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成人T细胞白血病/淋巴瘤整合过程中I型人嗜T细胞病毒的克隆扩增及基因组特征分析

[Clonal expansion and genomic characterization of the human T-cell lymphotropic virus type I during the integration process in adult T-cell leukemia/lymphoma].

作者信息

Salcedo-Cifuentes Mercedes, Cabrera Jesús, Cuesta-Astroz Yesid, Carrasca Edwin, Eizuru Yoshito, Domínguez Martha C, Sánchez Adalberto, García-Vallejo Felipe

机构信息

Laboratorio de Biología Molecular y Patogénesis, Departamento de Ciencias Fisiológicas, Facultad de Salud, Universidad del Valle, Cali, Colombia.

出版信息

Biomedica. 2009 Jun;29(2):218-31.

PMID:20128347
Abstract

INTRODUCTION

Although the integration of human T-cell lymphotropic virus type I into the T-cells is not a random process, the mechanistic details are not understood.

OBJECTIVES

The characteristics of the flanking host chromatin were evaluated at the integration sites in adult T-cell leukaemia/lymphoma (ATLL) patients infected with the virus.

MATERIALS AND METHODS

From seven leukemic Colombian patients positive for the human T-cell lymphotropic virus type I (HTLV-I), lymphocyte DNA samples were extracted and amplified by inverse polymerase chain reaction (IPCR). Clonal expansion and human genome nucleotide composition in an extension of 50 bp was determined. To establish the characteristics of the human genome flanking provirus, 61 IPCR sequences from Colombian and Japanese ATLL patients, were analyzed in silico to obtain insights about the genomic structure, functions and nature of associated chromatin.

RESULTS

The clonal expansion of cell clones was predominantly oligoclonal. From 61 IPCR sequences, 155 alignments with homology higher than 95% (e-value < 0.05) were screened. Seventy-five percent of those sequences corresponded to non coding elements that include repetitive and non-repetitive DNA. Fifty percent of the proviral integrations were associated with chromosomes of A and B groups. Viral DNA integration tended to favor exons of genes that replicated early, controlled the cell cycle, or were involved in signal transduction.

CONCLUSIONS

The results indicated that HTLV-I integration was preferentially directed towards genomic environments with high C:G content, and toward genes that replicate early, regulate cell cycle or involved with signal transduction.

摘要

引言

虽然人类嗜T细胞病毒I型整合到T细胞中并非随机过程,但其机制细节尚不清楚。

目的

评估感染该病毒的成人T细胞白血病/淋巴瘤(ATLL)患者整合位点侧翼宿主染色质的特征。

材料与方法

从7例人类嗜T细胞病毒I型(HTLV-I)阳性的哥伦比亚白血病患者中提取淋巴细胞DNA样本,并通过反向聚合酶链反应(IPCR)进行扩增。测定50bp延伸范围内的克隆扩增和人类基因组核苷酸组成。为确定前病毒侧翼人类基因组的特征,对来自哥伦比亚和日本ATLL患者的61条IPCR序列进行了计算机分析,以了解相关染色质的基因组结构、功能和性质。

结果

细胞克隆的克隆扩增主要为寡克隆。从61条IPCR序列中筛选出155条同源性高于95%(e值<0.05)的比对序列。其中75%的序列对应于包括重复和非重复DNA在内的非编码元件。50%的前病毒整合与A组和B组染色体相关。病毒DNA整合倾向于早期复制、控制细胞周期或参与信号转导的基因外显子。

结论

结果表明,HTLV-I整合优先靶向C:G含量高的基因组环境,以及早期复制、调节细胞周期或参与信号转导的基因。

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