Your search keyword '"Song, Ivy"' showing total 13 results

1. Population pharmacokinetics and exposure-response relationships of maribavir in transplant recipients with cytomegalovirus infection.

Author

Song IH, Chen G, Hayes S, Farrell C, Jomphe C, Gosselin NH, and Sun K

Subjects

Humans, Middle Aged, Male, Female, Adult, Aged, Transplant Recipients, Dose-Response Relationship, Drug, Cytomegalovirus drug effects, Models, Biological, Young Adult, Drug Resistance, Viral, Dichlororibofuranosylbenzimidazole analogs & derivatives, Cytomegalovirus Infections drug therapy, Ribonucleosides pharmacokinetics, Ribonucleosides administration & dosage, Ribonucleosides adverse effects, Ribonucleosides therapeutic use, Benzimidazoles pharmacokinetics, Benzimidazoles adverse effects, Benzimidazoles administration & dosage, Benzimidazoles therapeutic use, Antiviral Agents pharmacokinetics, Antiviral Agents therapeutic use, Antiviral Agents adverse effects, Antiviral Agents administration & dosage

Abstract

Maribavir is approved for management of post-transplant cytomegalovirus (CMV) infections refractory and/or resistant to CMV therapies at a dose of 400 mg twice daily (BID). Population pharmacokinetic (PopPK) and exposure-response analyses were conducted to support the appropriateness of 400 mg BID dosing. A PopPK model was developed using non-linear mixed-effects modeling with pooled maribavir plasma concentration-time data from phase 1 and 2 studies (from 100 mg up to 1200 mg as single or repeated doses) and the phase 3 SOLSTICE study (400 mg BID). Exposure-response analyses were performed for efficacy, safety, and viral resistance based on data collected in the SOLSTICE study. Maribavir PK after oral administration was adequately described by a two-compartment model with first-order elimination, first-order absorption, and an absorption lag-time. There was no evidence that maribavir PK was affected by age, sex, race, diarrhea, vomiting, disease characteristics, or concomitant use of histamine H 2 blockers, or proton pump inhibitors. In the SOLSTICE study, higher maribavir exposure was not associated with increased probability of achieving CMV DNA viremia clearance, nor with reduced probability of treatment-emergent maribavir-resistant CMV mutations. A statistically significant association with maribavir exposure was identified for taste disturbance, fatigue, and treatment-emergent serious adverse events, while transplant type, enrollment region, CMV DNA level at baseline, and/or CMV resistance at baseline were identified as additional risk factors for these safety outcomes. In conclusion, the findings of these PopPK and exposure-response analyses provide further support for the recommended maribavir dose of 400 mg BID., Competing Interests: Declarations. Competing interests: IH Song, G Chen, and K Sun are employees of Takeda Development Center Americas, Inc., and receive stocks (and stock options) from Takeda. S Hayes and C Farrell are employees of ICON plc. C Jomphe and NH Gosselin are employees of Certara., (© 2024. The Author(s).)

Published

2024

2. Maribavir: Mechanism of action, clinical, and translational science.

Author

Sun K, Fournier M, Sundberg AK, and Song IH

Subjects

Humans, Translational Science, Biomedical, Benzimidazoles, Antiviral Agents, Cytomegalovirus Infections chemically induced, Cytomegalovirus Infections drug therapy, Dichlororibofuranosylbenzimidazole analogs & derivatives

