RÉSUMÉ
This phase I thorough QTc, double-blind, randomized, placebo- and positive-controlled, parallel group, multiple-dose study evaluated avacopan's effect on cardiac repolarization using concentration-QTc (C-QTc) as the primary analysis. Avacopan 30 mg b.i.d. (therapeutic dose) was administered orally on days 1 through 7 followed by avacopan 100 mg b.i.d. (supratherapeutic dose) on days 8 through 14 in 29 healthy participants. Moxifloxacin 400 mg and placebo were administered on days 1 and 15 in a nested crossover design for assay sensitivity in separate cohorts to 28 participants. Time-matched plasma concentrations and up to 10 replicate ECGs were obtained on prespecified days at baseline and postdose on days 1, 7, 14, and 15. The mean change from baseline on QTcF for avacopan (-5.5 to 3.5 ms) was similar to placebo (-6.9 to 1.4 ms) across days 1, 7, and 14. The mean effect on ΔΔQTcF (90% CI) was estimated as 1.5 ms (-0.17 to 3.09) and 0.8 ms (-2.41 to 4.05) for 30 and 100 mg avacopan b.i.d. treatments, respectively. Based on the C-QTc analysis, avacopan's effect on ΔΔQTcF >10 ms can be excluded within the observed plasma concentration range of up to ~1220 and ~335 ng/mL for avacopan and active major metabolite, M1, respectively. The estimated population slopes showed a shallow relationship, which was not statistically significant. There was no clinically meaningful effect of avacopan on heart rate or cardiac conduction (PR and QRS intervals). Avacopan appeared to be generally well tolerated in this study population.
Sujet(s)
Études croisées , Relation dose-effet des médicaments , Électrocardiographie , Volontaires sains , Rythme cardiaque , Humains , Mâle , Adulte , Femelle , Méthode en double aveugle , Jeune adulte , Rythme cardiaque/effets des médicaments et des substances chimiques , Adulte d'âge moyen , Moxifloxacine/administration et posologie , Moxifloxacine/effets indésirables , Moxifloxacine/pharmacocinétique , AdolescentRÉSUMÉ
Obesity is a major public health crisis. Multi-specific peptides have emerged as promising therapeutic strategies for clinical weight loss. Glucagon-like peptide-1 (GLP-1) and glucose-dependent insulinotropic polypeptide (GIP) are endogenous incretins that regulate weight through their receptors (R). AMG 133 (maridebart cafraglutide) is a bispecific molecule engineered by conjugating a fully human monoclonal anti-human GIPR antagonist antibody to two GLP-1 analogue agonist peptides using amino acid linkers. Here, we confirm the GIPR antagonist and GLP-1R agonist activities in cell-based systems and report the ability of AMG 133 to reduce body weight and improve metabolic markers in male obese mice and cynomolgus monkeys. In a phase 1, randomized, double-blind, placebo-controlled clinical study in participants with obesity ( NCT04478708 ), AMG 133 had an acceptable safety and tolerability profile along with pronounced dose-dependent weight loss. In the multiple ascending dose cohorts, weight loss was maintained for up to 150 days after the last dose. These findings support continued clinical evaluation of AMG 133.
Sujet(s)
Glucagon-like peptide 1 , Récepteur du peptide-1 similaire au glucagon , Perte de poids , Animaux , Humains , Mâle , Souris , Glucagon-like peptide 1/analogues et dérivés , Obésité/traitement médicamenteux , Obésité/métabolisme , Peptides/usage thérapeutique , Récepteur du peptide-1 similaire au glucagon/antagonistes et inhibiteursRÉSUMÉ
BACKGROUND: Approved systemic treatment options are limited for pediatric patients with moderate to severe plaque psoriasis. OBJECTIVE: To assess the efficacy and safety of apremilast over 16 weeks in pediatric patients with plaque psoriasis. METHODS: SPROUT (NCT03701763) was a phase 3, multicenter, randomized, double-blind, placebo-controlled study of apremilast in patients aged 6-17 years with moderate-to-severe psoriasis (Psoriasis Area and Severity Index [PASI] ≥12, body surface area ≥10%, static Physician Global Assessment [sPGA] ≥3) inadequately controlled by/inappropriate for topical therapy. Patients were stratified by age group and randomized (2:1) to apremilast (20 or 30 mg BID based on weight) or placebo for 16 weeks, followed by apremilast extension to 52 weeks. RESULTS: Of 245 patients randomized (apremilast: 163; placebo: 82), 221 (90%) completed the double-blind phase (apremilast: 149; placebo: 72). Significantly more patients achieved sPGA response and ≥75% reduction in PASI with apremilast than placebo, regardless of baseline age, weight, or disease severity. No new safety signals were observed. LIMITATIONS: Sample size of subgroup analyses. CONCLUSIONS: Improvements in global disease activity and skin involvement were significantly greater in pediatric patients treated with apremilast versus placebo. Adverse events were consistent with the known apremilast safety profile.
