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Article ; Online: Allele-specific recognition by LILRB3 and LILRA6 of a cytokeratin 8-associated ligand on necrotic glandular epithelial cells.

Jones, Des C / Hewitt, Colin R A / López-Álvarez, María R / Jahnke, Martin / Russell, Alasdair I / Radjabova, Valeria / Trowsdale, Alice R Z / Trowsdale, John

Oncotarget

2016  Volume 7, Issue 13, Page(s) 15618–15631

Abstract: The LILRs are a family of receptors that regulate the activities of myelomonocytic cells. We found that specific allelic variants of two related members of the LILR family, LILRB3 and LILRA6, interact with a ligand exposed on necrotic glandular ... ...

Abstract The LILRs are a family of receptors that regulate the activities of myelomonocytic cells. We found that specific allelic variants of two related members of the LILR family, LILRB3 and LILRA6, interact with a ligand exposed on necrotic glandular epithelial cells. The extracellular domains of LILRB3 and LILRA6 are very similar and their genes are highly polymorphic. A commonly occurring allele, LILRB3*12, displayed particularly strong binding of these necrotic cells and further screening of the products of LILRB3 alleles identified motifs that correlated with binding. Immunoprecipitation of the ligand from epithelial cell lysates using recombinant LILRB3*12, identified cytokeratins 8, 18 and 19. Purified proteins obtained from epithelial cell lysates, using anti-cytokeratin 8 antibodies, were able to activate LILRB3*12 reporter cells. Knock-down of cytokeratin 8 in epithelial cells abrogated expression of the LILRB3 ligand, while staining with recombinant LILRB3*12 showed co-localisation with cytokeratin 8 and 18 in permeabilised breast cancer cells. Necrosis is a common feature of tumours. The finding of a necrosis-associated ligand for these two receptors raises the possibility of a novel interaction that alters immune responses within the tumour microenvironment. Since LILRB3 and LILRA6 genes are highly polymorphic the interaction may influence an individual's immune response to tumours.
MeSH term(s) Alleles ; Antigens, CD/genetics ; Antigens, CD/immunology ; Antigens, CD/metabolism ; Cell Line ; Epithelial Cells/metabolism ; Epithelial Cells/pathology ; Humans ; Keratin-8/metabolism ; Necrosis/immunology ; Necrosis/metabolism ; Polymorphism, Single Nucleotide ; Receptors, Immunologic/genetics ; Receptors, Immunologic/immunology ; Receptors, Immunologic/metabolism
Chemical Substances Antigens, CD ; Keratin-8 ; LILRA6 protein, human ; LILRB3 protein, human ; Receptors, Immunologic
Language English
Publishing date 2016-01-14
Publishing country United States
Document type Journal Article
ZDB-ID 2560162-3
ISSN 1949-2553 ; 1949-2553
ISSN (online) 1949-2553
ISSN 1949-2553
DOI 10.18632/oncotarget.6905
Database MEDical Literature Analysis and Retrieval System OnLINE

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