Tipranavir (TPV) Genotypic Inhibitory Quotient Predicts Virological Response at 48 Weeks to TPV-Based Salvage Regimens

Requena, Daniel González de; Bonora, Stefano; Calcagno, Andrea; D’Avolio, Antonio; Siccardi, Marco; Fontana, Silvia; Milia, Maria Grazia; Sciandra, Mauro; Garazzino, Silvia; Garbo, Antonio Di; Baietto, Lorena; Trentini, Laura; Perri, Giovanni Di

doi:10.1128/aac.01063-07

Cited by 15 publications

(7 citation statements)

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“…Genotypic inhibitory quotients (GIQ) were calculated for each PI by dividing the C trough by the number of specific DRM detected in the GRT1 [13,14] and classified as therapeutic/subtherapeutic on the basis of GIQ efficacy thresholds extrapolated from the literature (C0.220 lg/ml/ mutation for atazanavir; C1.800 lg/ml/mutation for darunavir; C0.300 lg/ml/mutation for fosamprenavir; C1.000 lg/ml/mutation for lopinavir; C0.040 lg/ml/ mutation for saquinavir; C14.501 lg/ml/mutation for tipranavir) [15][16][17][18][19][20].…”

Section: Drug Levelsmentioning

confidence: 99%

Relationship between antiretroviral plasma concentration and emergence of HIV-1 resistance mutations at treatment failure

et al. 2011

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Section: Drug Levelsmentioning

confidence: 99%

Relationship between antiretroviral plasma concentration and emergence of HIV-1 resistance mutations at treatment failure

et al. 2011

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“…The genotypic sensitivity score, sometimes referred to as an optimized background score considers the number of drugs in the optimized background regimen which have been shown to be active through genotypic testing 65–67. For adult patients with a genotypic sensitivity score of ≥2, 64.2% achieved a virologic response, compared with a 20% virologic response rate for those with a score <2 66. This trend was not observed in pediatric patients, possibly due to the small number of patients enrolled, and very few having a genotypic sensitivity score of ≥2 67.…”

Section: Newer Arv Treatment Options For Hiv-positive Adults and Chilmentioning

confidence: 93%

“…When correlating gIQ, tipranavir trough, tipranavir mutation score, use of enfuvirtide, and genotypic sensitivity score with virologic response in adult patients using logistic regression, gIQ was found to be the most significant predictor of virologic response ( P = 0.03) 63. At 48 weeks, a significantly greater reduction in viral load was observed in adult patients who had a gIQ > 14,500 ng/mL/mutation (83.3% versus 38.4%) 66. At 48 weeks, pediatric patients with a gIQ above the first quartile (0.56–7.19) were more likely to achieve a viral load of <400 copies/mL (8% versus 52–68%) 67.…”

Section: Newer Arv Treatment Options For Hiv-positive Adults and Chilmentioning

confidence: 94%

“… 65 – 67 For adult patients with a genotypic sensitivity score of ≥2, 64.2% achieved a virologic response, compared with a 20% virologic response rate for those with a score <2. 66 This trend was not observed in pediatric patients, possibly due to the small number of patients enrolled, and very few having a genotypic sensitivity score of ≥2. 67 An inhibitory quotient is calculated by dividing the tipranavir trough by the tipranavir IC 50 .…”

Section: Newer Arv Treatment Options For Hiv-positive Adults and Chilmentioning

confidence: 95%

“…The genotypic inhibitory quotient (gIQ) is calculated by dividing the tipranavir serum trough concentration by the number of tipranavir resistance conferring mutations genotyped from the patient’s HIV strain 62,63,66,67,70. The measure of gIQ had the highest correlation with virologic success in both children and adults.…”

Section: Newer Arv Treatment Options For Hiv-positive Adults and Chilmentioning

confidence: 99%

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Role of tipranavir in treatment of patients with multidrug-resistant HIV

Courter

Teevan²,

Li³

et al. 2010

TCRM

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The worldwide emergence of multidrug-resistant human immunodeficiency virus (HIV)-1 strains has the driven the development of new antiretroviral (ARV) agents. Over the past 5 years, HIV-entry and integrase inhibitor ARVs, as well as improved non-nucleoside reverse transcriptase inhibitors (NRTIs) and protease inhibitors (PIs), have become available for treatment. It is important to assess how these new ARVs might be most judiciously used, paying close attention to viral susceptibility patterns, pharmacodynamic parameters, and the likelihood that patients will adhere to their therapy. Herein we review published material in Medline, EMBASE, and ISI for each antiretroviral agent/classes currently approved and summarize the available data on their efficacy, safety, and pharmacologic parameters. We focus on the role of tipranavir, a recently approved nonpeptidic PI, for treating HIV-infected children, adolescents, and adults with a history of multidrug-resistant HIV.

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Trifluoromethyl-substituted pyridyl- and pyrazolylboronic acids and esters: synthesis and Suzuki–Miyaura cross-coupling reactions

2009

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The synthesis of trifluoromethyl-substituted pyridylboronic acids and pyrazolylboronic esters is described via lithiation-boronation protocols (Schemes 1, 3 and 4). A study of their palladium-catalysed cross-couplings with heteroaryl halides is presented. CF3-substituted aryl/heteroaryl-pyridines are thereby obtained (51-98% yields). Analogous cross-couplings have yielded heteroaryl-3-(trifluoromethyl)pyrazoles (60-85% yields); homocoupling of the pyrazolylboronic esters is suppressed by the addition of potassium formate, although competing protodeboronation is observed. Halogenation of the 4-position of selected pyrazole coupling products allows for further cross-couplings to yield tetra-substituted pyrazolyl derivatives (Scheme 5). X-Ray crystal structures are reported for selected pyridylboronic acids, pyrazolylboronic esters and derived trifluoromethyl-substituted heterobiaryl systems. These multi-ring CF3-substituted systems are of interest as building blocks for drug discovery and materials chemistry.

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Tipranavir (TPV) Genotypic Inhibitory Quotient Predicts Virological Response at 48 Weeks to TPV-Based Salvage Regimens

Cited by 15 publications

References 15 publications

Relationship between antiretroviral plasma concentration and emergence of HIV-1 resistance mutations at treatment failure

Relationship between antiretroviral plasma concentration and emergence of HIV-1 resistance mutations at treatment failure

Role of tipranavir in treatment of patients with multidrug-resistant HIV

Trifluoromethyl-substituted pyridyl- and pyrazolylboronic acids and esters: synthesis and Suzuki–Miyaura cross-coupling reactions

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