Abstract

Maribavir is an oral benzimidazole riboside for treatment of post-transplant cytomegalovirus (CMV) infection/disease that is refractory to prior antiviral treatment (with or without resistance). Through competitive inhibition of adenosine triphosphate, maribavir prevents the phosphorylation actions of UL97 to inhibit CMV DNA replication, encapsidation, and nuclear egress. Maribavir is active against CMV strains with viral DNA polymerase mutations that confer resistance to other CMV antivirals. After oral administration, maribavir is rapidly and highly absorbed (fraction absorbed >90%). The approved dose of 400 mg twice daily (b.i.d.) achieves a steady-state area under the curve per dosing interval of 128 h*μg/mL and trough concentration of 4.90 μg/mL (13.0 μM). Maribavir is highly bound to human plasma proteins (98%) with a small apparent volume of distribution of 27.3 L. Maribavir is primarily cleared by hepatic CYP3A4 metabolism; its major metabolite, VP44669 (pharmacologically inactive), is excreted in the urine and feces. There is no clinically relevant impact on maribavir pharmacokinetics by age, sex, race/ethnicity, body weight, transplant type, or hepatic/renal impairment status. In phase II dose-ranging studies, maribavir showed similar rates of CMV viral clearance across 400, 800, or 1200 mg b.i.d. groups, ranging from 62.5-70% in study 202 (NCT01611974) and 74-83% in study 203 (EudraCT 2010-024247-32). In the phase III SOLSTICE trial (NCT02931539), maribavir 400 mg b.i.d. demonstrated superior CMV viremia clearance at week 8 versus investigator-assigned treatments, with lower treatment discontinuation rates. Dysgeusia, nausea, vomiting, and diarrhea were commonly experienced adverse events among patients treated with maribavir in clinical trials., (© 2024 Takeda Development Center Americas, Inc. Clinical and Translational Science published by Wiley Periodicals LLC on behalf of American Society for Clinical Pharmacology and Therapeutics.)

Published

2024

3. Pharmacokinetics and Safety Evaluation of Maribavir in Healthy Japanese and Matched White Participants: A Phase 1, Open-Label Study.

Author

Song I, Suttle B, Wu J, and Ilic K

Subjects

Adult, Humans, Area Under Curve, East Asian People, White People, Antiviral Agents pharmacokinetics, Dichlororibofuranosylbenzimidazole analogs & derivatives, Dichlororibofuranosylbenzimidazole pharmacokinetics

Abstract

This phase I study compared pharmacokinetics and safety of maribavir in Japanese and White participants, and evaluated dose proportionality in Japanese participants. Under fasting conditions, 12 healthy adult participants of Japanese descent and 12 matched White participants received a single 400-mg dose of maribavir. Japanese participants received 2 further doses of maribavir: 200 mg and 800 mg, or 800 mg and 200 mg, separated by a ≥72-hour washout period. Serial blood samples were collected up to 24 hours after dosing for pharmacokinetic assessments. Following the 400-mg dose, the geometric mean ratios (90% confidence interval) of Japanese versus White participants were 110% (91.7%-133%) for maximum plasma concentration, 122% (96.8%-155%) for area under the plasma concentration-time curve (AUC) from time of dosing to the last measurable concentration, and 125% (98.0%-160%) for AUC extrapolated to infinity. In Japanese participants, maribavir AUC extrapolated to infinity and AUC from time of dosing to the last measurable concentration increased in a dose-proportional fashion over 200-800 mg; maximum plasma concentration increased less than dose proportionally. Seven participants reported treatment-emergent adverse events (TEAEs; Japanese participants, 400 mg: 2 [16.7%], 200 mg: 1 [8.3%]; White participants, 400 mg: 4 [33.3%]), all mild and most commonly dysgeusia. No serious TEAEs or TEAEs leading to discontinuation were reported. This study demonstrated higher maribavir systemic exposure in Japanese than White participants and similar safety outcomes. This difference in exposure is not considered clinically important and its significance remains to be determined., (© 2023 Takeda Development Center Americas, Inc. Clinical Pharmacology in Drug Development published by Wiley Periodicals LLC on behalf of American College of Clinical Pharmacology.)

Published

2023

4. Evaluation of the Effect of Maribavir on Cardiac Repolarization in Healthy Participants: Thorough QT/QTc Study.

Author

Ilic K, Song I, Wu J, and Martin P

Subjects

Administration, Oral, Adolescent, Adult, Antiviral Agents adverse effects, Benzimidazoles adverse effects, Blood Pressure drug effects, Cross-Over Studies, Dose-Response Relationship, Drug, Double-Blind Method, Dysgeusia diagnosis, Female, Healthy Volunteers, Heart Rate drug effects, Humans, Long QT Syndrome chemically induced, Male, Middle Aged, Moxifloxacin administration & dosage, Ribonucleosides adverse effects, Young Adult, Antiviral Agents administration & dosage, Benzimidazoles administration & dosage, Dysgeusia chemically induced, Electrocardiography drug effects, Long QT Syndrome diagnosis, Ribonucleosides administration & dosage

