Randomised clinical trial: safety, tolerability, pharmacokinetics and pharmacodynamics of repeated doses of TAK‐438 (vonoprazan), a novel potassium‐competitive acid blocker, in healthy male subjects

Summary Background TAK‐438 (vonoprazan) is a potassium‐competitive acid blocker that reversibly inhibits gastric H+, K+‐ATPase. Aim To evaluate the safety, tolerability, pharmacokinetics and pharmacodynamics of TAK‐438 in healthy Japanese and non‐Japanese men. Methods In two Phase I, randomised, dou...

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Published in	Alimentary pharmacology & therapeutics Vol. 41; no. 7; pp. 636 - 648
Main Authors	Jenkins, H., Sakurai, Y., Nishimura, A., Okamoto, H., Hibberd, M., Jenkins, R., Yoneyama, T., Ashida, K., Ogama, Y., Warrington, S.
Format	Journal Article
Language	English
Published	England Blackwell Publishing Ltd 01.04.2015
Subjects	Adult Asian Continental Ancestry Group Dose-Response Relationship, Drug Double-Blind Method European Continental Ancestry Group Gastric Acid Gastrointestinal Agents - adverse effects Gastrointestinal Agents - pharmacokinetics Gastrointestinal Agents - pharmacology Half-Life Humans Japan Male Metabolic Clearance Rate Middle Aged Nervous System Diseases Potassium - pharmacology Pyrroles - adverse effects Pyrroles - pharmacokinetics Pyrroles - pharmacology Randomised Clinical Trials Sulfonamides - adverse effects Sulfonamides - pharmacokinetics Sulfonamides - pharmacology United Kingdom Young Adult
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Abstract	Summary Background TAK‐438 (vonoprazan) is a potassium‐competitive acid blocker that reversibly inhibits gastric H+, K+‐ATPase. Aim To evaluate the safety, tolerability, pharmacokinetics and pharmacodynamics of TAK‐438 in healthy Japanese and non‐Japanese men. Methods In two Phase I, randomised, double‐blind, placebo‐controlled studies, healthy men (Japan N = 60; UK N = 48) received TAK‐438 10–40 mg once daily at a fixed dose level for 7 consecutive days. Assessments included safety, tolerability, pharmacokinetics and pharmacodynamics (intragastric pH). Results Plasma concentration–time profiles of TAK‐438 at all dose levels showed rapid absorption (median Tmax ≤2 h). Mean elimination half‐life was up to 9 h. Exposure was slightly greater than dose proportional, with no apparent time‐dependent inhibition of metabolism. There was no important difference between the two studies in AUC0‐tau on Day 7. TAK‐438 caused dose‐dependent acid suppression. On Day 7, mean 24‐h intragastric pH>4 holding time ratio (HTR) with 40 mg TAK‐438 was 100% (Japan) and 93.2% (UK), and mean night‐time pH>4 HTR was 100% (Japan) and 90.4% (UK). TAK‐438 was well tolerated. The frequency of adverse events was similar at all dose levels and there were no serious adverse events. There were no important increases in serum alanine transaminase activity. Serum gastrin and pepsinogen I and II concentrations increased with TAK‐438 dose. Conclusions TAK‐438 in multiple rising oral dose levels of 10–40 mg once daily for 7 days was safe and well tolerated in healthy men and caused rapid, profound and sustained suppression of gastric acid secretion throughout each 24‐h dosing interval. Clinicaltrials.gov identifiers: NCT02123953 and NCT02141711.