Sujet(s)
Anti-inflammatoires non stéroïdiens , Psoriasis , Indice de gravité de la maladie , Thalidomide , Humains , Thalidomide/analogues et dérivés , Thalidomide/usage thérapeutique , Thalidomide/effets indésirables , Thalidomide/administration et posologie , Psoriasis/traitement médicamenteux , Adolescent , Enfant , Méthode en double aveugle , Mâle , Femelle , Anti-inflammatoires non stéroïdiens/usage thérapeutique , Anti-inflammatoires non stéroïdiens/administration et posologie , Anti-inflammatoires non stéroïdiens/effets indésirables , Résultat thérapeutique , Inhibiteurs de la phosphodiestérase-4/effets indésirables , Inhibiteurs de la phosphodiestérase-4/usage thérapeutique , Inhibiteurs de la phosphodiestérase-4/administration et posologie , Relation dose-effet des médicamentsRÉSUMÉ
Glecaprevir (GLE)/pibrentasvir (PIB) is an all-oral, interferon- and ribavirin-free, pan-genotypic fixed-dose combination regimen approved for the treatment of all major genotypes of hepatitis C virus (HCV) infection in many countries worldwide. To support clinical development in China, an open-label, single-center phase 1 study was conducted to evaluate the pharmacokinetics, safety, and tolerability of GLE/PIB in healthy Chinese adults in Mainland China. Eighteen participants received 3 tablets of coformulated GLE/PIB 100/40 mg once daily (QD) for 7 days. Following GLE/PIB 300 mg/120 mg administration, GLE and PIB reached maximum concentration in 4-5 hours with a terminal elimination half-life of 5.9 and 25 hours, respectively. Both GLE and PIB reached steady state by day 5, with no-to-minimal accumulation (≤17% higher). GLE/PIB exposures in healthy Chinese participants were similar to historical observations across phase 1 studies in healthy Western participants. GLE/PIB was safe and well-tolerated, with most adverse events being mild. These pharmacokinetics and safety data, together with existing global efficacy and safety data in healthy and HCV-infected Western participants, support the use of GLE/PIB 300 mg/120 mg QD in adult Chinese patients with chronic HCV infection.
Sujet(s)
Antiviraux , Hépatite C , Adulte , Humains , Peuples d'Asie de l'Est , Hepacivirus/génétique , Hépatite C/traitement médicamenteux , ComprimésRÉSUMÉ
BACKGROUND AND OBJECTIVE: Omecamtiv mecarbil (OM) is a novel cardiac myosin activator in development for the treatment of heart failure with reduced ejection fraction. The objective of this study was to evaluate the potential for OM to affect the pharmacokinetics of metformin. METHODS: This was an open-label, fixed-sequence study in 14 healthy subjects. On Day 1, subjects received an 850 mg oral dose of metformin. From Days 4 to 9, subjects received twice-daily 25 mg oral doses of OM tablets. On Day 10, subjects received an 850 mg oral dose of metformin and a single 25 mg tablet of OM. Blood and urine samples were collected up to 36 h post-dose following administration of metformin on Days 1 and 10 to characterize concentrations of metformin in plasma and urine. RESULTS: The ratios of the geometric least square means of metformin coadministered with OM compared to metformin alone were 98.7%, 99.3%, and 110.2% for AUCinf, AUClast, and Cmax, respectively. The mean renal clearance of metformin was similar following metformin administered alone (34.2 L/h) compared to metformin coadministered with OM (32.9 L/h). All adverse events were mild in severity and resolved prior to the end of the study. No serious adverse events or treatment-emergent adverse events led to discontinuation from the study. CONCLUSIONS: There was no clinically relevant effect of OM on the pharmacokinetics of metformin in healthy subjects.
Sujet(s)
Metformine/pharmacocinétique , Transporteurs de cations organiques/métabolisme , Urée/analogues et dérivés , Administration par voie orale , Adulte , Aire sous la courbe , Diarrhée/étiologie , Interactions médicamenteuses/physiologie , Femelle , Période , Volontaires sains , Humains , Méthode des moindres carrés , Mâle , Metformine/administration et posologie , Metformine/effets indésirables , Metformine/composition chimique , Adulte d'âge moyen , Courbe ROC , Spécificité du substrat , Comprimés/composition chimique , Urée/administration et posologie , Urée/effets indésirables , Urée/composition chimiqueRÉSUMÉ
Omecamtiv mecarbil (OM) is a cardiac myosin activator in clinical development for the treatment of heart failure. The effect of food on the pharmacokinetics (PK) of 25, 37.5, and 50 mg strength modified release (MR) tablets and the bioequivalence of two 25 mg tablets versus one 50 mg MR tablet were evaluated in two open-label, randomized, cross-over studies in healthy subjects. Subjects received two 25 mg tablets or one 50 mg OM MR tablet under fed or fasted states in Study 1 (n = 39), and single oral doses of 25 and 37.5 mg OM MR tablets and to assess its relative bioavailability to the 25 mg MR tablet, a 25 mg oral solution under fed or fasted states in Study 2 (n = 34). The area under the concentration-time curve (AUC) and the maximum observed concentration (Cmax ) of 25, 37.5, or 50 mg OM MR tablets were approximately 13%-22% higher and 31%-40% higher, respectively, when taken with food. The two 25 mg and one 50 mg OM MR tablets were bioequivalent (90% confidence intervals) of the geometric mean ratios for Cmax and AUC of OM were within 0.8-1.25 under the fasted or fed state. OM was well tolerated and all treatment-emergent events were mild in severity and resolved by the end of the study. In conclusion, these studies demonstrated that the effect of food on the PK of OM was minimal at all three studied strengths of the MR tablets, and two 25 mg MR tablets may be switched for one 50 mg MR tablet (EudraCT Number: 2019-003683-44).