Abstract

Maribavir is an orally bioavailable benzimidazole riboside in clinical development for treatment of cytomegalovirus infection in patients who undergo transplantation. Maribavir was evaluated in a thorough QT (TQT) study to determine any effects on cardiac repolarization. The effect of maribavir 100 and 1,200 mg oral doses on the baseline-adjusted and placebo-adjusted corrected QT (QTc) interval (delta delta QTc (ddQTc)) and other electrocardiogram (ECG) parameters was assessed in a randomized, phase I, placebo-controlled, four-period crossover study in healthy participants (men and women ages 18-50 years). Additionally, maribavir pharmacokinetics, safety, and tolerability were investigated. Moxifloxacin (400 mg) was used as a positive control to demonstrate the study's ability to detect QT prolongation. Digital 12-lead Holter ECG monitoring was performed over 22 hours following study drug administration. Individual, Fridericia's, and Bazett's QTc intervals were calculated. Of 52 randomized participants (29 ± 8.1 years old; 31 men (60%)), 50 (96%) completed the study. For both 100-mg and 1200-mg doses of maribavir, analysis of ddQTc demonstrated that the upper bound of the two-sided 90% confidence interval was below the 10-ms threshold at all time points. The concentration-effect analysis demonstrated no relationship between ddQTc and plasma concentrations of maribavir (and its metabolite). There were no clinically meaningful changes in heart rate and systolic blood pressure. The most common adverse event was dysgeusia; no serious adverse events were reported. This TQT study demonstrated that maribavir did not have impact on cardiac repolarization., (© 2020 Takeda Pharmaceuticals International Company. Clinical and Translational Science published by Wiley Periodicals LLC on behalf of the American Society for Clinical Pharmacology and Therapeutics.)

Published

2020

5. Effects of Maribavir on P-Glycoprotein and CYP2D6 in Healthy Volunteers.

Author

Song IH, Ilic K, Murphy J, Lasseter K, and Martin P

Subjects

Adult, Antiviral Agents administration & dosage, Antiviral Agents blood, Antiviral Agents pharmacokinetics, Benzimidazoles administration & dosage, Benzimidazoles blood, Benzimidazoles pharmacokinetics, Cytochrome P-450 CYP2D6 genetics, Cytomegalovirus Infections drug therapy, Dextromethorphan administration & dosage, Dextromethorphan blood, Dextromethorphan pharmacokinetics, Digoxin administration & dosage, Digoxin blood, Digoxin pharmacokinetics, Drug Interactions, Female, Genotype, Healthy Volunteers, Humans, Male, Middle Aged, Ribonucleosides administration & dosage, Ribonucleosides blood, Ribonucleosides pharmacokinetics, Young Adult, ATP Binding Cassette Transporter, Subfamily B, Member 1 metabolism, Antiviral Agents pharmacology, Benzimidazoles pharmacology, Cytochrome P-450 CYP2D6 metabolism, Ribonucleosides pharmacology

Abstract

Maribavir is an investigational drug being evaluated in transplant recipients with cytomegalovirus infection. To understand potential drug-drug interactions, we examined the effects of multiple doses of maribavir on cytochrome P450 (CYP) 2D6 and P-glycoprotein (P-gp) activity using probe substrates in healthy volunteers. During this phase 1 open-label study (NCT02775240), participants received the probe substrates digoxin (0.5 mg) and dextromethorphan (30 mg) before and after maribavir (400 mg twice daily for 8 days). Serial plasma samples were analyzed for digoxin, dextromethorpha, dextrorphan, and maribavir concentrations. Pharmacokinetic parameters were calculated (noncompartmental analysis) and analyzed with a linear mixed-effects model for treatment comparison to estimate geometric mean ratios (GMRs) and 90% confidence intervals (CIs). CYP2D6 polymorphisms were genotyped using polymerase chain reaction. Overall, 17 of 18 participants (94.4%) completed the study. All participants were genotyped as CYP2D6 intermediate/extensive metabolizers. GMR (90%CI) of digoxin C max , AUC last , and AUC 0-∞ with and without maribavir was 1.257 (1.139-1.387), 1.187 (1.088-1.296), and 1.217 (1.110-1.335), respectively, outside the "no-effect" window (0.8-1.25). GMR (90%CI) of dextromethorphan AUC last and AUC last ratio of dextromethorphan/dextrorphan were 0.877 (0.692-1.112) and 0.901 (0.717-1.133), respectively, marginally outside the no-effect window, although large variability was observed in these pharmacokinetic parameters. Pharmacokinetic parameters of dextrorphan were unaffected. Maribavir inhibited P-gp activity but did not affect CYP2D6 activity. Maribavir's effect on the pharmacokinetics of P-gp substrates should be evaluated individually, and caution should be exercised with P-gp substrates with narrow therapeutic windows., (© 2019 Shire Plc. The Journal of Clinical Pharmacology published by Wiley Periodicals, Inc. on behalf of American College of Clinical Pharmacology.)

