| Literature DB >> 23891328 |
Sabina Victoria1, Jairo R Temerozo, Livia Gobbo, Haynna K Pimenta-Inada, Dumith Chequer Bou-Habib.
Abstract
Patients infected with HIV-1, the etiological agent of AIDS, have increased intestinal permeability, which allows for the passage of microbial products, including Toll-like receptor (TLR) ligands, into circulation. The exposure of HIV-1-infected cells to certain TLR agonists affects viral replication, but studies associating viral production with the activation of TLR2 in HIV-1-infected cells are rare and controversial. Here, we report that the TLR2 ligands Zymosan and Pam3CSK4 potently inhibit HIV-1 replication in acutely infected monocyte-derived macrophages and the exposure to TLR2 ligands prior to infection renders macrophages refractory to HIV-1 production. Macrophage treatment with Pam3CSK4 did not change the cellular expression of the HIV-1 entry receptors CD4 and CCR5. Both TLR2 ligands increased the macrophage production of β-chemokines and IL-10, and the blockage of these soluble factors prevented the inhibitory effect of TLR2 activation on HIV-1 replication. Our findings show that the direct engagement of TLR2 in HIV-1-infected macrophages increase cellular resistance to HIV-1 infection, and that controlling HIV-1 replication with agonists for TLR2 might have implications for the development of antiretroviral therapies.Entities:
Keywords: AIDS; HIV; HIV-1; IL; IL-10; LPS; Macrophages; PAMP; PBMCs; PHA; TLR; Toll-like receptor; Toll-like receptors.; acquired immunodeficiency syndrome; human immunodeficiency virus type-1; interleukin; lipopolysaccharide; pathogen-associated molecular patterns; peripheral blood mononuclear cells; phytohemagglutinin; β-Chemokines
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Year: 2013 PMID: 23891328 DOI: 10.1016/j.imbio.2013.06.006
Source DB: PubMed Journal: Immunobiology ISSN: 0171-2985 Impact factor: 3.144