Natural Variation in Vif: Differential Impact on APOBEC3G/3F and a Potential Role in HIV-1 Diversification
نویسندگان
چکیده
The HIV-1 Vif protein counteracts the antiviral activity exhibited by the host cytidine deaminases APOBEC3G and APOBEC3F. Here, we show that defective vif alleles can readily be found in HIV-1 isolates and infected patients. Single residue changes in the Vif protein sequence are sufficient to cause the loss of Vif-induced APOBEC3 neutralization. Interestingly, not all the detected defects lead to a complete inactivation of Vif function since some mutants retained selective neutralizing activity against APOBEC3F but not APOBEC3G or vice versa. Concordantly, independently hypermutated proviruses with distinguishable patterns of G-to-A substitution attributable to cytidine deamination induced by APOBEC3G, APOBEC3F, or both enzymes were present in individuals carrying proviruses with completely or partly defective Vif variants. Natural variation in Vif function may result in selective and partial neutralization of cytidine deaminases and thereby promote viral sequence diversification within HIV-1 infected individuals.
منابع مشابه
تولید سلول های ناپذیرا برای مطالعه HIV-1 vif
سابقه و هدف: مولکول APOBEC3G ، به عنوان فاکتور سلولی دخیل در میانکنش با vif HIV-1 عمل میکند که برای بررسی میانکنش آن با vif HIV-1 ، از سلولهای ناپذیرای طبیعی و ذاتی مثل H9 و PBMC انسانی مولد APOBEC3G استفاده میشود. به دلیل ناکارآمدی آنها در این نوع بررسیها، نیازمند سلولهای ناپذیرایی بودیم که به طور ثابت و به میزان بالا تولید APOBEC3G بنماید. لذا از سلولهای 293T برای ایجاد این دسته از سلول...
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ورودعنوان ژورنال:
- PLoS Pathogens
دوره 1 شماره
صفحات -
تاریخ انتشار 2005