1. Negative mucosal synergy between Herpes simplex type 2 and HIV in the female genital tract
- Author
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Charles Wachihi, Sanja Huibner, Keith R. Fowke, Tony Mazzulli, Walter Jaoko, Rupert Kaul, Anuradha Rebbapragada, Christopher Pettengell, Francis A. Plummer, Blake T. Ball, and Sherzana Sunderji
- Subjects
Adult ,Chemokine ,Sexual transmission ,Immunology ,HIV Infections ,Cervix Uteri ,Biology ,medicine.disease_cause ,Virus ,Immune system ,Acquired immunodeficiency syndrome (AIDS) ,T-Lymphocyte Subsets ,Immunopathology ,medicine ,Humans ,Immunology and Allergy ,Immunity, Mucosal ,Herpes Genitalis ,Mucous Membrane ,virus diseases ,Dendritic Cells ,Genitalia, Female ,Middle Aged ,medicine.disease ,biology.organism_classification ,Sex Work ,Virology ,Virus Shedding ,Cross-Sectional Studies ,Infectious Diseases ,Herpes simplex virus ,Chronic Disease ,Vagina ,Lentivirus ,HIV-1 ,biology.protein ,Female - Abstract
Objective: There is substantial epidemiological evidence that infection by Herpes simplex virus type 2 (HSV2) enhances both HIV susceptibility and subsequent sexual transmission. Both infections are extremely common in female sex workers (FSWs) in sub-Saharan Africa, and up to 80% of new HIV infections in urban men in the region are acquired via transactional sex. The present study aimed to elucidate the mucosal immune interactions between HIV and HSV2 in the genital tract. Methods: Endocervical immune cell populations, cytokine/chemokine protein levels in cervico-vaginal secretions and cervical immune gene expression profiles were measured in a well-defined cohort of HIV-infected and uninfected Kenyan FSWs. Associations between the genital immune milieu and infection by and/or shedding of common genital co-pathogens were examined. Results: HIV-infected FSWs were much more likely to be infected by HSV2, and to shed HSV2 DNA in the genital tract. There was also a profound negative 'mucosal synergy' between these viruses. In HIV uninfected FSWs, HSV2 infection was associated with a ten-fold increase in cervical immature dendritic cells (iDC) expressing DC-SIGN, and a three-fold increase in cervical CD4+ T cells expressing CCR5. HIV infection was associated with iDC depletion in the cervix, and with increased HSV2 genital reactivation, which in turn was associated with HIV shedding levels. Conclusions: The findings suggest a mucosal vicious circle in which HSV2 infection increases HIV target cells in the genital mucosa, subsequent HIV infection impairs HSV2 mucosal immune control, and local HSV2 reactivation enhances both HSV2 and HIV transmission.
- Published
- 2007
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