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用烷基溶血磷脂清除白血病缓解期骨髓的临床前和临床结果。

Purging leukemia remission marrows with alkyl-lysophospholipids, preclinical and clinical results.

作者信息

Vogler W R, Olson A C, Berdel W E, Okamoto S, Glasser L

机构信息

Department of Medicine, Emory University School of Medicine, Atlanta, Georgia 30322.

出版信息

Prog Clin Biol Res. 1990;333:1-18; discussion 19-20.

PMID:2308973
Abstract

Alkyl-lysophospholipids are unique compounds which have selective anti-cancer activity with relative sparing of normal bone marrow stem cells. Thus, they would appear to be ideal candidates for marrow purging. In contrast to most anti-cancer drugs, these compounds act on the cell membrane resulting in inhibition of phosphatidylcholine biosynthesis. In addition, these compounds inhibit protein kinase C activity and may interfere with signal transmission. In low doses in in vitro systems, they have been shown to induce differentiation in leukemic cell lines. Lethally irradiated Balb/c mice were injected with normal bone marrow cells containing 1-2% leukemic cells (WEHI III-B) to simulate a remission marrow after the cells were incubated in vitro for 24 hours with 0-100 ug/ml of 1-0-octadecyl-2-0-methyl-rac-glycero-3-phosphocholine (ALP). All the mice given cells not treated with ALP succumbed to leukemia, whereas there was a dose-response increase in survival in those given ALP treated cells. Similar results were observed when the cells were cryopreserved and thawed before injection. Very little effect of ALP was noted on stem cells as measured by the spleen colony assay. In vitro studies using human marrow progenitor assays (CFU-GEMM) were undertaken in which marrow was mixed with 0.1% HL60 cells and exposed for 1 or 4 hours to ALP at 0, 25 and 50 ug/ml. The cells were plated and assayed for CFU-GEMM and leukemic colonies. At 50 ug/ml, HL60 colonies were eliminated and there was no significant reduction in normal marrow progenitor cells. Clinical trials were initiated. Eleven patients with acute leukemia in remission who were candidates for autologous bone marrow transplantation had marrow harvested, incubated with 50 ug/ml of ALP and cryopreserved. CFU-GEMM assays before and after purging showed no differences. There was a similar significant reduction after cryopreservation regardless of whether marrows were purged. Two patients were transplanted with purged marrow, one in early relapse and one in a marrow remission, but had evidence of CNS leukemia. In both, ablative therapy consisted of cytosine arabinoside, 3 gm/m2 x 12 doses, followed by fractionated TBI to a total of 12 Gy prior to reinfusion of thawed marrow. The patient in early relapse had progression of leukemia by day 28. The patient in marrow remission is disease-free 9 months after transplantation. These studies indicate that purging marrow with ALP is a promising approach and further clinical studies are indicated.

摘要

烷基溶血磷脂是一类独特的化合物,具有选择性抗癌活性,对正常骨髓干细胞的损伤相对较小。因此,它们似乎是骨髓净化的理想候选物。与大多数抗癌药物不同,这些化合物作用于细胞膜,导致磷脂酰胆碱生物合成受到抑制。此外,这些化合物还能抑制蛋白激酶C的活性,并可能干扰信号传递。在体外系统中,低剂量的这些化合物已被证明能诱导白血病细胞系分化。对致死剂量照射的Balb/c小鼠注射含有1%-2%白血病细胞(WEHI III-B)的正常骨髓细胞,以模拟缓解期骨髓,然后将细胞与0-100μg/ml的1-0-十八烷基-2-0-甲基-rac-甘油-3-磷酸胆碱(ALP)在体外孵育24小时。所有接受未用ALP处理细胞的小鼠均死于白血病,而接受ALP处理细胞的小鼠存活率呈剂量依赖性增加。当细胞在注射前进行冷冻保存和解冻时,也观察到了类似的结果。通过脾集落试验检测,发现ALP对干细胞的影响很小。进行了使用人骨髓祖细胞检测(CFU-GEMM)的体外研究,将骨髓与0.1%的HL60细胞混合,并分别用0、25和50μg/ml的ALP处理1小时或4小时。将细胞接种并检测CFU-GEMM和白血病集落。在50μg/ml时,HL60集落被清除,而正常骨髓祖细胞没有显著减少。于是开展了临床试验。11例急性白血病缓解期且适合进行自体骨髓移植的患者采集了骨髓,用50μg/ml的ALP孵育后进行冷冻保存。净化前后的CFU-GEMM检测没有差异。无论骨髓是否经过净化,冷冻保存后都有类似的显著减少。两名患者接受了净化后的骨髓移植,一名处于早期复发阶段,一名处于骨髓缓解期,但都有中枢神经系统白血病的证据。在这两名患者中,清髓疗法包括阿糖胞苷,3g/m²,共12剂,然后在回输解冻骨髓前进行分次全身照射,总剂量为12Gy。早期复发的患者在第28天白血病进展。骨髓缓解期的患者在移植后9个月无病生存。这些研究表明,用ALP净化骨髓是一种有前景的方法,需要进一步开展临床研究。

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