| Literature DB >> 27491564 |
Maria Liljevald1, Maria Rehnberg2, Magnus Söderberg3, Marie Ramnegård2, Jenny Börjesson4, Donatella Luciani2, Nina Krutrök2, Lena Brändén3, Camilla Johansson3, Xiufeng Xu4, Mikael Bjursell4, Anna-Karin Sjögren3, Jorrit Hornberg3, Ulf Andersson3, David Keeling2, Johan Jirholt2.
Abstract
RORγ is a nuclear hormone receptor which controls polarization of naive CD4+ T-cells into proinflammatory Th17 cells. Pharmacological antagonism of RORγ has therapeutic potential for autoimmune diseases; however, this mechanism may potentially carry target-related safety risks, as mice deficient in Rorc, the gene encoding RORγ, develop T-cell lymphoma with 50% frequency. Due to the requirement of RORγ during development, the Rorc knockout (KO) animals lack secondary lymphoid organs and have a dysregulation in the generation of CD4+ and CD8+ T cells. We wanted to extend the evaluation of RORγ deficiency to address the question whether lymphomas, similar to those observed in the Rorc KO, would develop in an animal with an otherwise intact adult immune system. Accordingly, we designed a conditional RORγ knockout mouse (Rorc CKO) where the Rorc locus could be deleted in adult animals. Based on these studies we can confirm that these animals also develop lymphoma in a similar time frame as embryonic Rorc knockouts. This study also suggests that in animals where the gene deletion is incomplete, the thymus undergoes a rapid selection process replacing Rorc deficient cells with remnant thymocytes carrying a functional Rorc locus and that subsequently, these animals do not develop lymphoblastic lymphoma.Entities:
Keywords: Adult induced knockout mouse model; Lymphoblastic lymphoma; NHR; RORγ; RORγt; Rorc; Th17 cells
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Year: 2016 PMID: 27491564 DOI: 10.1016/j.autrev.2016.07.036
Source DB: PubMed Journal: Autoimmun Rev ISSN: 1568-9972 Impact factor: 9.754