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[Preprint]. 2025 Sep 5:2025.08.28.672927.

doi: 10.1101/2025.08.28.672927.

Identifying a Vaginal Microbiome-Derived Selective Antibiotic Metabolite via Microbiome Pharmacology Analysis

Smrutiti Jena¹, Damilola Lawore¹, Javier Muñoz Briones¹, Kenzie Birse^{2

3}, Alana Lamont², Romel D Mackelprang⁴, Laura Noel-Romas^{2

3}, Michelle Perner⁵, Xuanlin Hou⁴, Elizabeth Irungu⁶, Nelly Mugo^{4

6}, Samantha Knodel^{2

3}, Stephanie Doran Brubaker⁷, Timothy R Muwonge⁸, Elly Katabira⁸, Sean M Hughes⁹, Fernanda L Calienes¹⁰, Raymond Krajci³, Rachel Liu³, Dalí Nemecio³, Florian Hladik^{9

10

11}, Jairam Lingappa^{4

11

12}, Adam D Burgener^{2

3

13}, Alicia R Berard^{2

3}, Leopold N Green¹, Douglas K Brubaker^{3

14}

Affiliations

¹ Weldon School of Biomedical Engineering, Purdue University, West Lafayette IN.
² Department of Obstetrics and Gynecology, University of Manitoba, Winnipeg Canada.
³ Center for Global Health and Disease, Department of Pathology, Case Western Reserve University, Cleveland OH.
⁴ Department of Global Health, University of Washington, Seattle USA.
⁵ Medical Microbiology and Infectious Disease University of Manitoba, Winnipeg Canada.
⁶ Partners in Health Research and Development, Kenya Medical Research Institute, Nairobi Kenya.
⁷ Graduate School of Public Health, University of Pittsburgh, Pittsburgh USA.
⁸ Infectious Disease Institute, Makerere University, Makerere, Kampala Uganda.
⁹ Department of Obstetrics and Gynecology, University of Washington, Seattle USA.
¹⁰ Fred Hutchinson Cancer Research Center, Seattle USA.
¹¹ Department of Medicine, University of Washington, Seattle USA.
¹² Department of Pediatrics, University of Washington, Seattle USA.
¹³ Department of Medicine Solna, Karolinska Institutet, Framstegsgatan Sweden.
¹⁴ The Blood Heart Lung Immunology Research Center, Case Western Reserve University, University Hospitals of Cleveland, Cleveland, OH, USA.

PMID: 40909525
PMCID: PMC12407940
DOI: 10.1101/2025.08.28.672927

Identifying a Vaginal Microbiome-Derived Selective Antibiotic Metabolite via Microbiome Pharmacology Analysis

Smrutiti Jena et al. bioRxiv. 2025.

[Preprint]. 2025 Sep 5:2025.08.28.672927.

doi: 10.1101/2025.08.28.672927.

Authors

Affiliations

¹ Weldon School of Biomedical Engineering, Purdue University, West Lafayette IN.
² Department of Obstetrics and Gynecology, University of Manitoba, Winnipeg Canada.
³ Center for Global Health and Disease, Department of Pathology, Case Western Reserve University, Cleveland OH.
⁴ Department of Global Health, University of Washington, Seattle USA.
⁵ Medical Microbiology and Infectious Disease University of Manitoba, Winnipeg Canada.
⁶ Partners in Health Research and Development, Kenya Medical Research Institute, Nairobi Kenya.
⁷ Graduate School of Public Health, University of Pittsburgh, Pittsburgh USA.
⁸ Infectious Disease Institute, Makerere University, Makerere, Kampala Uganda.
⁹ Department of Obstetrics and Gynecology, University of Washington, Seattle USA.
¹⁰ Fred Hutchinson Cancer Research Center, Seattle USA.
¹¹ Department of Medicine, University of Washington, Seattle USA.
¹² Department of Pediatrics, University of Washington, Seattle USA.
¹³ Department of Medicine Solna, Karolinska Institutet, Framstegsgatan Sweden.
¹⁴ The Blood Heart Lung Immunology Research Center, Case Western Reserve University, University Hospitals of Cleveland, Cleveland, OH, USA.