Published

2020

6. No clinically significant pharmacokinetic interactions between dolutegravir and daclatasvir in healthy adult subjects.

Author

Ross LL, Song IH, Arya N, Choukour M, Zong J, Huang SP, Eley T, Wynne B, and Buchanan AM

Subjects

Adolescent, Adult, Aged, Antiviral Agents blood, Carbamates, Cross-Over Studies, Drug Administration Schedule, Drug Interactions, Female, HIV Integrase Inhibitors blood, HIV Integrase Inhibitors pharmacokinetics, Healthy Volunteers, Heterocyclic Compounds, 3-Ring blood, Humans, Imidazoles blood, Male, Middle Aged, Outcome Assessment, Health Care, Oxazines, Piperazines, Pyridones, Pyrrolidines, Valine analogs & derivatives, Young Adult, Antiviral Agents pharmacokinetics, Area Under Curve, Heterocyclic Compounds, 3-Ring pharmacokinetics, Imidazoles pharmacokinetics

Abstract

Background: Daclatasvir (DCV) is an NS5A replication complex inhibitor recently approved for chronic hepatitis C virus treatment., Methods: To assess drug interactions between the HIV integrase strand transfer inhibitor dolutegravir (DTG) and DCV, subjects were randomized into 1 of 2 sequences in an open-label, 3-period, crossover study. Subjects received either DTG 50 mg once daily or DCV 60 mg once daily for 5 days in periods 1 and 2 and DTG 50 mg plus DCV 60 mg once daily for 5 days in period 3, with no washout between periods 2 and 3. Between periods 1 and 2, there was a washout period of at least 7 days., Results: The geometric least-squares mean ratios (90 % confidence intervals) of DCV area under the concentration-time curve over a dosing interval (AUC0-τ), maximum observed concentration (Cmax), and concentration at the end of the dosing interval (Cτ) were 0.978 (0.831-1.15), 1.03 (0.843-1.25), and 1.06 (0.876-1.29), respectively, when DCV was administered with DTG compared with DCV alone. Compared with DTG alone, coadministration of DTG with DCV increased DTG AUC0-τ, Cmax, and Cτ by approximately 33, 29, and 45 %, respectively., Conclusions: DCV plasma exposure was not meaningfully affected by DTG. Coadministration of DTG with DCV resulted in slight increases in DTG AUC0-τ, Cmax, and Cτ. Accumulated safety and tolerability data in humans receiving DTG to date suggests this effect is not considered clinically significant. DTG and DCV can be coadministered without dose adjustment., Trial Registration: Registered on March 6, 2014 with ClinicalTrials.gov; registration number: NCT02082808 and as Study ID: 201102 on the ViiV Clinical Study Registry.

Published

2016

7. Physiologically Based Pharmacokinetic Modeling for Maribavir to Inform Dosing in Drug‐Drug Interaction Scenarios with CYP3A4 Inducers and Inhibitors.

Author

Chen, Grace, Sun, Kefeng, Michon, Ingrid, Barter, Zoe, Neuhoff, Sibylle, Ghosh, Lipika, Ilic, Katarina, and Song, Ivy H.

