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不协调成熟作为慢性粒细胞白血病的主要生物学缺陷。

Discordant maturation as the primary biological defect in chronic myelogenous leukemia.

作者信息

Strife A, Lambek C, Wisniewski D, Wachter M, Gulati S C, Clarkson B D

机构信息

Laboratory of Hematopoietic Cell Kinetics, Sloan-Kettering Institute, New York, New York.

出版信息

Cancer Res. 1988 Feb 15;48(4):1035-41.

PMID:3422181
Abstract

Comparative studies of the in vitro growth characteristics of normal and chronic myelogenous leukemic (CML) progenitor cells have provided further evidence that discordant maturation is the primary biological defect in CML. The in vitro growth of total normal and CML granulocyte/macrophage colony forming unit (CFU-GM) populations were compared with early and intermediate (HLA-DR positive) CFU-GM derived from the same marrows. The absolute number of total CML CFU-GM exceeded the number generated by normal marrow through 7 days of culture due entirely to an excess of CML CFU-GM with limited proliferative capacity. Unlike normal colonies, relatively few of the leukemic colonies grew to a large size; the early and intermediate (HLA-DR positive) CML progenitors also exhibited limited proliferative capacity compared to normal. Highly enriched progenitor populations were prepared, and it was observed that the primitive (small) CML CFU-GM also had greatly reduced proliferative potential compared to primitive normal progenitors, but rather behaved similarly to normal mature (large) CFU-GM. Similarly, CML erythroid burst forming units were at a more advanced stage of maturation than normal erythroid burst forming units as evidenced by their reduced proliferative capacity, the observation that a reduced proportion required burst promoting activity to enable them to respond to erythropoietin and the observation that a larger fraction than normal could sustain a limited period of erythropoietin deprivation in the absence of burst promoting activity. Based on these findings and supporting evidence from our previous studies and those reported by other investigators, it is concluded that the dominance of the leukemic population is not due to unregulated proliferation but rather to discordant maturation resulting in expansion in the later maturational compartments which are not under strict regulatory control.

摘要

对正常和慢性粒细胞白血病(CML)祖细胞的体外生长特性进行的比较研究,进一步证明了成熟失调是CML的主要生物学缺陷。将正常和CML粒细胞/巨噬细胞集落形成单位(CFU-GM)群体的体外生长情况,与来自同一骨髓的早期和中期(HLA-DR阳性)CFU-GM进行了比较。在7天的培养过程中,CML CFU-GM的总数超过了正常骨髓产生的数量,这完全是由于增殖能力有限的CML CFU-GM数量过多所致。与正常集落不同,白血病集落中相对较少能生长到较大尺寸;与正常情况相比,早期和中期(HLA-DR阳性)的CML祖细胞也表现出有限的增殖能力。制备了高度富集的祖细胞群体,观察到原始(小)CML CFU-GM与原始正常祖细胞相比,其增殖潜力也大大降低,但表现与正常成熟(大)CFU-GM相似。同样,CML红系爆式集落形成单位比正常红系爆式集落形成单位处于更成熟的阶段,这表现为它们增殖能力降低,观察发现需要爆式促进活性才能对促红细胞生成素作出反应的比例降低,以及观察到在没有爆式促进活性的情况下,能在有限时间内耐受促红细胞生成素剥夺的比例比正常情况更大。基于这些发现以及我们之前研究和其他研究者报告的支持证据,得出结论:白血病群体占优势并非由于增殖不受调控,而是由于成熟失调导致在后期成熟区室中扩张,而这些区室并未受到严格的调控。

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