Your search keyword '"Chandorkar G"' showing total 12 results

1. Intrapulmonary penetration of ceftolozane/tazobactam and piperacillin/tazobactam in healthy adult subjects

Author

Chandorkar, G., primary, Huntington, J. A., additional, Gotfried, M. H., additional, Rodvold, K. A., additional, and Umeh, O., additional

Published

2012

2. 972 VX-950: the discovery of an inhibitor of the hepatitis C NS3·4A protease and a potential hepatitis C virus therapeutic

Author

PERNI, R, primary, CHANDORKAR, G, additional, CHATURVEDI, P, additional, COURTNEY, L, additional, DECKER, C, additional, GATES, C, additional, HARBESON, S, additional, KWONG, A, additional, LIN, C, additional, and LUONG, Y, additional

Published

2003

3. Pharmacokinetics of surotomycin from phase 1 single and multiple ascending dose studies in healthy volunteers.

Author

Chandorkar G, Zhan Q, Donovan J, Rege S, and Patino H

Subjects

Adolescent, Adult, Aged, Cohort Studies, Dose-Response Relationship, Drug, Double-Blind Method, Female, Follow-Up Studies, Healthy Volunteers, Humans, Lipopeptides blood, Male, Middle Aged, Peptides, Cyclic blood, Young Adult, Lipopeptides administration & dosage, Lipopeptides pharmacokinetics, Peptides, Cyclic administration & dosage, Peptides, Cyclic pharmacokinetics

Abstract

Background: Surotomycin, a novel, orally administered, cyclic, lipopeptide antibacterial in development for the treatment of Clostridium difficile-associated diarrhea, has demonstrated minimal intestinal absorption in animal models., Methods: Safety, tolerability, and plasma pharmacokinetics of single and multiple ascending oral doses (SAD/MAD) of surotomycin in healthy volunteers were characterized in two randomized, double-blind, placebo-controlled, phase 1 studies., Results: Participants were sequentially enrolled into one of four SAD (500, 1000, 2000, 4000 mg surotomycin) or three MAD (250, 500, 1000 mg surotomycin twice/day for 14 days) cohorts. Ten subjects were randomized 4:1 into each cohort to receive surotomycin or placebo. Surotomycin plasma concentrations rose as dose increased (maximum plasma concentration [C max ]: 10.5, 21.5, 66.6, and 86.7 ng/mL). Systemic levels were generally low, with peak median surotomycin plasma concentrations observed 6-12 h after the first dose. In the MAD study, surotomycin plasma concentrations were higher on day 14 (C max : 25.5, 37.6, and 93.5 ng/mL) than on day 1 (C max : 6.8, 11.0, and 21.1 ng/mL for increasing doses), indicating accumulation. In the SAD study, <0.01% of the administered dose was recovered in urine. Mean surotomycin stool concentration from the 1000 mg MAD cohort was 6394 μg/g on day 5. Both cohorts were well tolerated with all adverse events reported as mild to moderate., Conclusion: Both SAD and MAD studies of surotomycin demonstrated minimal systemic exposure, with feces the primary route of elimination following oral administration; consistent with observations with similar compounds, such as fidaxomicin. Results of these phase 1 studies support the continued clinical development of surotomycin for the treatment of Clostridium difficile-associated diarrhea., Trial Registration: NCT02835118 and NCT02835105 . Retrospectively registered, July 13 2016.

Published

2017

4. Population pharmacokinetics of ceftolozane/tazobactam in healthy volunteers, subjects with varying degrees of renal function and patients with bacterial infections.

