Vaginal lIve Biotherapeutic RANdomized Trial

Phase 1 Trial of Multi-strain Lactobacillus Crispatus Vaginal Live Biotherapeutic Product

Status

Completed

Phases

Early Phase 1

Study type

Interventional

Source

ClinicalTrials.gov

Registry ID

NCT06135974

Acronym

VIBRANT

Enrollment

Registered

2023-11-18

Start date

2024-02-01

Completion date

2025-02-18

Last updated

2025-03-25

For informational purposes only — not medical advice. Sourced from public registries and may not reflect the latest updates. Terms

Conditions

Bacterial Vaginosis

Keywords

live biotherapeutic, bacterial vaginosis, vaginitis

Brief summary

The goal of this randomized clinical trial is to evaluate safety and biologic effect of a multi-strain vaginal L. crispatus live biotherapeutic product (LBP) in people receiving antibiotic treatment for bacterial vaginosis (BV). The main question\[s\] it aims to answer are whether the intervention is safe, and whether the strains of L. crispatus will colonize recipients' vagina. The study will evaluate one LBP with 6 strains of L. crispatus (LC106) and one LBP with 15 strains (LC115) vs. placebo. Participants will: * be treated with oral antibiotics for BV * receive 7 days of vaginal study product * collect daily home swabs and make short daily diary entries for 5 weeks, including the week of antibiotic treatment and the week of study product treatment. Researchers will compare the 3 groups receiving different dosing strategies of LC106 and 1 group receiving LC115 vs. 1 group receiving placebo to see if the live biotherapeutic strains colonize the vagina after antibiotic treatment for BV.

Detailed description

This is a Phase I randomized trial of a novel live biotherapeutic intervention containing multiple strains of L. crispatus. L. crispatus is a species of Lactobacillus commonly found in the human vagina, which is associated with optimal reproductive health outcomes. Detection of, and dominance of the community by, L. crispatus is associated with lower risk for bacterial vaginosis (BV), but no intervention to date has demonstrated the ability to durably shift the vaginal microbiome to L. crispatus dominance in a majority of treated people. In this study, we will compare safety and biologic effects of two formulations of a consortia of L. crispatus strains, and a variety of dosing strategies in women with BV who receive antibiotic treatment. Our primary outcome is colonization with any of the L. crispatus strains contained in the live biotherapeutic product. All participants will have menses suppressed with either injectable progesterone contraception or continuous oral contraceptive pills for the duration of the study. All participants will receive 7 days of oral metronidazole (500mg twice daily) and will be randomized to one of five groups: 1. Placebo daily for 7d after metronidazole treatment 2. LC-106 daily for 7d after metronidazole treatment 3. LC-106 daily for 3d + 4 days of placebo, starting after metronidazole treatment 4. LC-106 daily for 7d, starting on day 3 of metronidazole treatment 5. LC-115 daily for 7d after metronidazole treatment

Interventions

DRUGLC106

Tablet containing at least 2 x 10\^6 CFU/tablet, and comprised of 6 strains of Lactobacillus crispatus

DRUGLC115

Tablet containing at least 2 x 10\^6 CFU/tablet, and comprised of 15 strains of Lactobacillus crispatus

DRUGPlacebo

Vaginal tablets containing primarily microcrystalline cellulose and no live bacteria

DRUGMetronidazole Oral

Metronidazole tablet orally twice daily for 7 days

Study design

Allocation

RANDOMIZED

Intervention model

PARALLEL

Primary purpose

TREATMENT

Masking

QUADRUPLE (Subject, Caregiver, Investigator, Outcomes Assessor)

Masking description

Study product is labeled in a blinded manner with a code. Only pharmacy will have the link to the code and treatment assignment. However, the one arm starting study product during antibiotic treatment will be unblinded for both participants and investigators. However, the laboratory staff conducting the analyses for the primary and secondary outcomes will remain masked.

