Cell-Extrinsic Defective Lymphocyte Development in Lmna-/- Mice |
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| Authors: | J. Scott Hale Richard L. Frock Sara A. Mamman Pamela J. Fink Brian K. Kennedy |
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| Affiliation: | 1. Department of Immunology, University of Washington, Seattle, Washington, United States of America.; 2. Department of Biochemistry, University of Washington, Seattle, Washington, United States of America.;New York University, United States of America |
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| Abstract: | BackgroundMutations in the LMNA gene, which encodes all A-type lamins, result in a variety of human diseases termed laminopathies. Lmna-/- mice appear normal at birth but become runted as early as 2 weeks of age and develop multiple tissue defects that mimic some aspects of human laminopathies. Lmna-/- mice also display smaller spleens and thymuses. In this study, we investigated whether altered lymphoid organ sizes are correlated with specific defects in lymphocyte development.Principal FindingsLmna-/- mice displayed severe age-dependent defects in T and B cell development which coincided with runting. Lmna-/- bone marrow reconstituted normal T and B cell development in irradiated wild-type recipients, driving generation of functional and self-MHC restricted CD4+ and CD8+ T cells. Transplantation of Lmna-/- neonatal thymus lobes into syngeneic wild-type recipients resulted in good engraftment of thymic tissue and normal thymocyte development.ConclusionsCollectively, these data demonstrate that the severe defects in lymphocyte development that characterize Lmna-/- mice do not result directly from the loss of A-type lamin function in lymphocytes or thymic stroma. Instead, the immune defects in Lmna-/- mice likely reflect indirect damage, perhaps resulting from prolonged stress due to the striated muscle dystrophies that occur in these mice. |
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