Author

Chandorkar G, Xiao A, Mouksassi MS, Hershberger E, and Krishna G

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Anti-Bacterial Agents blood, Cephalosporins blood, Female, Healthy Volunteers, Humans, Male, Middle Aged, Penicillanic Acid blood, Penicillanic Acid pharmacokinetics, Tazobactam, Young Adult, Anti-Bacterial Agents pharmacokinetics, Bacterial Infections metabolism, Cephalosporins pharmacokinetics, Models, Biological, Penicillanic Acid analogs & derivatives, Renal Insufficiency metabolism

Abstract

Ceftolozane/tazobactam is a novel antipseudomonal cephalosporin and β-lactamase inhibitor in clinical development for treatment of complicated urinary tract (cUTI) and intra-abdominal (cIAI) infections and nosocomial pneumonia. The population pharmacokinetics of ceftolozane/tazobactam were characterized in healthy volunteers, subjects with varying degrees of renal function, and patients with cIAI or cUTI. Serum concentration data from 376 adults who received ceftolozane/tazobactam in doses ranging from 500 to 3000 mg were analyzed to identify factors contributing to the pharmacokinetic variability. Ceftolozane/tazobactam pharmacokinetics were well described by a linear two-compartment model with first-order elimination and moderate between-subject variability in both clearance and volume of distribution (Vc). For both ceftolozane and tazobactam, clearance was highly correlated with renal function with creatinine clearance influencing exposure, and infection influencing Vc. Body weight was an additional covariate affecting the Vc of ceftolozane. Other covariates tested, such as age, body weight, sex, ethnicity, and presence of infection, had no clinically relevant effects on exposure. The final pharmacokinetic models adequately described the plasma concentrations of ceftolozane and tazobactam and form the basis for further modeling and simulation including evaluation of probability of target attainment in a diverse population with varying demographics, degrees of renal function, and infection status., (© 2014 The Authors. The Journal of Clinical Pharmacology Published by Wiley Periodicals, Inc. on behalf of American College of Clinical Pharmacology.)

Published

2015

5. Impact of renal function on the pharmacokinetics and safety of ceftolozane-tazobactam.

Author

Wooley M, Miller B, Krishna G, Hershberger E, and Chandorkar G

Subjects

Adolescent, Adult, Aged, Cephalosporins adverse effects, Cephalosporins blood, Female, Humans, Kidney Failure, Chronic blood, Male, Middle Aged, Penicillanic Acid adverse effects, Penicillanic Acid blood, Penicillanic Acid pharmacokinetics, Penicillanic Acid therapeutic use, Prospective Studies, Tazobactam, Young Adult, Cephalosporins pharmacokinetics, Cephalosporins therapeutic use, Kidney Failure, Chronic drug therapy, Penicillanic Acid analogs & derivatives

Abstract

Ceftolozane-tazobactam is a novel antipseudomonal cephalosporin with a β-lactamase inhibitor. We investigated the pharmacokinetics (PK) and safety of ceftolozane-tazobactam in subjects with various degrees of renal function. In two phase I, open-label studies, a single dose of ceftolozane-tazobactam was administered as a 1-h intravenous infusion to 24 subjects with normal, mild, or moderate renal impairment (1,000/500 mg) and six subjects with severe renal impairment (500/250 mg). Six subjects with end-stage renal disease (ESRD) received two doses of ceftolozane-tazobactam (500/250 mg each), pre- and posthemodialysis (post-HD). PK parameters were determined by noncompartmental methods. Plasma exposure to ceftolozane-tazobactam increased as renal function declined with only slightly increased exposures in subjects with mild renal impairment; the median area under the concentration-time curve from time zero to infinity (AUC0-∞) for ceftolozane and tazobactam increased 1.4- and 1.2-fold, respectively. In subjects with moderate renal impairment, the AUC0-∞ increased 2.5- and 2.2-fold for ceftolozane and tazobactam, respectively. In subjects with severe renal impairment, the dose-normalized median AUC0-∞ for ceftolozane and tazobactam increased 4.4- and 3.8-fold, respectively. In ESRD subjects, ceftolozane and tazobactam concentrations declined rapidly following the start of HD, with approximately 66 and 56% reductions in overall exposure based on the AUC0-∞ before and after dialysis. Slight increases in exposure with mild renal impairment do not warrant a dose adjustment; however, subjects with moderate or severe renal impairment and those on HD require a decrease in the dose, a change in the frequency of administration, or both to achieve exposures within the established safety and efficacy margins of ceftolozane-tazobactam. Ceftolozane-tazobactam was well tolerated by all renal impairment groups.

