Tenofovir/Levonorgestrel Intravaginal Ring and Tenofovir Intravaginal Ring

Phase 2

• Conditions: HIV; Anti-Retroviral Agent; Contraception; Prevention
• Interventions: Drug: Placebo IVR; Drug: TFV IVR; Drug: TFV/LNG IVR

• Registration Number: NCT03762382
• Lead Sponsor: CONRAD

Brief Summary

The purpose of the study is to evaluate the safety, pharmacokinetics and pharmacodynamics of, and the tolerability and acceptance of an intravaginal ring (IVR) delivering both tenofovir and levonorgestrel (TFV/LNG) and an IVR delivering TFV only, compared to a placebo IVR, in women in Western Kenya.

Detailed Description

This Phase 2a clinical trial will evaluate the safety, pharmacokinetics and pharmacodynamics of, and the tolerability and adherence to two novel intravaginal rings (IVRs). The tenofovir/levonorgestrel (TFV/LNG) IVR and TFV IVRs are designed to provide HIV (and HSV-2) prevention with and without contraceptive for pregnancy prevention, respectively. Women will be protected from pregnancy by abstinence from vaginal intercourse or agreeing to consistently use condoms; concurrent use of a non-hormonal copper intrauterine device is permitted.

The study will enroll healthy, HIV-negative, non-pregnant, menstruating women aged 18-34 years, inclusive, and not currently infected with hepatitis B virus, who are assessed to be at lower risk for HIV. The goal is to enroll fifty (50) women in Western Kenya. The participants will be randomized 2:2:1 to use one of the following continuous delivery IVRs: twenty (20) women to use the TFV/LNG IVR; ten (10) women to use the TFV IVR; and ten (10) women to use the placebo IVR. Participants will attend up to ten (10) routine study visits that may include physical and pelvic exams, collection of venous blood, vaginal fluid and cervical mucus, and behavioral questionnaires. A subset of twenty (20) women will participate in in-depth interviews.

Study Timeline

• Study First Submitted: 2018-11-16
• Study First Submitted QC: 2018-11-30
• Study First Posted: 2018-12-03
• Study Start: 2018-12-12
• Primary Completion: 2019-08-20
• Status Verified: 2020-01
• Last Update Submitted: 2020-01-13
• Last Update Posted: 2020-01-14
• Study Completion: 2020-04

Recruitment & Eligibility

• Status: UNKNOWN
• Sex: Female
• Target Recruitment: 50

Inclusion Criteria

• Female, aged 18-34 years, inclusive

• General good health (by history and per clinician discretion) without any clinically significant systemic disease (including, but not limited to significant liver disease/hepatitis, gastrointestinal disease, kidney disease, thyroid disease, osteoporosis or bone disease, and diabetes), uterus, and cervix

• Not pregnant or planning to become pregnant

• Pre-screening HIV risk score ≤4

• Currently having regular menstrual cycles (approximately 24-35 days) OR with a history of having regular menstrual cycles before contraceptive use, by report, and resumed some menstruation or spotting (with biochemical confirmation of ovulation)

• Willing to undergo Visual Inspection with Lugol's Iodine (VILI) for cervical abnormalities during pelvic exam

• Willing to abstain from use of vaginal products other than the study product, including tampons (except for during menses) , menstrual cups, vaginally inserted cloths or other materials, spermicides, lubricants, and douches for the whole study

• Willing to abstain from any vaginal intercourse starting 48 hours before certain study visits

• Vaginal and cervical anatomy that, in the opinion of the clinician, lends itself to easy genital tract sample collection and is absent of vesicles and ulcers

• No use of hormonal contraceptives within the following periods specified for each type of contraception method:

  • Oral contraceptives (combined or progestin-only), contraceptive patch or contraceptive vaginal ring in at least two (2) months
  • Last DMPA injection received at least four (4) months ago and has resumed regular menstruation
  • Hormonal IUD/IUS removed at least four (4) months ago and has resumed regular menstruation
  • Hormonal implant removed at least six (6) months ago and has resumed regular menstruation

