AUTHOR=Murshid Ayesha , Borges Thiago J. , Lang Benjamin J. , Calderwood Stuart K. 

TITLE=The Scavenger Receptor SREC-I Cooperates with Toll-Like Receptors to Trigger Inflammatory Innate Immune Responses

JOURNAL=Frontiers in Immunology

VOLUME=Volume 7 - 2016

YEAR=2016

URL=https://www.frontiersin.org/journals/immunology/articles/10.3389/fimmu.2016.00226

DOI=10.3389/fimmu.2016.00226

ISSN=1664-3224

ABSTRACT=3	SREC-I is a Class F scavenger receptor expressed by immune cells with a significant role in

4	CD8+ and CD4+-mediated T cell immunity. This receptor can also modulate the function of Toll

5	like receptors (TLR) which play essential roles in innate immunity. Here we will discuss how
	
65	SREC-I alters double stranded RNA (dsRNA)-mediated TLR3 activation. Earlier it was found

76	that human monocyte/macrophage THP1 cells as well as bone marrow derived macrophages

87	from mice exhibited increased responses to polyinosine-polycytidylic acid (poly I:C, PIC) and

98	CpG	(unmethylated)	DNA	and	enhanced	production	of	inflammatory	cytokines	with

109	overexpressed SREC-I. Our data also showed that intracellular/endocytic TLR3 and TLR9 could

1110	directly interact with SREC-I in the presence of their respective ligands. We also observed that

1211	the internalized ligand along with TLR3/TLR9 colocalized in the endosome in macrophages and

1312	THP-1 cells over expressing these receptors. In the absence of these ligands there was no

1413	detectable colocalization between the SREC-I and endocytic TLRs. It was shown earlier that

1514	SREC-I stimulated dsRNA/CpGDNA mediated TLR3/TLR9 activation of the innate immune

1615	response by triggering signaling through the NF-κB, IRF3 and MAP kinase pathways leading to

1716	transcription of cytokine genes. We also established that SREC-I can associate with plasma

1817	membrane TLRs, like TLR2 and TLR4. We demonstrated that SREC-I-TLR4 signals more

1918	efficiently from lipid microdomain in which LPS can associate with SREC-I-TLR4 complex. We

2019	also proved that SREC-I is an alternate receptor for LPS capable of internalizing the complex

2120	and for endocytic TLR ligands as well. This binding activated endocytic TLR mediated

2221	downstream cytokine production in THP1 cells and macrophages. Finally, SREC-I could also

2322	form complexes with TLR2 and induce the release of cytokines in the presence of bacterial, viral

2423	and fungal ligands.