Subjects

IN vitro studies, SECONDARY analysis, RECEIVER operating characteristic curves, RESEARCH funding, CYTOMEGALOVIRUS diseases, ENZYME inhibitors, ANTIVIRAL agents, DRUG interactions, DRUG development, RIFAMPIN

Abstract

Maribavir, an orally available antiviral agent, has been approved in multiple countries for the treatment of patients with refractory post‐transplant cytomegalovirus (CMV) infection and/or disease. Maribavir is primarily metabolized by CYP3A4; coadministration with CYP3A4 inducers and inhibitors may significantly alter maribavir exposure, thereby affecting its efficacy and safety. The effect of CYP3A4 inducers and inhibitors on maribavir exposure was evaluated based on a drug‐drug interaction (DDI) study and physiologically‐based pharmacokinetic (PBPK) modeling. The effect of rifampin (a strong inducer of CYP3A4 and moderate inducer of CYP1A2), administered at a 600 mg dose once daily, on maribavir pharmacokinetics was assessed in a clinical phase 1 DDI study in healthy participants. A full PBPK model for maribavir was developed and verified using in vitro and clinical pharmacokinetic data from phase 1 studies. The verified PBPK model was then used to simulate maribavir DDI interactions with various CYP3A4 inducers and inhibitors. The DDI study results showed that coadministration with rifampin decreased the maribavir maximum plasma concentration (Cmax), area under the plasma concentration‐time curve (AUC), and trough concentration (Ctrough) by 39%, 60%, and 82%, respectively. Based on the results from the clinical DDI study, the coadministration of maribavir with rifampin is not recommended. The PBPK model did not predict a clinically significant effect of CYP3A4 inhibitors on maribavir exposure; however, it predicted that strong or moderate CYP3A4 inducers, including carbamazepine, efavirenz, phenobarbital, and phenytoin, may reduce maribavir exposure to a clinically significant extent, and may prompt the consideration of a maribavir dosing increase, in accordance with local approved labels and/or regulations. [ABSTRACT FROM AUTHOR]

Published

2024

8. Maribavir Pharmacokinetics and Safety in Participants With Moderate Hepatic Impairment: A Phase 1, Open-Label, Single-Dose, Parallel Group Study.

Author

Song, Ivy, Chen, Grace, Jingyang Wu, and Ilic, Katarina

Subjects

*LIVER physiology, *CONFIDENCE intervals, *TASTE disorders, *CYTOMEGALOVIRUS diseases, *ORAL drug administration, *BLOOD plasma, *ANTIVIRAL agents, *SEVERITY of illness index, *LIVER diseases, *RESEARCH funding, *DRUG side effects, *PATIENT safety, *METABOLITES, *DISEASE risk factors

Abstract

Maribavir, an orally bioavailable antiviral, has shown superior activity against posttransplant cytomegalovirus infection compared with conventional antivirals. It is primarily metabolized in the liver. This open-label, single-center study evaluated the effect of hepatic impairment on the pharmacokinetics of maribavir in nontransplant participants. A single 200-mg dose of maribavir was administered orally under fasting conditions to participants with moderate hepatic impairment (Child-Pugh class B) (n = 10) and healthy controls (n = 10) matched for age, weight, sex, and smoking status. Compared with participants with normal hepatic function, maximum plasma concentration (Cmax) and area under the plasma concentration-time curve (AUC) from time 0 to infinity values for maribavir in participants with moderate hepatic impairment were 1.346-fold (90%CI of geometric mean ratio, 1.091-1.660) and 1.261-fold (0.889-1.787) higher, respectively. However, Cmax and AUC values for unbound maribavir were comparable. For VP 44469, the main metabolite of maribavir, the Cmax and AUC from time 0 to infinity values were 1.190-fold (0.836-1.693) and 1.309-fold (1.007-1.702) higher, respectively, in participants with moderate hepatic impairment. In total, 7 mild treatment-emergent adverse events were reported, all in the moderate hepatic impairment group. Dysgeusia was the most frequently reported treatment-emergent adverse event, at a frequency of 50%. These results indicated that total maribavir concentrations were mildly increased in participants with moderate hepatic impairment, while unbound concentrations were unaffected. Similar maribavir pharmacokinetics in participants with moderate hepatic impairment and normal hepatic function suggest that dose adjustment may not be required for patients with moderate hepatic impairment. [ABSTRACT FROM AUTHOR]

Published

2023

9. Effects of enzyme inducers efavirenz and tipranavir/ritonavir on the pharmacokinetics of the HIV integrase inhibitor dolutegravir.

