TY - JOUR
T1 - Two novel human cytomegalovirus NK cell evasion functions target MICA for lysosomal degradation
AU - Fielding, Ceri A
AU - Aicheler, Rebecca
AU - Stanton, Richard J
AU - Wang, Eddie C Y
AU - Han, Song
AU - Seirafian, Sepehr
AU - Davies, James
AU - McSharry, Brian P
AU - Weekes, Michael P
AU - Antrobus, P Robin
AU - Prod'homme, Virginie
AU - Blanchet, Fabien P
AU - Sugrue, Daniel
AU - Cuff, Simone
AU - Roberts, Dawn
AU - Davison, Andrew J
AU - Lehner, Paul J
AU - Wilkinson, Gavin W G
AU - Tomasec, Peter
PY - 2014/5
Y1 - 2014/5
N2 - NKG2D plays a major role in controlling immune responses through the regulation of natural killer (NK) cells, αβ and γδ T-cell function. This activating receptor recognizes eight distinct ligands (the MHC Class I polypeptide-related sequences (MIC) A andB, and UL16-binding proteins (ULBP)1-6) induced by cellular stress to promote recognition cells perturbed by malignant transformation or microbial infection. Studies into human cytomegalovirus (HCMV) have aided both the identification and characterization of NKG2D ligands (NKG2DLs). HCMV immediate early (IE) gene up regulates NKGDLs, and we now describe the differential activation of ULBP2 and MICA/B by IE1 and IE2 respectively. Despite activation by IE functions, HCMV effectively suppressed cell surface expression of NKGDLs through both the early and late phases of infection. The immune evasion functions UL16, UL142, and microRNA(miR)-UL112 are known to target NKG2DLs. While infection with a UL16 deletion mutant caused the expected increase in MICB and ULBP2 cell surface expression, deletion of UL142 did not have a similar impact on its target, MICA. We therefore performed a systematic screen of the viral genome to search of addition functions that targeted MICA. US18 and US20 were identified as novel NK cell evasion functions capable of acting independently to promote MICA degradation by lysosomal degradation. The most dramatic effect on MICA expression was achieved when US18 and US20 acted in concert. US18 and US20 are the first members of the US12 gene family to have been assigned a function. The US12 family has 10 members encoded sequentially through US12-US21; a genetic arrangement, which is suggestive of an 'accordion' expansion of an ancestral gene in response to a selective pressure. This expansion must have be an ancient event as the whole family is conserved across simian cytomegaloviruses from old world monkeys. The evolutionary benefit bestowed by the combinatorial effect of US18 and US20 on MICA may have contributed to sustaining the US12 gene family.
AB - NKG2D plays a major role in controlling immune responses through the regulation of natural killer (NK) cells, αβ and γδ T-cell function. This activating receptor recognizes eight distinct ligands (the MHC Class I polypeptide-related sequences (MIC) A andB, and UL16-binding proteins (ULBP)1-6) induced by cellular stress to promote recognition cells perturbed by malignant transformation or microbial infection. Studies into human cytomegalovirus (HCMV) have aided both the identification and characterization of NKG2D ligands (NKG2DLs). HCMV immediate early (IE) gene up regulates NKGDLs, and we now describe the differential activation of ULBP2 and MICA/B by IE1 and IE2 respectively. Despite activation by IE functions, HCMV effectively suppressed cell surface expression of NKGDLs through both the early and late phases of infection. The immune evasion functions UL16, UL142, and microRNA(miR)-UL112 are known to target NKG2DLs. While infection with a UL16 deletion mutant caused the expected increase in MICB and ULBP2 cell surface expression, deletion of UL142 did not have a similar impact on its target, MICA. We therefore performed a systematic screen of the viral genome to search of addition functions that targeted MICA. US18 and US20 were identified as novel NK cell evasion functions capable of acting independently to promote MICA degradation by lysosomal degradation. The most dramatic effect on MICA expression was achieved when US18 and US20 acted in concert. US18 and US20 are the first members of the US12 gene family to have been assigned a function. The US12 family has 10 members encoded sequentially through US12-US21; a genetic arrangement, which is suggestive of an 'accordion' expansion of an ancestral gene in response to a selective pressure. This expansion must have be an ancient event as the whole family is conserved across simian cytomegaloviruses from old world monkeys. The evolutionary benefit bestowed by the combinatorial effect of US18 and US20 on MICA may have contributed to sustaining the US12 gene family.
KW - Adult
KW - Bacterial Proteins/metabolism
KW - Cells, Cultured
KW - Cytomegalovirus/immunology
KW - Enzyme Inhibitors/pharmacology
KW - Histocompatibility Antigens Class I/metabolism
KW - Humans
KW - Immune Evasion/drug effects
KW - Killer Cells, Natural/drug effects
KW - Leupeptins/pharmacology
KW - Luminescent Proteins/metabolism
KW - Lysosomes/drug effects
KW - Macrolides/pharmacology
KW - NK Cell Lectin-Like Receptor Subfamily K/physiology
KW - Proteolysis/drug effects
KW - Recombinant Proteins/metabolism
KW - Viral Proteins/physiology
UR - http://www.scopus.com/inward/record.url?scp=84901647915&partnerID=8YFLogxK
UR - http://www.scopus.com/inward/citedby.url?scp=84901647915&partnerID=8YFLogxK
U2 - 10.1371/journal.ppat.1004058
DO - 10.1371/journal.ppat.1004058
M3 - Article
C2 - 24787765
AN - SCOPUS:84901647915
SN - 1553-7366
VL - 10
SP - 1
EP - 17
JO - PLoS Pathogens
JF - PLoS Pathogens
IS - 5
M1 - e1004058
ER -