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[人类嗜T淋巴细胞逆转录病毒(HTLV)的分子生物学]

[Molecular biology of human T-lymphotropic retroviruses (HTLV)].

作者信息

Dorner F, Barrett P N, Schmidt B L, Bodemer W

出版信息

Wien Med Wochenschr. 1986 Apr 30;136(7-8):181-8.

PMID:2425498
Abstract

The first human retroviruses have been discovered during the past seven years. They cause two diseases which involve disturbances of the growth of the T4-lymphocyte. This target cell type, which is central to the regulation of the immune system is induced by human T-lymphotropic virus type I (HTLV-I) to excessive proliferation (leukaemia) and by HTLV-III/LAV (lymphadenopathy associated virus) to premature death (acquired immune deficiency syndrome [AIDS]). Both also seem to be indirectly involved in several other disorders. The genetic structures of these retroviruses and the mechanisms by which they usurp host-cell functions are novel among retroviruses. The continuous increase in the number of AIDS cases for whom no effective therapy is currently possible mandates attempts at developing primary prevention by a vaccine. Based on past attempts at developing vaccines against retroviruses, the most feasible configuration will be the glycoprotein linked to its transmembrane protein. Any virus preparation containing nucleic acids could be considered less safe. Potential problems exist in that there is extensive heterogeneity among various HTLV-III isolates, particularly in the env-gene. This fact and the known relationship of HTLV-III to some Lentiviruses suggest that functional antigenic variation could be encountered. The methodology of developing a vaccine against the retroviruses causing AIDS should also be helpful in designing vaccine strategies against human leukaemia and lymphomas caused by other members of this virus family.

摘要

在过去七年中发现了首批人类逆转录病毒。它们引发两种疾病,这两种疾病都涉及T4淋巴细胞生长的紊乱。这种对免疫系统调节至关重要的靶细胞类型,被I型人类嗜T淋巴细胞病毒(HTLV-I)诱导过度增殖(白血病),被HTLV-III/LAV(淋巴结病相关病毒)诱导过早死亡(获得性免疫缺陷综合征[艾滋病])。两者似乎也间接涉及其他几种疾病。这些逆转录病毒的基因结构以及它们篡夺宿主细胞功能的机制在逆转录病毒中是新颖的。目前尚无有效治疗方法的艾滋病病例数量持续增加,这就要求尝试通过疫苗进行一级预防。基于过去开发抗逆转录病毒疫苗的尝试,最可行的构型将是与其跨膜蛋白相连的糖蛋白。任何含有核酸的病毒制剂都可能被认为安全性较低。存在潜在问题,因为各种HTLV-III分离株之间存在广泛的异质性,特别是在env基因方面。这一事实以及HTLV-III与某些慢病毒的已知关系表明可能会遇到功能性抗原变异。开发针对导致艾滋病的逆转录病毒的疫苗的方法,也应有助于设计针对由该病毒家族其他成员引起的人类白血病和淋巴瘤的疫苗策略。

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