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Interleukin-22 regulates neutrophil recruitment in ulcerative colitis and is associated with resistance to ustekinumab therapy
by
Ding, Yuchun
, Yang, Feifei
, Pavlidis, Polychronis
, Niazi, Umar
, Powell, Nick
, Lamb, Christopher
, Lo, Jonathan W.
, Cozzetto, Domenico
, Tsakmaki, Anastasia
, Bewick, Gavin
, Pantazi, Eirini
, Li, Katherine
, Macdonald, Thomas T.
, Long, Anna K.
, Lord, Graham M.
, Madgwick, Matthew
, Alberts, Elena
, Friedman, Joshua
, Sa, Ana Caroline Costa
, Saqi, Mansoor
, Treveil, Agatha
, Digby- Bell, Jonathan
, Carey, Christopher D.
, Gul, Leila
, Korcsmaros, Tamas
in
13/100
/ 13/21
/ 13/31
/ 38/61
/ 38/91
/ 631/250/127/1213
/ 631/250/2502/2055
/ 631/250/2504/223/1699
/ 631/250/347
/ 64
/ 64/60
/ 692/4020/1503/257
/ Biopsy
/ Cell activation
/ Chemokines
/ Chemokines, CXC - metabolism
/ Chemotaxis
/ Colitis, Ulcerative - drug therapy
/ Colitis, Ulcerative - genetics
/ Colon
/ CXCR2 protein
/ Cytokines
/ Enrichment
/ Gene regulation
/ Homeostasis
/ Humanities and Social Sciences
/ Humans
/ Immune system
/ Inflammatory bowel disease
/ Inflammatory bowel diseases
/ Interleukin 22
/ Interleukin 23
/ Interleukin-8 - metabolism
/ Interleukins
/ Leukocytes (neutrophilic)
/ Microorganisms
/ Monoclonal antibodies
/ multidisciplinary
/ Neutrophil Infiltration
/ Neutrophils
/ Neutrophils - metabolism
/ Organoids
/ Patients
/ Receptors, Interleukin-8B - metabolism
/ Recruitment
/ Science
/ Science (multidisciplinary)
/ Stat3 protein
/ Transcription
/ Ulcerative colitis
/ Ustekinumab - pharmacology
/ Ustekinumab - therapeutic use
2022
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Interleukin-22 regulates neutrophil recruitment in ulcerative colitis and is associated with resistance to ustekinumab therapy
by
Ding, Yuchun
, Yang, Feifei
, Pavlidis, Polychronis
, Niazi, Umar
, Powell, Nick
, Lamb, Christopher
, Lo, Jonathan W.
, Cozzetto, Domenico
, Tsakmaki, Anastasia
, Bewick, Gavin
, Pantazi, Eirini
, Li, Katherine
, Macdonald, Thomas T.
, Long, Anna K.
, Lord, Graham M.
, Madgwick, Matthew
, Alberts, Elena
, Friedman, Joshua
, Sa, Ana Caroline Costa
, Saqi, Mansoor
, Treveil, Agatha
, Digby- Bell, Jonathan
, Carey, Christopher D.
, Gul, Leila
, Korcsmaros, Tamas
in
13/100
/ 13/21
/ 13/31
/ 38/61
/ 38/91
/ 631/250/127/1213
/ 631/250/2502/2055
/ 631/250/2504/223/1699
/ 631/250/347
/ 64
/ 64/60
/ 692/4020/1503/257
/ Biopsy
/ Cell activation
/ Chemokines
/ Chemokines, CXC - metabolism
/ Chemotaxis
/ Colitis, Ulcerative - drug therapy
/ Colitis, Ulcerative - genetics
/ Colon
/ CXCR2 protein
/ Cytokines
/ Enrichment
/ Gene regulation
/ Homeostasis
/ Humanities and Social Sciences
/ Humans
/ Immune system
/ Inflammatory bowel disease
/ Inflammatory bowel diseases
/ Interleukin 22
/ Interleukin 23
/ Interleukin-8 - metabolism
/ Interleukins
/ Leukocytes (neutrophilic)
/ Microorganisms
/ Monoclonal antibodies
/ multidisciplinary
/ Neutrophil Infiltration
/ Neutrophils
/ Neutrophils - metabolism
/ Organoids
/ Patients
/ Receptors, Interleukin-8B - metabolism
/ Recruitment
/ Science
/ Science (multidisciplinary)
/ Stat3 protein
/ Transcription
/ Ulcerative colitis
/ Ustekinumab - pharmacology
/ Ustekinumab - therapeutic use
2022
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Interleukin-22 regulates neutrophil recruitment in ulcerative colitis and is associated with resistance to ustekinumab therapy
by
Ding, Yuchun
, Yang, Feifei
, Pavlidis, Polychronis
, Niazi, Umar
, Powell, Nick
, Lamb, Christopher
, Lo, Jonathan W.