• Willing to refrain from using any hormonal contraceptives for the entire study and to use only study-provided non-spermicidal male condoms with or without a study-provided Cu-IUD

• P4 ≥3.0 ng/ml

• Estimated glomerular filtration rate (eGFR) ≥90ml/min/1.73m2

• Willing to give voluntary consent and sign/mark an informed consent form

• Willing and able to comply with protocol requirements

Exclusion Criteria

• Body mass index (BMI) ≥30 kg/m
• History of hysterectomy
• Currently pregnant or within less than three (3) calendar months of the last pregnancy outcome.
• Currently breastfeeding or having breastfed an infant in the last two (2) months, or planning to breastfeed during the course of the study
• Contraindication to any study products-LNG, TFV, or excipient ingredients
• Contraindication to LNG
• In the last three (3) months, diagnosed with or treated for any STI or pelvic inflammatory disease
• Positive test for HIV-1, syphilis, Trichomonas vaginalis (TV), Neisseria gonorrhea (GC), Chlamydia trachomatis (CT) or HBsAg
• Nugent score greater than or equal to 7 or a symptomatic BV clinical diagnosis as defined by Amsel's criteria
• Suspected breast cancer or other progestin-sensitive cancer
• Suspected hepatic disease, including cirrhosis or viral hepatitis
• History of bleeding or coagulation problems
• Known current drug or alcohol abuse which could impact study compliance
• Grade 2 or higher laboratory abnormality, per the Division of AIDS, National Institute of Allergy and Infectious Disease (DAIDS) Table for Grading the Severity of Adverse Events, or clinically significant laboratory abnormality as determined by the clinician
• Use of any concomitant medications
• Participation in any other investigational trial with use of a drug/device within the last 30 days or planned participation in any other investigational trial with use of a drug/device during the study
• History of gynecological procedures (including genital piercing) on the external genitalia, vagina, or cervix within the last 14 days
• Labial elongation (due to pulling practices and use of botanicals or caustic agents)
• Abnormal finding on laboratory or physical examination or a social or medical condition in the volunteer which, in the opinion of the site co-PI(s), would make participation in the study unsafe or would complicate interpretation of data
• Currently using, or has used within the preceding one (1) month, emtricitabine/tenofovir disoproxil fumarate (TDF/FTC or Truvada®) or any other tenofovir product, and/or has plans to use a non-study tenofovir product in any form during the study

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
Placebo IVR (Non-eluting)	Placebo IVR	Placebo Intravaginal Ring
TFV IVR (10mg) (Continuous)	TFV IVR	Tenofovir Intravaginal Ring
TFV/LNG IVR (10mg/20μg) (Continuous)	TFV/LNG IVR	Tenofovir/Levonorgestrel Intravaginal Ring

Primary Outcome Measures

Name	Time	Method
Mucosal safety	Change from Baseline to up to 90 days of IVR use	Changes in cervicovaginal mucosa by visual inspection
Safety Laboratory Assessments- complete blood counts	Change from Baseline to up to 90 days of IVR use	Number of participants with abnormal complete blood counts
Treatment-emergent adverse events (TEAEs)	Change from Baseline to up to 90 days of IVR use	Participants with Grade 2 or higher local female genital TEAEs as defined by DAIDS Table for Grading the Severity of Adult and Pediatric AEs (version 2.1) and DAIDS Table for Grading the Severity of Adult and Pediatric Adverse Events Addendum 1 Female Genital Grading Table for Use in Microbicide Studies
Safety Laboratory Assessments- lipids	Change from Baseline to up to 90 days of IVR use	Number of participants with abnormal lipids
Safety Laboratory Assessments- Serum chemistry	Change from Baseline to up to 90 days of IVR use	Number of participants with abnormal serum chemistry

