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Titlebook: Entry Inhibitors in HIV Therapy; Jacqueline D. Reeves,Cynthia A. Derdeyn Book 2007 Birkhäuser Basel 2007 AIDS.HIV.HIV Therapy.HIV infectio

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Classification and Diagnosis of Urticaria,g up to 30% difference within HIV-1 and up to 55% between HIV-1 and HIV-2 (www.hiv.lanl.gov). Most entry inhibitors have been designed and tested based on HIV-1 subtype B viruses, and would therefore be expected to be most effective against viruses of this genetic subtype. There are few studies that
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https://doi.org/10.1007/978-3-662-10733-1 for the treatment of HIV: the RTIs - either nucleoside or non-nucleoside - and PIs. Although combinations of these agents brought about dramatic improvements in HIV therapy, the limitations of therapeutic regimens based solely on RTIs and PIs were already evident and problematic when enfuvirtide en
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Inhibitors that target gp120 interactions with coreceptor,eference largely explains cell tropism. The importance of CCR5 in viral transmission and as a target for therapeutic intervention was underscored by the discovery of a 32-base pair deletion in the human CCR5 coding region (Δ32 mutation) which, when homozygous, prevents CCR5 surface expression and HI
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Enfuvirtide: from basic science to FDA approval, for the treatment of HIV: the RTIs - either nucleoside or non-nucleoside - and PIs. Although combinations of these agents brought about dramatic improvements in HIV therapy, the limitations of therapeutic regimens based solely on RTIs and PIs were already evident and problematic when enfuvirtide en
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Entry Inhibitors in HIV Therapy978-3-7643-7783-0Series ISSN 2296-6056 Series E-ISSN 2296-6064
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