Sujet(s)
Urée/analogues et dérivés , Administration par voie orale , Adulte , Aire sous la courbe , Myosines cardiaques , Études croisées , Préparations à action retardée , Substitution de médicament , Jeûne/métabolisme , Femelle , Interactions aliments-médicaments , Volontaires sains , Humains , Mâle , Adulte d'âge moyen , Comprimés , Équivalence thérapeutique , Urée/administration et posologie , Urée/effets indésirables , Urée/sang , Urée/pharmacocinétiqueRÉSUMÉ
Omecamtiv mecarbil (OM) is a novel selective cardiac myosin activator under investigation for the treatment of heart failure with reduced ejection fraction. OM is primarily eliminated via metabolism mediated by multiple cytochrome P450 enzymes. This phase 1 single-dose, multicenter, open-label, nonrandomized study evaluated the pharmacokinetics (PK) of OM and major metabolites M3 and M4, safety, and tolerability following oral administration of a single dose of 25-mg MR tablet in subjects with mild (n = 6) or moderate (n = 6) hepatic impairment (according to Child-Pugh classification) versus subjects with normal hepatic function (n = 6). Relative to subjects with normal hepatic function, for subjects with mild or moderate hepatic impairment, OM AUCinf was 103.2% (90%CI, 58.0%-183.6%) and 94.8% (90%CI, 54.7%-164.1%), respectively, and OM Cmax was 126.8% (90%CI, 85.7%-187.7%) and 117.3% (90%CI, 80.7%-170.5%), respectively. Exposures to M3 were similar across groups, whereas slightly lower exposures were observed for M4 with worsening hepatic function. The OM, M3, and M4 tmax and t1/2 values were similar between groups. There were no serious adverse events (AEs) or treatment-related treatment-emergent AEs. Overall, OM, M3, and M4 PK were not meaningfully affected by mild or moderate hepatic impairment, suggesting the same dosing strategy can be used in subjects with mild or moderate hepatic impairment.
Sujet(s)
Urée , Administration par voie orale , Aire sous la courbe , Humains , Comprimés , Urée/effets indésirables , Urée/analogues et dérivésRÉSUMÉ
BACKGROUND AND OBJECTIVE: Omecamtiv mecarbil is a novel selective cardiac myosin activator (myotrope) under investigation for the treatment of heart failure with reduced ejection fraction. The objective of this clinical study was to estimate the effect of varying degrees of renal impairment on the pharmacokinetics of omecamtiv mecarbil single dose (50 mg) under fasted conditions. METHODS: This phase I, open-label, non-randomized, parallel-group study evaluated the pharmacokinetics, safety, and tolerability of a single oral dose of omecamtiv mecarbil 50 mg in individuals with normal renal function or mild, moderate, and severe renal impairment, including end-stage renal disease requiring dialysis. Geometric least-squares mean ratios of maximum observed concentration (Cmax) and area under the plasma concentration-time curve (AUC) and 90% confidence intervals were derived for comparisons of renal impairment vs normal renal function. Participants were monitored for adverse events. RESULTS: Thirty-one participants received treatment and completed the study. Geometric mean exposures were similar for participants with renal impairment (AUC∞ range, 2550-3220 h*ng/mL; Cmax range, 78.9-107 ng/mL) and participants with normal renal function (AUC∞, 2790 h*ng/mL; Cmax, 92.6 ng/mL), with geometric least-squares mean ratios of 85.2-125.9. Exposure was similar on dialysis vs non-dialysis days in participants with end-stage renal disease (AUC0-24, 1650 vs 1700 h*ng/mL; Cmax, 100.0 vs 107.0 ng/mL). Four participants (12.9%) reported four treatment-emergent adverse events. No deaths, treatment-emergent adverse events leading to discontinuation, or serious adverse events occurred. CONCLUSIONS: Omecamtiv mecarbil pharmacokinetics were not meaningfully affected by renal function or hemodialysis, suggesting the same dosing strategy can be used in individuals with normal renal function or renal impairment. Oral administration of omecamtiv mecarbil was not associated with major tolerability findings. This study supports omecamtiv mecarbil for the treatment of heart failure in individuals with or without renal impairment.
Sujet(s)
Défaillance cardiaque , Urée , Administration par voie orale , Aire sous la courbe , Myosines cardiaques/métabolisme , Myosines cardiaques/usage thérapeutique , Défaillance cardiaque/traitement médicamenteux , Humains , Urée/analogues et dérivés , Urée/usage thérapeutiqueRÉSUMÉ
PURPOSE: Fixed-dose combination glecaprevir (GLE) 300 mg + pibrentasvir (PIB) 120 mg is an orally administered once daily antiviral regimen approved for the treatment of hepatitis C virus (HCV) infection. The objective of this study was to evaluate the potential for cardiac repolarization following GLE + PIB administration in healthy adults. METHODS: This placebo- and active-controlled, randomized, single-dose, 4-period, 4-sequence crossover study enrolled 48 healthy subjects. The doses of GLE 400 mg + PIB 120 mg were selected to provide exposures comparable to those with the doses that are therapeutic in the HCV-infected population, GLE 300 mg + PIB 120 mg. The doses of GLE 600 mg + PIB 240 mg were selected to provide supratherapeutic exposures without exceeding the exposures of the GLE + PIB maximal tolerated doses. Moxifloxacin 400 mg (active control/open label) was used for confirming the sensitivity of the ECG assay in detecting QTc prolongation. Time-matched plasma concentrations and triplicate ECGs were obtained on treatment days -1 and 1. The primary end point was time-matched, placebo-corrected, baseline-adjusted Fridericia-corrected QT interval (ΔΔQTcF). Pharmacokinetic-pharmacodynamic analyses characterized the relationship between GLE and PIB plasma concentrations and ΔΔQTcF using a linear regression model and linear mixed-effects model. Findings from categorical analyses of ECG-interval data were also summarized. Tolerability was evaluated through adverse-events monitoring, physical examination including vital sign measurements, ECGs, and laboratory tests. FINDINGS: A total of 48 subjects (22 women [46%], 26 men [54%]), were enrolled in the study, and 47 subjects completed all 4 periods. None of the subjects had a change from baseline in QTcF interval of >30 msec or an absolute QTcF interval of >450 msec. Peak ΔΔQTcF values observed at 5 h postdose (Tmax) were 2.9 msec (upper 95% confidence limit, 4.9 msec) with the therapeutic dose and 3.1 msec (upper 95% confidence limit, 5.1 msec) with the supratherapeutic dose, with both upper 95% confidence limits well below the 10-msec threshold. Assay sensitivity was confirmed by peak ΔΔQTcF in the positive control (12.8 ms at 2 h postdose). No statistically significant GLE or PIB concentration-dependent effects on ΔΔQTcF were observed. Headache and skin irritation from ECG electrodes were the most commonly reported AEs. No clinically significant vital sign measurements, ECG findings, or laboratory measurements were observed. There were no patterns of T- and U-wave morphologic abnormalities. IMPLICATIONS: The fixed-dose combination regimen of GLE/PIB does not prolong the QTc interval. ClinicalTrials.gov identifier.
