Clinical Trials/NCT01622673

NCT01622673

Completed

Phase 1

A Study to Evaluate the Effect of Metal Cation-Containing Antacids on Raltegravir Pharmacokinetics in HIV-Infected Subjects on a Stable Raltegravir-Containing Regimen

Merck Sharp & Dohme LLC0 sites27 target enrollmentJune 2012

ConditionsHIV Infections

InterventionsRaltegravir TUMS® Ultra Strength MINTOX® Maximum Strength

DrugsRaltegravir TUMS® Ultra Strength MINTOX® Maximum Strength

Overview

Phase: Phase 1
Intervention: Raltegravir
Conditions: HIV Infections
Sponsor: Merck Sharp & Dohme LLC
Enrollment: 27
Primary Endpoint: Least Squares Mean Steady State Plasma Concentration (C12hrs) of Raltegravir After Coadministration of Antacid (Primary Hypothesis)
Status: Completed
Last Updated: 9 years ago

Overview Investigators Eligibility Criteria Arms & Interventions Outcomes Similar Trials

Overview

Brief Summary

This study will evaluate: (1) the effect of co-administration of single doses of calcium carbonate antacid and magnesium/aluminum hydroxide antacid on the steady-state plasma pharmacokinetic profile of raltegravir in human immunodeficiency virus (HIV)-infected participants; and (2) the effect of staggered dosing of a single dose of a magnesium/aluminum hydroxide antacid 2 hours before and 2 hours after administration of raltegravir on the steady-state plasma pharmacokinetic profile of raltegravir in the same participants.

The study will determine whether (1) the C12hrs of steady-state raltegravir after co-administration of single doses of calcium carbonate antacid is decreased to a clinically meaningful degree compared with C12hrs after administration of raltegravir alone; and whether (2) the C12hrs of steady-state raltegravir after co-administration of a single dose of magnesium/aluminum hydroxide antacid is decreased to a clinically meaningful degree compared with the C12hrs after administration of raltegravir alone.

Registry

clinicaltrials.gov

Start Date

June 2012

End Date

October 2012

Last Updated

9 years ago

Study Type

Interventional

Study Design

Crossover

Sex

All

Investigators

Sponsor

Merck Sharp & Dohme LLC

Responsible Party

Sponsor

Eligibility Criteria

Inclusion Criteria

•HIV-infected participant on a stable raltegravir dose (400 mg every 12 hours) as part of a stable anti-retroviral regimen (ARV) for at least 1 month and will maintain current ARV therapy throughout the study
•Body Mass Index ≤32 kg/m\^2
•Good general health
•Can be a current smoker and/or user of nicotine or nicotine-containing products, but use of nicotine-containing products will not be permitted during the stay at the clinical research site

Exclusion Criteria

•History of gastric bypass surgery
•Pregnant or nursing
•Mentally or legally incapacitated, has significant emotional problems, or has a history of a clinically significant psychiatric disorder; participants who have had situational depression may be enrolled at the discretion of the investigator.
•History of stroke, chronic seizures, or major neurological disorder
•History of clinically significant endocrine, gastrointestinal, cardiovascular, hematological, hepatic, immunological, renal, respiratory, or genitourinary abnormalities or diseases (excluding HIV); participants with a history of uncomplicated kidney stones or childhood asthma may be enrolled at the discretion of the investigator.
•Active neoplastic disease deemed unstable or progressing by the investigator
•Currently taking rifampin or unable to refrain from use of any proton pump inhibitor and any histamine-2 (H2)-blockers, over-the-counter antacids, calcium supplements, or multivitamins during the study
•Consumes excessive amounts of alcohol
•Consumes excessive amounts of coffee, tea, cola, or other caffeinated beverages
•Major surgery or blood donation within the past 4 weeks

Arms & Interventions

RAL, TUMS+RAL, MINTOX+RAL, MINTOX Before RAL, MINTOX After RAL

Participants received Raltegravir in treatment period 1, followed by TUMS® + Raltegravir in treatment period 2, followed by MINTOX® + Raltegravir in treatment period 3, followed by MINTOX® 2 hours before Raltegravir in treatment period 4, followed by MINTOX® 2 hours After Raltegravir in treatment period 5. There was a 2-day washout between treatment periods.

