Your search keyword '"Rao N.V.S. Mamidi"' showing total 23 results

1. Niraparib Shows Superior Tissue Distribution and Efficacy in a Prostate Cancer Bone Metastasis Model Compared with Other PARP Inhibitors

Author

Linda A. Snyder, Rajendra Damle, Shefali Patel, Jared Bohrer, Anna Fiorella, Jenny Driscoll, Rebecca Hawkins, Christopher F. Stratton, Carol D. Manning, Kanaka Tatikola, Volha Tryputsen, Kathryn Packman, and Rao N.V.S. Mamidi

Subjects

Male, Cancer Research, Indazoles, Prostate, Prostatic Neoplasms, Bone Neoplasms, Poly(ADP-ribose) Polymerase Inhibitors, Mice, Piperidines, Oncology, Animals, Humans, Tissue Distribution, Poly(ADP-ribose) Polymerases

Abstract

Patients with prostate cancer whose tumors bear deleterious mutations in DNA-repair pathways often respond to PARP inhibitors. Studies were conducted to compare the activity of several PARP inhibitors in vitro and their tissue exposure and in vivo efficacy in mice bearing PC-3M-luc-C6 prostate tumors grown subcutaneously or in bone. Niraparib, olaparib, rucaparib, and talazoparib were compared in proliferation assays, using several prostate tumor cell lines and in a cell-free PARP-trapping assay. PC-3M-luc-C6 cells were approximately 12- to 20-fold more sensitive to PARP inhibition than other prostate tumor lines, suggesting that these cells bear a DNA damage repair defect. The tissue exposure and efficacy of these PARP inhibitors were evaluated in vivo in PC-3M-luc-C6 subcutaneous and bone metastasis tumor models. A steady-state pharmacokinetic study in PC-3M-luc-C6 tumor-bearing mice showed that all of the PARP inhibitors had favorable subcutaneous tumor exposure, but niraparib was differentiated by superior bone marrow exposure compared with the other drugs. In a PC-3M-luc-C6 subcutaneous tumor efficacy study, niraparib, olaparib, and talazoparib inhibited tumor growth and increased survival to a similar degree. In contrast, in the PC-3M-luc-C6 bone metastasis model, niraparib showed the most potent inhibition of bone tumor growth compared with the other therapies (67% vs. 40%–45% on day 17), and the best survival improvement over vehicle control [hazard ratio (HR), 0.28 vs. HR, 0.46–0.59] and over other therapies (HR, 1.68–2.16). These results show that niraparib has superior bone marrow exposure and greater inhibition of tumor growth in bone, compared with olaparib, rucaparib, and talazoparib.

Published

2022

2. Supplementary Figure from Niraparib Shows Superior Tissue Distribution and Efficacy in a Prostate Cancer Bone Metastasis Model Compared with Other PARP Inhibitors

Author

Rao N.V.S. Mamidi, Kathryn Packman, Volha Tryputsen, Kanaka Tatikola, Carol D. Manning, Christopher F. Stratton, Rebecca Hawkins, Jenny Driscoll, Anna Fiorella, Jared Bohrer, Shefali Patel, Rajendra Damle, and Linda A. Snyder

Abstract

Supplementary Figure from Niraparib Shows Superior Tissue Distribution and Efficacy in a Prostate Cancer Bone Metastasis Model Compared with Other PARP Inhibitors

Published

2023

3. Prediction of the drug–drug interaction potential of the α1‐acid glycoprotein bound, CYP3A4/CYP2C9 metabolized oncology drug, erdafitinib

Author

Frank Jacobs, Loeckie de Zwart, I. Goris, Mario Monshouwer, Rao N.V.S. Mamidi, Lilian Y. Li, Italo Poggesi, Jan Snoeys, Peter Verboven, Ellen Scheers, and Inneke Wynant

Subjects

Physiologically based pharmacokinetic modelling, Genotype, CYP3A, Antineoplastic Agents, RM1-950, Pharmacology, Models, Biological, Article, Pharmacokinetics, Quinoxalines, Cytochrome P-450 CYP3A, Cytochrome P-450 Enzyme Inhibitors, Humans, Drug Interactions, Pharmacology (medical), Growth factor receptor inhibitor, CYP2C9, Cytochrome P-450 CYP2C9, Cytochrome P-450 Enzyme Inducers, CYP3A4, biology, Chemistry, Research, Cytochrome P450, Transporter, Articles, Orosomucoid, Modeling and Simulation, biology.protein, Pyrazoles, Therapeutics. Pharmacology

Abstract

Erdafitinib is a potent oral pan‐fibroblast growth factor receptor inhibitor being developed as oncology drug for patients with alterations in the fibroblast growth factor receptor pathway. Erdafitinib binds preferentially to α1‐acid glycoprotein (AGP) and is primarily metabolized by cytochrome P450 (CYP) 2C9 and 3A4. This article describes a physiologically based pharmacokinetic (PBPK) model for erdafitinib to assess the drug–drug interaction (DDI) potential of CYP3A4 and CYP2C9 inhibitors and CYP3A4/CYP2C9 inducers on erdafitinib pharmacokinetics (PK) in patients with cancer exhibiting higher AGP levels and in populations with different CYP2C9 genotypes. Erdafitinib's DDI potential as a perpetrator for transporter inhibition and for time‐dependent inhibition and/or induction of CYP3A was also evaluated. The PBPK model incorporated input parameters from various in vitro and clinical PK studies, and the model was verified using a clinical DDI study with itraconazole and fluconazole. Erdafitinib clearance in the PBPK model consisted of multiple pathways (CYP2C9/3A4, renal, intestinal; additional hepatic clearance), making the compound less susceptible to DDIs. In poor‐metabolizing CYP2C9 populations carrying the CYP2C9*3/*3 genotype, simulations shown clinically relevant increase in erdafitinib plasma concentrations. Simulated luminal and enterocyte concentration showed potential risk of P‐glycoprotein inhibition with erdafitinib in the first 5 h after dosing, and simulations showed this interaction can be avoided by staggering erdafitinib and digoxin dosing. Other than a simulated ~ 60% exposure reduction with strong CYP3A/2C inducers such as rifampicin, other DDI liabilities were minimal and considered not clinically relevant.