Intervention model description

This is a randomized trial with 5 arms

Eligibility

Sex/Gender

FEMALE

Age

18 Years to 40 Years

Healthy volunteers

Inclusion criteria

* Premenopausal individuals, 18- 40 years old * BV by Amsel criteria (at least 3 of 4 criteria must be present) * Abnormal Nugent score: ≥ 7 * Willing and able to provide written informed consent. * HIV uninfected (by HIV Ab/Ag test at enrollment) * Not pregnant by pregnancy test at enrollment, and unlikely to have an early pregnancy per clinician's assessment of last menstrual period and recent sexual activity. * On continuous oral contraceptives (US site) or injectable progestin contraceptives (South African site) that suppress menstrual cycles, or willing to suppress menstrual cycles with one of these types of hormonal contraceptives * Willing and able to attend study visits and comply with study procedures

Exclusion criteria

* History of clinically significant vaginal, cervical, or uterine disease including but not limited to: cancer of the female reproductive tract * Prior hysterectomy * Diagnosed with cervicovaginal infection (inclusive of gonorrhoeae, chlamydia, trichomonas) within the 30 days prior (or at enrollment visit). Yeast and bacterial vaginosis are not exclusionary. * Use of antibiotics in the past 30 days * Syphilis (positive screen at enrollment) * Vulvovaginal candidiasis (positive microscopy at enrollment) * Allergy to or contraindication to use of oral metronidazole * High grade abnormal Pap (HSIL, AGC \[Atypical Glandular Cells\], ASCUS-H) at enrollment (LSIL, ASCUS, or HPV+ are all non-exclusionary) * Currently participating in another study of an investigational product (excluding COVID vaccine studies) * Use of long-acting systemic investigational product (e.g. injectable PrEP) within the past year * Subject taking any of the following medications currently or in the past 30 days: systemic steroids (inhaled or nasal steroid therapy is permitted), interleukins, systemic interferons (e.g. local injection of interferon alpha for treatment of human papillomavirus is permitted) or systemic chemotherapy. * History of coronary artery disease, myocardial infarction, chronic obstructive pulmonary disease, chronic renal failure, decompensated cirrhosis, or any other condition that in the opinion of the investigator will compromise ability to participate in the study. * Use of an IUD (intrauterine device) * Use of probiotics, prebiotics or synbiotics (supplements and products, oral or vaginal) within past 30 days. (NOTE: Oral yogurt with live cultures is allowed, as are fermented foods.) * Active COVID-19 infection (determined by a positive PCR test of a nasal or nasopharyngeal swab) or recent exposure (\< 14 days) to someone with confirmed COVID-19 infection (an exposure is considered being within 6 feet/180 cm of someone without a mask for more than 15 minutes). Potential participants who meet these criteria can delay screening until they have completed isolation or quarantine. * Vaginal cleansing practices in the past 30 days (i.e. vaginal products for cleaning or drying, vaginal douching) (by eligibility questionnaire) * Any other condition or situation that in the opinion of the investigator will compromise ability to participate in the study. * Menopause: surgical; or absence of periods not due to hormonal contraception and in the setting of prior chemotherapy * Use of testosterone for any reason * Systolic blood pressure \> 180 or diastolic blood pressure \> 110 at screening or enrollment * Hemoglobin \< 9 * Less than 2 weeks since 2nd COVID vaccination (mRNA) or 1st vaccination (J&J) or booster * Either breastfeeding/lactating or pregnant within 8 weeks prior to study entry

Design outcomes

Primary

Measure	Time frame	Description
Adverse events	Over 12 weeks	Assessment of safety by comparing number and severity of adverse events
Detection of LBP strains by metagenomic sequencing	Over 5 weeks	Detection of any one strain from the LBP at 5% relative abundance or greater, or any combination of strains at 10% relative abundance or greater using shotgun metagenomic sequencing

Secondary

Measure	Time frame	Description
Recurrent BV by Amsel and Nugent criteria	Over 12 weeks	Presence of BV by Amsel criteria and/or Nugent criteria
Non-iners Lactobacillus dominance and abundance	Over 12 weeks	Using 16S rRNA sequencing, relative abundance of non-iners Lactobacillus species in the vaginal fluid, and proportion with dominance by these species (\> 50% relative abundance)
Proportion of participants reporting product was acceptable to use	Over 12 weeks	Participant perceptions of and preferences for the vaginal LBP treatment
Alpha and beta diversity of the microbial community	Over 12 weeks	Comparison of alpha and beta diversity metrics between arms before and after treatment with LBP
Kinetics of colonization	Over 12 weeks	Presence and quantity of each strain contained in the LBP measured by strain-specific quantitative PCR

Other

Measure	Time frame	Description
Comparison of detection of LBP strains by metagenomics between US and South Africa	Over 12 weeks	Comparison of all outcome measures at the US site vs. the South African site

Countries

South Africa, United States

Outcome results

None listed

Source: ClinicalTrials.gov · Data processed: Feb 4, 2026