Author

Song, Ivy, Borland, Julie, Chen, Shuguang, Guta, Phyllis, Lou, Yu, Wilfret, David, Wajima, Toshihiro, Savina, Paul, Peppercorn, Amanda, Castellino, Stephen, Wagner, David, Hosking, Louise, Mosteller, Michael, Rubio, Justin, and Piscitelli, Stephen

Subjects

*ANTIVIRAL agents, *CLINICAL trials, *CONFIDENCE intervals, *DRUG interactions, *DRUG side effects, *HIV infections, *MATHEMATICAL statistics, *RESEARCH funding, *PARAMETERS (Statistics), *DATA analysis software, *TIPRANAVIR (Drug), *EFAVIRENZ, *RITONAVIR

Abstract

Purpose: Dolutegravir (DTG) is an unboosted, integrase inhibitor for the treatment of HIV infection. Two studies evaluated the effects of efavirenz (EFV) and tipranavir/ritonavir (TPV/r) on DTG pharmacokinetics (PK) in healthy subjects. Methods: The first study was an open-label crossover where 12 subjects received DTG 50 mg every 24 hours (q24h) for 5 days, followed by DTG 50 mg and EFV 600 mg q24h for 14 days. The second study was an open-label crossover where 18 subjects received DTG 50 mg q24h for 5 days followed by TPV/r 500/200 mg every 12 hours (q12h) for 7 days and then DTG 50 mg q24h and TPV/r 500/200 mg q12h for a further 5 days. Safety assessments and serial PK samples were collected. Non-compartmental PK analysis and geometric mean ratios and 90 % confidence intervals were generated. Results: The combination of DTG with EFV or TPV/r was generally well tolerated. Four subjects discontinued the TPV/r study due to increases in alanine aminotransferase that were considered related to TPV/r. Co-administration with EFV resulted in decreases of 57, 39 and 75 % in DTG AUC, C and C, respectively. Co-administration with TPV/r resulted in decreases of 59, 46 and 76 % in DTG AUC, C and C, respectively. Conclusions: Given the reductions in exposure and PK/pharmacodynamic relationships in phase II/III trials, DTG should be given at an increased dose of 50 mg twice daily when co-administered with EFV or TPV/r, and alternative regimens without inducers should be considered in integrase inhibitor-resistant patients. [ABSTRACT FROM AUTHOR]

Published

2014

10. ING116070: A Study of the Pharmacokinetics and Antiviral Activity of Dolutegravir in Cerebrospinal Fluid in HIV-1–Infected, Antiretroviral Therapy–Naive Subjects.

Author

Letendre, Scott L., Mills, Anthony M., Tashima, Karen T., Thomas, Deborah A., Min, Sherene S., Chen, Shuguang, Song, Ivy H., and Piscitelli, Stephen C.

Subjects

ANTIVIRAL agents, HIV infections, THERAPEUTICS, INTEGRASE inhibitors, CEREBROSPINAL fluid, ANTIRETROVIRAL agents, ABACAVIR-lamivudine (Drug), PHARMACOKINETICS

Abstract

Median dolutegravir concentrations in cerebrospinal fluid were similar to unbound concentrations in plasma and all subjects exceeded the in vitro 50% inhibitory concentration for wild-type viruses (0.2 ng/mL) by ≥66-fold, suggesting therapeutic concentrations are achieved in cerebrospinal fluid..Background. Dolutegravir (DTG), a once-daily, human immunodeficiency virus type 1 (HIV-1) integrase inhibitor, was evaluated for distribution and antiviral activity in cerebrospinal fluid (CSF).Methods. ING116070 is an ongoing, single-arm, open-label, multicenter study in antiretroviral therapy–naive, HIV-1–infected adults. Subjects received DTG (50 mg) plus abacavir/lamivudine (600/300 mg) once daily. The CSF and plasma (total and unbound) DTG concentrations were measured at weeks 2 and 16. The HIV-1 RNA levels were measured in CSF at baseline and weeks 2 and 16 and in plasma at baseline and weeks 2, 4, 8, 12, and 16.Results. Thirteen white men enrolled in the study; 2 withdrew prematurely, 1 because of a non–drug-related serious adverse event (pharyngitis) and 1 because of lack of treatment efficacy. The median DTG concentrations in CSF were 18 ng/mL (range, 4–23 ng/mL) at week 2 and 13 ng/mL (4–18 ng/mL) at week 16. Ratios of DTG CSF to total plasma concentration were similar to the unbound fraction of DTG in plasma. Median changes from baseline in CSF (n = 11) and plasma (n = 12) HIV-1 RNA were −3.42 and −3.04 log10 copies/mL, respectively. Nine of 11 subjects (82%) had plasma and CSF HIV-1 RNA levels <50 copies/mL and 10 of 11 (91%) had CSF HIV-1 RNA levels <2 copies/mL at week 16.Conclusions. The DTG concentrations in CSF were similar to unbound plasma concentrations and exceeded the in vitro 50% inhibitory concentration for wild-type HIV (0.2 ng/mL), suggesting that DTG achieves therapeutic concentrations in the central nervous system. The HIV-1 RNA reductions were similar in CSF and plasma.Clinical Trials Registration. NCT01499199. [ABSTRACT FROM AUTHOR]