Published

2021

4. Metabolism and disposition in rats, dogs, and humans of erdafitinib, an orally administered potent pan-fibroblast growth factor receptor (FGFR) tyrosine kinase inhibitor

Author

Italo Poggesi, Hilde Bohets, Chi Keung, Inneke Wynant, Filip Cuyckens, Rao N.V.S. Mamidi, Ellen Scheers, Laurent Leclercq, and Carine Borgmans

Subjects

Male, medicine.drug_class, Health, Toxicology and Mutagenesis, Administration, Oral, Pharmacology, Toxicology, 030226 pharmacology & pharmacy, Biochemistry, Tyrosine-kinase inhibitor, Rats, Sprague-Dawley, Excretion, Feces, 03 medical and health sciences, Dogs, Glucuronides, 0302 clinical medicine, Species Specificity, Pharmacokinetics, Biotransformation, Erdafitinib, Quinoxalines, medicine, Animals, Bile, Humans, Protein Kinase Inhibitors, Chemistry, General Medicine, Disposition, Metabolism, Receptors, Fibroblast Growth Factor, Rats, Fibroblast growth factor receptor, Area Under Curve, 030220 oncology & carcinogenesis, Pyrazoles

Abstract

This article describes in vivo biotransformation and disposition of erdafitinib following single oral dose of 3H-erdafitinib and 14C-erdafitinib to intact and bile duct-cannulated (BC) rats (4 mg/k...

Published

2020

5. Sample Preparation for LC‐MS Bioanalysis of Liposomal Samples

Author

Rao N.V.S. Mamidi, Wenying Jian, and Naidong Weng

Subjects

Bioanalysis, Liposome, Chromatography, Chemistry, Liquid chromatography–mass spectrometry, Ultrafiltration, Sample preparation, Free drug, Solid phase extraction

Published

2019

6. Niraparib with androgen receptor-axis-targeted therapy in patients with metastatic castration-resistant prostate cancer: safety and pharmacokinetic results from a phase 1b study (BEDIVERE)

Author

Byron M. Espina, Julie N. Graff, Alex Yu, Peter St. John Francis, Jean Baptiste Lattouf, Fred Saad, Rao N.V.S. Mamidi, Eugene Zhu, Neal D. Shore, Vinny Hayreh, Anasuya Hazra, Branislav Bradic, Marc De Meulder, Arash Rezazadeh Kalebasty, Edwin M. Posadas, and Kim N. Chi

Subjects

Oncology, Male, Cancer Research, medicine.medical_specialty, Indazoles, medicine.medical_treatment, Phases of clinical research, Niraparib, Poly(ADP-ribose) Polymerase Inhibitors, Toxicology, MCRPC, Targeted therapy, 03 medical and health sciences, chemistry.chemical_compound, Prostate cancer, 0302 clinical medicine, Piperidines, Prednisone, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, medicine, Humans, Pharmacology (medical), Pharmacokinetics, 030212 general & internal medicine, Adverse effect, PARP inhibitors, Aged, Pharmacology, Aged, 80 and over, Androgen-signaling-targeted therapy, business.industry, Apalutamide, Abiraterone acetate, Middle Aged, medicine.disease, Discontinuation, Prostatic Neoplasms, Castration-Resistant, chemistry, Thiohydantoins, Receptors, Androgen, DRD genes, 030220 oncology & carcinogenesis, Androstenes, Original Article, business, medicine.drug

Abstract

Purpose To assess the safety and pharmacokinetics and determine the recommended phase 2 dose (RP2D) of niraparib with apalutamide or abiraterone acetate plus prednisone (AAP) in patients with metastatic castration-resistant prostate cancer (mCRPC). Methods BEDIVERE was a multicenter, open-label, phase 1b study of niraparib 200 or 300 mg/day with apalutamide 240 mg or AAP (abiraterone acetate 1000 mg; prednisone 10 mg). Patients with mCRPC were previously treated with ≥ 2 lines of systemic therapy, including ≥ 1 androgen receptor-axis-targeted therapy for prostate cancer. Results Thirty-three patients were enrolled (niraparib-apalutamide, 6; niraparib-AAP, 27). No dose-limiting toxicities (DLTs) were reported when combinations included niraparib 200 mg; five patients receiving niraparib 300 mg experienced DLTs [niraparib-apalutamide, 2/3 patients (66.7%); niraparib-AAP, 3/8 patients (37.5%)]. Although data are limited, niraparib exposures were lower when given with apalutamide compared with historical niraparib monotherapy exposures in patients with solid tumors. Because of the higher incidence of DLTs, the niraparib–apalutamide combination and niraparib 300 mg combination with AAP were not further evaluated. Niraparib 200 mg was selected as the RP2D with AAP. Of 19 patients receiving niraparib 200 mg with AAP, 12 (63.2%) had grade 3/4 treatment-emergent adverse events, the most common being thrombocytopenia (26.3%) and hypertension (21.1%). Five patients (26.3%) had adverse events leading to treatment discontinuation. Conclusions These results support the choice of niraparib 200 mg as the RP2D with AAP. The niraparib–AAP combination was tolerable in patients with mCRPC, with no new safety signals. An ongoing phase 3 study is further assessing this combination in patients with mCRPC. Trial registration no. NCT02924766 (ClinicalTrials.gov).

Published

2020

7. Rosuvastatin Myotoxicity After Starting Canagliflozin Treatment

Author

Norman Rosenthal, Don Sun, Yshai Yavin, Damayanthi Devineni, and Rao N.V.S. Mamidi

Subjects

Canagliflozin, business.industry, MEDLINE, General Medicine, Myotoxicity, Pharmacology, Internal Medicine, Humans, Medicine, Rosuvastatin, Hydroxymethylglutaryl-CoA Reductase Inhibitors, Rosuvastatin Calcium, business, medicine.drug

Published

2021

8. Renal tubular and adrenal medullary tumors in the 2-year rat study with canagliflozin confirmed to be secondary to carbohydrate (glucose) malabsorption in the 15-month mechanistic rat study

Author

Godelieve Lammens, Bianca Feyen, Petra Vinken, Jim Proctor, Mark D. Johnson, Rao N.V.S. Mamidi, and Sandra De Jonghe

Subjects

Male, 0301 basic medicine, medicine.medical_specialty, Malabsorption, Adrenal Gland Neoplasms, Toxicology, Rats, Sprague-Dawley, 03 medical and health sciences, 0302 clinical medicine, Dietary Sucrose, Internal medicine, medicine, Animals, Hypoglycemic Agents, Canagliflozin, Kidney, Leydig cell, business.industry, General Medicine, Hyperplasia, medicine.disease, Kidney Neoplasms, Rats, Glucose, Kidney Tubules, 030104 developmental biology, medicine.anatomical_structure, Endocrinology, Glucose-galactose malabsorption, 030220 oncology & carcinogenesis, SGLT2 Inhibitor, business, Adrenal medulla, medicine.drug

Abstract

During preclinical development of canagliflozin, an SGLT2 inhibitor, treatment-related pheochromocytomas, renal tubular tumors (RTT), and testicular Leydig cell tumors were reported in the 2-year rat toxicology study. In a previous 6-month rat mechanistic study, feeding a glucose free diet prevented canagliflozin effects on carbohydrate malabsorption as well as the increase in cell proliferation in adrenal medulla and kidneys, implicating carbohydrate malabsorption as the mechanism for tumor formation. In this chronic study male Sprague-Dawley rats were dosed orally with canagliflozin at high dose-levels (65 or 100 mg/kg/day) for 15 months and received either a standard diet or a glucose-free diet. Canagliflozin-dosed rats on standard diet showed presence of basophilic renal tubular tumors (6/90) and an increased incidence of adrenal medullary hyperplasia (35/90), which was fully prevented by feeding a glucose-free diet (no RTT's; adrenal medullary hyperplasia in ≤5/90). These data further confirm that kidney and adrenal medullary tumors in the 2-year rat study were secondary to carbohydrate (glucose) malabsorption and were not due to a direct effect of canagliflozin on these target tissues.

