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CXCR2

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Immunopharmacology Ligand  Target has curated data in GtoImmuPdb

Target id: 69

Nomenclature: CXCR2

Family: Chemokine receptors

This receptor has a proposed ligand; see the Latest Pairings page for more information.

Gene and Protein Information Click here for help
class A G protein-coupled receptor
Species TM AA Chromosomal Location Gene Symbol Gene Name Reference
Human 7 360 2q35 CXCR2 C-X-C motif chemokine receptor 2 53,69
Mouse 7 359 1 38.41 cM Cxcr2 C-X-C motif chemokine receptor 2 11
Rat 7 359 9q33 Cxcr2 C-X-C motif chemokine receptor 2 23
Previous and Unofficial Names Click here for help
IL8RB [53] | IL-8R2 | KC receptor [11] | CD182 | CXC-R2 | GRO/MGSA receptor | high affinity interleukin-8 receptor B | CD128 | Gpcr16 | chemokine (C-X-C motif) receptor 2
Database Links Click here for help
Specialist databases
GPCRdb cxcr2_human (Hs), cxcr2_mouse (Mm), cxcr2_rat (Rn)
Other databases
Alphafold
ChEMBL Target
Ensembl Gene
Entrez Gene
Human Protein Atlas
KEGG Gene
OMIM
Pharos
RefSeq Nucleotide
RefSeq Protein
UniProtKB
Wikipedia
Natural/Endogenous Ligands Click here for help
CXCL1 {Sp: Human}
CXCL6 {Sp: Human}
CXCL8 {Sp: Human}
CXCL2 {Sp: Human}
CXCL3 {Sp: Human}
CXCL5 {Sp: Human}
CXCL7 {Sp: Human}
CXCL1 {Sp: Mouse}
CXCL2 {Sp: Mouse}
CXCL3 {Sp: Mouse}
CXCL5 {Sp: Mouse}
CXCL1 {Sp: Rat}
CXCL2 {Sp: Rat}
CXCL3 {Sp: Rat}
CXCL5 {Sp: Rat}
Comments: macrophage derived lectin is a proposed ligand, single publication

Download all structure-activity data for this target as a CSV file go icon to follow link

Agonists
Key to terms and symbols Click column headers to sort
Ligand Sp. Action Value Parameter Reference
[125I]CXCL8 (human) Peptide Click here for species-specific activity table Ligand is labelled Ligand is radioactive Hs Full agonist 9.0 – 9.4 pKd 34,79
pKd 9.0 – 9.4 (Kd 1.02x10-9 – 3.98x10-10 M) [34,79]
[125I]KC-Tyr Peptide Ligand is labelled Ligand is radioactive Mm Full agonist 8.4 pKd 11
pKd 8.4 [11]
CXCL6 {Sp: Human} Peptide Click here for species-specific activity table Ligand is endogenous in the given species Immunopharmacology Ligand Hs Full agonist 7.0 pKd 95
pKd 7.0 [95]
HIV-1 matrix protein p17 Peptide Hs Agonist 6.9 pKd 30
pKd 6.9 (Kd 1.3x10-7 M) [30]
CXCL8 {Sp: Human} Peptide Click here for species-specific activity table Ligand is endogenous in the given species Immunopharmacology Ligand Hs Full agonist 8.8 – 9.5 pKi 8,34,53,91,94
pKi 8.8 – 9.5 [8,34,53,91,94]
CXCL1 {Sp: Human} Peptide Ligand is endogenous in the given species Immunopharmacology Ligand Hs Full agonist 8.4 – 9.7 pKi 34,53,94
pKi 8.4 – 9.7 [34,53,94]
CXCL1 {Sp: Human} Peptide Immunopharmacology Ligand Mm Full agonist 8.1 pKi 11
pKi 8.1 [11]
CXCL1 {Sp: Rat} Peptide Immunopharmacology Ligand Mm Full agonist 7.2 – 8.8 pKi 11
pKi 8.8 [11]
pKi 7.2 [11]
CXCL8 {Sp: Human} Peptide Immunopharmacology Ligand Mm Full agonist 6.4 pKi 11
pKi 6.4 [11]
CXCL3 {Sp: Human} Peptide Ligand is endogenous in the given species Immunopharmacology Ligand Hs Full agonist 7.8 – 9.2 pIC50 4
pIC50 7.8 – 9.2 [4]
vCXCL1 Peptide Click here for species-specific activity table Hs Agonist 8.3 pIC50 58
pIC50 8.3 (IC50 5.6x10-9 M) [58]
CXCL2 {Sp: Human} Peptide Ligand is endogenous in the given species Immunopharmacology Ligand Hs Full agonist 7.0 – 9.1 pIC50 4
pIC50 7.0 – 9.1 [4]
CXCL5 {Sp: Human} Peptide Ligand is endogenous in the given species Immunopharmacology Ligand Hs Full agonist 6.9 – 9.0 pIC50 4
pIC50 6.9 – 9.0 [4]
CXCL7 {Sp: Human} Peptide Ligand is endogenous in the given species Immunopharmacology Ligand Hs Full agonist 6.3 – 9.3 pIC50 4
pIC50 6.3 – 9.3 [4]
View species-specific agonist tables
Agonist Comments
The cathelicidin peptide LL-37 may act as a functional ligand for CXCR2 on human neutrophils, but binding affinity was not determined [98].
