细胞免受阿霉素的细胞毒性;然而,这种非造血细胞系在氯化血红素诱导下会发生树突形成。细胞荧光分析细胞内阿霉素含量以及用[3H]柔红霉素进行的标记研究表明,在K562红白血病细胞中,氯化血红素可使这些蒽环类药物的细胞内积累减少50%以上。这些研究表明,小剂量的氯化血红素可防止蒽环类药物在细胞内积累,从而显著降低其对细胞的毒性。由于这种保护作用在造血细胞中更为明显,因此有可能利用这一发现来保护骨髓免受蒽环类药物在非造血肿瘤治疗期间的细胞毒性作用。

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