Published

2017

9. Abstract 4128: Niraparib shows superior tissue distribution and efficacy in a prostate bone metastasis model compared with other PARP inhibitors

Author

Shefali Patel, Linda A. Snyder, Jenny Driscoll, Carol Manning, Volha Tryputsen, Rajendra N. Damle, Kanaka Tatikola, Rao N.V.S. Mamidi, Jared Bohrer, Kathryn Packman, Rebecca Hawkins, and Christopher F. Stratton

Subjects

Cancer Research, business.industry, Cancer, Bone metastasis, medicine.disease, In vitro, Olaparib, chemistry.chemical_compound, Prostate cancer, medicine.anatomical_structure, Breast cancer, Oncology, chemistry, Prostate, medicine, Cancer research, Bone marrow, business

Abstract

Patients whose prostate tumors bear deleterious mutations in genes that cause DNA repair defects (DRD), such as breast cancer (BRCA)2, respond to inhibitors of poly (ADP-ribose) [PAR] polymerase (PARP)-1 and PARP-2. Several PARP inhibitors, including niraparib, are in clinical development for the treatment of late stage prostate cancer. Prostate cancer typically metastasizes to bone marrow, and it is possible that efficacy of PARP inhibitors could differ based on their ability to penetrate and inhibit tumor growth in bone. Nonclinical studies were conducted to evaluate activity of PARP inhibitors in vitro, and to compare tissue exposure and efficacy in mice bearing PC-3-luc-C6 prostate tumors grown either subcutaneously (SC) or in bone. PC-3-luc-C6 cells do not have identifiable mutations in DRD genes, but they were >10-fold more sensitive in vitro to PARP inhibition than other prostate tumor lines. Treatment with niraparib induced a pattern of γ-H2AX and RAD51 staining that indicated the cells are deficient in DNA repair. Niraparib and olaparib exhibited similar potency in a biochemical PARP trapping assay, but in vitro cellular cytotoxicity studies of PC-3-luc-C6 cells demonstrated that niraparib was ~8-fold more potent than olaparib. A steady state PK study in mice bearing PC-3-luc-C6 SC prostate tumors demonstrated distinct patterns of tissue exposure of PARP inhibitors. For example, niraparib was detected for 12 or 24 hours in all tissues tested, including in plasma, tumor, and bone marrow. In contrast, olaparib was detected for up to 12-24 hours in plasma and tumor, but only transient exposure was observed in bone marrow. Mean AUC24 ratio estimates showed that niraparib had several-fold higher distribution to tumor and bone marrow as compared with olaparib. Efficacy studies were performed in the PC-3-luc-C6 tumor model, implanted either SC or by intracardiac injection to seed bone metastases. In the soft tissue SC tumor model, efficacy of the PARP inhibitors was similar, increasing lifespan by up to ~30%. However, the PARP inhibitors were differentiated by efficacy in the bone metastasis model. Niraparib significantly inhibited bone tumor growth and prolonged survival by ~30% over control mice, while olaparib did not prolong survival. This result is consistent with the hypothesis that niraparib's superior bone marrow exposure results in greater inhibition of tumor growth in bone. It further suggests that prostate cancer patients may derive greater benefit from PARP inhibitors that can penetrate the bone marrow. Citation Format: Linda A. Snyder, Rajendra N. Damle, Shefali Patel, Jared Bohrer, Jenny Driscoll, Rebecca Hawkins, Christopher F. Stratton, Carol Manning, Kanaka Tatikola, Volha Tryputsen, Kathryn Packman, Rao Mamidi. Niraparib shows superior tissue distribution and efficacy in a prostate bone metastasis model compared with other PARP inhibitors [abstract]. In: Proceedings of the Annual Meeting of the American Association for Cancer Research 2020; 2020 Apr 27-28 and Jun 22-24. Philadelphia (PA): AACR; Cancer Res 2020;80(16 Suppl):Abstract nr 4128.

Published

2020

10. In vitro metabolism of canagliflozin in human liver, kidney, intestine microsomes, and recombinant uridine diphosphate glucuronosyltransferases (UGT) and the effect of genetic variability of UGT enzymes on the pharmacokinetics of canagliflozin in humans

Author

Bhavna Solanki, Ellen Scheers, Andrew Jadwin, Rao N.V.S. Mamidi, Reyna Favis, Damayanthi Devineni, and Stephan Francke

Subjects

Adult, Male, Glucuronosyltransferase, Genotype, Cmax, Pharmacology, Kidney, Gene Expression Regulation, Enzymologic, chemistry.chemical_compound, Pharmacokinetics, Microsomes, medicine, Humans, Hypoglycemic Agents, Pharmacology (medical), Canagliflozin, Intestinal Mucosa, chemistry.chemical_classification, biology, Genetic Variation, Metabolism, Middle Aged, Recombinant Proteins, Uridine diphosphate, Enzyme, Liver, chemistry, biology.protein, Microsome, Female, medicine.drug

Abstract

O-glucuronidation is the major metabolic elimination pathway for canagliflozin. The objective was to identify enzymes and tissues involved in the formation of 2 major glucuronidated metabolites (M7 and M5) of canagliflozin and subsequently to assess the impact of genetic variations in these uridine diphosphate glucuronosyltransferases (UGTs) on in vivo pharmacokinetics in humans. In vitro incubations with recombinant UGTs revealed involvement of UGT1A9 and UGT2B4 in the formation of M7 and M5, respectively. Although M7 and M5 were formed in liver microsomes, only M7 was formed in kidney microsomes. Participants from 7 phase 1 studies were pooled for pharmacogenomic analyses. A total of 134 participants (mean age, 41 years; men, 63%; white, 84%) were included in the analysis. In UGT1A9*3 carriers, exposure of plasma canagliflozin (Cmax,ss , 11%; AUCτ,ss , 45%) increased relative to the wild type. An increase in exposure of plasma canagliflozin (Cmax,ss , 21%; AUCt,ss , 18%) was observed in participants with UGT2B4*2 genotype compared with UGT2B4*2 noncarriers. Metabolites further delineate the role of both enzymes. The pharmacokinetic findings in participants carrying the UGT1A9*3 and UGT2B4*2 allele implicate that UGT1A9 and UGT2B4 are involved in the metabolism of canagliflozin to M7 and M5, respectively.

