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Merck

Immunotherapeutic Blockade of CD47 Inhibitory Signaling Enhances Innate and Adaptive Immune Responses to Viral Infection.

Cell reports (2020-04-16)
Lamin B Cham, Laughing Bear Torrez Dulgeroff, Michal Caspi Tal, Tom Adomati, Fanghui Li, Hilal Bhat, Anfei Huang, Philipp A Lang, Mary E Moreno, Jose M Rivera, Sofiya A Galkina, Galina Kosikova, Cheryl A Stoddart, Joseph M McCune, Lara M Myers, Irving L Weissman, Karl S Lang, Kim J Hasenkrug
RESUMEN

Paradoxically, early host responses to infection include the upregulation of the antiphagocytic molecule, CD47. This suggests that CD47 blockade could enhance antigen presentation and subsequent immune responses. Indeed, mice treated with anti-CD47 monoclonal antibody following lymphocytic choriomeningitis virus infections show increased activation of both macrophages and dendritic cells (DCs), enhancement of the kinetics and potency of CD8+ T cell responses, and significantly improved virus control. Treatment efficacy is critically dependent on both APCs and CD8+ T cells. In preliminary results from one of two cohorts of humanized mice infected with HIV-1 for 6 weeks, CD47 blockade reduces plasma p24 levels and restores CD4+ T cell counts. The results indicate that CD47 blockade not only enhances the function of innate immune cells but also links to adaptive immune responses through improved APC function. As such, immunotherapy by CD47 blockade may have broad applicability to treat a wide range of infectious diseases.

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Sigma-Aldrich
N,N-Dimetilformamida, for molecular biology, ≥99%
Sigma-Aldrich
L-Glutamine–Penicillin–Streptomycin solution, L-glutamine 200 mM, streptomycin 10 mg/mL, penicillin 10,000 units, 0.1 μm filtered, BioReagent, suitable for cell culture