Antagonists
Key to terms and symbols View all chemical structures Click column headers to sort
Ligand Sp. Action Value Parameter Reference
navarixin Small molecule or natural product Primary target of this compound Click here for species-specific activity table Immunopharmacology Ligand Hs Antagonist 10.3 pIC50 6,24
pIC50 10.3 (IC50 4.9x10-11 M) [6,24]
AZD5069 Small molecule or natural product Primary target of this compound Click here for species-specific activity table Immunopharmacology Ligand Hs Antagonist 9.1 pIC50 71
pIC50 9.1 (IC50 7.9x10-10 M) [71]
Description: Measuring displacement of CXCL8 binding to recombinant CXCR2 in HEK cell membrane preparations.
danirixin Small molecule or natural product Immunopharmacology Ligand Hs Antagonist 7.9 pIC50 66
pIC50 7.9 (IC50 1.25x10-8 M) [66]
SB 225002 Small molecule or natural product Immunopharmacology Ligand Hs Antagonist 7.7 pIC50 90
pIC50 7.7 (IC50 1.99x10-8 M) [90]
elubirixin Small molecule or natural product Primary target of this compound Immunopharmacology Ligand Hs Antagonist 7.7 pIC50 6
pIC50 7.7 (IC50 2.2x10-8 M) [6]
SX-517 Small molecule or natural product Hs Antagonist 7.2 pIC50 59
pIC50 7.2 (IC50 6x10-8 M) [59]
NSC 157449 Small molecule or natural product Hs Antagonist 6.3 pIC50 90
pIC50 6.3 [90]
Allosteric Modulators
Key to terms and symbols View all chemical structures Click column headers to sort
Ligand Sp. Action Value Parameter Reference
reparixin Small molecule or natural product Immunopharmacology Ligand Hs Negative 6.4 pIC50 8
pIC50 6.4 (IC50 4x10-7 M) [8]
Allosteric Modulator Comments
The mechanism of inhibition exhibited by reparixin is not fully resolved. The compound may act as a negative allosteric modulator, rather than an antagonist.
Ladarixin (DF2156A, a reparixin derivative; Pubchem CID 11372270) is a dual CXCR1/2 non‐competitive allosteric modulator that inhibits CXCL1- and CXCL8-induced leukocyte chemotaxis [9]. It is compound 57 in Moriconi et al.'s 2007 J Med Chem paper [67]. DF2156A reached Phase 2 clinical evaluation in patients with the autoimmune pruritic skin disease bullous pemphigoid, but the study was terminated due to limited efficacy in the first tranche of enrolled participants (see NCT01571895). Ladarixin has since been reported to show potential therapeutic utility in the treatment of experimental cutaneous and uveal melanomas [49], and is being studied as a therapeutic option in newly diagnosed type I diabetes patients (see NCT02814838). DF2755A and DF2726 are non-competitive negative allosteric modulators of CXCL8 signalling via CXCR1 and CXCR2 [12,56].
