Youdong Pan 1 , Tian Tian 1 , Chang Ook Park 1 , Serena Y Lofftus 1 , Shenglin Mei 2 , Xing Liu 3 , Chi Luo 4 , John T O'Malley 1 , Ahmed Gehad 1 , Jessica E Teague 1 , Sherrie J Divito 1 , Robert Fuhlbrigge 1 , Pere Puigserver 4 , James G Krueger 5 , Gökhan S Hotamisligil 6 , Rachael A Clark 1 , 7 , Thomas S Kupper 1 , 7
Feb 20 2017
Tissue-resident memory T (TRM) cells persist indefinitely in epithelial barrier tissues and protect the host against pathogens. However, the biological pathways that enable the long-term survival of TRM cells are obscure. Here we show that mouse CD8(+) TRM cells generated by viral infection of the skin differentially express high levels of several molecules that mediate lipid uptake and intracellular transport, including fatty-acid-binding proteins 4 and 5 (FABP4 and FABP5). We further show that T-cell-specific deficiency of Fabp4 and Fabp5 (Fabp4/Fabp5) impairs exogenous free fatty acid (FFA) uptake by CD8(+) TRM cells and greatly reduces their long-term survival in vivo, while having no effect on the survival of central memory T (TCM) cells in lymph nodes. In vitro, CD8(+) TRM cells, but not CD8(+) TCM cells, demonstrated increased mitochondrial oxidative metabolism in the presence of exogenous FFAs; this increase was not seen in Fabp4/Fabp5 double-knockout CD8(+) TRM cells. The persistence of CD8(+) TRM cells in the skin was strongly diminished by inhibition of mitochondrial FFA β-oxidation in vivo. Moreover, skin CD8(+) TRM cells that lacked Fabp4/Fabp5 were less effective at protecting mice from cutaneous viral infection, and lung Fabp4/Fabp5 double-knockout CD8(+) TRM cells generated by skin vaccinia virus (VACV) infection were less effective at protecting mice from a lethal pulmonary challenge with VACV. Consistent with the mouse data, increased FABP4 and FABP5 expression and enhanced extracellular FFA uptake were also demonstrated in human CD8(+) TRM cells in normal and psoriatic skin. These results suggest that FABP4 and FABP5 have a critical role in the maintenance, longevity and function of CD8(+) TRM cells, and suggest that CD8(+) TRM cells use exogenous FFAs and their oxidative metabolism to persist in tissue and to mediate protective immunity.