RT Journal Article SR Electronic T1 P2.091 A Repeated Low Dose Co-Challenge Model of SHIV-RT and HSV-2 in Rhesus Macaques JF Sexually Transmitted Infections JO Sex Transm Infect FD BMJ Publishing Group Ltd SP A116 OP A116 DO 10.1136/sextrans-2013-051184.0355 VO 89 IS Suppl 1 A1 Kenney, J A1 Derby, N A1 Aravantinou, M A1 Rana, S A1 Lifson, J D A1 Piatak, M A1 Gettie, A A1 Blanchard, J A1 Robbiani, M YR 2013 UL http://sti.bmj.com/content/89/Suppl_1/A116.1.abstract AB Background HIV acquisition is facilitated by HSV-2 infection, making microbicides that block both viruses desirable for limiting HIV transmission. We have tested microbicides in a stringent efficacy model: vaginal co-challenge with a single high dose of SHIV-RT (103 TCID50) and HSV-2 (2 × 108 pfu) in DepoProvera (DP)-treated macaques. Here we established a model mimicking real world exposure: repeated low dose SHIV/HSV-2 co-challenge in non-DP-treated animals. Methods Two groups of macaques were co-challenged weekly for 11wks with SHIV (10 or 50 TCID50) and HSV-2 (107 pfu) after which the SHIV dose was increased to 200 TCID50 in all animals for 9 more co-challenges. HSV-2 shedding in vaginal swabs and SHIV plasma viremia were determined. Antibodies (Abs) to SIV and HSV-2, HSV-2-specific T cell responses and the hormones estradiol and progesterone were measured in the blood. Results After 11 co-challenges, SHIV infections were detected in 1/3 animals from the 10 TCID50 SHIV group and 1/3 from the 50 TCID50 SHIV group (after 2 and 8 challenges, respectively). Upon increasing the SHIV dose, two more animals became infected (after 1 and 5 more co-challenges), but the last two remained uninfected. SHIV viremia was similar in all infected animals, which all developed SIV-specific Abs. All animals (6/6) became HSV-2 infected. Initial analyses suggest that the frequency of HSV-2 shedding was greater in non-DP-treated animals repeatedly exposed to 107 pfu than we previously observed for DP-treated animals that received a single 2 × 108 pfu dose of HSV-2 with SHIV (p < 0.0001). HSV-2-specific IgG responses were not detected; T cell responses are being analysed. Conclusion We have developed a repeated low dose co-challenge model to evaluate microbicides against SHIV and HSV-2. SHIV infection frequency was 67% in this model, similar to the single high dose co-challenge. HSV-2 infection was enhanced compared to the single high dose model.