Other Binding Ligands
Key to terms and symbols Click column headers to sort
Ligand Sp. Action Value Parameter Reference
Mz438 Small molecule or natural product Ligand is labelled N/A - 8.4 pKd 41
pKd 8.4 (Kd 4.17x10-9 M) [41]
Description: Binding affinity in a cellular context
Immunopharmacology Comments
CXCR2 is one of more than 20 distinct chemokine receptors expressed in human leukocytes. Chemokines primarily act to promote leukocyte chemotaxis to sites of inflammation. CXCR2 is discussed in relation to immuno-oncology in [2]. From a therapeutic perspective, small molecule CXCR2 antagonists (e.g., AZD5069, danirixin) have been developed to selectively block neutrophilic inflammatory pathways in chronic inflammatory lung diseases. In addition to blocking excessive neutrophil recruitment in blood [73] and to the lungs of more severe asthma patients [88], AZD5069 can also act as a NET-stabilizing agent to disrupt NET formation in sputum neutrophils derived from patients with COPD [77,87].
Immuno Process Associations
Immuno Process:  Inflammation
Immuno Process:  Antigen presentation
Immuno Process:  Immune regulation
Immuno Process:  Cytokine production & signalling
Immuno Process:  Chemotaxis & migration
Immuno Process:  Cellular signalling
Primary Transduction Mechanisms Click here for help
Transducer Effector/Response
Gi/Go family Adenylyl cyclase inhibition
Calcium channel
Comments:  The βγ subunit of the Gi G protein is necessary for chemotaxis [70] and calcium mobilisation [34].
References:  27,34,70
Secondary Transduction Mechanisms Click here for help
Transducer Effector/Response
Calcium channel
Other - See Comments
Comments:  Additional information on signaling pathways can be found in [89]. Agonists at high concentrations induce phosphorylation of CXCR2, leading to homologous desensitization, receptor internalization and partial degradation [7,18,26,68]. CXCR2 couples mainly to G protein-coupled receptor kinase 6 (GRK6) to negatively regulate receptor sensitization and trafficking [78].
References:  46
Tissue Distribution Click here for help
Neutrophils.
Species:  Human
Technique:  Western blotting.
References:  57
CX3CR1low CD14+ monocytes.
Species:  Human
Technique:  FACS
References:  29
CNS: hippocampus, dentate nucleus, pontine nuclei, locus coeruleus, paraventricular nucleus, and in the anterior horn, interomediolateral cell column, and Clarke's column of the spinal cord.
Species:  Human
Technique:  Immunohistochemistry.
References:  38
Polymorphonuclear neutrophils.
Species:  Human
Technique:  Flow cytometry.
References:  22
Bronchial epithelial cells.
Species:  Human
Technique:  RT-PCR and flow cytometry.
References:  25
Urinary tract epithelial cells.
Species:  Human
Technique:  Immunohistochemistry.
References:  31
Chondrocytes.
Species:  Human
Technique:  Flow cytometry.
References:  61
Umbilical vein endothelial cells (HUVECs).
Species:  Human
Technique:  immunocytochemistry.
References:  54
Basophils.
Species:  Human
Technique:  Flow cytometry and RT-PCR
References:  42,74
Mast cells.
Species:  Human
Technique:  RNAse protection assay and flow cytometry.
References:  72
NK cells and lymphocytes.
Species:  Human
Technique:  FACS
References:  16
Peritoneal exudate cells.
Species:  Mouse
Technique:  Northern blotting.
References:  11
Alveolar macrophages.
Species:  Mouse
Technique:  Immunohistochemistry.
References:  65
NKT cells.
Species:  Mouse
Technique:  FACS
References:  40
Bone-marrow endothelial progenitor cell (EPC).
Species:  Mouse
Technique:  FACS
References:  37
Hippocampal neurons.
Species:  Rat
Technique:  RT-PCR.
References:  62
Lung, speen, neutrophil.
Species:  Rat
Technique:  RNase protection assay and Northern blotting.
References:  23
Tissue Distribution Comments
The expression of CXCR1 and CXCR2 on NK cells is under debate. CXCR2 is also expressed by many non-hematopoietic cells, including endothelial cells and tumor cells.
Expression Datasets Click here for help

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Log average relative transcript abundance in mouse tissues measured by qPCR from Regard, J.B., Sato, I.T., and Coughlin, S.R. (2008). Anatomical profiling of G protein-coupled receptor expression. Cell, 135(3): 561-71. [PMID:18984166] [Raw data: website]

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Functional Assays Click here for help
Measurement of intracellular Ca2+ levels in HEK 293 cells transfected with the human CXCR2 receptor.
Species:  Human
Tissue:  HEK 293 cells.
Response measured:  Increase in intracellular Ca2+.
References:  53,95-96
Measurement of intracellular Ca2+ levels in HEK 293 cells transfected with the rat CXCR2 receptor.
