Mcgowan, I and Hoesley, C and Cranston, RD and Andrew, P and Janocko, L and Dai, JY and Carballo-Dieguez, A and Ayudhya, RKN and Piper, J and Hladik, F and Mayer, K
(2013)
A Phase 1 Randomized, Double Blind, Placebo Controlled Rectal Safety and Acceptability Study of Tenofovir 1% Gel (MTN-007).
PLoS ONE, 8 (4).
Abstract
Objective: Rectal microbicides are needed to reduce the risk of HIV acquisition associated with unprotected receptive anal intercourse. The MTN-007 study was designed to assess the safety (general and mucosal), adherence, and acceptability of a new reduced glycerin formulation of tenofovir 1% gel. Methods: Participants were randomized 1:1:1:1 to receive the reduced glycerin formulation of tenofovir 1% gel, a hydroxyethyl cellulose placebo gel, a 2% nonoxynol-9 gel, or no treatment. Each gel was administered as a single dose followed by 7 daily doses. Mucosal safety evaluation included histology, fecal calprotectin, epithelial sloughing, cytokine expression (mRNA and protein), microarrays, flow cytometry of mucosal T cell phenotype, and rectal microflora. Acceptability and adherence were determined by computer-administered questionnaires and interactive telephone response, respectively. Results: Sixty-five participants (45 men and 20 women) were recruited into the study. There were no significant differences between the numbers of ≥ Grade 2 adverse events across the arms of the study. Likelihood of future product use (acceptability) was 87% (reduced glycerin formulation of tenofovir 1% gel), 93% (hydroxyethyl cellulose placebo gel), and 63% (nonoxynol-9 gel). Fecal calprotectin, rectal microflora, and epithelial sloughing did not differ by treatment arms during the study. Suggestive evidence of differences was seen in histology, mucosal gene expression, protein expression, and T cell phenotype. These changes were mostly confined to comparisons between the nonoxynol-9 gel and other study arms. Conclusions: The reduced glycerin formulation of tenofovir 1% gel was safe and well tolerated rectally and should be advanced to Phase 2 development. Trial Registration: ClinicalTrials.gov NCT01232803.
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| Item Type: |
Article
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| Status: |
Published |
| Creators/Authors: |
| Creators | Email | Pitt Username | ORCID  |
|---|
| Mcgowan, I | imcgowan@pitt.edu | IMCGOWAN | | | Hoesley, C | | | | | Cranston, RD | rdc27@pitt.edu | RDC27 | | | Andrew, P | | | | | Janocko, L | | | | | Dai, JY | | | | | Carballo-Dieguez, A | | | | | Ayudhya, RKN | | | | | Piper, J | | | | | Hladik, F | | | | | Mayer, K | | | |
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| Date: |
3 April 2013 |
| Date Type: |
Publication |
| Journal or Publication Title: |
PLoS ONE |
| Volume: |
8 |
| Number: |
4 |
| DOI or Unique Handle: |
10.1371/journal.pone.0060147 |
| Schools and Programs: |
School of Medicine > Medicine |
| Refereed: |
Yes |
| PubMed ID: |
23573238 |
| Date Deposited: |
22 Apr 2013 16:11 |
| Last Modified: |
13 Oct 2017 18:55 |
| URI: |
http://d-scholarship.pitt.edu/id/eprint/18323 |
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