Sujet(s)
Acides amino-isobutyriques/administration et posologie , Benzimidazoles/administration et posologie , Cyclopropanes/administration et posologie , Rythme cardiaque/effets des médicaments et des substances chimiques , Coeur/effets des médicaments et des substances chimiques , Lactames macrocycliques/administration et posologie , Leucine/analogues et dérivés , Proline/analogues et dérivés , Quinoxalines/administration et posologie , Sulfonamides/administration et posologie , Adulte , Acides amino-isobutyriques/sang , Acides amino-isobutyriques/pharmacocinétique , Benzimidazoles/sang , Benzimidazoles/pharmacocinétique , Études croisées , Cyclopropanes/sang , Cyclopropanes/pharmacocinétique , Méthode en double aveugle , Association médicamenteuse , Électrocardiographie/effets des médicaments et des substances chimiques , Femelle , Volontaires sains , Coeur/physiologie , Humains , Lactames macrocycliques/sang , Lactames macrocycliques/pharmacocinétique , Leucine/administration et posologie , Leucine/sang , Leucine/pharmacocinétique , Syndrome du QT long , Mâle , Adulte d'âge moyen , Proline/administration et posologie , Proline/sang , Proline/pharmacocinétique , Pyrrolidines , Quinoxalines/sang , Quinoxalines/pharmacocinétique , Méthode en simple aveugle , Sulfonamides/sang , Sulfonamides/pharmacocinétique , Jeune adulteRÉSUMÉ
BACKGROUND: Treatment of patients coinfected with hepatitis C and human immunodeficiency viruses (HCV; HIV) requires careful consideration of potential drug-drug interactions between HCV direct-acting antiviral agents (DAA) and HIV antiretrovirals. Glecaprevir/pibrentasvir is a fixed-dose combination of an NS3/4A protease inhibitor and an NS5A inhibitor approved for the treatment of chronic HCV genotype 1-6 infection, including patients with HIV coinfection. METHODS: A series of phase 1 studies was conducted to evaluate potential interactions of glecaprevir and pibrentasvir with elvitegravir/cobicistat/emtricitabine/tenofovir alafenamide, abacavir/dolutegravir/lamivudine, raltegravir, rilpivirine, atazanavir/ritonavir, darunavir/ritonavir, lopinavir/ritonavir, or efavirenz/emtricitabine/tenofovir disoproxil fumarate. Pharmacokinetics of the antiretrovirals and DAAs were characterized when administered alone and in combination to quantify changes in systemic drug exposure. RESULTS: Glecaprevir area under the curve increased >4-fold in the presence of ritonavir-boosted HIV protease inhibitors, while pibrentasvir concentrations were not significantly affected; elevations in alanine transaminase occurred in combination with atazanavir/ritonavir only. Exposures of glecaprevir and pibrentasvir may be significantly decreased by efavirenz. Coadministration with glecaprevir and pibrentasvir did not result in clinically significant changes in the exposure of any antiretroviral agents. CONCLUSIONS: Atazanavir is contraindicated with glecaprevir/pibrentasvir and use of boosted protease inhibitors or efavirenz is not recommended. No clinically significant interactions were observed with other studied antiretrovirals.
Sujet(s)
Antirétroviraux/pharmacologie , Benzimidazoles/pharmacologie , Co-infection/traitement médicamenteux , Interactions médicamenteuses , Infections à VIH/traitement médicamenteux , Hépatite C chronique/traitement médicamenteux , Pyrrolidines/pharmacologie , Quinoxalines/pharmacologie , Sulfonamides/pharmacologie , Adulte , Antirétroviraux/pharmacocinétique , Antirétroviraux/usage thérapeutique , Benzimidazoles/pharmacocinétique , Benzimidazoles/usage thérapeutique , Contre-indications aux médicaments , Association médicamenteuse , Femelle , Hépatite C chronique/complications , Humains , Mâle , Pyrrolidines/pharmacocinétique , Pyrrolidines/usage thérapeutique , Quinoxalines/pharmacocinétique , Quinoxalines/usage thérapeutique , Sulfonamides/pharmacocinétique , Sulfonamides/usage thérapeutiqueRÉSUMÉ
Glecaprevir (GLE)/pibrentasvir (PIB) 300 mg/120 mg once daily (Mavyret/Maviret) is an all-oral, pangenotypic, interferon- and ribavirin-free combination regimen approved for the treatment of chronic hepatitis C virus (HCV) infection. The objective of the current analyses was to characterize the pharmacokinetics (PK) of GLE/PIB in HCV-infected Japanese patients. Data from 332 subjects enrolled in 2 Japan phase 3 trials, CERTAIN-1 and CERTAIN-2, were used in the analyses. Pharmacokinetics of GLE/PIB were characterized using a nonlinear mixed-effects modeling. The analyses evaluated the impact of covariates (concomitant medications and demographic and clinical covariates such as renal impairment, effect of cirrhotic status) on GLE/PIB PK. GLE and PIB PK were described by 1- and 2-compartment models, respectively. Presence of cirrhosis, age, and body weight were identified as significant covariates on GLE/PIB PK. A trend toward higher GLE and PIB exposures in older patients and higher PIB exposures in heavier patients was observed; however, these increases were not considered clinically meaningful. GLE and PIB exposures were higher in HCV-infected subjects with cirrhosis (Child-Pugh A; GLE area under the plasma concentration-time curve was 160% higher, and PIB area under the plasma concentration-time curve was 21% higher) compared to subjects without cirrhosis. Renal function (including subjects with end-stage renal disease with dialysis) had no impact on GLE or PIB exposures. The GLE/PIB dose was well tolerated in the Japanese population, and no dose adjustment is needed for the evaluated intrinsic and extrinsic factors.