Published

2014

6. The effect of CYP3A inhibitors and inducers on the pharmacokinetics of telaprevir in healthy volunteers.

Author

Garg V, Chandorkar G, Yang Y, Adda N, McNair L, Alves K, Smith F, and van Heeswijk RP

Subjects

Adult, Alkynes, Area Under Curve, Clinical Trials as Topic, Cyclopropanes, Drug Combinations, Drug Interactions, Female, Humans, Male, Middle Aged, Benzoxazines pharmacology, Cytochrome P-450 CYP3A metabolism, Cytochrome P-450 CYP3A Inhibitors, Enzyme Inhibitors pharmacology, Ketoconazole pharmacology, Oligopeptides pharmacokinetics, Rifampin pharmacology

Abstract

Aim: To evaluate the effects of ketoconazole, rifampicin and efavirenz on the pharmacokinetics of telaprevir in healthy volunteers., Method: Results from three clinical studies are described. (1) Volunteers received a single 750 mg dose telaprevir with and without a single 400 mg dose ketoconazole. (2) Volunteers received (a) 1250 mg telaprevir followed by three 750 mg doses given every 8 h and (b) four 1250 mg telaprevir doses given every 8 h, with a single 400 mg dose ketoconazole given with the fourth dose of telaprevir. (3) Volunteers received either a single 750 mg dose telaprevir with or without 600 mg once daily rifampicin, or 750 mg every 8 h telaprevir with and without 600 mg once daily efavirenz., Results: A single 400 mg dose of ketoconazole increased single dose telaprevir exposure: the geometric least-squares mean ratio (GLSMR, with 90% confidence limits) was 1.24 (1.10, 1.41) for C(max) and 1.62 (1.45, 1.81) for AUC(0,∞). However, after multiple doses of telaprevir, there was no discernible effect of ketoconazole on telaprevir exposure. Co-administration of rifampicin at steady-state markedly reduced single dose telaprevir exposure with GLSMRs of 0.14 (0.11, 0.18) for C(max) and 0.08 (0.07, 0.11) for AUC(0,∞), whereas efavirenz had a smaller effect on telaprevir exposure when both drugs were co-administered at steady-state, with GLSMRs of 0.91 (0.81, 1.02) for C(max) , 0.53 (0.44, 0.65) for C(min), and 0.74 (0.65, 0.84) for AUC(0,8 h)., Conclusion: CYP3A inducers, rifampicin and efavirenz, can reduce telaprevir exposure to varying degrees based on their potency. The effect of ketoconazole as an inhibitor of telaprevir metabolism is more pronounced after a single dose of telaprevir than after repeated administration., (© 2012 Vertex Pharmaceuticals Incorporated. British Journal of Clinical Pharmacology © 2012 The British Pharmacological Society.)

Published

2013

7. Effect of telaprevir on the pharmacokinetics of midazolam and digoxin.

Author

Garg V, Chandorkar G, Farmer HF, Smith F, Alves K, and van Heeswijk RP

Subjects

ATP Binding Cassette Transporter, Subfamily B, Member 1 antagonists & inhibitors, ATP Binding Cassette Transporter, Subfamily B, Member 1 metabolism, Adolescent, Adult, Antiviral Agents blood, Antiviral Agents pharmacokinetics, Area Under Curve, Cytochrome P-450 CYP3A metabolism, Digoxin administration & dosage, Digoxin blood, Digoxin urine, Drug Interactions, Female, Humans, Male, Midazolam administration & dosage, Midazolam analogs & derivatives, Midazolam blood, Middle Aged, Oligopeptides blood, Oligopeptides pharmacokinetics, Protease Inhibitors blood, Protease Inhibitors pharmacokinetics, Young Adult, Antiviral Agents administration & dosage, Cytochrome P-450 CYP3A Inhibitors, Digoxin pharmacokinetics, Midazolam pharmacokinetics, Oligopeptides administration & dosage, Protease Inhibitors administration & dosage

