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使用细胞周期进程抑制剂戈拉替德增强对人祖细胞进行热疗净化的选择性。

Enhanced selectivity of hyperthermic purging of human progenitor cells using Goralatide, an inhibitor of cell cycle progression.

作者信息

Wierenga P K, Brenner M K, Konings A W

机构信息

Department Radiobiology, University of Groningen, The Netherlands.

出版信息

Bone Marrow Transplant. 1998 Jan;21(1):73-8. doi: 10.1038/sj.bmt.1701045.

Abstract

Recurrence of leukemia is a major problem after autologous stem cell transplantation. One potential means of reducing this risk is to purge the autologous transplant in vitro by hyperthermia. We have demonstrated that after a hyperthermic treatment of 120 min at 43 degrees C, the leukemic progenitor cells (CFU-AML) are decreased by 5-log but the normal hematopoietic committed progenitor cells (CFU-GM, BFU-E and CFU-E) are reduced by only 1-log. Moreover, the hyperthermic sensitivity coincides with the stem cell hierarchy, ie CFU-GM are less heat sensitive than BFU-E, while CFU-E are the most sensitive. The impact of pretreatment with the tetrapeptide AcSDKP (Goralatide) on the proliferative activity and heat sensitivity of the normal and leukemic progenitor cells was determined. An incubation of 21 h at 37 degrees C with 10(-9) M Goralatide reduces the number of normal hematopoietic progenitor cells in S-phase and concomitantly decreases their hyperthermic sensitivity. This effect implies that the proliferative activity is the major determinant for the detected differences in hyperthermic sensitivity of the subsets in the normal hematopoietic stem cell compartment. In contrast, the cell cycle progression of leukemic progenitor cells is not affected and hence these cells are not protected from hyperthermia-induced cell killing after preincubation with Goralatide. Thus, the treatment with Goralatide increases the therapeutic window of hyperthermia and increases the potential value of this physical purging technique.

摘要

白血病复发是自体干细胞移植后的一个主要问题。降低这种风险的一种潜在方法是通过热疗在体外净化自体移植细胞。我们已经证明,在43摄氏度下进行120分钟的热疗后,白血病祖细胞(CFU-AML)减少了5个对数,但正常造血定向祖细胞(CFU-GM、BFU-E和CFU-E)仅减少了1个对数。此外,热敏感性与干细胞层次结构一致,即CFU-GM比BFU-E对热的敏感性低,而CFU-E最敏感。测定了四肽AcSDKP(戈拉替德)预处理对正常和白血病祖细胞增殖活性和热敏感性的影响。在37摄氏度下用10^(-9) M戈拉替德孵育21小时可减少处于S期的正常造血祖细胞数量,并同时降低其热敏感性。这种效应意味着增殖活性是正常造血干细胞区室中各亚群热敏感性差异的主要决定因素。相反,白血病祖细胞的细胞周期进程不受影响,因此在与戈拉替德预孵育后,这些细胞不能免受热诱导的细胞杀伤。因此,戈拉替德治疗增加了热疗的治疗窗口,并增加了这种物理净化技术的潜在价值。

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