Sujet(s)
Acides amino-isobutyriques/pharmacocinétique , Antiviraux/pharmacocinétique , Benzimidazoles/pharmacocinétique , Cyclopropanes/pharmacocinétique , Hépatite C chronique/traitement médicamenteux , Lactames macrocycliques/pharmacocinétique , Leucine/analogues et dérivés , Proline/analogues et dérivés , Quinoxalines/pharmacocinétique , Sulfonamides/pharmacocinétique , Administration par voie orale , Adulte , Facteurs âges , Sujet âgé , Sujet âgé de 80 ans ou plus , Acides amino-isobutyriques/administration et posologie , Acides amino-isobutyriques/effets indésirables , Antiviraux/administration et posologie , Antiviraux/effets indésirables , Aire sous la courbe , Benzimidazoles/administration et posologie , Benzimidazoles/effets indésirables , Biodisponibilité , Poids , Cyclopropanes/administration et posologie , Cyclopropanes/effets indésirables , Calendrier d'administration des médicaments , Association médicamenteuse , Femelle , Hépatite C chronique/sang , Humains , Japon , Lactames macrocycliques/administration et posologie , Lactames macrocycliques/effets indésirables , Leucine/administration et posologie , Leucine/effets indésirables , Leucine/pharmacocinétique , Cirrhose du foie/génétique , Cirrhose du foie/métabolisme , Mâle , Adulte d'âge moyen , Modèles biologiques , Proline/administration et posologie , Proline/effets indésirables , Proline/pharmacocinétique , Pyrrolidines , Quinoxalines/administration et posologie , Quinoxalines/effets indésirables , Sulfonamides/administration et posologie , Sulfonamides/effets indésirables , Jeune adulteRÉSUMÉ
BACKGROUND AND OBJECTIVE: Risankizumab, a humanized monoclonal interleukin-23 antagonist antibody, has efficacy for treatment of plaque psoriasis, generalized pustular psoriasis (GPP) and erythrodermic psoriasis (EP). These analyses characterized the relationships between risankizumab exposures and key efficacy and safety variables in Japanese patients with moderate-to-severe plaque psoriasis, GPP, or EP following treatment with 75 or 150 mg subcutaneous doses at weeks 0, 4, and every 12 weeks thereafter. METHODS: Risankizumab average plasma concentrations (Cavg) were correlated with probabilities of achieving efficacy end points (PASI 75, PASI 90, PASI 100, and sPGA 0/1) using data from Japanese patients (N = 225) and non-Japanese patients (N = 1678) with moderate-to-severe plaque psoriasis enrolled in global trials, or a Japan Phase 2/3 trial. RESULTS: The exposure-efficacy relationships in Japanese patients were consistent with relationships for patients in global Phase 3 trials. At Week 16, a plateau of efficacy was demonstrated for 150 mg subcutaneous dose providing estimated PASI 90 and sPGA 0/1 response probabilities of 77%, and 88%, respectively. The exposures for 75 mg dose appeared to be suboptimal for PASI 100 response and other efficacy responses in heavier patients. Exposure-safety analyses (N = 242) indicated no apparent relationship between risankizumab Cavg and key safety variables, including any adverse event, serious adverse event, infection and infestation, and serious infection during treatment, consistent with observations in the global trials. CONCLUSIONS: Overall, risankizumab 150 mg maximized efficacy, including PASI 100 response, in Japanese patients with psoriasis with no apparent relationship between exposure and evaluated safety variables. CLINICAL TRIAL REGISTRATION: NCT03000075, NCT03022045, NCT02672852, NCT02684357, NCT02684370, NCT02694523, NCT02054481.