Species:  Rat
Tissue:  HEK 293 cells.
Response measured:  Increase in intracellular Ca2+.
References:  23
Measurement of chemotaxis of mouse peripheral blood leukocytes endogenously expressing the CXCR2 receptor.
Species:  Mouse
Tissue:  Peripheral blood leukocytes.
Response measured:  Chemotaxis.
References:  11
Measurement of Ca2+ levels in Jurkat cells transfected with the human CXCR2 receptor.
Species:  Human
Tissue:  Jurkat cells.
Response measured:  Ca2+ mobilisation.
References:  45-46,92
Measurement of elastase released by human neutrophils endogenously expressing the CXCR2 receptor.
Species:  Human
Tissue:  Neutrophils.
Response measured:  Release of elastase.
References:  45-46,92
Measurement of chemotaxis of human mast cells, HMC-1, endogenously expressing the CXCR2 receptor.
Species:  Human
Tissue:  HMC-1 cells.
Response measured:  Chemotaxis.
References:  72
Measurement of focal adhesion kinase (FAK) activity and chemotaxis of HEK 293 and RBL cells transfected with the CXCR2 receptor.
Species:  Human
Tissue:  HEK 293 and RBL cells.
Response measured:  FAK phosphorylation and chemotaxis.
References:  27
Measurement of chemotaxis of HEK 293 cells transfected with the human CXCR2 receptor.
Species:  Human
Tissue:  HEK 293 cells.
Response measured:  Chemotaxis.
References:  27,95
Measurement of cAMP levels in CHO cells transfected with the human CXCR2 receptor.
Species:  Human
Tissue:  CHO cells.
Response measured:  Inhibition of cAMP accumulation.
References:  34
Phosphorylation of focal adhesion kinase.
Species:  Human
Tissue:  Human CXCR2-transfected RBL 2H3 cells.
Response measured:  Elevated spreading.
References:  18
Measurement of neutrophil extracellular traps (NETs) formation of COPD-sputum-derived neutrophils endogenously expressing the human CXCR2 receptor.
Species:  Human
Tissue:  Sputum neutrophils
Response measured:  NET formation
References:  77,87
Physiological Functions Click here for help
Angiogenesis.
Species:  Rat
Tissue:  Cornea.
References:  3
Bacterial sepsis.
Species:  Mouse
Tissue: 
References:  84
Macrophage recruitment.
Species:  Rat
Tissue:  In vivo (kidney).
References:  97
Macrophage recruitment.
Species:  Mouse
Tissue:  In vivo.
References:  10
Chemotaxis.
Species:  Human
Tissue:  Mast cells.
References:  72
Chemotaxis.
Species:  Human
Tissue:  Neutrophils.
References:  90
Hypertrophic differentiation.
Species:  Human
Tissue:  Chondrocytes.
References:  61
Cell proliferation and inhibition of apoptosis.
Species:  Human
Tissue:  Umbilical vein endothelial cells.
References:  54
Cutaneous wound repair.
Species:  Mouse
Tissue:  In vivo.
References:  20,64
Chemotaxis.
Species:  Human
Tissue:  Microvascular endothelial cells (HMVECs).
References:  3
Neovascularisation (angiogenesis).
Species:  Rat
Tissue:  Cornea.
References:  3
Neutrophil recruitment.
Species:  Mouse
Tissue:  In vivo.
References:  19,32,35,50,64
Transendothelial movement of mast cell progenitors into intestinal tissue.
Species:  Mouse
Tissue:  In vivo (small intestine).
References:  1
Ergress from bone marrow.
Species:  Mouse
Tissue:  Neutrophils.
References:  52
Host defense in murine urinary tract infection.
Species:  Mouse
Tissue:  Neutrophils.
References:  75
Proliferation and migration of endothelial cells.
Species:  Human
Tissue:  HUVECs and HMECs.
References:  3,55
Neutrophil recruitment to skin following infection by HSV-1.
Species:  Mouse
Tissue:  Neutrophils.
References:  83
Angiogenesis.
Species:  Mouse
Tissue:  Bone marrow-derived endothelial progenitor cells (EPCs).
References:  39
Neutrophil infiltration to pancreas during autoimmune diabetes.
Species:  Mouse
Tissue:  Neutrophils.
References:  21
Neutrophil infiltration to the bronchial tissue and sputum in severe asthma.
Species:  Human
Tissue: 
References:  88
Neutrophil recruitment in peripheral circulation: human and non-human primates.