Published

2015

11. Effects of rifampin, cyclosporine A, and probenecid on the pharmacokinetic profile of canagliflozin, a sodium glucose co-transporter 2 inhibitor, in healthy participants

Author

Hans Stieltjes, Christopher R. Curtin, Sveta Weiner, Shean-Sheng Wang, Ewa Wajs, Jay Ariyawansa, Nicholas A. Di Prospero, Nicole Vaccaro, Joseph Murphy, Rao N.V.S. Mamidi, Paul Rothenberg, and Damayanthi Devineni

Subjects

Adult, Male, drug-drug interactions, medicine.medical_specialty, Sodium, MRP, Cmax, chemistry.chemical_element, Thiophenes, P-glycoprotein, Pharmacology, Glucosides, Pharmacokinetics, Diabetes mellitus, Internal medicine, polycyclic compounds, medicine, Humans, Drug Interactions, Pharmacology (medical), Canagliflozin, Sodium-Glucose Transporter 2 Inhibitors, Probenecid, business.industry, Area under the curve, Transporter, medicine.disease, Endocrinology, chemistry, Cyclosporine, Female, Rifampin, business, pharmacokinetics, UGT, Research Article, medicine.drug

Abstract

Objective: Canagliflozin, a sodium-glucose co-transporter 2 inhibitor, approved for the treatment of type-2 diabetes mellitus (T2DM), is metabolized by uridine diphosphate-glucuronosyltransferases (UGT) 1A9 and UGT2B4, and is a substrate of P-glycoprotein (P-gp). Canagliflozin exposures may be affected by coadministration of drugs that induce (e.g., rifampin for UGT) or inhibit (e.g. probenecid for UGT; cyclosporine A for P-gp) these pathways. The primary objective of these three independent studies (single-center, open-label, fixed-sequence) was to evaluate the effects of rifampin (study 1), probenecid (study 2), and cyclosporine A (study 3) on the pharmacokinetics of canagliflozin in healthy participants. Methods: Participants received; in study 1: canagliflozin 300 mg (days 1 and 10), rifampin 600 mg (days 4 – 12); study 2: canagliflozin 300 mg (days 1 – 17), probenecid 500 mg twice daily (days 15 – 17); and study 3: canagliflozin 300 mg (days 1 – 8), cyclosporine A 400 mg (day 8). Pharmacokinetics were assessed at pre-specified intervals on days 1 and 10 (study 1); on days 14 and 17 (study 2), and on days 2 – 8 (study 3). Results: Rifampin decreased the maximum plasma canagliflozin concentration (Cmax) by 28% and its area under the curve (AUC) by 51%. Probenecid increased the Cmax by 13% and the AUC by 21%. Cyclosporine A increased the AUC by 23% but did not affect the Cmax. Conclusion: Coadministration of canagliflozin with rifampin, probenecid, and cyclosporine A was well-tolerated. No clinically meaningful interactions were observed for probenecid or cyclosporine A, while rifampin coadministration modestly reduced canagliflozin plasma concentrations and could necessitate an appropriate monitoring of glycemic control.

Published

2015

12. Effect of canagliflozin, a sodium glucose co-transporter 2 inhibitor, on the pharmacokinetics of oral contraceptives, warfarin, and digoxin in healthy participants

Author

Damayanthi Devineni, Hans Stieltjes, Sue Sha, Nicole Vaccaro, Paul Rothenberg, Sveta Weiner, Rao N.V.S. Mamidi, Donna Skee, Apexa Bernard, Prasarn Manitpisitkul, and Hong Tian

Subjects

Adult, Male, Digoxin, Cardiotonic Agents, Metabolic Clearance Rate, Cmax, Levonorgestrel, Thiophenes, Pharmacology, Ethinyl Estradiol, Risk Assessment, Drug Administration Schedule, Young Adult, Glucosides, Sodium-Glucose Transporter 2, Pharmacokinetics, Humans, Hypoglycemic Agents, Medicine, Drug Dosage Calculations, Drug Interactions, Pharmacology (medical), International Normalized Ratio, Canagliflozin, Blood Coagulation, Sodium-Glucose Transporter 2 Inhibitors, Cross-Over Studies, business.industry, Area under the curve, Warfarin, Anticoagulants, Middle Aged, Crossover study, Healthy Volunteers, Contraceptives, Oral, Combined, Drug Combinations, Area Under Curve, Pharmacodynamics, Polypharmacy, Female, business, Half-Life, medicine.drug

Abstract

OBJECTIVE Drug-drug interactions between canagliflozin, a sodium glucose co-transporter 2 inhibitor approved for the management of type-2 diabetes mellitus, and an oral contraceptive (OC), warfarin, and digoxin were evaluated in three phase 1 studies in healthy participants. METHODS All studies were open-label; study 1 included a fixed-sequence design, and studies 2 and 3 used a crossover design. Regimens were: study 1: OC (levonorgestrel (150 μg) + ethinyl estradiol (30 μg))/day (day 1), canagliflozin 200 mg/day (days 4 - 8), and canagliflozin with OC (day 9); study 2: canagliflozin 300 mg/day (days 1 - 12) with warfarin 30 mg/day (day 6) in period 1, and only warfarin 30 mg/day (day 1) in period 2, or vice versa; study 3: digoxin alone (0.5 mg/day (day 1) + 0.25 mg/day (days 2 - 7)) in period 1, and with canagliflozin 300 mg/day (days 1 - 7) in period 2, or vice versa. Pharmacokinetics (PK) were assessed at prespecified intervals; OC: days 1 and 9, canagliflozin: days 8 - 9 (study 1); warfarin: days 6 (period 1) and 1 (period 2) (study 2); and digoxin: days 5 - 7 (periods 1 and 2) (study 3). Warfarin's pharmacodynamics (PD; International Normalized Ratio (INR)) was assessed on days 6 (period 1) and 1 (period 2). RESULTS Canagliflozin increased the plasma exposure of OC (maximum plasma concentration (Cmax): 22%, area under the curve (AUC): 6%) and digoxin (Cmax: 36%, AUC: 20%); but did not alter warfarin'€™s PK and PD. No clinically relevant safety findings (including hypoglycemia) were noted. CONCLUSION Canagliflozin can be coadministered with OC, warfarin, or digoxin without dose adjustments. All treatments were well-tolerated.

