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Publication : γδT cells are prevalent in the proximal aorta and drive nascent atherosclerotic lesion progression and neutrophilia in hypercholesterolemic mice.

First Author  Vu DM Year  2014
Journal  PLoS One Volume  9
Issue  10 Pages  e109416
PubMed ID  25313857 Mgi Jnum  J:223560
Mgi Id  MGI:5649499 Doi  10.1371/journal.pone.0109416
Citation  Vu DM, et al. (2014) gammadeltaT cells are prevalent in the proximal aorta and drive nascent atherosclerotic lesion progression and neutrophilia in hypercholesterolemic mice. PLoS One 9(10):e109416
abstractText  Unique innate immunity-linked gammadeltaT cells have been seen in early human artery lesions, but their role in lesion development has received little attention. Here we investigated whether gammadeltaT cells modulate atherogenesis in apolipoprotein E-deficient (ApoE KO) mice. We found that gammadeltaT cell numbers were markedly increased in the proximal aorta of ApoE-deficient vs. wild-type mice during early atherogenesis, particularly in the aortic root and arch, where they comprised most of the T cells and lesion progression is most rapid. gammadeltaT cells infiltrated intimal lesions in ApoE KO mice, but only the adventitia in wild-type mice, and were more prevalent than CD4+ T cells in early nascent lesions, as evaluated by en face confocal microscopy. These aortic gammadeltaT cells produced IL-17, but not IFN-gamma, analyzed by ex vivo FACS. Furthermore, aortic arch lipid accumulation correlated strongly with abundance of IL-17-expressing splenic gammadeltaT cells in individual ApoE KO mice. To investigate the role of these gammadeltaT cells in early atherogenesis, we analyzed ApoE/gammadeltaT double knockout (DKO) compared to ApoE KO mice. We observed reduced early intimal lipid accumulation at sites of nascent lesion formation, both in chow-fed (by 40%) and Western diet-fed (by 44%) ApoE/gammadeltaT DKO mice. In addition, circulating neutrophils were drastically reduced in these DKO mice on Western diet, while expansion of inflammatory monocytes and splenic Th1 or Th17 lymphocytes was not affected. These data reveal, for the first time, a pathogenic role of gammadeltaT cells in early atherogenesis in ApoE KO mice, by mechanisms likely to involve their IL-17 production and induction of neutrophilia. Targeting gammadeltaT cells thus might offer therapeutic benefit in atherosclerosis or other inflammatory vascular diseases.
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