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Role of Methylation-Controlled J protein in CD8 function and persistent viral infection of the placenta

$195,000R21FY2019AINIH

University Of Vermont & St Agric College, Burlington VT

Investigators

Abstract

Infectious organisms are a major cause of poor pregnancy outcome, including prematurity, growth retardation, stillbirth, congenital deformity and neonatal morbidity and mortality. Even if the maternal circulation is cleared of infection, persistent viral infection of the placenta is a major outcome of maternal infection, with severe consequences for the infant. Further, the placenta can be a source of persistent maternal systemic infection. Despite the dire consequences of persistent placental infection, we do not fully understand the mechanisms enough to generate targeted interventions in infected mothers. We have developed a mouse model of maternal infection with Lymphocytic Choriomeningitis virus LCMV and observed that although the maternal circulation is cleared within 8 days of infection, the placenta remains persistently infected and so does the uterus many days post-partum. We have evidence suggesting that this is related to CD8 T cell function, as manipulation of the cytokine milieu increases both presence and function of these cells and is associated with decreased viral load. Understanding mechanisms for metabolic change in immune cells is becoming a major area of interest. Due to their exponential expansion in response to antigen stimulation, the effect of metabolism in T cells is recognized as critical. In addition to proliferation, changes in metabolism can also affect effector function (e.g. cytokine secretion, cytotoxicity). We, like others, have found that this is particularly true for CD8 T cells and through our collaborator, Dr. Rincon and her examination of this, she has discovered a unique protein, Methylation-Controlled J protein (MCJ) that regulates mitochondrial metabolism in CD8 T cells. Importantly, deficiency in this molecule leads to enhanced metabolism and function, as well as overall improvement in immunologic memory in the setting of influenza infection. In this R21 application, we propose to i) test the hypothesis that there is downregulation of placental CD8 T cell effector function through upregulation in MCJ and ii) test the hypothesis that deficiency in MCJ leads to decreased placental virus after maternal infection with LCMV. These studies are in keeping with renewed interest in maternal immunity in NIAID, as they will advance our understanding of microbe-vector-host interactions and their influence on pregnancy outcomes.

View original record on NIH RePORTER →