Pharmacodynamics, Safety, and Pharmacokinetics of BMS-663068, an Oral HIV-1 Attachment Inhibitor in HIV-1-Infected Subjects

Nettles, Richard E.; Schürmann, Dirk; Zhu, Li; Stonier, Michele; Huang, Shu-Pang; Chang, Ih; Chien, Caly; Krystal, Mark; Wind‐Rotolo, Megan; Ray, Neelanjana; Hanna, George J.; Bertz, Richard; Grasela, Dennis M.

doi:10.1093/infdis/jis432

Cited by 94 publications

(84 citation statements)

References 9 publications

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“…(q12h) plus RTV at 100 mg q12h or every morning with those in subjects receiving BMS-663068 alone at 1,200 mg q12h (15). The moderate increase in BMS-626529 systemic exposure observed in the presence of RTV is consistent with the metabolic profile of the compound, in that RTV inhibits the CYP3A-mediated metabolism of BMS-626529 but has a minimal effect on the esterase-mediated hydrolysis pathway.…”

Section: Discussionsupporting

confidence: 55%

“…As both ATV and RTV are potent inhibitors of CYP3A4 (12,13), it was anticipated that coadministration of ATV and RTV with BMS-663068 could result in greater systemic exposures of BMS-626529. This is supported by results from earlyphase pharmacokinetic (PK) studies (14)(15)(16) that have shown that RTV moderately increases BMS-626529 systemic exposure. In contrast, as neither BMS-663068 nor BMS-626529 inhibits CYP3A4 in vitro, coadministration of BMS-663068 with RTV and/or ATV is not expected to affect RTV or ATV exposures.…”

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confidence: 64%

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Pharmacokinetic Interactions between BMS-626529, the Active Moiety of the HIV-1 Attachment Inhibitor Prodrug BMS-663068, and Ritonavir or Ritonavir-Boosted Atazanavir in Healthy Subjects

Zhu

Hruska

Hwang

et al. 2015

Antimicrob Agents Chemother

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BMS-663068 is a prodrug of BMS-626529, a first-in-class attachment inhibitor that binds directly to HIV-1 gp120, preventing initial viral attachment and entry into host CD4 ؉ T cells. This open-label, multiple-dose, four-sequence, crossover study addressed potential two-way drug-drug interactions following coadministration of BMS-663068 (BMS-626529 is a CYP3A4 substrate), atazanavir (ATV), and ritonavir (RTV) (ATV and RTV are CYP3A4 inhibitors). Thirty-six healthy subjects were randomized 1:1:1:1 to receive one of four treatment sequences with three consecutive treatments: BMS-663068 at 600 mg twice daily (BID), BMS-663068 at 600 mg BID plus RTV at 100 mg once daily (QD), ATV at 300 mg QD plus RTV at 100 mg QD (

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Section: Discussionsupporting

confidence: 55%

mentioning

confidence: 64%

Pharmacokinetic Interactions between BMS-626529, the Active Moiety of the HIV-1 Attachment Inhibitor Prodrug BMS-663068, and Ritonavir or Ritonavir-Boosted Atazanavir in Healthy Subjects

Zhu

Hruska

Hwang

et al. 2015

Antimicrob Agents Chemother

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“…Baseline viral drug susceptibility appeared to be the most influential factor in determining the magnitude of the decline in HIV-1 RNA levels during BMS-663068 monotherapy, in line with observations from the AI438006 study (6,10), and the most compelling exposure-response relationships were observed with log etransformed PBAIC 50 -adjusted C ss,avg and C tau . There were no significant differences between the C ss,avg and C tau models, so, as C tau is generally considered to be a better predictor of antiviral activity, the C tau model was selected for the modeling and simulation analysis.…”

Section: Discussionsupporting

confidence: 75%

“…Only subjects with a baseline BMS-626529 half-maximal (50%) inhibitory concentration (IC 50 ) of Ͻ100 nM were included in the AI438011 study (7); the baseline BMS-626529 IC 50 was not an exclusion criterion for the AI438006 study. Plasma samples were analyzed for BMS-626529 concentrations by a validated liquid chromatography-mass spectrometry/mass spectrometry (LC-MS/MS) assay as previously described (6).…”

