Microbicides The Population Council Experience and Future Directions Don E. Waldron Medical Director Don E. Waldron Medical Director
HistoryHistory Early research in the late 80’s identified large molecular structured entity derived from sea weed as a potential HIV blocking agent In vitro tissue studies showed Carraguard ® protective against HIV In vivo mouse and monkey experiments demonstrated blocking Methyl cellulose placebo was not protective against HIV Early research in the late 80’s identified large molecular structured entity derived from sea weed as a potential HIV blocking agent In vitro tissue studies showed Carraguard ® protective against HIV In vivo mouse and monkey experiments demonstrated blocking Methyl cellulose placebo was not protective against HIV
Phase I Trials conducted in many countries including South Africa (SA) Results showed that Carraguard ® is safe and acceptable Couples study for male tolerance and acceptability is under analysis Two studies in HIV positive cohorts are underway Trials conducted in many countries including South Africa (SA) Results showed that Carraguard ® is safe and acceptable Couples study for male tolerance and acceptability is under analysis Two studies in HIV positive cohorts are underway
Phase II Experience (Preliminary Observations) Two trials conducted in Thailand (165) and SA (400), two arms, Intent to Treat (ITT) Safety and acceptability confirmed Condom use similar in both arms with condom usage in Thailand higher than in SA Recruitment and retention similar for both arms Seroconversions only in SA, 8 in each arm Two trials conducted in Thailand (165) and SA (400), two arms, Intent to Treat (ITT) Safety and acceptability confirmed Condom use similar in both arms with condom usage in Thailand higher than in SA Recruitment and retention similar for both arms Seroconversions only in SA, 8 in each arm
Gel & Condom Usage During Sex Acts, Phase II SA (ITT)
Phase III Overall Design Considerations A classic placebo controlled, two arm, double blind ITT trial in 4500 non infected women in SA The active arm Carraguard® and a methyl cellulose placebo Maximum trial duration is 48 months with a 24 month maximum subject participation We are examining a design of closing the trial 12 months after the last patient is enrolled A classic placebo controlled, two arm, double blind ITT trial in 4500 non infected women in SA The active arm Carraguard® and a methyl cellulose placebo Maximum trial duration is 48 months with a 24 month maximum subject participation We are examining a design of closing the trial 12 months after the last patient is enrolled
Trial Criteria Two major exclusion criteria –Women who test positive for HIV –Pregnant women Women with STIs will be accepted Primary endpoint: HIV seroconversion Safety endpoints: STIs & vaginal lesions Two major exclusion criteria –Women who test positive for HIV –Pregnant women Women with STIs will be accepted Primary endpoint: HIV seroconversion Safety endpoints: STIs & vaginal lesions
Compliance Methods Compliance will be tested using several methods –Visit questionnaires administered by clinic staff –Applicator tracking using bar code –Compliance with visit schedule –Applicator usage test under evaluation Non compliant subjects will be excluded from the ITT analyses Compliance will be tested using several methods –Visit questionnaires administered by clinic staff –Applicator tracking using bar code –Compliance with visit schedule –Applicator usage test under evaluation Non compliant subjects will be excluded from the ITT analyses