Published

2015

13. Absolute oral bioavailability and pharmacokinetics of canagliflozin: A microdose study in healthy participants

Author

Ellen Scheers, Joseph Murphy, Paul Rothenberg, Shean-Sheng Wang, Hans Stieltjes, Rao N.V.S. Mamidi, and Damayanthi Devineni

Subjects

Canagliflozin, business.industry, Cmax, Pharmaceutical Science, Urine, Pharmacology, Bioavailability, Tolerability, Pharmacokinetics, MicroDose, Oral administration, Medicine, Pharmacology (medical), business, medicine.drug

Abstract

Absolute oral bioavailability of canagliflozin was assessed by simultaneous oral administration with intravenous [(14) C]-canagliflozin microdose infusion in nine healthy men. Pharmacokinetics of canagliflozin, [(14) C]-canagliflozin, and total radioactivity, and safety and tolerability were assessed at prespecified timepoints. On day 1, single-dose oral canagliflozin (300 mg) followed 105 minutes later by intravenous [(14) C]-canagliflozin (10 µg, 200 nCi) was administered. After oral administration, the mean (SD) Cmax of canagliflozin was 2504 (482) ng/mL at 1.5 hours, AUC∞ 17,375 (3555) ng.h/mL, and t1/2 11.6 (0.70) hours. After intravenous administration, the mean (SD) Cmax of unchanged [(14) C]-canagliflozin was 17,605 (6901) ng/mL, AUC∞ 27,100 (10,778) ng.h/mL, Vdss 83.5 (29.2) L, Vdz 119 (41.6) L, and CL 12.2 (3.79) L/h. Unchanged [(14) C]-canagliflozin and metabolites accounted for about 57% and 43% of the plasma total [(14) C] radioactivity AUC∞ , respectively. For total [(14) C] radioactivity, the mean (SD) Cmax was 15,981 (2721) ng-eq/mL, and AUC∞ 53,755 (15,587) ng-eq.h/mL. Renal (34.5% in urine) and biliary (34.1% in feces) excretions were the major elimination pathways for total [(14) C] radioactivity. The absolute oral bioavailability of canagliflozin was 65% (90% confidence interval: 55.41; 76.07). Overall, oral canagliflozin 300 mg coadministered with intravenous [(14) C]-canagliflozin (10 µg) was generally well-tolerated in healthy men, with no treatment-emergent adverse events.

Published

2014

14. Carcinogenicity in rats of the SGLT2 inhibitor canagliflozin

Author

Petra Vinken, Sandra De Jonghe, Jim Proctor, Mark D. Johnson, Bianca Feyen, Dirk Mariën, Helena Geys, Inneke Wynant, and Rao N.V.S. Mamidi

Subjects

Male, endocrine system, medicine.medical_specialty, Carcinogenesis, Carcinogenicity Tests, Adrenal Gland Neoplasms, chemistry.chemical_element, Parathyroid hormone, Pheochromocytoma, Thiophenes, Calcium, Toxicology, Rats, Sprague-Dawley, Structure-Activity Relationship, Glucosides, Sodium-Glucose Transporter 2, Testicular Neoplasms, Internal medicine, medicine, Animals, Canagliflozin, Sodium-Glucose Transporter 2 Inhibitors, Calcium metabolism, Kidney, Dose-Response Relationship, Drug, Leydig cell, Chemistry, General Medicine, Kidney Neoplasms, Urinary calcium, Rats, Kidney Tubules, medicine.anatomical_structure, Endocrinology, SGLT2 Inhibitor, Luteinizing hormone, Leydig Cell Tumor

Abstract

The carcinogenicity potential of canagliflozin, an inhibitor of SGLT2, was evaluated in a 2-year rat study (10, 30, and 100 mg/kg). Rats showed an increase in pheochromocytomas, renal tubular tumors, and testicular Leydig cell tumors. Systemic exposure multiples at the highest dose relative to the maximum clinical dose were 12- to 21-fold. Pheochromocytomas and renal tubular tumors were noted in both sexes at 100 mg/kg. Leydig cell tumors were observed in males in all dose groups and were associated with increased luteinizing hormone levels. Hyperplasia was increased in the adrenal medulla at 100 mg/kg, but only a limited increase in simple tubular hyperplasia was observed in the kidney of males at 100 mg/kg. Hyperostosis occurred and was accompanied by substantial effects on calcium metabolism, including increased urinary calcium excretion and decreased levels of calcium regulating hormones (1,25-dihydroxyvitamin D and parathyroid hormone). A separate study with radiolabeled calcium confirmed that increased urinary calcium excretion was mediated via increased calcium absorption from the gastrointestinal tract. It was hypothesized that, at high doses, canagliflozin might have inhibited glucose absorption in the intestine via SGLT1 inhibition that resulted in glucose malabsorption, which increased calcium absorption by stimulating colonic glucose fermentation and reducing intestinal pH. Pheochromocytomas and adrenal medullary hyperplasia were attributed to altered calcium homeostasis, which have a known relationship in the rat. In conclusion, Leydig cell tumors were associated with increased luteinizing hormone levels and pheochromocytomas were most likely related to glucose malabsorption and altered calcium homeostasis. Renal tubular tumors may also have been linked to glucose malabsorption.

Published

2014

15. Successful Integration of Nonclinical and Clinical Findings in Interpreting the Clinical Relevance of Rodent Neoplasia with a New Chemical Entity

Author

Sandra De Jonghe, Kirk Ways, Jim Proctor, Calvert Louden, Rao N.V.S. Mamidi, and Mark D. Johnson

Subjects

Male, Oncology, medicine.medical_specialty, Pathology, endocrine system diseases, Carcinogenicity Tests, Toxicology, medicine.disease_cause, Pathology and Forensic Medicine, Mice, Internal medicine, New chemical entity, medicine, Animals, Humans, Hypoglycemic Agents, Testosterone, Clinical significance, Canagliflozin, Sodium-Glucose Transporter 2 Inhibitors, Molecular Biology, Clinical Trials as Topic, Leydig cell, Mechanism (biology), business.industry, Type 2 Diabetes Mellitus, Neoplasms, Experimental, Cell Biology, Rats, medicine.anatomical_structure, Diabetes Mellitus, Type 2, SGLT2 Inhibitor, business, Carcinogenesis, medicine.drug

Abstract

Canagliflozin, a sodium glucose co-transporter 2 (SGLT2) inhibitor, has been developed for the treatment of adults with type 2 diabetes mellitus (T2DM). During the phase 3 program, treatment-related pheochromocytomas, renal tubular tumors, and testicular Leydig cell tumors were reported in the 2-year rat toxicology study. Treatment-related tumors were not seen in the 2-year mouse study. A cross-functional, mechanism-based approach was undertaken to determine whether the mechanisms responsible for tumorigenesis in the rat were of relevance to humans. Based on findings from nonclinical and clinical studies, the treatment-related tumors observed in rats were not deemed to be of clinical relevance. Here, we describe the scientific and regulatory journey from learning of the 2-year rat study findings to the approval of canagliflozin for the treatment of T2DM.

