A hepatocyte-specific cytochromecoxidase deficiency in mice leads to a lymphopenia owing to deficiencies in bone marrow progenitors

Abstract

SummaryMutations that negatively impact mitochondrial function are highly prevalent in humans and lead to disorders with a wide spectrum of disease phenotypes, including deficiencies in immune cell development and/or function. Previous analyses of mice with a hepatocyte-specific cytochromecoxidase (COX) deficiency revealed an unexpected peripheral blood leukopenia associated with splenic and thymic atrophy. Here, we use mice with a hepatocyte-specific deletion of the COX assembly factorSco1to show that metabolic defects extrinsic to the hematopoietic compartment lead to a pan-lymphopenia represented by severe losses in both B and T cells. We further demonstrate that immune defects in these mice are associated with the loss of bone marrow lymphoid progenitors common to both lineages and early signs of autoantibody-mediated autoimmunity. Our findings collectively point to a significant role for hepatocyte dysfunction as an instigator of immunodeficiency in patients with congenital mitochondrial defects who suffer from chronic or recurrent infections.