Published

2014

11. The Effect of Lopinavir/Ritonavir and Darunavir/Ritonavir on the HIV Integrase Inhibitor S/GSK1349572 in Healthy Participants.

Author

Song, Ivy, Min, Sherene S., Borland, Julie, Yu Lou, Shuguang Chen, Patel, Parul, Ishibashi, Toru, and Piscitelli, Stephen C.

Subjects

*ANALYSIS of variance, *ANTIVIRAL agents, *COMBINATION drug therapy, *CLINICAL trials, *COMPUTER software, *CONFIDENCE intervals, *CROSSOVER trials, *HIGH performance liquid chromatography, *MASS spectrometry, *ORAL drug administration, *RESEARCH funding, *STATISTICAL sampling, *DATA analysis, *PROTEASE inhibitors, *DARUNAVIR, *LOPINAVIR-ritonavir, *HIV integrase inhibitors

Abstract

S/GSK1349572 is an unboosted, once-daily integrase inhibitor with a novel resistance profile. As standard of care for patients infected with HIV is combination therapy, the potential interaction between S/GSK1349572 and ritonavir-boosted protease inhibitors was evaluated. In an open-label, repeat-dose, 2-period, 2-sequence crossover study in healthy participants, S/GSK1349572 was administered at 30 mg once daily for 5 days, followed by randomization to lopinavir/ritonavir 400/100 mg twice daily or darunavir/ritonavir 600/100 mg twice daily coad-ministered with S/GSK1349572 30 mg once daily for 14 days. There was no washout between periods. Serial pharmacokinetic (PK) samples and safety assessments were obtained throughout the study. Thirty of 31 participants completed the study (15 participants per group). Treatment comparisons of steady-state S/GSK1349572 PK parameters demonstrated that coadministration of lopinavir/ritonavir had no significant effect on steady-state PK of S/GSK1349572. Coadministration of darunavir/ritonavir resulted in a nonclinically significant reduction in steady-state plasma S/GSK1349572 exposures. Plasma S/GSK1349572 AUC(0-τ ), Cmax, and Cτdecreased by 22%, 11%, and 38%, respectively, on average. S/GSK1349572 was well tolerated with no serious adverse events (AEs) or withdrawals due to drug-related AEs. The most frequent drug-related AEs were diarrhea, dizziness, and headache. No dosage adjustment for S/ GSK1349572 is required when used with lopinavir/ritonavir or darunavir/ritonavir. [ABSTRACT FROM PUBLISHER]

Published

2011

12. Summary of Maribavir (SHP620) Drug–Drug Interactions Based on Accumulated Clinical and Nonclinical Data.

Author

Song, Ivy, Sun, Kefeng, Ilic, Katarina, and Martin, Patrick

Subjects

*ANTIVIRAL agents, *GLUCURONOSYLTRANSFERASE, *CYTOCHROME P-450, *DRUG interactions, *CLINICAL trials