Species:  Human
Tissue: 
References:  47,73,86
Physiological Functions Comments
CXCR2 is implicated in ischemic injury, trauma and multiple sclerosis [81], and in NET formation [87].
Physiological Consequences of Altering Gene Expression Click here for help
CXCR2 knockin mice have been developed, where the mouse CXCR2 receptor is replaced by human CXCR2. This mouse model demonstrates that both the mouse and human forms of the receptor are functionally equivalent. This model allows us to test the role of the human receptor using animal studies.
Species:  Mouse
Tissue: 
Technique:  Gene targeting in embryonic stem cells.
References:  63
CXCR2 knockout mice exhibit impaired corneal neovascular (angiogenic) response.
Species:  Mouse
Tissue: 
Technique:  Gene targeting in embryonic stem cells.
References:  3
CXCR2 knockout mice exhibit impaired neutrophil recruitment during inflammatory responses.
Species:  Mouse
Tissue: 
Technique:  Gene targeting in embryonic stem cells.
References:  19,32,35,44,50,64
CXCR2 receptor knockout mice exhibit delayed cutaneous wound healing (delayed epithelialisation and decreased neovascularisation). They have defective neutrophil recruitment as well as altered monocyte recruitment and Il-1β secretion.
Species:  Mouse
Tissue: 
Technique:  Gene targeting in embryonic stem cells.
References:  20
CXCR2 receptor knockout mice exhibit decreased airway hyperreactivity in response to respiratory syncytial virus (RSV) infection compared to wild-type mice.
Species:  Mouse
Tissue: 
Technique:  Gene targeting in embryonic stem cells.
References:  65
CXCR2 knockout mice subjected to ischaemia-reperfusion exhibit reduced myocardial infarct size and reduced inflammatory cell recruitment compared to wild-type mice.
Species:  Mouse
Tissue: 
Technique:  Gene targeting in embryonic stem cells.
References:  85
CXCR2 receptor knockout mice exhibit a decreased number of mast cell progenitors found in the small intestine.
Species:  Mouse
Tissue: 
Technique:  Gene targeting in embryonic stem cells.
References:  1
CXCR2 receptor knockout mice exhibit a dysfunctional neutrophil response to infection. The neutrophils are unable to cross epithelial barriers and therefore accumulate in large quantities the subepithelial tissue. Unable to clear the infection, the mice develop swollen kidneys, neutrophil abscesses, high numbers of bacteria and renal scarring.
Species:  Mouse
Tissue: 
Technique:  Gene targeting in embryonic stem cells.
References:  31,36
CXCR2 knockout mice exhibit enhanced numbers of myeloid progenitor cells in the femur, spleen and blood.
Species:  Mouse
Tissue: 
Technique:  Gene targeting in embryonic stem cells.
References:  13
CXCR2 is involved in development of acute and chronic pancreatitis.
Species:  Mouse
Tissue:  Pancreas.
Technique:  Overall knockout and specific deletion of Cxcr2 from myeloid cells.
References:  82
CXCR2(-/-) mice failed to show PMN infiltration into the mucosa in a chronic colitis model, and showed limited signs of mucosal damage and reduced clinical symptoms.
Species:  Mouse
Tissue:  Colonic mucosa; PMN
Technique:  Gene knock-outs
References:  14
Reduced CXCR2 leads to lymphadenopathy due to increase in B cells and to splenomegaly, resulting from an increase in metamyelocytes, band, and mature neutrophils.
Species:  Mouse
Tissue:  B cells; Neutrophils
Technique:  Gene targeting in embryonic stem cells.
References:  15
CXCR2 deficiency leads to defects in clearing bacteria from kidneys and bladders and development of bacteremia and symptoms of systemic disease.
Species:  Mouse
Tissue:  Kidneys; Bladders; Neutrophils
Technique:  Gene knock-outs
References:  28
CXCR2 is involved in cerebral endothelial activation and leukocyte recruitment during neuroinflammation.
Species:  Mouse
Tissue:  CNS; Endothelial cells; Leukocytes
Technique:  Gene knock-outs
References:  93
XCR2 is involved in EPC-mediated advanced atherosclerosis.
Species:  Mouse
Tissue:  Bone-marrow endothelial progenitor cell (EPC)
Technique:  Adoptive transfer of Cxcr2-/- Tie2-GFP+ EPCs.