Published

2014

16. Effect of canagliflozin on the pharmacokinetics of glyburide, metformin, and simvastatin in healthy participants

Author

Donna Skee, Prasarn Manitpisitkul, Joseph Murphy, Shean-Sheng Wang, Damayanthi Devineni, Hans Stieltjes, Rao N.V.S. Mamidi, Ewa Wajs, Hong Tian, An Vandebosch, Keith Usiskin, and Tom Verhaeghe

Subjects

Canagliflozin, medicine.medical_specialty, GLYBURIDE/METFORMIN, business.industry, Cmax, nutritional and metabolic diseases, Pharmaceutical Science, Half-life, Metformin, Endocrinology, Pharmacokinetics, Simvastatin, Internal medicine, medicine, Pharmacology (medical), Adverse effect, business, medicine.drug

Abstract

Drug-drug interactions between canagliflozin, a sodium glucose co-transporter 2 inhibitor, and glyburide, metformin, and simvastatin were evaluated in three phase-1 studies in healthy participants. In these open-label, fixed sequence studies, participants received: Study 1-glyburide 1.25 mg/day (Day 1), canagliflozin 200 mg/day (Days 4-8), canagliflozin with glyburide (Day 9); Study 2-metformin 2,000 mg/day (Day 1), canagliflozin 300 mg/day (Days 4-7), metformin with canagliflozin (Day 8); Study 3-simvastatin 40 mg/day (Day 1), canagliflozin 300 mg/day (Days 2-6), simvastatin with canagliflozin (Day 7). Pharmacokinetic parameters were assessed at prespecified intervals. Co-administration of canagliflozin and glyburide did not affect the overall exposure (maximum plasma concentration [Cmax ] and area under the plasma concentration-time curve [AUC]) of glyburide and its metabolites (4-trans-hydroxy-glyburide and 3-cis-hydroxy-glyburide). Canagliflozin did not affect the peak concentration of metformin; however, AUC increased by 20%. Though Cmax and AUC were slightly increased for simvastatin (9% and 12%) and simvastatin acid (26% and 18%) following coadministration with canagliflozin, compared with simvastatin administration alone; however, no effect on active 3-hydroxy-3-methyl-glutaryl-CoA (HMG-CoA) reductase inhibitory activity was observed. There were no serious adverse events or hypoglycemic episodes. No drug-drug interactions were observed between canagliflozin and glyburide, metformin, or simvastatin. All treatments were well-tolerated in healthy participants.

Published

2014

17. Carbohydrate malabsorption mechanism for tumor formation in rats treated with the SGLT2 inhibitor canagliflozin

Author

Bianca Feyen, Sandra De Jonghe, Calvert Louden, Petra Vinken, Stewart Bryant, Godelieve Lammens, Rao N.V.S. Mamidi, Sandra Snook, Mark D. Johnson, Esther Moesen, Michael F. Kelley, Jim Proctor, Kirk Ways, and Jing Ying Ma

Subjects

Male, medicine.medical_specialty, Malabsorption, Carcinogenesis, chemistry.chemical_element, Thiophenes, Calcium, Kidney, Toxicology, Rats, Sprague-Dawley, Excretion, Glucosides, Malabsorption Syndromes, Internal medicine, medicine, Animals, Hypercalciuria, Canagliflozin, Sodium-Glucose Transporter 2 Inhibitors, Cell Proliferation, Chemistry, General Medicine, medicine.disease, Immunohistochemistry, Urinary calcium, Rats, Endocrinology, medicine.anatomical_structure, SGLT2 Inhibitor, Cell Adhesion Molecules, Carbohydrate Metabolism, Inborn Errors, medicine.drug

Abstract

Canagliflozin is an SGLT2 inhibitor used for the treatment of type 2 diabetes mellitus. Studies were conducted to investigate the mechanism responsible for renal tubular tumors and pheochromocytomas observed at the high dose in a 2-year carcinogenicity study in rats. At the high dose (100mg/kg) in rats, canagliflozin caused carbohydrate malabsorption evidenced by inhibition of intestinal glucose uptake, decreased intestinal pH and increased urinary calcium excretion. In a 6-month mechanistic study utilization of a glucose-free diet prevented carbohydrate malabsorption and its sequelae, including increased calcium absorption and urinary calcium excretion, and hyperostosis. Cell proliferation in the kidney and adrenal medulla was increased in rats maintained on standard diet and administered canagliflozin (100mg/kg), and in addition an increase in the renal injury biomarker KIM-1 was observed. Increased cell proliferation is considered as a proximal event in carcinogenesis. Effects on cell proliferation, KIM-1 and calcium excretion were inhibited in rats maintained on the glucose-free diet, indicating they are secondary to carbohydrate malabsorption and are not direct effects of canagliflozin.

Published

2014

18. LC–ESI-MS/MS quantification of 4β-hydroxycholesterol and cholesterol in plasma samples of limited volume

Author

Lisa Smith, Heng-Keang Lim, Naidong Weng, Jose Silva, Yang Yuan, Rick Edom, Rao N.V.S. Mamidi, David C. Evans, and Yaodong Xu

Subjects

Spectrometry, Mass, Electrospray Ionization, Analyte, Electrospray, Clinical Biochemistry, Pharmaceutical Science, Mass spectrometry, Analytical Chemistry, Mice, chemistry.chemical_compound, Tandem Mass Spectrometry, Drug Discovery, medicine, Animals, Humans, Derivatization, Chromatography, High Pressure Liquid, Spectroscopy, Chromatography, Chemistry, Elution, Cholesterol, Selected reaction monitoring, Human serum albumin, Hydroxycholesterols, lipids (amino acids, peptides, and proteins), medicine.drug

Abstract

A liquid chromatography-electrospray ionization-tandem mass spectrometry (LC-ESI-MS/MS) assay was developed and qualified for analyzing 4β-hydroxycholesterol and cholesterol in 5 μl of human and mouse plasma. Stable isotope-labeled d7-analogs of both analytes were used as internal standards and 4.2% (w/v) human serum albumin in phosphate-buffered saline was used as the surrogate matrix for preparation of calibration curves and QCs. The assay is capable of quantification of 4β-hydroxycholesterol and cholesterol from 5 to 500 ng/ml and 50 to 2000 μg/ml, respectively, with acceptable accuracy and precision following evaluation of recovery of analytes, autosampler stability and potential contribution of chemical oxidation to the formation of 4β-hydroxycholesterol. The final reconstituted solution was diluted for quantification of cholesterol typically present at 1000 fold higher concentration than 4β-hydroxycholesterol in the same samples used for 4β-hydroxycholesterol quantification. The successful quantification using a low plasma volume was achieved by quantification of total forms (free and conjugated) of both analytes after alkaline hydrolysis, followed by derivatization to form electrospray ionization-sensitive picolinyl esters, which upon collision-induced dissociation gave high mass precursor-product ion pair for selective detection by multiple reaction monitoring. In addition, chromatographic separation using a 16-min reversed phase gradient elution on a 1.9 μm particle size, C18 column, overcame interference from other isobaric plasma oxysterols during detection by multiple-reaction monitoring. This assay was compared to an orthogonal enzymatic assay for cholesterol and all samples, but one, provided values that were within 10% of each other. In addition, this assay passed the incurred sample tests for both analytes in human and mouse plasma samples according to reported acceptance criteria for incurred sample reanalysis. The quantification of both analytes permitted the determination of 4β-hydroxycholesterol compared to its ratio to cholesterol as an endogenous biomarker for CYP3A4/5 activity. The LC-ESI-MS/MS assay was also successfully applied to quantification of 4β-hydroxycholesterol and cholesterol in plasma samples from untreated human and mice including FRG™ KO C57Bl/6 chimeric mice with humanized livers. The preliminary data indicated that the plasma 4β-hydroxycholesterol concentrations or their ratio to cholesterol from mice including chimeric mice were higher than those from human.