Abstract

In this open-label study, 24 healthy volunteers received a single intravenous (IV) dose of 0.5 mg of midazolam on day 1 and a single oral dose each of 2 mg of midazolam and 0.5 mg of digoxin on day 3. Telaprevir 750 mg every 8 hours was administered from day 8 through day 23, along with a single IV dose of 0.5 mg of midazolam on day 17 and single oral doses of 2 mg of midazolam and 0.5 mg of digoxin on day 19. Midazolam, 1'-hydroxymidazolam, digoxin, and telaprevir concentrations in plasma and digoxin concentrations in urine were measured and pharmacokinetic parameters calculated. On comparing administration with versus without telaprevir, the geometric least squares mean ratios (with 90% confidence limits) for IV midazolam were 1.02 (0.80, 1.31) for maximum observed concentrations (C(max)) and 3.40 (3.04, 3.79) for area under the curve from 0 to 24 hours (AUC(0-24h)); for oral midazolam 2.86 (2.52, 3.25) for C(max) and 8.96 (7.75, 10.35) for AUC(0-24h); and for oral digoxin 1.50 (1.36, 1.65) for C(max) and 1.85 (1.70, 2.00) for area under the curve from 0 to infinity (AUC(0-∞)). Coadministration of telaprevir with oral midazolam resulted in approximately 3-fold decrease in the mean AUC(0-∞) of 1'-hydroxymidazolam. The renal clearance of digoxin was similar with or without telaprevir. Results show that telaprevir is an inhibitor of CYP3A and P-glycoprotein.

Published

2012

8. Single-dose pharmacokinetics and tolerability of daptomycin 8 to 10 mg/kg in children aged 2 to 6 years with suspected or proved Gram-positive infections.

Author

Abdel-Rahman SM, Chandorkar G, Akins RL, Bradley JS, Jacobs RF, Donovan J, and Benziger DP

Subjects

Anti-Bacterial Agents administration & dosage, Area Under Curve, Biological Availability, Child, Child, Preschool, Daptomycin administration & dosage, Female, Half-Life, Humans, Injections, Intravenous, Male, Metabolic Clearance Rate, Plasma chemistry, Anti-Bacterial Agents adverse effects, Anti-Bacterial Agents pharmacokinetics, Daptomycin adverse effects, Daptomycin pharmacokinetics, Gram-Positive Bacterial Infections drug therapy

Abstract

A pharmacokinetic analysis was performed for single intravenous doses of daptomycin 8 or 10 mg/kg in subjects aged 2 to 6 years. Proportional increases in maximum plasma concentration (68.4 μg/mL, 79.2 μg/mL) and area under the curve (429.1 μg · h/mL, 549.7 μg · h/mL) were observed for each dose cohort, respectively. Half-life, clearance, and distribution volume were similar between groups. Both doses were well tolerated.

Published

2011

9. Merimepodib, pegylated interferon, and ribavirin in genotype 1 chronic hepatitis C pegylated interferon and ribavirin nonresponders.

Author

Rustgi VK, Lee WM, Lawitz E, Gordon SC, Afdhal N, Poordad F, Bonkovsky HL, Bengtsson L, Chandorkar G, Harding M, McNair L, Aalyson M, Alam J, Kauffman R, Gharakhanian S, and McHutchison JG

Subjects

Adolescent, Adult, Aged, Carbamates adverse effects, Carbamates pharmacokinetics, Double-Blind Method, Drug Therapy, Combination, Female, Humans, Interferon alpha-2, Male, Middle Aged, Phenylurea Compounds adverse effects, Phenylurea Compounds pharmacokinetics, Recombinant Proteins, Antiviral Agents administration & dosage, Carbamates administration & dosage, Hepatitis C, Chronic drug therapy, Interferon-alpha administration & dosage, Phenylurea Compounds administration & dosage, Polyethylene Glycols administration & dosage, Ribavirin administration & dosage