References:  37
CXCR2 is a negative determinant for pancreatic islet survival after transplantation.
Species:  Mouse
Tissue:  Pancreatic islets; Polymorphonuclear leukocytes and NKT cells.
Technique:  Genetic and pharmacological blockade.
References:  17
CXCR2 regulates bone marrow blood vessel repair/regeneration and haematopoietic recovery following myeloablation and bone marrow transplantation.
Species:  Mouse
Tissue:  Bone marrow.
Technique:  Gene knock-outs
References:  33
Loss of CXCR2 suppresses chronic colonic inflammation and colitis-associated tumorigenesis.
Species:  Mouse
Tissue:  Colon; Myeloid-derived suppressor cells (MDSCs).
Technique:  Gene knock-outs
References:  48
Phenotypes, Alleles and Disease Models Click here for help Mouse data from MGI

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Allele Composition & genetic background Accession Phenotype Id Phenotype Reference
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
C.129S2(B6)-Cxcr2/J
MGI:105303  MP:0002334 abnormal airway responsiveness PMID: 11801688 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
involves: 129S2/SvPas * C57BL/6J
MGI:105303  MP:0002397 abnormal bone marrow morphology PMID: 8036519 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
C.129S2(B6)-Cxcr2/J
MGI:105303  MP:0008721 abnormal chemokine level PMID: 11801688 
Cxcr2tm1Mwm|Dstncorn1 Dstncorn1/Dstncorn1,Cxcr2tm1Mwm/Cxcr2tm1Mwm
involves: 129S2/SvPas * A/WySn * BALB/c * brachy stock
MGI:105303  MGI:1929270  MP:0001312 abnormal cornea morphology PMID: 18628996 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
C.129S2(B6)-Cxcr2/J
MGI:105303  MP:0003009 abnormal cytokine secretion PMID: 11714818 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
C.129S2(B6)-Cxcr2/J
MGI:105303  MP:0002465 abnormal eosinophil physiology PMID: 11801688 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
involves: 129S2/SvPas * C57BL/6J
MGI:105303  MP:0008111 abnormal granulocyte differentiation PMID: 8036519 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
C.129S2(B6)-Cxcr2/J
MGI:105303  MP:0008751 abnormal interleukin level PMID: 11801688  14707102 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
C.129S2(B6)-Cxcr2/J
MGI:105303  MP:0002442 abnormal leukocyte physiology PMID: 15356099 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
involves: 129S2/SvPas * C57BL/6J
MGI:105303  MP:0002348 abnormal lymph node medulla PMID: 8036519 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
C.129S2(B6)-Cxcr2/J
MGI:105303  MP:0000920 abnormal myelination PMID: 12176324 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
involves: 129S2/SvPas * C57BL/6J
MGI:105303  MP:0001601 abnormal myelopoiesis PMID: 8036519 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
involves: 129S2/SvPas * BALB/c
MGI:105303  MP:0001601 abnormal myelopoiesis PMID: 16094689 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
C.129S2(B6)-Cxcr2/J
MGI:105303  MP:0002463 abnormal neutrophil physiology PMID: 11801688  15466624 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
involves: 129S2/SvPas * BALB/c
MGI:105303  MP:0002463 abnormal neutrophil physiology PMID: 16094689 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
C.129S2(B6)-Cxcr2/J
MGI:105303  MP:0008042 abnormal NK T cell physiology PMID: 11123307 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
C.129S2(B6)-Cxcr2/J
MGI:105303  MP:0002281 abnormal respiratory mucosa goblet cell morphology PMID: 12626595 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
C.129S2(B6)-Cxcr2/J
MGI:105303  MP:0000955 abnormal spinal cord morphology PMID: 12176324 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
involves: 129S2/SvPas * C57BL/6J
MGI:105303  MP:0002357 abnormal spleen white pulp morphology PMID: 8036519 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
C.129S2(B6)-Cxcr2/J
MGI:105303  MP:0002444 abnormal T cell physiology PMID: 11801688 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
C.129S2(B6)-Cxcr2/J
MGI:105303  MP:0005465 abnormal T-helper 1 physiology PMID: 11801688 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
C.129S2(B6)-Cxcr2/J
