Interleukin (IL)-1, IL-6, and IL-8 Predict Mucosal Toxicity of Vaginal Microbicidal Contraceptives

doi:10.1095/biolreprod.104.029603

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Immunology

Interleukin (IL)-1, IL-6, and IL-8 Predict Mucosal Toxicity of Vaginal Microbicidal Contraceptives¹

R.N. Fichorova²^,3, M. Bajpai⁴, N. Chandra⁴, J.G. Hsiu⁵, M. Spangler³, V. Ratnam³, and G.F. Doncel⁴

Department of Obstetrics,³ Gynecology and Reproductive Biology, Brigham and Women's Hospital, Harvard Medical School, Boston, Massachusetts 02115 CONRAD,⁴ Department of Obstetrics and Gynecology, Department of Pathology,⁵ Eastern Virginia Medical School, Norfolk, Virginia 23507

Inflammation of the female reproductive tract increases susceptibilityto HIV-1 and other viral infections and, thus, it becomes aserious liability for vaginal products. Excessive release ofproinflammatory cytokines may alter the mucosal balance betweentissue destruction and repair and be linked to enhanced penetrationand replication of viral pathogens upon chemical insult. Thepresent study evaluates four surface-active microbicide candidates,nonoxynol-9 (N-9), benzalkonium chloride (BZK), sodium dodecylsulfate, and sodium monolaurate for their activity against humansperm and HIV, and their capacity to induce an inflammatoryresponse on human vaginal epithelial cells and by the rabbitvaginal mucosa. Spermicidal and virucidal evaluations rankedN-9 as the most potent compound but were unable to predict theimpact of the compounds on vaginal cell viability. Interleukin(IL)-1 release in vitro reflected their cytotoxicity profilesmore accurately. Furthermore, IL-1 concentrations in vaginalwashings correlated with cumulative mucosal irritation scoresafter single and multiple applications (P < 0.01), showingBZK as the most damaging agent for the vaginal mucosa. BZK inducedrapid cell death, IL-1 release, and IL-6 secretion. The othercompounds required either more prolonged or repeated contactwith the vaginal epithelium to induce a significant inflammatoryreaction. Increased IL-8 levels after multiple applicationsin vivo identified compounds with the highest cumulative mucosaltoxicity (P < 0.01). In conclusion, IL-1, IL-6, and IL-8in the vaginal secretions are sensitive indicators of compound-inducedmucosal toxicity. The described evaluation system is a valuabletool in identifying novel vaginal contraceptive microbicides,selecting out candidates that may enhance, rather than decrease,HIV transmission.

¹ Supported by grants CSA-01-300 and MSA-02-304 (R.N.F.) and intramuralfunds (G.F.D.) from the CONRAD program, Eastern Virginia MedicalSchool, under a Cooperative Agreement with the U.S. Agency forInternational Development (USAID). The views expressed by theauthors do not necessarily reflect those of CONRAD or USAID.

² Correspondence: Raina Fichorova, 221 Longwood Avenue, RF468,Boston, MA 02115. FAX: 617 713 3018; rfichorova{at}rics.bwh.harvard.edu

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