AbstractList	TAK-438 (vonoprazan) is a potassium-competitive acid blocker that reversibly inhibits gastric H(+) , K(+) -ATPase. To evaluate the safety, tolerability, pharmacokinetics and pharmacodynamics of TAK-438 in healthy Japanese and non-Japanese men. In two Phase I, randomised, double-blind, placebo-controlled studies, healthy men (Japan N = 60; UK N = 48) received TAK-438 10-40 mg once daily at a fixed dose level for 7 consecutive days. Assessments included safety, tolerability, pharmacokinetics and pharmacodynamics (intragastric pH). Plasma concentration-time profiles of TAK-438 at all dose levels showed rapid absorption (median Tmax ≤2 h). Mean elimination half-life was up to 9 h. Exposure was slightly greater than dose proportional, with no apparent time-dependent inhibition of metabolism. There was no important difference between the two studies in AUC0-tau on Day 7. TAK-438 caused dose-dependent acid suppression. On Day 7, mean 24-h intragastric pH>4 holding time ratio (HTR) with 40 mg TAK-438 was 100% (Japan) and 93.2% (UK), and mean night-time pH>4 HTR was 100% (Japan) and 90.4% (UK). TAK-438 was well tolerated. The frequency of adverse events was similar at all dose levels and there were no serious adverse events. There were no important increases in serum alanine transaminase activity. Serum gastrin and pepsinogen I and II concentrations increased with TAK-438 dose. TAK-438 in multiple rising oral dose levels of 10-40 mg once daily for 7 days was safe and well tolerated in healthy men and caused rapid, profound and sustained suppression of gastric acid secretion throughout each 24-h dosing interval. Clinicaltrials.gov identifiers: NCT02123953 and NCT02141711. TAK-438 (vonoprazan) is a potassium-competitive acid blocker that reversibly inhibits gastric H(+) , K(+) -ATPase.BACKGROUNDTAK-438 (vonoprazan) is a potassium-competitive acid blocker that reversibly inhibits gastric H(+) , K(+) -ATPase.To evaluate the safety, tolerability, pharmacokinetics and pharmacodynamics of TAK-438 in healthy Japanese and non-Japanese men.AIMTo evaluate the safety, tolerability, pharmacokinetics and pharmacodynamics of TAK-438 in healthy Japanese and non-Japanese men.In two Phase I, randomised, double-blind, placebo-controlled studies, healthy men (Japan N = 60; UK N = 48) received TAK-438 10-40 mg once daily at a fixed dose level for 7 consecutive days. Assessments included safety, tolerability, pharmacokinetics and pharmacodynamics (intragastric pH).METHODSIn two Phase I, randomised, double-blind, placebo-controlled studies, healthy men (Japan N = 60; UK N = 48) received TAK-438 10-40 mg once daily at a fixed dose level for 7 consecutive days. Assessments included safety, tolerability, pharmacokinetics and pharmacodynamics (intragastric pH).Plasma concentration-time profiles of TAK-438 at all dose levels showed rapid absorption (median Tmax ≤2 h). Mean elimination half-life was up to 9 h. Exposure was slightly greater than dose proportional, with no apparent time-dependent inhibition of metabolism. There was no important difference between the two studies in AUC0-tau on Day 7. TAK-438 caused dose-dependent acid suppression. On Day 7, mean 24-h intragastric pH>4 holding time ratio (HTR) with 40 mg TAK-438 was 100% (Japan) and 93.2% (UK), and mean night-time pH>4 HTR was 100% (Japan) and 90.4% (UK). TAK-438 was well tolerated. The frequency of adverse events was similar at all dose levels and there were no serious adverse events. There were no important increases in serum alanine transaminase activity. Serum gastrin and pepsinogen I and II concentrations increased with TAK-438 dose.RESULTSPlasma concentration-time profiles of TAK-438 at all dose levels showed rapid absorption (median Tmax ≤2 h). Mean elimination half-life was up to 9 h. Exposure was slightly greater than dose proportional, with no apparent time-dependent inhibition of metabolism. There was no important difference between the two studies in AUC0-tau on Day 7. TAK-438 caused dose-dependent acid suppression. On Day 7, mean 24-h intragastric pH>4 holding time ratio (HTR) with 40 mg TAK-438 was 100% (Japan) and 93.2% (UK), and mean night-time pH>4 HTR was 100% (Japan) and 90.4% (UK). TAK-438 was well tolerated. The frequency of adverse events was similar