Published

2013

19. In vitro and physiologically‐based pharmacokinetic based assessment of drug–drug interaction potential of canagliflozin

Author

Jan Snoeys, Ellen Scheers, David C. Evans, Carlo Sensenhauser, Heng-Keang Lim, Laurent Leclercq, Peter Verboven, Shannon Dallas, Michael F. Kelley, Mark D. Johnson, Filip Cuyckens, and Rao N.V.S. Mamidi

Subjects

Physiologically based pharmacokinetic modelling, Organic anion transporter 1, CYP2B6, In Vitro Techniques, Pharmacology, Models, Biological, 030226 pharmacology & pharmacy, Xenopus laevis, 03 medical and health sciences, 0302 clinical medicine, Cytochrome P-450 Enzyme System, Pharmacokinetics, medicine, Animals, Humans, Hypoglycemic Agents, Pharmacology (medical), Drug Interactions, Canagliflozin, CYP2C8, Letter to the Editor, biology, CYP3A4, Chemistry, Membrane Transport Proteins, Repaglinide, Area Under Curve, 030220 oncology & carcinogenesis, biology.protein, medicine.drug

Abstract

Aims Canagliflozin is a recently approved drug for use in the treatment of type 2 diabetes. The potential for canagliflozin to cause clinical drug-drug interactions (DDIs) was assessed. Methods DDI potential of canagliflozin was investigated using in vitro test systems containing drug metabolizing enzymes or transporters. Basic predictive approaches were applied to determine potential interactions in vivo. A physiologically-based pharmacokinetic (PBPK) model was developed and clinical DDI simulations were performed to determine the likelihood of cytochrome P450 (CYP) inhibition by canagliflozin. Results Canagliflozin was primarily metabolized by uridine 5'-diphospho-glucuronosyltransferase 1A9 and 2B4 enzymes. Canagliflozin was a substrate of efflux transporters (P-glycoprotein, breast cancer resistance protein and multidrug resistance-associated protein-2) but was not a substrate of uptake transporters (organic anion transporter polypeptide isoforms OATP1B1, OATP1B3, organic anion transporters OAT1 and OAT3, and organic cationic transporters OCT1, and OCT2). In inhibition assays, canagliflozin was shown to be a weak in vitro inhibitor (IC50 ) of CYP3A4 (27 μmol l -1 , standard error [SE] 4.9), CYP2C9 (80 μmol l -1 , SE 8.1), CYP2B6 (16 μmol l-1 , SE 2.1), CYP2C8 (75 μmol l -1 , SE 6.4), P-glycoprotein (19.3 μmol l -1 , SE 7.2), and multidrug resistance-associated protein-2 (21.5 μmol l -1 , SE 3.1). Basic models recommended in DDI guidelines (US Food & Drug Administration and European Medicines Agency) predicted moderate to low likelihood of interaction for these CYPs and efflux transporters. PBPK DDI simulations of canagliflozin with CYP probe substrates (simvastatin, S-warfarin, bupropion, repaglinide) did not show relevant interaction in humans since mean areas under the concentration-time curve and maximum plasma concentration ratios for probe substrates with and without canagliflozin and its 95% CIs were within 0.80-1.25. Conclusions In vitro DDI followed by a predictive or PBPK approach was applied to determine DDI potential of canagliflozin. Overall, canagliflozin is neither a perpetrator nor a victim of clinically important interactions.

Published

2016

20. De-Risking Bio-therapeutics for Possible Drug Interactions Using Cryopreserved Human Hepatocytes

Author

Cindy Zakszewski, Rao N.V.S. Mamidi, Michael McMillia, Chao Han, Monica Singer, Carlo Sensenhauser, Shannon Dallas, Ameesha Batheja, Honghui Zhou, Jose Silva, and Maria Markowska

Subjects

Male, Drug, Gene isoform, medicine.medical_specialty, media_common.quotation_subject, medicine.medical_treatment, Clinical Biochemistry, Biology, Pharmacology, Cytochrome P-450 Enzyme System, Risk Factors, Internal medicine, Psoriasis, Gene expression, medicine, Humans, Drug Interactions, media_common, Cryopreservation, chemistry.chemical_classification, Biological Products, Messenger RNA, CYP1A2, Middle Aged, medicine.disease, Endocrinology, Enzyme, Cytokine, chemistry, Child, Preschool, Hepatocytes, Cytokines, Female

Abstract

Inflammatory diseases such as rheumatoid arthritis and psoriasis are characterized by increases in circulating cytokines, which play an important role in modulation of the disease state. Several marketed bio-therapeutics target cytokines and act as effective treatment strategies. Previous in-vitro and in-vivo studies have suggested that cytokines may have both direct and indirect effects on drug metabolizing enzyme levels in the liver. Few studies have characterized models to evaluate the risk of potential drug interactions that might be mediated by changes in cytokine levels. In the present studies the potential of three cytokines (IL-2, IL-6 and TNF-α) to modulate gene expression and activity of the major human cytochrome P450 (CYP) enzymes (CYP1A2, 2B6, 2C9, 2C19, 2D6, and 3A4) in cryopreserved human hepatocytes (CHH) was investigated. Significant decreases in the activity of all 6 CYP isoforms occurred in hepatocytes incubated with TNF-α or IL-6 (17-85%; and 22-76% of untreated control values, respectively). TNF-α down-regulated the gene expression of CYP1A2, 2D6 and 3A4 only, whereas IL-6 down-regulated gene expression of all of the tested CYP isoforms except 2D6. IL-2 had only mild effects on CYP activity and mRNA levels of examined isoforms. In CHH exposed to TNF-α, changes in CYP activity were not always paralleled by gene expression alterations for three of the examined CYP isoforms. These studies highlight several potential pitfalls in using isolated human hepatocytes for determination of drug interactions by bio-therapeutics including lack of correlation of mRNA and activity measurements for some CYP isoforms when using single time point determinations, and appropriateness of the model for indirect acting cytokine and cytokine modulators.

