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髓系核型与慢性粒细胞白血病的恶性期

Myeloid karyotype and the malignant phase of chronic granulocytic leukaemia.

作者信息

Lilleyman J S, Potter A M, Watmore A E, Cooke P, Sokol R J, Wood J K

出版信息

Br J Haematol. 1978 Jul;39(3):317-23. doi: 10.1111/j.1365-2141.1978.tb01104.x.

Abstract

During the course of a 30 month study period, 26 patients with typical chronic granulocytic leukaemia (CGL) developed karyotype abnormalities in addition to the Philadelphia (Ph1) chromosome. All cases had received at least 14 months continuous low dose busulphan, and the chromosome changes were found before clinical transformation in six patients and at the time this occurred in 20. Survival following the discovery of these additional abnormalities was short, with a median of 11 weeks for the whole group. Trisomy 8 was the commonest additional chromosome abnormality, but no one karyotype change was clearly associated with shorter survival than another. 23 of the 26 have died as a direct result of their disease, forming part of a total of 40 deaths from typical CGL encountered during the study period where karyotype analyses were performed during the terminal stages of disease. Of these 40, only two (5%) patients showed no chromosome abnormalities extra to the Ph1 prior to death. (The 17 non-study patients who died were similar in all respects to the 23 from the study group, but had no prior chromosome studies performed during the chronic phase of the disease.) It is suggested that an expanding aneuploid or pseudodiploid clone arising from the leukaemic cells during the benign phase of CGL can be used to mark the sometimes ill-defined onset of the malignant phase in all but a small proportion of cases.

摘要

在为期30个月的研究期间,26例典型慢性粒细胞白血病(CGL)患者除了有费城(Ph1)染色体外,还出现了核型异常。所有病例均接受了至少14个月的持续低剂量白消安治疗,其中6例患者在临床转化前发现染色体改变,20例在临床转化时发现。发现这些额外异常后的生存期较短,全组中位生存期为11周。三体8是最常见的额外染色体异常,但没有一种核型改变与比其他改变更短的生存期明显相关。26例中有23例直接死于该病,这是研究期间典型CGL总共40例死亡的一部分,这些死亡病例在疾病终末期进行了核型分析。在这40例中,只有2例(5%)患者在死亡前除了Ph1染色体外没有其他染色体异常。(17例非研究患者的死亡情况在各方面与研究组的23例相似,但在疾病慢性期未进行过染色体研究。)有人提出,在CGL的良性阶段,白血病细胞产生的不断扩大的非整倍体或假二倍体克隆可用于标记除一小部分病例外,恶性阶段有时不明确的发病情况。

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