at all dose levels and there were no serious adverse events. There were no important increases in serum alanine transaminase activity. Serum gastrin and pepsinogen I and II concentrations increased with TAK-438 dose.TAK-438 in multiple rising oral dose levels of 10-40 mg once daily for 7 days was safe and well tolerated in healthy men and caused rapid, profound and sustained suppression of gastric acid secretion throughout each 24-h dosing interval. Clinicaltrials.gov identifiers: NCT02123953 and NCT02141711.CONCLUSIONSTAK-438 in multiple rising oral dose levels of 10-40 mg once daily for 7 days was safe and well tolerated in healthy men and caused rapid, profound and sustained suppression of gastric acid secretion throughout each 24-h dosing interval. Clinicaltrials.gov identifiers: NCT02123953 and NCT02141711. Summary Background TAK‐438 (vonoprazan) is a potassium‐competitive acid blocker that reversibly inhibits gastric H+, K+‐ATPase. Aim To evaluate the safety, tolerability, pharmacokinetics and pharmacodynamics of TAK‐438 in healthy Japanese and non‐Japanese men. Methods In two Phase I, randomised, double‐blind, placebo‐controlled studies, healthy men (Japan N = 60; UK N = 48) received TAK‐438 10–40 mg once daily at a fixed dose level for 7 consecutive days. Assessments included safety, tolerability, pharmacokinetics and pharmacodynamics (intragastric pH). Results Plasma concentration–time profiles of TAK‐438 at all dose levels showed rapid absorption (median Tmax ≤2 h). Mean elimination half‐life was up to 9 h. Exposure was slightly greater than dose proportional, with no apparent time‐dependent inhibition of metabolism. There was no important difference between the two studies in AUC0‐tau on Day 7. TAK‐438 caused dose‐dependent acid suppression. On Day 7, mean 24‐h intragastric pH>4 holding time ratio (HTR) with 40 mg TAK‐438 was 100% (Japan) and 93.2% (UK), and mean night‐time pH>4 HTR was 100% (Japan) and 90.4% (UK). TAK‐438 was well tolerated. The frequency of adverse events was similar at all dose levels and there were no serious adverse events. There were no important increases in serum alanine transaminase activity. Serum gastrin and pepsinogen I and II concentrations increased with TAK‐438 dose. Conclusions TAK‐438 in multiple rising oral dose levels of 10–40 mg once daily for 7 days was safe and well tolerated in healthy men and caused rapid, profound and sustained suppression of gastric acid secretion throughout each 24‐h dosing interval. Clinicaltrials.gov identifiers: NCT02123953 and NCT02141711.
Author	Hibberd, M. Jenkins, R. Okamoto, H. Jenkins, H. Yoneyama, T. Nishimura, A. Ogama, Y. Ashida, K. Sakurai, Y. Warrington, S.
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BackLink	https://www.ncbi.nlm.nih.gov/pubmed/25707624$$D View this record in MEDLINE/PubMed
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Snippet	Summary Background TAK‐438 (vonoprazan) is a potassium‐competitive acid blocker that reversibly inhibits gastric H+, K+‐ATPase. Aim To evaluate the safety,... TAK-438 (vonoprazan) is a potassium-competitive acid blocker that reversibly inhibits gastric H(+) , K(+) -ATPase. To evaluate the safety, tolerability,... TAK-438 (vonoprazan) is a potassium-competitive acid blocker that reversibly inhibits gastric H(+) , K(+) -ATPase.BACKGROUNDTAK-438 (vonoprazan) is a...
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SubjectTerms	Adult Asian Continental Ancestry Group Dose-Response Relationship, Drug Double-Blind Method European Continental Ancestry Group Gastric Acid Gastrointestinal Agents - adverse effects Gastrointestinal Agents - pharmacokinetics Gastrointestinal Agents - pharmacology Half-Life Humans Japan Male Metabolic Clearance Rate Middle Aged Nervous System Diseases Potassium - pharmacology Pyrroles - adverse effects Pyrroles - pharmacokinetics Pyrroles - pharmacology Randomised Clinical Trials Sulfonamides - adverse effects Sulfonamides - pharmacokinetics Sulfonamides - pharmacology United Kingdom Young Adult
Title	Randomised clinical trial: safety, tolerability, pharmacokinetics and pharmacodynamics of repeated doses of TAK‐438 (vonoprazan), a novel potassium‐competitive acid blocker, in healthy male subjects
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