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在选择性药物压力下,重组导致HIV-1双重耐药突变体迅速出现。

Recombination leads to the rapid emergence of HIV-1 dually resistant mutants under selective drug pressure.

作者信息

Moutouh L, Corbeil J, Richman D D

机构信息

Department of Pathology, University of California, San Diego, 92093-0679, USA.

出版信息

Proc Natl Acad Sci U S A. 1996 Jun 11;93(12):6106-11. doi: 10.1073/pnas.93.12.6106.

Abstract

The potential contribution of recombination to the development of HIV-1 resistance to multiple drugs was investigated. Two distinct viruses, one highly resistant to a protease inhibitor (SC-52151) and the other highly resistant to zidovudine, were used to coinfect T lymphoblastoid cells in culture. The viral genotypes could be distinguished by four mutations conferring drug resistance to each drug and by other sequence differences specific for each parental virus. Progeny virions recovered from mixed infection were passaged in the presence and absence of both zidovudine and SC-52151. Dually resistant mutants emerged rapidly under selective conditions, and these viruses were genetic recombinants. These results emphasize that genetic recombination could contribute to high-level multiple-drug resistance and that this process must be considered in chemotherapeutic strategies for HIV infection.

摘要

研究了重组对HIV-1产生多重耐药性的潜在作用。使用两种不同的病毒,一种对蛋白酶抑制剂(SC-52151)高度耐药,另一种对齐多夫定高度耐药,在培养中共同感染T淋巴母细胞。病毒基因型可通过赋予每种药物耐药性的四个突变以及每种亲本病毒特有的其他序列差异来区分。从混合感染中回收的子代病毒颗粒在有和没有齐多夫定及SC-52151的情况下传代。在选择性条件下,双重耐药突变体迅速出现,这些病毒是基因重组体。这些结果强调基因重组可能导致高水平的多重耐药性,并且在HIV感染的化疗策略中必须考虑这一过程。

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