| Literature DB >> 33463537 |
Stephanie Kim1,2, Rami Khoriaty1,3, Lu Li1, Madison McClune1, Theodosia A Kalfa4,5, Julia Wu1,2, Daniel Peltier6, Hideaki Fujiwara1, Yaping Sun1, Katherine Oravecz-Wilson1, Richard A King1, David Ginsburg1,6,7,8,9,10, Pavan Reddy1.
Abstract
T cell-mediated responses are dependent on their secretion of key effector molecules. However, the critical molecular determinants of the secretion of these proteins are largely undefined. Here, we demonstrate that T cell activation increases trafficking via the ER-to-Golgi pathway. To study the functional role of this pathway, we generated mice with a T cell-specific deletion in SEC23B, a core subunit of coat protein complex II (COPII). We found that SEC23B critically regulated the T cell secretome following activation. SEC23B-deficient T cells exhibited a proliferative defect and reduced effector functions in vitro, as well as in experimental models of allogeneic and xenogeneic hematopoietic cell transplantation in vivo. However, T cells derived from 3 patients with congenital dyserythropoietic anemia II (CDAII), which results from Sec23b mutation, did not exhibit a similar phenotype. Mechanistic studies demonstrated that unlike murine KO T cells, T cells from patients with CDAII harbor increased levels of the closely related paralog, SEC23A. In vivo rescue of murine KO by expression of Sec23a from the Sec23b genomic locus restored T cell functions. Together, our data demonstrate a critical role for the COPII pathway, with evidence for functional overlap in vivo between SEC23 paralogs in the regulation of T cell immunity in both mice and humans.Entities:
Keywords: Bone marrow transplantation; Cell Biology; Immunology; T cells
Year: 2021 PMID: 33463537 PMCID: PMC7810489 DOI: 10.1172/JCI136574
Source DB: PubMed Journal: J Clin Invest ISSN: 0021-9738 Impact factor: 14.808