Abstract

Unlabelled: Merimepodib (MMPD) is an orally administered, inosine monophosphate dehydrogenase inhibitor that has shown antiviral activity in nonresponders with chronic hepatitis C (CHC) when combined with pegylated interferon alfa 2a (Peg-IFN-alfa-2a) and ribavirin (RBV). We conducted a randomized, double-blind, multicenter, phase 2b study to evaluate the antiviral activity, safety, and tolerability of MMPD in combination with Peg-IFN-alfa-2a and RBV in patients with genotype 1 CHC who were nonresponders to prior therapy with Peg-IFN and RBV. Patients received 50 mg MMPD, 100 mg MMPD, or placebo every 12 hours, in addition to Peg-IFN-alfa-2a and RBV, for 24 weeks. Patients with a 2-log or more decrease from baseline or undetectable hepatitis C virus (HCV) RNA levels at week 24 were then eligible to continue Peg-IFN-alfa-2a and RBV for a further 24 weeks, followed by 24 weeks of follow-up. The primary efficacy endpoint was sustained virological response (SVR) rate at week 72 in all randomized patients who received at least one dose of study drug and had a history of nonresponse to standard therapy. A total of 354 patients were randomized to treatment (117 to placebo; 119 to 50 mg MMPD; 118 to 100 mg MMPD), and 286 completed the core study. The proportion of patients who achieved SVR was similar among the treatment groups: 6% (6/107) for 50 mg MMPD, 4% (5/112) for 100 mg MMPD, and 5% (5/104) for placebo (P = 0.8431). Adverse-event profiles for the MMPD combination groups were similar to that for Peg-IFN-alfa and RBV alone. Nausea, arthralgia, cough, dyspnea, neutropenia, and anemia were more common in patients taking MMPD., Conclusion: The addition of MMPD to Peg-IFN-alfa-2a and RBV combination therapy did not increase the proportion of nonresponder patients with genotype 1 CHC achieving an SVR.

Published

2009

10. Inhibitors of hepatitis C virus NS3.4A protease. Effect of P4 capping groups on inhibitory potency and pharmacokinetics.

Author

Perni RB, Chandorkar G, Cottrell KM, Gates CA, Lin C, Lin K, Luong YP, Maxwell JP, Murcko MA, Pitlik J, Rao G, Schairer WC, Van Drie J, and Wei Y

Subjects

Animals, Antiviral Agents chemical synthesis, Binding Sites, Cell Line, Crystallography, X-Ray, Drug Design, Hepacivirus enzymology, Hydrogen Bonding, Mice, Microbial Sensitivity Tests, Oligopeptides antagonists & inhibitors, Protease Inhibitors chemical synthesis, Structure-Activity Relationship, Virus Replication physiology, Antiviral Agents pharmacokinetics, Hepacivirus drug effects, Protease Inhibitors pharmacokinetics, Viral Nonstructural Proteins antagonists & inhibitors, Virus Replication drug effects

Abstract

Reversible tetrapeptide-based compounds have been shown to effectively inhibit the hepatitis C virus NS3.4A protease. Inhibition of viral replicon RNA production in Huh-7 cells has also been demonstrated. We show herein that the inclusion of hydrogen bond donors on the P4 capping group of tetrapeptide-based inhibitors result in increased binding potency to the NS3.4A protease. The capping groups also impart significant effects on the pharmacokinetic profile of these inhibitors.

Published

2007

11. Preclinical profile of VX-950, a potent, selective, and orally bioavailable inhibitor of hepatitis C virus NS3-4A serine protease.

Author

Perni RB, Almquist SJ, Byrn RA, Chandorkar G, Chaturvedi PR, Courtney LF, Decker CJ, Dinehart K, Gates CA, Harbeson SL, Heiser A, Kalkeri G, Kolaczkowski E, Lin K, Luong YP, Rao BG, Taylor WP, Thomson JA, Tung RD, Wei Y, Kwong AD, and Lin C

