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Vertebrate reproductive science and technology
RESEARCH ARTICLE

284. Leukocyte trafficking in the ovary of mice immunised with recombinant murine cyclomegalovirus expressing murine zona pellucida 3

S. O’Leary A , M. L. Lloyd B , G. R. Shellam B and S. Maddocks C
+ Author Affiliations
- Author Affiliations

A Animal Science, University of Adelaide, Roseworthy, SA, Australia

B School of Biomedical and Chemical Sciences, University of Western Australia, Nedlands, WA, Australia

C South Australian Research and Development Institute, Roseworthy, WA, Australia

Reproduction, Fertility and Development 17(9) 119-119 https://doi.org/10.1071/SRB05Abs284
Submitted: 26 July 2005  Accepted: 26 July 2005   Published: 5 September 2005

Abstract

Inoculation of female BALB/c mice with recombinant murine cytomegalovirus encoding murine zona pellucida antigen (MCMV-ZP3) confers infertility characterised by depletion in ovarian tertiary follicles by day 21 post inoculation followed by a progressive depletion in primordial follicles.1 Cell mediated immune responses begin as early as day 10 post immunisation with MCMV-ZP32 with the recruitment of leukocytes before serum antibody can be clearly detected in mice. The physiological mechanisms leading to infertility in inoculated mice are being progressively delineated with the role of leukocyte subsets implicated in early pathological changes in ovarian architecture. The aim of this study was to investigate the effect of MCMV-ZP3 infection on leukocytes including T cells recruited into the ovary following infection with recombinant virus. Fifteen BALB/c female mice were randomly allocated into three groups of five animals at 6 weeks of age. Group one received an injection of PBS, group two and three received intraperitoneal inoculations of 2 × 104 pfu of MCMV and MCMV-ZP3 respectively. Ovaries were retrieved at day 10, 21 and 35 post inoculation and one ovary from each mouse was sectioned for immunohistochemical analysis of resident leukocytes using mAb CD45 reactive with all leukocyte lineages and mAb for CD4 and CD8 positive T cells. MCMV-ZP3 inoculation increased the abundance of ovarian leukocytes including CD4 and CD8 positive T cells for all time points post immunisation except for CD8 positive T cells 21 days post infection (Table 1).

These results suggest that leukocytes, including T cells, are involved in causing early changes in the ovary post infection with MCMV-ZP3 that lead to the depletion of existing ovarian follicles leading to life long infertility in mice. Further experiments are underway to investigate the role of antibody and changes in leukocyte populations in the ovary as the course of infection with recombinant virus progresses.

This study is funded by the Cooperative Research Centre for Pest Animal Control.

   (1) Lloyd ML, et al. (2003). Biol. Reprod. 68, 2024–32.
   (2) O’Leary S, et al. (2004). Reprod. Fertil. Devel. 16(Supplement), 77.


Table 1.    Abundance of positively stained leukocytes (CD45) and T cells (CD4 and CD8) in mouse ovarian sections at day 10, 21 and 35 post immunisation with MCMV-ZP3
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