Phorbol ester induces down-regulation of CD4 molecule expression and resistance to in vitro infection by HIV1.

Thymus Pub Date : 1992-12-01
J L Touraine, K Sanhadji, I Benard
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Abstract

In vitro infectivity of the MT4 lymphoid cell line with human immunodeficiency virus (HIV) has been studied in correlation with the degree of expression of the CD4 molecule at the cell surface. To modulate this CD4 expression in vitro, pre-incubation with phorbol myristate acetate (PMA) was used. The lowest CD4 expression was obtained after 1 to 5 hours. Thereafter, a partial re-expression of OKT4 was observed, e.g., when the incubation time with PMA was extended to 20 hours. Reverse transcriptase (RT) activity decreased and was delayed proportionally to the length of incubation of cells with PMA. This observation was confirmed by the comparable variation of cytopathic effects and of p24 antigen release in culture supernatants. The decrease in HIV infectivity hence correlated with that of OKT4 expression when PMA treatment did not exceed a few hours. By contrast, after extended treatment, infectivity remained decreased although OKT4 expression reappeared.

佛波酯诱导CD4分子表达下调及抗hiv体外感染。
研究了MT4淋巴样细胞系感染人类免疫缺陷病毒(HIV)的体外感染性与细胞表面CD4分子表达程度的相关性。为了在体外调节这种CD4的表达,用肉豆蔻酸酯佛波酯(PMA)预孵育。1 ~ 5小时后CD4表达最低。之后,观察到OKT4的部分再表达,例如,当PMA孵育时间延长至20小时时。逆转录酶(RT)活性降低,并与PMA细胞孵育时间成比例地延迟。细胞病变效应和培养上清中p24抗原释放的类似变化证实了这一观察结果。因此,当PMA治疗不超过几个小时时,HIV传染性的降低与OKT4表达的降低相关。相比之下,延长治疗后,尽管OKT4表达重新出现,但感染性仍然下降。
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