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体内HTLV-1相关白血病发生的分子和细胞层面

Molecular and cellular aspects of HTLV-1 associated leukemogenesis in vivo.

作者信息

Mortreux F, Gabet A-S, Wattel E

机构信息

Unité d'Oncogenèse Virale, UMR5537 CNRS-Université Claude Bernard, Centre Léon Bérard, Lyon, France.

出版信息

Leukemia. 2003 Jan;17(1):26-38. doi: 10.1038/sj.leu.2402777.

DOI:10.1038/sj.leu.2402777
PMID:12529656
Abstract

Most cancers and leukemias are preceded by a prolonged period of clinical latency during which cellular, chromosomal and molecular aberrations help move normal cell towards the malignant phenotype. The problem is that premalignant cells are usually indistinguishable from their normal counterparts, thereby ruling out the possibility to investigate the events that govern early leukemogenesis in vivo. Adult T cell leukemia/lymphoma (ATLL) is a T cell malignancy that occurs after a 40-60-year period of clinical latency in about 3-5% of HTLV-1-infected individuals. ATLL cells are monoclonally expanded and harbor an integrated provirus. A persistent oligo/polyclonal expansion of HTLV-1-bearing cells has been shown to precede ATLL, supporting the fact that in ATLL tumor cells arise from a clonally expanding non-malignant cell. It is possible to isolate infected, ie preleukemic, cells during the premalignant asymptomatic phase of the infection, thus providing an exceptional system to study the mechanisms underlying human cancers. Here we review some of the consequences of HTLV-1 on its host cell in vivo, at different stages of infection.

摘要

大多数癌症和白血病之前都有一段较长的临床潜伏期,在此期间,细胞、染色体和分子异常促使正常细胞向恶性表型转变。问题在于,癌前细胞通常与正常细胞难以区分,因此排除了在体内研究早期白血病发生过程中相关事件的可能性。成人T细胞白血病/淋巴瘤(ATLL)是一种T细胞恶性肿瘤,在约3%-5%的人类嗜T淋巴细胞病毒1型(HTLV-1)感染个体中,经过40-60年的临床潜伏期后发病。ATLL细胞呈单克隆扩增,并含有整合的前病毒。研究表明,携带HTLV-1的细胞持续寡克隆/多克隆扩增先于ATLL出现,这支持了ATLL肿瘤细胞源自克隆性扩增的非恶性细胞这一事实。在感染的癌前无症状阶段,可以分离出受感染的即白血病前期细胞,从而提供了一个研究人类癌症潜在机制的特殊系统。在此,我们综述了HTLV-1在感染的不同阶段对其宿主细胞在体内产生的一些影响。

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