Sujet(s)
Anticorps monoclonaux/usage thérapeutique , Psoriasis , Anticorps monoclonaux/pharmacocinétique , Relation dose-effet des médicaments , Humains , Japon , Psoriasis/traitement médicamenteux , Indice de gravité de la maladie , Résultat thérapeutiqueRÉSUMÉ
Risankizumab, a humanized monoclonal antibody that targets interleukin-23 p19 subunit, was developed for the treatment of psoriasis. This work characterizes risankizumab pharmacokinetics in Japanese and Chinese healthy subjects compared with white healthy subjects and in Japanese patients with moderate to severe plaque psoriasis, generalized pustular psoriasis, or erythrodermic psoriasis. A phase 1, single-dose study evaluated risankizumab pharmacokinetics and safety/tolerability in healthy white (18 and 300 mg subcutaneous [SC]), Japanese (18, 90, and 300 mg SC and 200, 600, and 1200 mg intravenous [IV]), and Chinese (18, 90, and 300 mg SC) subjects; pharmacokinetic data were analyzed using noncompartmental methods. Risankizumab pharmacokinetic data from phase 2/3 studies in Japanese patients with plaque psoriasis, generalized pustular psoriasis, or erythrodermic psoriasis following multiple SC doses of 75 mg or 150 mg were analyzed using a population pharmacokinetic approach along with data from the phase 1 and global phase 1 to 3 studies. Risankizumab plasma exposures (peak plasma concentration and area under the concentration-time curve) were approximately dose-proportional across 18- to 300-mg SC or 200- to 1200-mg IV doses. Risankizumab terminal elimination half-life (harmonic mean 27-34 days) was comparable across doses and ethnicities. Risankizumab exposures were approximately 20% to 30% higher in Japanese and Chinese healthy subjects compared with white healthy subjects or in Japanese patients compared with non-Japanese patients. After accounting for body-weight differences, risankizumab exposures were comparable across ethnicities. Overall, there was no ethnic impact on risankizumab pharmacokinetics, and the small difference in exposure due to body weight has no clinical relevance.
Sujet(s)
Anticorps monoclonaux humanisés/pharmacocinétique , Anticorps monoclonaux humanisés/usage thérapeutique , Anticorps monoclonaux/pharmacocinétique , Anticorps monoclonaux/usage thérapeutique , Psoriasis/traitement médicamenteux , Adulte , Sujet âgé , Sujet âgé de 80 ans ou plus , Asiatiques , Méthode en double aveugle , Femelle , Volontaires sains , Humains , Injections sous-cutanées/méthodes , Mâle , Adulte d'âge moyen , Indice de gravité de la maladie , , Jeune adulteRÉSUMÉ
BACKGROUND & AIMS: Proton pump inhibitors (PPIs) are commonly prescribed to treat acid-related disorders. Some direct-acting antiviral regimens for chronic hepatitis C virus (HCV) infection have reduced efficacy in patients taking concomitant acid-reducing agents, including PPIs, due to interactions between drugs. We analyzed data from 9 multicenter, phase 2 and 3 trials to determine the efficacy and pharmacokinetics of an HCV therapeutic regimen comprising glecaprevir and pibrentasvir (glecaprevir/pibrentasvir) in patients taking concomitant acid-reducing agents. METHODS: We analyzed data from 2369 patients infected with HCV genotypes 1-6 and compensated liver disease treated with an all-oral regimen of glecaprevir/pibrentasvir for 8-16 weeks. We compared efficacy and pharmacokinetics among patients receiving at least 1 dose of an acid-reducing agent (a PPI, an H2 blocker, or antacid). High-dose PPI was defined as daily dose greater than 20 mg omeprazole dose equivalent. The objectives were to evaluate rate of sustained virologic response 12 weeks post-treatment (SVR12) and to assess steady-state glecaprevir and pibrentasvir exposures in patients on acid-reducing agents. RESULTS: Of the 401 patients (17%) who reported use of acid-reducing agents, 263 took PPIs (11%; 109 patients took a high-dose PPI and 154 patients took a low-dose PPI). Rates of SVR12 were 97.0% among patients who used acid-reducing agents and 97.5% among those not using acid-reducing agents (P = .6). An SVR12 was achieved in 96.3% taking a high-dose PPI and 97.4% taking a low-dose PPI, with no virologic failures in those receiving a high-dose PPI (P = .7). Glecaprevir, but not pibrentasvir, bioavailability was affected; its exposure decreased by 41% in patients taking a high-dose PPI. CONCLUSIONS: In an analysis of data from 9 clinical trials, we observed a high rate of SVR12 (approximately 97%) among patients treated with glecaprevir/pibrentasvir for HCV infection-even among patients taking concomitant ARA or high-dose PPI. This was despite decreased glecaprevir exposures in patients when on high-dose PPIs. ClinicalTrials.gov numbers, NCT02243280 (SURVEYOR-I), NCT02243293 (SURVEYOR-II), NCT02604017 (ENDURANCE-1), NCT02640482 (ENDURANCE-2), NCT02640157 (ENDURANCE-3), NCT02636595 (ENDURANCE-4), NCT02642432 (EXPEDITION-1), NCT02651194 (EXPEDITION-4), NCT02446717 (MAGELLAN-I).
Sujet(s)
Antiviraux/administration et posologie , Antiviraux/pharmacocinétique , Benzimidazoles/administration et posologie , Benzimidazoles/pharmacocinétique , Hépatite C chronique/traitement médicamenteux , Inhibiteurs de la pompe à protons/administration et posologie , Pyrrolidines/administration et posologie , Pyrrolidines/pharmacocinétique , Quinoxalines/administration et posologie , Quinoxalines/pharmacocinétique , Sulfonamides/administration et posologie , Sulfonamides/pharmacocinétique , Administration par voie orale , Adulte , Sujet âgé , Sujet âgé de 80 ans ou plus , Animaux , Essais cliniques de phase II comme sujet , Essais cliniques de phase III comme sujet , Association médicamenteuse , Interactions médicamenteuses , Femelle , Humains , Mâle , Adulte d'âge moyen , Réponse virologique soutenue , Résultat thérapeutique , Jeune adulteRÉSUMÉ
Glecaprevir (GLE) and pibrentasvir (PIB) are direct-acting antivirals coformulated as a combination tablet for once-daily treatment of chronic hepatitis C virus infection. The objective of this study was to evaluate the effect of different methods of tablet manipulations-cutting in half, grinding into powder, or crushing-on the bioavailability of GLE and PIB relative to whole film-coated bilayer tablets. This was a phase 1, single-dose, open-label, randomized, 5-period, nonfasting crossover study in 25 healthy adult male and female subjects. Intensive pharmacokinetic measurements were carried out up to 48 h after dosing on day 1 of each period. Safety and tolerability was assessed throughout the study. Compared with the reference whole tablets, cutting into half had minimal impact on GLE and PIB exposures (≤15% difference), whereas grinding or crushing the tablets resulted in lower exposures (27% to 61%) for GLE and higher exposures (21% to 83%) for PIB. These results provide guidance on appropriate administration of GLE/PIB in patients who have difficulty swallowing whole tablets.