Abstract

Introduction Maribavir, a potent and orally bioavailable antiviral, is being evaluated in Phase 3 trials for the treatment of cytomegalovirus (CMV) infections in transplant patients. Often numerous concomitant medications are administered to these patients to manage their comorbidities. A thorough evaluation of maribavir potential for drug–drug interactions (DDIs) is warranted and required for the regulatory approval. Objectives To thoroughly evaluate potential DDIs for maribavir. Methods Extensive in vitro studies were conducted to evaluate the potential involvement of cytochrome P450s (CYPs), uridine diphosphate glucuronosyltransferases (UGTs) and transporters on the disposition of maribavir, as well as the inhibitory and induction effect of maribavir on these enzymes and transporters. Clinical Phase 1 studies included a human mass-balance study, two probe-cocktail studies, and five DDI studies with ketoconazole, rifampin, antacid, voriconazole, and tacrolimus. Results Maribavir is metabolized primarily in the liver through CYP3A4 (70–85%) and CYP1A2 (15–30%). Renal clearance is a minor route (<5%). Maribavir is a substrate of P-gp and UGTs, however, the contribution of glucuronidation to the overall clearance of maribavir is considered low. Maribavir is not a clinically significant inhibitor of CYPs, UGTs, and transporters, except for weak inhibition for CYP2C19, P-gp, and possibly UGT1A1. Maribavir is not a clinically significant inducer for CYP1A2, 2B6, and 3A4. Maribavir's exposure is increased 46% by ketoconazole and decreased 61% by rifampin and not affected by antacids. Maribavir increases tacrolimus exposure by 51% and does not affect voriconazole. Conclusions Maribavir has low risk for DDI. Inhibitors of CYP3A4 and/or P-gp may increase maribavir exposure, but dose adjustment of maribavir is not necessary. Potent inducers of CYP3A4 and P-gp decrease maribavir exposure, necessitating maribavir dose increase. Maribavir may increase exposure of immunosuppressants, such as tacrolimus. Therefore, monitoring of concomitant immunosuppressants' blood concentration should be considered at initiation, co-administration, and discontinuation of maribavir. Maribavir is not expected to interact with other concurrent medications. [ABSTRACT FROM AUTHOR]

Published

2019

13. Clinical Pharmacology of Maribavir (SHP620): A Comprehensive Overview.

Author

Song, Ivy, Ilic, Katarina, Sun, Kefeng, and Martin, Patrick

Subjects

*CYTOMEGALOVIRUS disease treatment, *ANTIVIRAL agents, *CLINICAL pharmacology, *PHARMACOKINETICS, *PHARMACODYNAMICS

Abstract

Introduction Maribavir, a potent and orally bioavailable antiviral, is being evaluated in Phase 3 trials for the treatment of CMV infections in transplant patients and received FDA Breakthrough Therapy designation. A thorough understanding of the clinical pharmacology of maribavir is necessary to guide the appropriate use of the drug in transplant patients who often have multiple comorbidities and require complex concurrent medication regimens. Objectives To summarize the clinical pharmacology data of maribavir. Methods Pharmacokinetic and pharmacodynamic assessments were performed in sixteen Phase 1 studies and three Phase 2 studies. Data were summarized to characterize maribavir's disposition (absorption, distribution, metabolism, and excretion) in healthy adult subjects and special populations (HIV-infected, hepatically impaired, renally impaired, and organ transplant recipients). A definitive QT study was conducted to evaluate the cardiac repolarization effect. The drug interaction risks were assessed using both nonclinical and clinical studies. Results Maribavir is primarily eliminated through the CYP3A4 pathway and has a half-life of 5–7 hours. Co-administration with food or antacid, or crushing the tablet, had no impact on maribavir's exposure. Maribavir binds to plasma proteins with unbound fraction estimated at 1.5% and can penetrate the blood–retinal barrier. No pharmacokinetic difference is found among healthy subjects, transplant patients, subjects with severe renal impairment, or moderate hepatic impairment. Maribavir's exposure is increased by 46% by ketoconazole and decreased by 61% by rifampin. Maribavir increases tacrolimus exposure by 51%, does not affect voriconazole exposure, and is not expected to affect exposures of most other concurrent medications. Maribavir has no effects on QT intervals. Conclusions Extensive clinical pharmacology data have been generated to support the clinical use and dose of maribavir for the treatment of CMV infections in transplant recipients. Maribavir can be taken with or without food. No maribavir dose adjustment is needed in patients with mild-to-moderate hepatic impairment or renal impairment or with concurrent medications, except for CYP3A4 inducers. [ABSTRACT FROM AUTHOR]

Published

2019