AI Article Synopsis

  • This study is the first to experimentally demonstrate transplacental transmission (TPT) of the wild-type Indian BTV-1 virus in pregnant mice, revealing its impact on fetal development and immune response.
  • TPT was observed to be more prevalent during mid-gestation (71.43%) compared to early gestation (57.14%), with significant effects including embryonic deaths and congenital defects in the fetuses.
  • The study also highlights the immune dynamics, showing changes in CD4 and CD8 T-lymphocytes and increased apoptotic cells during peak viral load, suggesting the need for improved control and vaccination strategies against BTV-1.

Article Abstract

Transplacental transmission (TPT) of wild-type Indian BTV-1 had never been experimentally proved. This study was first time investigated TPT of Indian BTV-1 (isolated from aborted and stillborn goat fetal spleens). The sequential pathology, virological and immune cell kinetics (CD4, CD8 T-lymphocytes and NK cells in spleen and PBMCs), and apoptosis in IFNAR1-blocked pregnant mice during early (infected on 1 GD) and mid (infected on 8 GD) gestation have been studied. There was higher rate of TPT during mid stage (71.43%) than early (57.14%) stage. In early stage reduced implantation sites, early embryonic deaths, abortions, and necro-haemorrhagic lesions had observed. Mid stage, congenital defects and neurological lesions in foetuses like haemorrhages, diffuse cerebral edema, necrotizing encephalitis and decreased bone size (Alizarin red staining) were noticed. BTV-1 antigen was first time demonstrable in cells of mesometrium, decidua of embryos, placenta, uterus, ovary, and brain of foetuses by immunohistochemistry and quantified by real-time qRT-PCR. BTV-inoculated mice were seroconverted by 7 and 5 dpi, and reached peak levels by 15 and 9 dpi in early and mid gestation, respectively. CD4 and CD8 cells were significantly decreased (increased ratio) on 7 dpi but subsequently increased on 15 dpi in early gestation. In mid gestation, increased CD8 cells (decreased ratio) were observed. Apoptotic cells in PBMCs and tissues increased during peak viral load. This first time TPT of wild-type Indian BTV-1 deserves to be reported for implementation of control strategies. This model will be very suitable for further research into mechanisms of TPT, overwintering, and vaccination strategies.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7005837PMC
http://dx.doi.org/10.1038/s41598-020-58268-0DOI Listing

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