生长激素和IGF-I对白血病患者活动性和缓解期造血细胞克隆生长的影响——初步报告

Z Zadik, Z Estrov, Y Karov, T Hahn, Y Barak
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引用次数: 52

摘要

用生长激素治疗生长迟缓的儿童白血病幸存者的数量正在增加。关于生长激素和胰岛素样生长因子I (IGF-I)与恶性肿瘤的发生或复发的直接或间接关系的争论,特别是在白血病患者中使用生长激素治疗的情况下,仍然没有解决。因此,我们研究了生长激素和IGF-I对急性白血病(ALL和AML)患者诊断和复发以及慢性白血病(CML)患者缓解期骨髓的影响。生长激素浓度为250 ng/ml和300 ng/ml时,生长激素可分别使blast菌落数量平均增加68%和77%。当IGF-I浓度分别为0.05、0.25和0.5 ng/ml时,ALL患者的blast菌落数量分别增加了50%、93%和105%,AML患者的blast菌落数量分别增加了33%、58%和65%。在3例缓解期的CML患者中,粒细胞-巨噬细胞集落形成试验未显示GH或IGF-I刺激外周血细胞集落形成。我们的体外数据(如先前报道的)表明生长激素和igf - 1可能促进母细胞增殖,在缓解期白血病患者中补充这些肽必须仔细监测早期复发。为了检验生长激素和igf - 1对这些细胞的影响,需要对缓解期白血病患者的骨髓细胞进行进一步的研究。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
The effect of growth hormone and IGF-I on clonogenic growth of hematopoietic cells in leukemic patients during active disease and during remission--a preliminary report.

The number of survivors of childhood leukemia treated with growth hormone for growth retardation is increasing. The debate about the direct or indirect relationship of GH and insulin-like growth factor I (IGF-I) to the occurrence or recurrence of malignancy, especially in the case of GH therapy in patients with leukemia, is still unresolved. We, therefore, studied the effect of GH and IGF-I on bone marrow of patients with acute leukemia (ALL and AML) in diagnosis and recurrence and in chronic leukemia patients (CML) in remission. GH increased blast colony numbers by a mean of 68% and 77% at GH concentrations of 250 and 300 ng/ml, respectively. IGF-I increased blast colony numbers in ALL patients by 50, 93 and 105%, and in AML patients by 33, 58 and 65%, at IGF-I concentrations of 0.05, 0.25 and 0.5 ng/ml, respectively. In 3 CML patients in remission a granulocyte-macrophage colony forming assay did not reveal stimulation of peripheral blood blast colony formation by GH or IGF-I. Our in vitro data (as previously reported) suggest that GH and IGF-I may promote blast cell proliferation, and the supplemental administration of these peptides in leukemia patients in remission must be carefully monitored for early relapse. Additional studies on bone marrow cells of leukemic patients in remission are needed in order to examine the effects of GH and IGF-I on these cells.

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