Section: Methodsmentioning

confidence: 99%

“…In a phase 2a study of BMS-663068 monotherapy with or without RTV boosting in treatment-naive and treatment-experienced subjects (AI438006 study; ClinicalTrials.gov registration num-ber NCT01009814), a maximum median decline in the plasma HIV-1 RNA level of 1.12 to 1.73 log 10 copies/ml was observed after 8 days of treatment (6). The greatest virologic response (a change in the HIV-1 RNA level from the baseline level of Ն1 log 10 copies/ ml) to BMS-663068 treatment was in subjects with a baseline BMS-626529 half-maximal (50%) inhibitory concentration (IC 50 ) of Յ100 nM, with no change in efficacy detected across a wide range of doses.…”

mentioning

confidence: 99%

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Model-Based Phase 3 Dose Selection for HIV-1 Attachment Inhibitor Prodrug BMS-663068 in HIV-1-Infected Patients: Population Pharmacokinetics/Pharmacodynamics of the Active Moiety, BMS-626529

Landry

Zhu

Tarif

et al. 2016

Antimicrob Agents Chemother

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BMS-663068 is an oral prodrug of the HIV-1 attachment inhibitor BMS-626529, which prevents viral attachment to host CD4؉ T cells by binding to HIV-1 gp120. To guide dose selection for the phase 3 program, pharmacokinetic/pharmacodynamic modeling was performed using data from two phase 2 studies with HIV-1-infected subjects (n ‫؍‬ 244). BMS-626529 population pharmacokinetics were described by a two-compartment model with first-order elimination from the central compartment, zero-order release of prodrug from the extended-release formulation into a hypothetical absorption compartment, and first-order absorption into the central compartment. The covariates of BMS-663068 formulation type, lean body mass, baseline CD8؉ T-cell percentage, and ritonavir coadministration were found to be significant contributors to intersubject variability. Exposure-response analyses showed a relationship between the log e -transformed concentration at the end of a dosing interval (C tau ) normalized for the protein binding-adjusted BMS-626529 half-maximal (50%) inhibitory concentration (PBAIC 50 ) and the change in the HIV-1 RNA level from the baseline level after 7 days of BMS-663068 monotherapy. The probability of achieving a decline in HIV-1 RNA level of >0.5 or >1.0 log 10 copies/ml as a function of the log e -transformed PBAIC 50 -adjusted C tau after 7 days of monotherapy was 99 to 100% and 57 to 73%, respectively, for proposed BMS-663068 doses of 400 mg twice daily (BID), 600 mg BID (not studied in the phase 2b study), 800 mg BID, 600 mg once daily (QD), and 1,200 mg QD. On the basis of a slight advantage in efficacy of BID dosing over QD dosing, similar responses for the 600-and 800-mg BID doses, and prior clinical observations, BMS-663068 at 600 mg BID was predicted to have the optimal benefit-risk profile and selected for further clinical investigation. (The phase 2a proof-of-concept study AI438006 and the phase 2b study AI438011 are registered at ClinicalTrials.gov under numbers NCT01009814 and NCT01384734, respectively.) A s the management of HIV-1 infection requires lifelong treatment with sequential combination antiretroviral therapy (cART), antiretrovirals with a novel mechanism of action that can be used in combination with other agents to form active regimens following virologic failure are needed. This is particularly relevant for heavily treatment-experienced patients who, by definition, have limited remaining treatment options due to viral drug resistance, toxicity, and drug-drug interactions (1). For such patients, treatment guidelines recommend construction of a new regimen containing two or, ideally, three fully active agents where possible, on the basis of treatment history, viral drug resistance, and/or a new mechanism of action (1, 2).BMS-663068 is an oral prodrug of the first-in-class HIV-1 attachment inhibitor BMS-626529, which prevents initial viral attachment to the host CD4 ϩ T cell by binding to the viral envelope protein gp120 (3). BMS-663068 is administered as an extendedrelease (ER) formulation, which...

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Antiviral Drug Discovery

Meanwell¹,

D’Andrea²,

Cianci³

et al. 2013

Drug Discovery

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Pharmacodynamics, Safety, and Pharmacokinetics of BMS-663068, an Oral HIV-1 Attachment Inhibitor in HIV-1-Infected Subjects

Cited by 94 publications

References 9 publications

Pharmacokinetic Interactions between BMS-626529, the Active Moiety of the HIV-1 Attachment Inhibitor Prodrug BMS-663068, and Ritonavir or Ritonavir-Boosted Atazanavir in Healthy Subjects

Pharmacokinetic Interactions between BMS-626529, the Active Moiety of the HIV-1 Attachment Inhibitor Prodrug BMS-663068, and Ritonavir or Ritonavir-Boosted Atazanavir in Healthy Subjects

Model-Based Phase 3 Dose Selection for HIV-1 Attachment Inhibitor Prodrug BMS-663068 in HIV-1-Infected Patients: Population Pharmacokinetics/Pharmacodynamics of the Active Moiety, BMS-626529

Antiviral Drug Discovery

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