Secondary Outcome Measures

Name	Time	Method
Maximum CV fluid concentration	6 and 24 hours post-IVR insertion; Menstrual cycle 1 day 14; Menstrual cycle 1 day 21-25; Menstrual cycle 2 day 21-25; Menstrual cycle 3, day 14; Day 90 of IVR use; and 24 hours post-IVR use (anticipated cycle length is 28 days)	Maximum CV fluid concentration of TFV
Confirmation of Ovulation	Pre-IVR insertion; Menstrual cycle 1, day 20-25; Menstrual cycle 2, day 20-25; Day 90 of IVR use (anticipated cycle length is 28 days)	Serum progesterone (P4) level.
Cervicovaginal (CV) fluid cytokines- IL-8	Change from Baseline to Day 90 of IVR use	Changes in IL-8 in CV fluid.
Changes in endogenous vaginal bacteria- Nugent score	Change from Baseline to Day 90 of IVR use	Changes in Nugent score (score 0-10)
Cervicovaginal (CV) fluid cytokines-IL-1α	Change from Baseline to Day 90 of IVR use	Changes in IL-1α in CV fluid.
Tolerability - Somatic and non-specific non-treatment emergent adverse events	Baseline; 6 and 24 hours post-IVR insertion; Menstrual cycle 1, day 14; Menstrual cycle 1, day 21-25; Menstrual cycle 2, day 21-25; Menstrual cycle 3, day 14; 90 days of IVR use; 24 hours post IVR use (anticipated cycle length is 28 days)	Subjective and objective assessment of new complaints (e.g., headache, nausea, weight change, breast tenderness, etc.)
Acceptability - Quantitative assessment of acceptability based on Questionnaires administered pre- and post-IVR use	Screening; 90 days of IVR use	Changes in responses to questionnaires pre- and post-IVR use on attitudes toward and perspectives of IVR use.
Percent (%) inhibition of HIV resulting from product use (Anti-HIV activity)	Baseline, Day 90 of IVR use	Anti-HIV and anti-HSV-2 activity in CV fluid (inhibition in cell assay)
Adherence - Drug concentrations	Baseline; 6 and 24 hours post-IVR insertion; Menstrual cycle 1, day 14; Menstrual cycle 1, day 21-25; Menstrual cycle 2, day 21-25; Menstrual cycle 3, day 14; 90 days of IVR use; 24 hours post-IVR use (anticipated cycle length is 28 days)	Plasma, serum, and vaginal fluid drug concentrations.
Adherence - Residual drug concentrations	Day 90 of IVR use	Residual drug (TFV and LNG) concentrations in returned TFV/LNG and TFV IVRs and residual excipients in returned placebo IVRs.
Maximum blood concentrations (Cmax)	Baseline; 6 and 24 hours post IVR insertion; Menstrual cycle 1, day 14; Menstrual cycle 1,day 21-25; Menstrual cycle 2, day 21-25; Menstrual cycle 3, day 14; Day 90 IVR use; 24 hours post-IVR use (anticipated cycle length is 28 days)	Maximum plasma concentration of TFV and maximum serum concentration of LNG
Percent (%) inhibition of HSV resulting from product use (Anti-HSV activity)	Baseline, Day 90 of IVR use	Anti-HSV-2 activity in CV fluid (inhibition in cell assay)
Cervical mucus assessment and quality score	Menstrual cycle 1, day 14; Menstrual cycle 3, day 14 (anticipated cycle length is 28 days)	Cervical mucus assessment and quality score (total summary score 0-15) as defined by WHO laboratory manual for the Examination and processing of human semen Fifth Edition, Appendix 5
Changes in endogenous vaginal bacteria	Change from Baseline to Day 90 of IVR use	Changes in endogenous vaginal bacteria in CV fluid
qPCR of Ring Microbiota	Day 90 of IVR use	Microbial growth on returned IVRs.
Tolerability - Self-reported complaints of changes in menstrual cycle	Screening; Menstrual cycle 1, day 14; Menstrual cycle 1, day 21-25; Menstrual cycle 2, day 21-25; Menstrual cycle 3, day 14; Day 90 of IVR use; 24 hours post-IVR use (anticipated cycle length is 28 days)	Percentage of women with changes in regularity of menstrual cycle
Adherence - Percentage of discontinuations	Up to Day 90 of IVR use	Percentage of IVR discontinuations

Trial Locations

Locations (1)

Kenya Medical Research Institute, Center for Global Health Research; 🇰🇪 Kisumu, Kisumu County, Kenya