PMID: 40909525
PMCID: PMC12407940
DOI: 10.1101/2025.08.28.672927

Abstract

The vaginal microbiome plays a critical role in maintaining immune and epithelial homeostasis in the female reproductive tract. Bacterial Vaginosis (BV) is deleterious to female health, causing the loss of beneficial Lactobacillus species, overgrowth of anaerobic taxa, changes in vaginal pH, breakdown of protective mucins and epithelial barriers, and activation of the immune system. Treatment with gel-based antibiotics (Metronidazole or Clindamycin) resolves BV for 85% of patients, but 50% of those cases recur, indicating a need to identify strategies for overcoming antibiotic resistance and achieving a more durable response. Here, we developed a systems biology approach termed Microbiome Pharmacology Analysis to characterize the antibiotic potential of vaginal microbes, their metabolites and functions, via computational fusion of human cohort multi-omics and post-drug perturbation transcriptomic profiles. We focused on Clindamycin and Metronidazole as candidate drugs and screened 780 vaginal microbiome-drug mimicry candidates to identify candidate taxa and metabolites with antibiotic potential. We demonstrate experimentally that Lactobacillus crispatus-derived Hydroxyisocaproate (HICA) selectively kills Gardnerella vaginalis and that HICA enhances epithelial barrier integrity in a human vagina-on-a-chip system. Our work demonstrates the first use of Pharmacobiome Analysis, for discovering novel, selective antibiotic metabolites for BV with implications for charting the full pharmacologic potential of the vaginal microbiome.

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Conflict of interest statement

COMPETING INTERESTS The authors declare no competing interests

Figures

**Figure 1.. Overview of Vaginal Pharmacobiome Analysis.**
**(A)** Vaginal microbiome multi-omics data is integrated with matched host transcriptomics via Spearman correlation analysis to generate microbe-gene, metabolite-gene, and bacterial functions-gene lists. Human vaginal microbiome-host gene lists are combined with LINCS characteristic direction signatures via Spearman correlation with False Discovery Rate correction to identify vaginal microbiome-drug mimicry associations.

**Figure 2.. Identification of Vaginal Microbiome Factors with Antibiotic Potential.**
Shown are correlation similarity scores (Spearman’s rho) for **(A)** relating the correlation coefficients between vaginal microbes and host gene expression to the CD perturbation values of clindamycin and metronidazole; **(B)** relating the correlation coefficients between vaginal metabolites and host gene expression to the CD perturbation values for clindamycin and metronidazole; **(C)** relating the correlation coefficients between vaginal bacterial metabolic functions and host gene expression to the CD perturbation values for clindamycin and metronidazole. See Methods for calculation of correlation similarity scores.

**Figure 3.**
(A) *L. crispatus* growth curve with different concentrations of HICA treatment. (B) Media pH changes at different timepoints of *L. crispatus* growth with HICA treatments (C) *G. vaginalis* growth curve with different concentrations of HICA treatment. (D) Media pH changes at different timepoints of *G. vaginalis* growth with HICA treatments.

**Figure 4.**
**(A)** Brightfield microscope image of vagina-chip system treated with 20mM of HICA versus pre-treatment and media control. (B) Apparent permeability of the vagina-chip epithelial layer after 48hours of HICA treatment shows increased barrier integrity (-log10(apparent permeability)).

See this image and copyright information in PMC

References

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This is a preprint.

Identifying a Vaginal Microbiome-Derived Selective Antibiotic Metabolite via Microbiome Pharmacology Analysis

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Identifying a Vaginal Microbiome-Derived Selective Antibiotic Metabolite via Microbiome Pharmacology Analysis

Authors

Affiliations

Abstract

Conflict of interest statement

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References

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