MGI:105303  MP:0005466 abnormal T-helper 2 physiology PMID: 11801688 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
B6.Cg-Il8rb
MGI:105303  MP:0003448 altered tumor morphology PMID: 14978086 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
C.129S2(B6)-Cxcr2/J
MGI:105303  MP:0005542 corneal vascularization PMID: 14707102 
Cxcr2tm1Mwm|Dstncorn1 Dstncorn1/Dstncorn1,Cxcr2tm1Mwm/Cxcr2tm1Mwm
involves: 129S2/SvPas * A/WySn * BALB/c * brachy stock
MGI:105303  MGI:1929270  MP:0005542 corneal vascularization PMID: 18628996 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
C.129S2(B6)-Cxcr2/J
MGI:105303  MP:0002335 decreased airway responsiveness PMID: 12626595 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
involves: 129S2/SvPas * BALB/c
MGI:105303  MP:0001265 decreased body size PMID: 16094689 
Cxcr2tm1(IL8RB)Dktr Cxcr2tm1(IL8RB)Dktr/Cxcr2tm1(IL8RB)Dktr
involves: 129S2/SvPas * C57BL/6
MGI:105303  MP:0003918 decreased kidney weight PMID: 16094689 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
B6.Cg-Il8rb
MGI:105303  MP:0001273 decreased metastatic potential PMID: 14978086 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
C.129S2(B6)-Cxcr2/J
MGI:105303  MP:0000954 decreased oligodendrocyte progenitor number PMID: 12176324 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
C.129S2(B6)-Cxcr2/J
MGI:105303  MP:0009764 decreased sensitivity to induced morbidity/mortality PMID: 14500678 
Cxcr2tm1(IL8RB)Dktr Cxcr2tm1(IL8RB)Dktr/Cxcr2tm1(IL8RB)Dktr
involves: 129S2/SvPas * C57BL/6
MGI:105303  MP:0004953 decreased spleen weight PMID: 16094689 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
C.129S2(B6)-Cxcr2/J
MGI:105303  MP:0005398 decreased susceptibility to fungal infection PMID: 11801688 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
C.129S2(B6)-Cxcr2/J
MGI:105303  MP:0003436 decreased susceptibility to induced arthritis PMID: 19109198 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
involves: 129S2/SvPas * BALB/c
MGI:105303  MP:0004956 decreased thymus weight PMID: 16094689 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
B6.Cg-Il8rb
MGI:105303  MP:0003447 decreased tumor growth/size PMID: 14978086 
Cxcr2tm1Mwm|Tg(TRAMP)8247Ng Cxcr2tm1Mwm/Cxcr2tm1Mwm,Tg(TRAMP)8247Ng/?
involves: 129S2/SvPas * BALB/c * C57BL/6
MGI:105303  MGI:2680364  MP:0003447 decreased tumor growth/size PMID: 16941672 
Cxcr2+|Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2+
C.129S2(B6)-Cxcr2/J
MGI:105303  MP:0002908 delayed wound healing PMID: 10951241 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
C.129S2(B6)-Cxcr2/J
MGI:105303  MP:0002908 delayed wound healing PMID: 10951241 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
involves: 129S2/SvPas * C57BL/6J
MGI:105303  MP:0008542 enlarged cervical lymph nodes PMID: 8036519 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
involves: 129S2/SvPas * C57BL/6J
MGI:105303  MP:0000702 enlarged lymph nodes PMID: 8036519 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
involves: 129S2/SvPas * C57BL/6J
MGI:105303  MP:0000691 enlarged spleen PMID: 8036519 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
involves: 129S2/SvPas * BALB/c
MGI:105303  MP:0000240 extramedullary hematopoiesis PMID: 16094689 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
involves: 129S2/SvPas * C57BL/6J
MGI:105303  MP:0008720 impaired neutrophil migration PMID: 8036519 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
C.129S2(B6)-Cxcr2/J
MGI:105303  MP:0008720 impaired neutrophil migration PMID: 11069247  11714818 
Cxcr2+|Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2+
C.129S2(B6)-Cxcr2/J
MGI:105303  MP:0008719 impaired neutrophil recruitment PMID: 10951241 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
C.129S2(B6)-Cxcr2/J
MGI:105303  MP:0008719 impaired neutrophil recruitment PMID: 10951241  11046063  15385471 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
involves: 129S2/SvPas * C57BL/6J
MGI:105303  MP:0005014 increased B cell number PMID: 8036519 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
involves: 129S2/SvPas * C57BL/6J
MGI:105303  MP:0008596 increased circulating interleukin-6 level PMID: 8036519 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