Published

2012

21. Metabolism and excretion of canagliflozin in mice, rats, dogs, and humans

Author

Dennis Kalamaridis, Ellen Scheers, Filip Cuyckens, Rao N.V.S. Mamidi, Michael F. Kelley, Mark D. Johnson, Heng-Keang Lim, Damayanthi Devineni, Jose Silva, Lin Ronghui, Sue Sha, David C. Evans, and Jie Chen

Subjects

Adult, Male, medicine.medical_specialty, Magnetic Resonance Spectroscopy, Glucuronidation, Pharmaceutical Science, Administration, Oral, Urine, Thiophenes, Pharmacology, Excretion, Rats, Sprague-Dawley, Feces, Mice, Young Adult, Dogs, Glucuronides, Glucosides, Species Specificity, In vivo, Internal medicine, Detoxification, medicine, Animals, Bile, Humans, Hypoglycemic Agents, Tissue Distribution, Carbon Radioisotopes, Canagliflozin, Chemistry, Reabsorption, Metabolism, Middle Aged, Rats, Endocrinology, Female, medicine.drug

Abstract

Canagliflozin is an oral antihyperglycemic agent used for the treatment of type 2 diabetes mellitus. It blocks the reabsorption of glucose in the proximal renal tubule by inhibiting the sodium-glucose cotransporter 2. This article describes the in vivo biotransformation and disposition of canagliflozin after a single oral dose of [ 14 C]canagliflozin to intact and bile duct-cannulated (BDC) mice and rats and to intact dogs and humans. Fecal excretion was the primary route of elimination of drug-derived radioactivity in both animals and humans. In BDC mice and rats, most radioactivity was excreted in bile. The extent of radioactivity excreted in urine as a percentage of the administered [ 14 C]canagliflozin dose was 1.2%– 7.6% in animals and approximately 33% in humans. The primary pathways contributing to the metabolic clearance of canagliflozin were oxidation in animals and direct glucuronidation of canagliflozin in humans. Unchanged canagliflozin was the major component in systemic circulation in all species. In human plasma, two pharmacologically inactive O-glucuronide conjugates of canagliflozin, M5 and M7, represented 19% and 14% of total drug-related exposure and were considered major human metabolites. Plasma concentrations of M5 and M7 in mice and rats from repeated dose safety studies were lower than those in humans given canagliflozin at the maximum recommended dose of 300 mg. However, biliary metabolite profiling in rodents indicated that mouse and rat livers had significant exposure to M5 and M7. Pharmacologic inactivity and high water solubility of M5 and M7 support glucuronidation of canagliflozin as a safe detoxification pathway.

Published

2014

22. Polymorphism of dextromethorphan oxidation in South Indian subjects

Author

Swaroopkumar V. S. Vakkalanka, Nataraj Brahmadevara, Madhusudana R. Chaluvadi, Shreeram Satyavageeswaran, Swaminathan Subramaniam, Govindadas Damodarram, Rao N.V.S. Mamidi, and Kasiram Katneni

Subjects

Adult, Male, animal structures, Adolescent, Metabolite, India, Urine, Pharmacology, Dextromethorphan, Fluorescence, Dextromethorphan Hydrobromide, chemistry.chemical_compound, Pharmacokinetics, Dextrorphan, medicine, Humans, Pharmacology (medical), Volunteer, Chromatography, High Pressure Liquid, Polymorphism, Genetic, Chemistry, Middle Aged, Phenotype, Female, Oxidation-Reduction, Pharmacogenetics, medicine.drug

Abstract

One hundred fifty-six unrelated healthy South Indian subjects were phenotyped according to their ability to metabolize dextromethorphan to its O-demethylated metabolite dextrorphan. Each volunteer was administered 25 mg oral dextromethorphan hydrobromide (19.3 mg dextromethorphan). Urine was collected during an 8-hour period after drug administration and was analyzed for dextromethorphan and dextrorphan by HPLC with fluorescence detection. This analysis was performed with and without previous deconjugation. The log 10 (metabolic ratio), calculated as the ratio of dextromethorphan to dextrorphan, was bimodally distributed, and it was inferred that the frequency of occurrence of poor metabolizers of dextromethorphan in South Indian subjects is 3.2%. Phenotype assignment remained the same with both methods of analysis. Furthermore, a fairly good correlation (Spearman rank order correlation coefficient [r s ] = 0.61; P < .0001) was observed between the log-transformed metabolic ratio derived from both methods. (Clin Pharmacol Ther 1999;66:193-200.)

Published

1999

23. Quantitative determination of DRF-1042 in human plasma by HPLC: validation and application in clinical pharmacokinetics ( This is publication number 275 from Dr Reddy's Laboratories Ltd.).

Author

Vijay V. Upreti, Rao N.V.S. Mamidi, Kasiram Katneni, and Nuggehally R. Srinivas

Subjects

LIQUID chromatography, PHARMACOKINETICS, PHARMACOLOGY, CHEMICAL kinetics, CLINICAL trials, MEDICAL experimentation on humans

Abstract

A simple and sensitive high-performance liquid chromatography (HPLC) method has been developed and validated for the determination of DRF-1042, a novel orally active camptothecin (CPT) analog, in human plasma. The sample preparation was a simple deproteinization with acidified methanol yielding almost 100% recovery of DRF-1042. An isocratic reverse-phase HPLC separation was developed on a Supelcosil-LC318 column (250 × 4.6 mm, 5 µm) with mobile phase consisting of 1% v/v triethylamine acetate, pH 5.5 and acetonitrile (80:20, v/v) at a flow rate of 1.0 mL/min. The eluate was monitored with a fluorescence detector set at excitation and emission wavelengths of 370 and 430 nm, respectively. The standard curves were linear (r2 > 0.999) in the concentration ranges 5.0–2004 ng/mL. The lower limit of quantification (LLQ) of the assay was 5 ng/mL. The mean measured quality control (QC) concentrations (range 5 ng/mL to 40 µg/mL) deviated from the nominal concentrations in the range of -10.5–0.08 and -14.5–7.97%, inter- and intra-day, respectively. The inter- and intra-day precisions in the measurement of QC samples at four tested concentrations, were in the range 0.64–5.89% relative standard deviation (RSD) and 0.33–14.7% RSD, respectively. The method was found to be suitable for measurement of plasma concentrations above the calibration curve after serial dilutions. Stability of DRF-1042 was confirmed in a battery of studies, viz., on bench-top, in the auto-sampler, in the stock solutions, after four quick freeze–thaw cycles, up to one month at -20C in human plasma and up to 2 months in the ex vivo samples. The method is simple, sensitive and reliable and has been successfully implemented to investigate the clinical pharmacokinetics of DRF-1042 in cancer patients in a phase I clinical trial. Copyright © 2003 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published

2003