Intervention: Raltegravir

RAL, TUMS+RAL, MINTOX+RAL, MINTOX Before RAL, MINTOX After RAL

Intervention: TUMS® Ultra Strength

RAL, TUMS+RAL, MINTOX+RAL, MINTOX Before RAL, MINTOX After RAL

Intervention: MINTOX® Maximum Strength

TUMS+RAL, MINTOX+RAL, RAL, MINTOX Before RAL, MINTOX After RAL

Participants received TUMS® + Raltegravir in treatment period 1, followed by MINTOX® + Raltegravir in treatment period 2, followed by Raltegravir in treatment period 3, followed by MINTOX® 2 hours before Raltegravir in treatment period 4, followed by MINTOX® 2 hours after Raltegravir in treatment period 5. There was a minimum 2-day washout between treatment periods.

Intervention: Raltegravir

TUMS+RAL, MINTOX+RAL, RAL, MINTOX Before RAL, MINTOX After RAL

Intervention: TUMS® Ultra Strength

TUMS+RAL, MINTOX+RAL, RAL, MINTOX Before RAL, MINTOX After RAL

Intervention: MINTOX® Maximum Strength

MINTOX+RAL, RAL, TUMS+RAL, MINTOX Before RAL, MINTOX After RAL

Participants received MINTOX® + Raltegravir in treatment period 1, followed by Raltegravir in treatment period 2, followed by TUMS® + Raltegravir in treatment period 3, followed by MINTOX® 2 hours before Raltegravir in treatment period 4, followed by MINTOX® 2 hours after Raltegravir in treatment period 5. There was a minimum 2-day washout between treatment periods.

Intervention: Raltegravir

MINTOX+RAL, RAL, TUMS+RAL, MINTOX Before RAL, MINTOX After RAL

Intervention: TUMS® Ultra Strength

MINTOX+RAL, RAL, TUMS+RAL, MINTOX Before RAL, MINTOX After RAL

Intervention: MINTOX® Maximum Strength

RAL, MINTOX+RAL, TUMS+RAL, MINTOX After RAL, MINTOX Before RAL

Participants received Raltegravir in treatment period 1, followed by MINTOX® + Raltegravir in treatment period 2, followed by TUMS® + Raltegravir in treatment period 3, followed by MINTOX® 2 hours after Raltegravir in treatment period 4, followed by MINTOX® 2 hours before Raltegravir in treatment period 5. There was a minimum 2-day washout between treatment periods.

Intervention: Raltegravir

RAL, MINTOX+RAL, TUMS+RAL, MINTOX After RAL, MINTOX Before RAL

Intervention: TUMS® Ultra Strength

RAL, MINTOX+RAL, TUMS+RAL, MINTOX After RAL, MINTOX Before RAL

Intervention: MINTOX® Maximum Strength

TUMS+RAL, RAL, MINTOX+RAL, MINTOX After RAL, MINTOX Before RAL

Participants received TUMS® + Raltegravir in treatment period 1, followed by Raltegravir in treatment period 2, followed by MINTOX® + Raltegravir in treatment period 3, followed by MINTOX® 2 hours after Raltegravir in treatment period 4, followed by MINTOX® 2 hours before Raltegravir in treatment period 5. There was a minimum 2-day washout between treatment periods.

Intervention: Raltegravir

TUMS+RAL, RAL, MINTOX+RAL, MINTOX After RAL, MINTOX Before RAL

Intervention: TUMS® Ultra Strength

TUMS+RAL, RAL, MINTOX+RAL, MINTOX After RAL, MINTOX Before RAL

Intervention: MINTOX® Maximum Strength

MINTOX+RAL, TUMS+RAL, RAL, MINTOX After RAL, MINTOX Before RAL

Participants received MINTOX® + Raltegravir in treatment period 1, followed by TUMS® + Raltegravir in treatment period 2, followed by Raltegravir in treatment period 3, followed by MINTOX® 2 hours after Raltegravir in treatment period 4, followed by MINTOX® 2 hours before Raltegravir in treatment period 5. There was a minimum 2-day washout between treatment periods.

