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一种新型人类内源性逆转录病毒家族:HERV-K(HML-6)的结构与基因组组织

Structure and genomic organization of a novel human endogenous retrovirus family: HERV-K (HML-6).

作者信息

Medstrand P, Mager D L, Yin H, Dietrich U, Blomberg J

机构信息

Department of Medical Microbiology, Lund University, Sweden.

出版信息

J Gen Virol. 1997 Jul;78 ( Pt 7):1731-44. doi: 10.1099/0022-1317-78-7-1731.

DOI:10.1099/0022-1317-78-7-1731
PMID:9225050
Abstract

Prototypic elements of a novel human endogenous retrovirus (HERV) family were identified and cloned from a human genomic library by the use of a pol fragment, HML-6, related to type A and type B retroviruses and class II HERVs. Out of 39 polhybridizing clones, five contained structures of full-length retroviral proviruses, with regions showing similarity to gag, pol and env, flanked by long terminal repeats (LTRs). Restriction mapping and partial sequence analysis of each full-length clone revealed few conserved restriction sites among HML-6 genomes, and about 20% sequence divergence over the reverse transcriptase region sequenced, suggesting that HML-6 constitutes a heterogeneous, but distinct family of elements belonging to the HERV-K superfamily. Sequence analysis of two clones, HML-6p and HML-6.17, revealed a lysine (K) tRNA UUU primer-binding site, and 40-68% nucleotide sequence similarity to LTR, gag, pro, pol and env regions of type B retroviruses and class II HERVs. HERV-K (HML-6) elements are present at about 30-40 copies per haploid genome. The HML-6 LTRs contain putative progesterone-responsive elements, which may be involved in the regulation of HML-6 expression. Furthermore, there are about 50 additional solitary HML-6 LTRs per haploid genome. Such LTRs were integrated within the pol region of two clones belonging to the same HML-6 family, indicating that some site preference may be involved in HERV integration.

摘要

通过使用与A、B型逆转录病毒及II类人内源性逆转录病毒(HERV)相关的pol片段HML-6,从人类基因组文库中鉴定并克隆出了一个新型人类内源性逆转录病毒(HERV)家族的原型元件。在39个发生杂交的克隆中,有5个包含全长逆转录病毒前病毒结构,其区域与gag、pol和env相似,两侧为长末端重复序列(LTR)。对每个全长克隆进行限制性图谱分析和部分序列分析发现,HML-6基因组中几乎没有保守的限制性位点,并且在测序的逆转录酶区域序列上有大约20%的序列差异,这表明HML-6构成了一个属于HERV-K超家族的异质性但独特的元件家族。对两个克隆HML-6p和HML-6.17的序列分析揭示了一个赖氨酸(K)tRNA UUU引物结合位点,并且与B型逆转录病毒和II类HERV的LTR、gag、pro、pol和env区域有40 - 68%的核苷酸序列相似性。HERV-K(HML-6)元件在每个单倍体基因组中约有30 - 40个拷贝。HML-6 LTR包含假定的孕酮反应元件,可能参与HML-6表达的调控。此外,每个单倍体基因组中还有约50个额外的单独HML-6 LTR。这些LTR整合在属于同一HML-6家族的两个克隆的pol区域内,表明HERV整合可能涉及一些位点偏好。

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