Sujet(s)
Antiviraux/sang , Benzimidazoles/sang , Quinoxalines/sang , Sulfonamides/sang , Adulte , Acides amino-isobutyriques , Antiviraux/administration et posologie , Antiviraux/effets indésirables , Aire sous la courbe , Benzimidazoles/administration et posologie , Benzimidazoles/effets indésirables , Biodisponibilité , Études croisées , Cyclopropanes , Femelle , Humains , Lactames macrocycliques , Leucine/analogues et dérivés , Mâle , Adulte d'âge moyen , Taille de particule , Proline/analogues et dérivés , Pyrrolidines , Quinoxalines/administration et posologie , Quinoxalines/effets indésirables , Sulfonamides/administration et posologie , Sulfonamides/effets indésirables , ComprimésRÉSUMÉ
BACKGROUND: The once-daily, all oral, RBV-free, pangenotypic direct-acting anti-viral regimen consisting of co-formulated NS3/4A protease inhibitor glecaprevir and NS5A inhibitor pibrentasvir (G/P), demonstrated high rates of sustained virologic response (SVR) in phase 2 and 3 studies outside Japan. METHODS: CERTAIN-1 is a phase 3, open-label, multicenter study assessing the safety and efficacy of G/P (300/120 mg) once daily in Japanese patients with chronic HCV GT1 infection. Patients without cirrhosis received 8 weeks of G/P or 12 weeks of ombitasvir/paritaprevir/ritonavir (OBV/PTV/r, 25/150/100 mg); patients with cirrhosis received G/P for 12 weeks. The primary efficacy endpoint was non-inferiority of G/P compared to OBV/PTV/r by assessing SVR at post-treatment week 12 (SVR12) among non-cirrhotic patients without the NS5A Y93H polymorphism. RESULTS: SVR12 was achieved by 128/129 (99.2%; one patient lost to follow-up) non-cirrhotic patients in the 8-week G/P Arm (including 23/23 patients with the NS5A Y93H polymorphism) and 52/52 (100%) patients in the 12-week OBV/PTV/r Arm. No patients from the G/P Arm prematurely discontinued the study drug or experienced a treatment-emergent serious adverse event (TESAE). Three patients from the OBV/PTV/r Arm experienced five TESAEs and one of these patients discontinued the study drug due to TESAEs. All 38 (100%) patients with compensated cirrhosis achieved SVR12; in this group, no TESAEs were reported and one patient discontinued treatment due to an AE. CONCLUSIONS: CERTAIN-1 study results demonstrate high efficacy and favorable tolerability of G/P in GT1-infected Japanese patients including those with the NS5A Y93H polymorphism, with no virologic failures observed.
Sujet(s)
Antiviraux/usage thérapeutique , Benzimidazoles/usage thérapeutique , Hépatite C chronique/traitement médicamenteux , Cirrhose du foie/traitement médicamenteux , Quinoxalines/usage thérapeutique , Sulfonamides/usage thérapeutique , Adulte , Répartition par âge , Sujet âgé , Sujet âgé de 80 ans ou plus , Acides amino-isobutyriques , Anilides/usage thérapeutique , Antiviraux/effets indésirables , Antiviraux/sang , Benzimidazoles/effets indésirables , Benzimidazoles/sang , Carbamates/usage thérapeutique , Cyclopropanes , Calendrier d'administration des médicaments , Association médicamenteuse , Association de médicaments , Femelle , Hepacivirus/génétique , Hepacivirus/isolement et purification , Hépatite C chronique/sang , Hépatite C chronique/complications , Hépatite C chronique/virologie , Humains , Lactames macrocycliques , Leucine/analogues et dérivés , Cirrhose du foie/sang , Cirrhose du foie/virologie , Composés macrocycliques/usage thérapeutique , Mâle , Adulte d'âge moyen , Proline/analogues et dérivés , Pyrrolidines , Quinoxalines/effets indésirables , Quinoxalines/sang , ARN viral/sang , Ritonavir/usage thérapeutique , Sulfonamides/effets indésirables , Sulfonamides/sang , Réponse virologique soutenue , Valine , Protéines virales non structurales/génétiqueRÉSUMÉ
Glecaprevir (nonstructural protein 3/4A protease inhibitor) and pibrentasvir (nonstructural protein 5A inhibitor) (G/P), a coformulated once-daily, all oral, ribavirin (RBV)-free, direct-acting antiviral regimen, was evaluated for safety and efficacy in hepatitis C virus genotype 2 (GT2)-infected Japanese patients, including those with compensated cirrhosis. CERTAIN-2 is a phase 3, open-label, multicenter study assessing the safety and efficacy of G/P (300/120 mg) once daily in treatment-naive and interferon ± RBV treatment-experienced Japanese patients without cirrhosis but with GT2 infection. Patients were randomized 2:1 to receive 8 weeks of G/P (arm A) or 12 weeks of sofosbuvir (400 mg once daily) + RBV (600-1000 mg weight-based, twice daily) (arm B). The primary endpoint was noninferiority of G/P compared to sofosbuvir + RBV by assessing sustained virologic response at posttreatment week 12 (SVR12) among patients in the intent-to-treat population. SVR12 was also assessed in treatment-naive and interferon ± RBV treatment-experienced patients with GT2 infection and compensated cirrhosis who received G/P for 12 weeks in the CERTAIN-1 study. A total of 136 patients were enrolled in CERTAIN-2. SVR12 was achieved by 88/90 (97.8%) patients in arm A and 43/46 (93.5%) patients in arm B. No patient in arm A experienced virologic failure, while 2 did in arm B. The primary endpoint was achieved. In CERTAIN-1, 100% (18/18) of GT2-infected patients with compensated cirrhosis achieved SVR12. Treatment-emergent serious adverse events were experienced by 2 patients without cirrhosis in each arm and no patient with cirrhosis. Conclusion: The results demonstrate high efficacy and favorable tolerability of G/P in GT2-infected Japanese patients. (Hepatology 2018;67:505-513).