Subjects

Administration, Oral, Animals, Area Under Curve, Binding Sites, Biological Availability, Cell Line, Cells, Cultured, Dogs, Dose-Response Relationship, Drug, Drug Evaluation, Preclinical, Half-Life, Hepacivirus drug effects, Hepatocytes drug effects, Humans, Inhibitory Concentration 50, Male, Mice, Mice, SCID, Oligopeptides administration & dosage, RNA, Viral physiology, Rats, Rats, Inbred F344, Rats, Sprague-Dawley, Replicon physiology, Serine Proteinase Inhibitors administration & dosage, Substrate Specificity, Hepacivirus enzymology, Oligopeptides pharmacokinetics, Oligopeptides pharmacology, Serine Proteinase Inhibitors pharmacokinetics, Serine Proteinase Inhibitors pharmacology

Abstract

VX-950 is a potent, selective, peptidomimetic inhibitor of the hepatitis C virus (HCV) NS3-4A serine protease, and it demonstrated excellent antiviral activity both in genotype 1b HCV replicon cells (50% inhibitory concentration [IC50] = 354 nM) and in human fetal hepatocytes infected with genotype 1a HCV-positive patient sera (IC50 = 280 nM). VX-950 forms a covalent but reversible complex with the genotype 1a HCV NS3-4A protease in a slow-on, slow-off process with a steady-state inhibition constant (K(i)*) of 7 nM. Dissociation of the covalent enzyme-inhibitor complex of VX-950 and genotype 1a HCV protease has a half-life of almost an hour. A >4-log10 reduction in the HCV RNA levels was observed after a 2-week incubation of replicon cells with VX-950, with no rebound of viral RNA observed after withdrawal of the inhibitor. In several animal species, VX-950 exhibits a favorable pharmacokinetic profile with high exposure in the liver. In a recently developed HCV protease mouse model, VX-950 showed excellent inhibition of HCV NS3-4A protease activity in the liver. Therefore, the overall preclinical profile of VX-950 supports its candidacy as a novel oral therapy against hepatitis C.

Published

2006

12. Functional expression of P-glycoprotein in primary cultures of human cytotrophoblasts and BeWo cells.

Author

Utoguchi N, Chandorkar GA, Avery M, and Audus KL

Subjects

ATP Binding Cassette Transporter, Subfamily B, Member 1 antagonists & inhibitors, ATP Binding Cassette Transporter, Subfamily B, Member 1 genetics, ATP-Binding Cassette Transporters antagonists & inhibitors, ATP-Binding Cassette Transporters metabolism, Adult, Blotting, Western, Culture Media, Conditioned chemistry, Cyclosporine pharmacology, Dipyridamole pharmacology, Drug Resistance, Multiple, Female, Fluoresceins metabolism, Fluorescent Dyes metabolism, Humans, Multidrug Resistance-Associated Proteins, Pregnancy, Quinidine pharmacology, Trophoblasts drug effects, Tumor Cells, Cultured, Verapamil antagonists & inhibitors, Vinblastine pharmacology, ATP Binding Cassette Transporter, Subfamily B, Member 1 metabolism, Choriocarcinoma metabolism, Trophoblasts metabolism

Abstract

The objective of this study was to investigate the functional expression of the efflux transporter, P-glycoprotein (P-gp), in primary cultures of human cytotrophoblasts and BeWo cell monolayers. Uptake studies with primary cultures of human cytotrophoblasts or BeWo cells were conducted with calcein-AM and vinblastine (P-gp markers) or fluorescein (MRP marker) in the presence of specific P-gp or MRP inhibitors. Results showed that the accumulation of P-gp substrates calcein-AM and vinblastine by BeWo cells or primary cultures of human cytotrophoblasts was significantly enhanced in the presence of a typical P-gp inhibitor, cyclosporin-A, or other inhibitors such as quinidine, verapamil, and dipyridamole. MRP inhibitors had no effect on the accumulation of calcein or fluorescein by BeWo cells. Western blots confirmed the presence of multidrug resistant gene product 1 (MDR1) in both primary cultures of human cytotrophoblasts and BeWo cells. This study demonstrates functional P-gp in term human trophoblasts and further supports the use of primary cultures of human cytotrophoblasts and BeWo cells as in vitro models of the trophoblast to investigate mechanisms regulating drug distribution across the placenta.

Published

2000