Mycobacterium tuberculosis impairs human memory CD4+ T cell recognition of M2 but not M1-like macrophages

结核分枝杆菌损害人类记忆 CD4+ T 细胞对 M2 型巨噬细胞的识别,但不影响 M1 型巨噬细胞的识别

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作者:Daniel P Gail, Vinicius G Suzart, Weinan Du, Avinaash Kaur Sandhu, Jessica Jarvela, Mary Nantongo, Ivan Mwebaza, Soumya Panigrahi, Michael L Freeman, David H Canaday, W Henry Boom, Richard F Silver, Stephen M Carpenter

Abstract

Direct recognition of Mycobacterium tuberculosis (Mtb)-infected cells is required for protection by CD4+ T cells. While impaired T cell recognition of Mtb-infected macrophages was demonstrated in mice, data are lacking for humans. Using T cells and monocyte-derived macrophages (MDMs) from individuals with latent Mtb infection (LTBI), we quantified the frequency of memory CD4+ T cell activation in response to autologous MDMs infected with virulent Mtb. We observed robust T cell activation in response to Mtb infection of M1-like macrophages differentiated using GM-CSF, while M2-like macrophages differentiated using M-CSF were poorly recognized. However, non-infected GM-CSF and M-CSF MDMs loaded with exogenous antigens elicited similar CD4+ T cell activation. IL-10 was preferentially secreted by infected M-CSF MDMs, and neutralization improved T cell activation. These results suggest that preferential infection of macrophages with an M2-like phenotype limits T cell-mediated protection against Mtb. Vaccine development should focus on T cell recognition of Mtb-infected macrophages.

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