involves: 129S2/SvPas * BALB/c
MGI:105303  MP:0004928 increased epididymis weight PMID: 16094689 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
involves: 129S2/SvPas * BALB/c
MGI:105303  MP:0000322 increased granulocyte number PMID: 16094689 
Cxcr2tm1(IL8RB)Dktr Cxcr2tm1(IL8RB)Dktr/Cxcr2tm1(IL8RB)Dktr
involves: 129S2/SvPas * C57BL/6
MGI:105303  MP:0000322 increased granulocyte number PMID: 16094689 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
C.129S2(B6)-Cxcr2/J
MGI:105303  MP:0002497 increased IgE level PMID: 11801688 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
involves: 129S2/SvPas * BALB/c
MGI:105303  MP:0003917 increased kidney weight PMID: 16094689 
Cxcr2tm1(IL8RB)Dktr Cxcr2tm1(IL8RB)Dktr/Cxcr2tm1(IL8RB)Dktr
involves: 129S2/SvPas * C57BL/6
MGI:105303  MP:0000218 increased leukocyte cell number PMID: 16094689 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
involves: 129S2/SvPas * C57BL/6J
MGI:105303  MP:0000219 increased neutrophil cell number PMID: 8036519 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
involves: 129S2/SvPas * BALB/c
MGI:105303  MP:0004909 increased seminal vesicle weight PMID: 16094689 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
involves: 129S2/SvPas * BALB/c
MGI:105303  MP:0004952 increased spleen weight PMID: 16094689 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
C.129S2(B6)-Cxcr2/J
MGI:105303  MP:0002412 increased susceptibility to bacterial infection PMID: 11069247 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
C.129S2(B6)-Cxcr2/J
MGI:105303  MP:0005027 increased susceptibility to parasitic infection PMID: 11714818 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
C.129S2(B6)-Cxcr2/J
MGI:105303  MP:0002418 increased susceptibility to viral infection PMID: 14707102 
Cxcr2tm1Mwm Cxcr2tm1Mwm/Cxcr2tm1Mwm
involves: 129S2/SvPas * C57BL/6J
MGI:105303  MP:0010373 myeloid hyperplasia PMID: 8036519 
Cxcr2tm1(IL8RB)Dktr Cxcr2tm1(IL8RB)Dktr/Cxcr2tm1(IL8RB)Dktr
involves: 129S2/SvPas * C57BL/6
MGI:105303  MP:0002768 small adrenal glands PMID: 16094689 
Cxcr2tm1(IL8RB)Dktr Cxcr2tm1(IL8RB)Dktr/Cxcr2tm1(IL8RB)Dktr
involves: 129S2/SvPas * C57BL/6
MGI:105303  MP:0000601 small liver PMID: 16094689 
Gene Expression and Pathophysiology Comments
In patients with type 1 diabetes the CXCR1/2 negative allosteric modulator reparixin improved outcome in a phase 2 randomized, open-label pilot study with a single infusion of allogeneic islets [17]. Administration of reparixin in on-pump coronary artery bypass grafting (CABG) patients appears to be feasible and safe. It concurrently attenuated postoperative granulocytosis in peripheral blood [76].
In many malignancies, elevated CXCR2 activity has been connected to increased tumor growth and metastasis.
Biologically Significant Variants Click here for help
Type:  Single nucleotide polymorphism
Species:  Human
Description:  Multiple single nucleotide polymorphisms in CXCR2 are associated with cystic fibrosis.
References:  51
Type:  Single nucleotide polymorphism
Species:  Human
Description:  Functional SNP in the 3'UTR of CXCR2 that is associated with reduced risk of lung cancer and provides protection from recurrent acute pyelonephritis
Amino acid change:  none
Nucleotide change:  C>T at position 127 of 3' UTR
SNP accession: 
References:  43,80
Type:  Single nucleotide polymorphism
Species:  Human
Description:  Single nucleotide polymorphisms in CXCR2 are associated with reduced WBC count.
References:  5
Type:  Frameshift mutation
Species:  Human
Description:  Family-based re-sequencing study in a pedigree with congenital neutropenia identified a loss-of-function mutation comprising a translational frameshift and premature termination codon after six novel amino acids.
Amino acid change:  H323fs6X
Nucleotide change:  968delA
References:  5
Type:  Single nucleotide polymorphism
Species:  Human
Description:  The 785C ->T polymorphism may be associated with a reduced risk of developing chronic obstructive pulmonary disease.
Nucleotide change:  785C>T
References:  60

References

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