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Background:
Objectives:
-To understand how HIV medicine and blood clot medicine interact, so doctors can choose what to prescribe for people who take both.
Eligibility:
Design:
Full description
Advances in antiretroviral (ARV) pharmacotherapy have translated to increased longevity and improved quality of life in people living with HIV; hence, elderly individuals comprise an increasing proportion of today s HIV population. Moreover, HIV infection itself has become recognized as a condition characterized by a hypercoaguable state and premature immunologic aging. Potential interactions between ARVs and anticoagulant medications are of particular concern considering that many elderly, and even non-elderly HIV patients will require short-term or chronic anticoagulation to prevent and/or treat systemic embolism. Dabigatran, administered as dabigatran etexilate, is an oral irreversible, competitive direct thrombin inhibitor, which has been shown to be superior to warfarin, and non-inferior to enoxaparin, in preventing thromboembolism in patients with atrial fibrillation and undergoing orthopedic surgery, respectively.
While dabigatran itself is not a substrate of Permeability-glycoprotein (P-gp), its inactivepro-drug, dabigatran etexilate, is a substrate of P-gp. Co-administration of dabigatran etexilate with P-gp modulators has resulted in significant changes in dabigatran exposure. The pharmacokinetic enhancers, ritonavir and cobicistat, as inhibitors of P-gp, are expected to increase plasma concentrations of dabigatran; however, neither agent has been studied in combination with dabigatran etexilate, to date. Hence, the purpose of this study is to determine whether the separate co-administration of ritonavir or cobicistat with dabigatran etexilate increases the systemic exposure of dabigatran in healthy volunteers, and if so, whether adjusting the administration times of these medications can circumvent this interaction.
In this open-label study, 32 healthy volunteers will be assigned to 1 of 2 groups. Group A will consist of 16 subjects who will take 22 days of ritonavir; Group B will consist of 16 subjects who will take 22 days of cobicistat. All subjects will receive 3 separated single doses of dabigatran etexilate. Pharmacokinetic (PK) and pharmacodynamics (PD) sampling for dabigatran will occur on Days 0 1, Day 19 1 20, and Day 26 1 27.
The PD effects of dabigatran will be characterized via ecarin clotting time (ECT) measurements. Dabigatran PK/PD parameters will be determined using non-compartmental methods with the WinNonlin professional computer program (version 5.2; Pharsight Corporation, Mountain View, CA). The following PK/PD parameters will be compared between the groups: area under the curve from 0 to 24 hours (AUC0-24), maximum total dabigatran plasma concentration (Cmax), area under the curve from 0 to infinity hours (AUC0- ), time to maximum plasma concentration (tmax), terminal half-life (T (Omega)), apparent oral clearance (CL/F), area under the effect curve from 0 to 24 hours (AUEC0-24), and the maximum effect ratio over baseline (ERmax).
Enrollment
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Inclusion and exclusion criteria
A subject will be considered eligible for this study only if all of the following criteria are met:
EXCLUSION CRITERIA:
A subject will be ineligible for this study if 1, or more, of the following criteria are met:
History of HIV exposure/infection, as determined by positive ELISA/ Western Blot.
History or presence of any of the following:
History or presence of the following:
bleeding/hematologic disorders (hemophilia, etc.)
serious/major bleeding event (intracranial, gastrointestinal, as assessed by patient interview)
c. current increased risk of bleeding (as indicated by aPTT >1.5 times ULN], platelets, PLT, <150,000/mm3, or Hgb <11 g/dL)
d. for female subjects, menorrhagia
Planned invasive or surgical procedure within (prior to, or following) 28 days of study participation.
Fasting total cholesterol >270 mg/dL or fasting triglycerides >270 mg/dL.
Fasting glucose >125 mg/dL.
Concomitant routine therapy with any prescription, over-the-counter, herbal, or holistic medications, including hormonal contraceptives by any route, or any investigational drugs for 30 days prior to receipt of any study medications (Day 0).
Concomitant therapy (chronic or intermittent) with any prescription, over-the-counter, herbal, or holistic medications will not be allowed during the study duration
Intermittent use of acetaminophen and loperamide will be allowed to have been taken, according to each manufacturer s recommendations, within 30 days prior to study participation
Intermittent use of acetaminophen, loperamide, and/or an antiemetic (as approved by the Principal Investigator) will be allowed to be taken according to each manufacturer s recommendations during the study. As P-gp substrates, loperamide and certain anti-emetics (i.e. ondansetron), should not be taken on the days of pharmacokinetic blood sampling
A daily multivitamin with minerals will be allowed during the study
Receipt of influenza vaccination will be allowed prior, during,
and/or after the study
Use of topical medications that are not significantly absorbed systemically will be allowed if approved by the Principal Investigator
Inability to obtain venous access for sample collection.
Inability to swallow whole capsules and/or tablets.
Positive serum or urine pregnancy test or breastfeeding female.
The presence of persistent diarrhea or malabsorption that could interferewith the subject s ability to absorb drugs.
Drug or alcohol use that may impair safety or adherence.
Use of nicotine-containing tobacco products, including cigarettes and chewing tobacco.
History of intolerance or allergic reaction (rash; hives; swollen lips;difficulty breathing) to DE, RTV, or COBI.
Organ transplant recipient.
Primary purpose
Allocation
Interventional model
Masking
40 participants in 2 patient groups
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Data sourced from clinicaltrials.gov
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