Intervention: Raltegravir

MINTOX+RAL, TUMS+RAL, RAL, MINTOX After RAL, MINTOX Before RAL

Intervention: TUMS® Ultra Strength

MINTOX+RAL, TUMS+RAL, RAL, MINTOX After RAL, MINTOX Before RAL

Intervention: MINTOX® Maximum Strength

Outcomes

Primary Outcomes

Least Squares Mean Steady State Plasma Concentration (C12hrs) of Raltegravir After Coadministration of Antacid (Primary Hypothesis)

Time Frame: 12 hours postdose

Participant blood samples were collected to measure the steady state plasma concentration of raltegravir 12 hours after administration alone or with a single dose of antacid. The primary hypothesis compared C12hrs of raltegravir when administered alone with C12hrs of raltegravir when coadministered with TUMS® or MINTOX®.

Least Squares Mean Steady State Area Under the Plasma Concentration-time Curve (AUC0-12hrs) of Raltegravir After Coadministration of Antacid (Primary Hypothesis)

Time Frame: Predose, 0.5, 1, 1.5, 2, 3, 4, 6, 8, and 12 hours postdose

Participant blood samples were collected to measure the steady state AUC of raltegravir up to 12 hours after administration alone or with a single dose of antacid. The primary hypothesis compared AUC0-12hrs of raltegravir when administered alone with AUC0-12hrs of raltegravir when coadministered with TUMS® or MINTOX®.

Least Squares Mean Steady State Area Under the Plasma Concentration-Time (AUC0-12hrs) of Raltegravir After Staggered Administration of Antacid (Secondary Hypothesis)

Time Frame: Predose, 0.5, 1, 1.5, 2, 3, 4, 6, 8, and 12 hours postdose

Participant blood samples were collected to measure the steady state AUC of raltegravir up to 12 hours after administration alone or before or after a single dose of antacid. The secondary hypothesis compared AUC0-12hrs of raltegravir when administered alone with AUC0-12hrs of raltegravir when administered 2 hours before or after MINTOX®.

Least Squares Mean Maximum Plasma Concentration (Cmax) of Raltegravir After Coadministration of Antacid (Primary Hypothesis)

Time Frame: Predose, 0.5, 1, 1.5, 2, 3, 4, 6, 8, and 12 hours postdose

Participant blood samples were collected to measure the steady state maximum plasma concentration of raltegravir when administered alone or with a single dose of antacid. The primary hypothesis compared Cmax of raltegravir when administered alone with Cmax of raltegravir when coadministered with TUMS® or MINTOX®.

Least Squares Mean Steady State Plasma Concentration (C12hrs) of Raltegravir After Staggered Administration of Antacid (Secondary Hypothesis)

Time Frame: 12 hours postdose

Participant blood samples were collected to measure the steady state plasma concentration of raltegravir 12 hours after administration alone or before or after a single dose of antacid. The secondary hypothesis compared C12hrs of raltegravir when administered alone with C12hrs of raltegravir when administered 2 hours before or after MINTOX®.

Least Squares Mean Maximum Plasma Concentration (Cmax) of Raltegravir After Staggered Administration of Antacid (Secondary Hypothesis)

Time Frame: Predose, 0.5, 1, 1.5, 2, 3, 4, 6, 8, and 12 hours postdose

Participant blood samples were collected to measure the maximum steady state plasma concentration of raltegravir after administration alone or before or after a single dose of antiacid. The secondary hypothesis compared Cmax of raltegravir when administered alone with Cmax of raltegravir when administered 2 hours before or after MINTOX®.

Mean Time to Maximum Plasma Concentration (Tmax) of Raltegravir

Time Frame: Predose, 0.5, 1, 1.5, 2, 3, 4, 6, 8, and 12 hours postdose

Participant blood samples were collected to measure the time to achieve the maximum steady state plasma concentration of raltegravir when administered alone or with a single dose of antacid

Number of Participants With Any Clinical or Laboratory Adverse Event (AE)

Time Frame: Up to 7 days after the last dose of study drug

An AE is defined as any unfavorable and unintended change in the structure, function, or chemistry of the body temporally associated with the use of the study drug, whether or not considered related to the use of the product. Any worsening of a preexisting condition which is temporally associated with the use of the study drug is also an adverse experience.