Human immunodeficiency virus reverse transcriptase codon 215 mutations diminish virologic response to didanosine-zidovudine therapy in subjects with non-syncytium-inducing phenotype
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作者:
Holodniy, M
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STANFORD UNIV,MED CTR,CTR AIDS RES,STANFORD,CA 94305STANFORD UNIV,MED CTR,CTR AIDS RES,STANFORD,CA 94305
Holodniy, M
[1
]
Katzenstein, D
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STANFORD UNIV,MED CTR,CTR AIDS RES,STANFORD,CA 94305STANFORD UNIV,MED CTR,CTR AIDS RES,STANFORD,CA 94305
Katzenstein, D
[1
]
Mole, L
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STANFORD UNIV,MED CTR,CTR AIDS RES,STANFORD,CA 94305STANFORD UNIV,MED CTR,CTR AIDS RES,STANFORD,CA 94305
Mole, L
[1
]
Winters, M
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STANFORD UNIV,MED CTR,CTR AIDS RES,STANFORD,CA 94305STANFORD UNIV,MED CTR,CTR AIDS RES,STANFORD,CA 94305
Winters, M
[1
]
Merigan, T
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STANFORD UNIV,MED CTR,CTR AIDS RES,STANFORD,CA 94305STANFORD UNIV,MED CTR,CTR AIDS RES,STANFORD,CA 94305
Merigan, T
[1
]
机构:
[1] STANFORD UNIV,MED CTR,CTR AIDS RES,STANFORD,CA 94305
Eight zidovudine-experienced subjects received zidovudine and didanosine for 30 weeks followed by 30 weeks of didanosine monotherapy. At study entry, plasma from 4 subjects had human immunodeficiency virus RNA pol T215Y/F mutant and 4 had codon 215 wild type. All 8 subjects had non-syncytium-inducing virus phenotype. Sustained 10-fold decreases in plasma RNA levels were seen only in subjects who initially had 215 wild type RNA, despite the development of a T215Y/F mutation during combination therapy. Virologic and immunologic benefits were maintained in this group with didanosine monotherapy. No subject developed a pol L74V codon mutation. Significant differences in plasma virus load and CD4 cell responses were seen in this zidovudine-didanosine combination pilot study relative to codon 215 genotype.