Sujet(s)
Antiviraux/administration et posologie , Benzimidazoles/administration et posologie , Hépatite C chronique/traitement médicamenteux , Quinoxalines/administration et posologie , Sulfonamides/administration et posologie , Adulte , Sujet âgé , Acides amino-isobutyriques , Benzimidazoles/effets indésirables , Benzimidazoles/pharmacocinétique , Cyclopropanes , Association de médicaments , Femelle , Génotype , Hépatite C chronique/virologie , Humains , Lactames macrocycliques , Leucine/analogues et dérivés , Mâle , Adulte d'âge moyen , Proline/analogues et dérivés , Pyrrolidines , Quinoxalines/effets indésirables , Quinoxalines/pharmacocinétique , Sulfonamides/effets indésirables , Sulfonamides/pharmacocinétique , Réponse virologique soutenueRÉSUMÉ
Unfortunately, in the original publication of this article, the copyright line was incorrectly published in PDF as "© The Author(s) 2017" instead of "©The Author(s) 2017 This article is an open access publication" and also the CC-BY description was not included. The description should be as follows.
RÉSUMÉ
BACKGROUND: Once-daily, orally administered, co-formulated glecaprevir (NS3/4A protease inhibitor) and pibrentasvir (NS5A inhibitor) (G/P) demonstrated pangenotypic activity and high sustained virologic response (SVR) rates in studies outside Japan. Here we report safety and efficacy in a subset of Japanese patients with chronic HCV infection who received G/P 300/120 mg in a phase 3, open-label, multicenter study (CERTAIN-1). METHODS: This analysis focuses on three difficult-to-treat subgroups: HCV GT1/2-infected patients who failed to achieve SVR after treatment with a direct acting antiviral (DAA)-containing regimen; GT1/2-infected patients with severe renal impairment (estimated glomerular filtration rate < 30 mL/min/1.73 m2); and GT3-infected patients. Patients in the renal impairment and GT3 cohorts were treatment-naive or interferon treatment-experienced. Noncirrhotic GT1/2-infected, DAA-naïve patients in the renal impairment cohort received G/P for 8 weeks; all other patients were treated for 12 weeks. Primary outcome was SVR (HCV RNA < 15 IU/mL) 12 weeks post-treatment (SVR12). RESULTS: The study enrolled 33 GT1/2-infected patients who failed previous DAA treatment (four with cirrhosis); 12 GT1/2-infected patients with severe renal impairment (two with cirrhosis); and 12 GT3-infected patients (two with cirrhosis). SVR12 was achieved by 31/33 (93.9%), 12/12 (100%), and 10/12 (83.3%) patients, respectively. One serious adverse event (fluid overload, not related to G/P) occurred in a patient on chronic intermittent hemodialysis. CONCLUSIONS: G/P achieved high SVR12 rates and was well tolerated in three difficult-to-treat patient subgroups with limited treatment options in Japan (DAA-experienced patients, patients with severe renal impairment, and GT3-infected patients). These results support the potential suitability of this regimen for these special populations in Japan.
Sujet(s)
Antiviraux/usage thérapeutique , Benzimidazoles/usage thérapeutique , Hepacivirus/génétique , Hépatite C chronique/traitement médicamenteux , Quinoxalines/usage thérapeutique , Insuffisance rénale/complications , Sulfonamides/usage thérapeutique , Adolescent , Adulte , Sujet âgé , Acides amino-isobutyriques , Antiviraux/effets indésirables , Benzimidazoles/effets indésirables , Cyclopropanes , Association de médicaments , Femelle , Génotype , Hepacivirus/isolement et purification , Hépatite C chronique/complications , Hépatite C chronique/virologie , Humains , Lactames macrocycliques , Leucine/analogues et dérivés , Mâle , Adulte d'âge moyen , Proline/analogues et dérivés , Pyrrolidines , Quinoxalines/effets indésirables , ARN viral/sang , Sulfonamides/effets indésirables , Réponse virologique soutenue , Échec thérapeutique , Résultat thérapeutique , Jeune adulteRÉSUMÉ
Glioblastoma (GBM) is a lethal and aggressive brain tumor that is resistant to conventional radiation and cytotoxic chemotherapies. Molecularly targeted agents hold great promise in treating these genetically heterogeneous tumors, yet have produced disappointing results. One reason for the clinical failure of these novel therapies can be the inability of the drugs to achieve effective concentrations in the invasive regions beyond the bulk tumor. In this review, we describe the influence of the blood-brain barrier on the distribution of anticancer drugs to both the tumor core and infiltrative regions of GBM. We further describe potential strategies to overcome these drug delivery limitations. Understanding the key factors that limit drug delivery into brain tumors will guide future development of approaches for enhanced delivery of effective drugs to GBM.
