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慢性髓性白血病中的良性造血祖细胞:现状与未来展望

Benign hematopoietic progenitors in chronic myeloid leukemia: current status and future prospects.

作者信息

Cervantes F, Rozman C

机构信息

Postgraduate School of Hematology Farreras Valenti, Servicio de Hematología, Hospital Clínic, Barcelona, Spain.

出版信息

Ann Hematol. 1994 Sep;69(3):99-105. doi: 10.1007/BF01695688.

Abstract

Many patients with chronic myeloid leukemia (CML) retain a certain degree of normal hematopoiesis at disease presentation. This fact, suspected on the basis of cytogenetic findings, has been confirmed by long-term bone marrow cultures (LTBMC) and the combined use of phenotypic and molecular studies. Based on the lack of HLA-DR expression, it has been possible to recognize a benign subpopulation within the stem-cell compartment in CML. Different in vitro techniques have been developed for the selection of these benign progenitors, including LTBMC, marrow incubation with cytolytic drugs or interferon, positive selection based on their phenotypic characteristics, and exposure to synthetic antisense oligodeoxynucleotides. In vivo selection with interferon or intensive chemotherapy is also possible. The primary goal of the selection of benign hematopoietic progenitors is their use for autotransplantation. To date, a few hundred CML patients have been submitted to the latter procedure using bone marrow or peripheral blood. The fact that the majority of them show evidence of persistent disease emphasizes the necessity for better selection methods of the benign progenitors, for intensifying the conditioning regimen to reduce the tumor burden as much as possible, and for the use of adjuvant therapy post-transplantation. Future trends include the refinement of positive selection methods, negative selection by taking advantage of the different stromal adhesiveness of the benign and malignant progenitors, or the use of autologous natural killer cells, antisense oligodeoxynucleotides, or specific antibodies to the bcr/abl junction region, and retroviral marking to determine the origin of relapse in autologous transplantation.

摘要

许多慢性粒细胞白血病(CML)患者在疾病初发时仍保留一定程度的正常造血功能。基于细胞遗传学发现所怀疑的这一事实,已通过长期骨髓培养(LTBMC)以及表型和分子研究的联合应用得到证实。基于缺乏HLA - DR表达,已能够在CML的干细胞区室中识别出一个良性亚群。已开发出不同的体外技术用于选择这些良性祖细胞,包括LTBMC、用细胞溶解药物或干扰素进行骨髓孵育、基于其表型特征的阳性选择以及暴露于合成反义寡脱氧核苷酸。用干扰素或强化化疗进行体内选择也是可行的。选择良性造血祖细胞的主要目标是将其用于自体移植。迄今为止,已有数百名CML患者接受了使用骨髓或外周血的后者程序。他们中的大多数显示出持续性疾病的证据这一事实强调了对于更好地选择良性祖细胞的方法、强化预处理方案以尽可能降低肿瘤负荷以及移植后使用辅助治疗的必要性。未来的趋势包括改进阳性选择方法、利用良性和恶性祖细胞不同的基质黏附性进行阴性选择、或使用自体自然杀伤细胞、反义寡脱氧核苷酸、或针对bcr/abl连接区的特异性抗体,以及进行逆转录病毒标记以确定自体移植中复发的起源。

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