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重组人促红细胞生成素(rHu-EPO)用于进展性多发性骨髓瘤的长期治疗。

Long-term therapy with recombinant human erythropoietin (rHu-EPO) in progressing multiple myeloma.

作者信息

Silvestris F, Romito A, Fanelli P, Vacca A, Dammacco F

机构信息

Department of Biomedical Sciences and Human Oncology Section of Internal Medicine and Clinical Oncology, University of Bari, Italy.

出版信息

Ann Hematol. 1995 Jun;70(6):313-8. doi: 10.1007/BF01696618.

Abstract

Recombinant human erythropoietin (rHu-EPO) is an effective growth factor for erythroid progenitor cells in anemia provoked by several conditions, including bone marrow tumors such as multiple myeloma (MM). We studied a group of 54 patients with MM undergoing second-induction chemotherapy. Thirty of them were randomly assigned to receive rHu-EPO at an initial dosage of 150 units/kg body weight three times a week, increased to 300 units/kg from the sixth week to the end of the 24-week study. Hemoglobin (Hb) levels increased in 77.7% of these patients by the eighth week. In addition, five transfusion-dependent patients in treatment with the VMCP protocol completed the trial without requiring blood supplement after the third month, whereas seven control patients required frequent supplements. Monthly assessment of hematologic parameters demonstrated the ability of rHu-EPO to increase reticulocyte counts, whereas five patients became resistant to the second-induction chemotherapy in apparent concurrence with their rHu-EPO therapy. The response to rHu-EPO in four of the five MM patients receiving cytotoxic protocols combined with alpha-interferon (alpha-IFN) included an increase of serum IgM after the third month. This effect was not demonstrable in any other group, including three rHu-EPO-untreated patients undergoing alpha-IFN + VMCP combined therapy, as well as rHu-EPO-treated patients not receiving alpha-IFN. Our data suggest that alpha-IFN plus rHu-EPO treatment in MM patients is effective in restoring normal B cell function. These results may reflect in vivo the modulation of normal human B cells and lymphoblasts by rHu-EPO observed in vitro.

摘要

重组人促红细胞生成素(rHu-EPO)是多种原因引起的贫血(包括骨髓肿瘤如多发性骨髓瘤(MM))中红系祖细胞的有效生长因子。我们研究了一组54例接受第二次诱导化疗的MM患者。其中30例被随机分配接受rHu-EPO治疗,初始剂量为150单位/千克体重,每周3次,从第6周起增加至300单位/千克体重,直至24周研究结束。到第8周时,这些患者中有77.7%的血红蛋白(Hb)水平升高。此外,5例接受VMCP方案治疗且依赖输血的患者在第三个月后完成试验,无需补充血液,而7例对照患者则需要频繁补充。每月对血液学参数的评估表明rHu-EPO能够增加网织红细胞计数,然而,5例患者在接受rHu-EPO治疗的同时明显对第二次诱导化疗产生了耐药性。在接受细胞毒性方案联合α干扰素(α-IFN)治疗的5例MM患者中,有4例对rHu-EPO的反应包括第三个月后血清IgM升高。在任何其他组中均未观察到这种效应,包括3例接受α-IFN + VMCP联合治疗但未接受rHu-EPO治疗的患者,以及未接受α-IFN治疗的rHu-EPO治疗患者。我们的数据表明,MM患者接受α-IFN加rHu-EPO治疗可有效恢复正常B细胞功能。这些结果可能在体内反映了体外观察到的rHu-EPO对正常人B细胞和成淋巴细胞的调节作用。

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