, Cozzetto, Domenico
, Tsakmaki, Anastasia
, Bewick, Gavin
, Pantazi, Eirini
, Li, Katherine
, Macdonald, Thomas T.
, Long, Anna K.
, Lord, Graham M.
, Madgwick, Matthew
, Alberts, Elena
, Friedman, Joshua
, Sa, Ana Caroline Costa
, Saqi, Mansoor
, Treveil, Agatha
, Digby- Bell, Jonathan
, Carey, Christopher D.
, Gul, Leila
, Korcsmaros, Tamas
in
13/100
/ 13/21
/ 13/31
/ 38/61
/ 38/91
/ 631/250/127/1213
/ 631/250/2502/2055
/ 631/250/2504/223/1699
/ 631/250/347
/ 64
/ 64/60
/ 692/4020/1503/257
/ Biopsy
/ Cell activation
/ Chemokines
/ Chemokines, CXC - metabolism
/ Chemotaxis
/ Colitis, Ulcerative - drug therapy
/ Colitis, Ulcerative - genetics
/ Colon
/ CXCR2 protein
/ Cytokines
/ Enrichment
/ Gene regulation
/ Homeostasis
/ Humanities and Social Sciences
/ Humans
/ Immune system
/ Inflammatory bowel disease
/ Inflammatory bowel diseases
/ Interleukin 22
/ Interleukin 23
/ Interleukin-8 - metabolism
/ Interleukins
/ Leukocytes (neutrophilic)
/ Microorganisms
/ Monoclonal antibodies
/ multidisciplinary
/ Neutrophil Infiltration
/ Neutrophils
/ Neutrophils - metabolism
/ Organoids
/ Patients
/ Receptors, Interleukin-8B - metabolism
/ Recruitment
/ Science
/ Science (multidisciplinary)
/ Stat3 protein
/ Transcription
/ Ulcerative colitis
/ Ustekinumab - pharmacology
/ Ustekinumab - therapeutic use
2022
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Interleukin-22 regulates neutrophil recruitment in ulcerative colitis and is associated with resistance to ustekinumab therapy
Journal Article
Interleukin-22 regulates neutrophil recruitment in ulcerative colitis and is associated with resistance to ustekinumab therapy
2022
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Overview
The function of interleukin-22 (IL-22) in intestinal barrier homeostasis remains controversial. Here, we map the transcriptional landscape regulated by IL-22 in human colonic epithelial organoids and evaluate the biological, functional and clinical significance of the IL-22 mediated pathways in ulcerative colitis (UC). We show that IL-22 regulated pro-inflammatory pathways are involved in microbial recognition, cancer and immune cell chemotaxis; most prominently those involving CXCR2
+
neutrophils. IL-22-mediated transcriptional regulation of CXC-family neutrophil-active chemokine expression is highly conserved across species, is dependent on STAT3 signaling, and is functionally and pathologically important in the recruitment of CXCR2
+
neutrophils into colonic tissue. In UC patients, the magnitude of enrichment of the IL-22 regulated transcripts in colonic biopsies correlates with colonic neutrophil infiltration and is enriched in non-responders to ustekinumab therapy. Our data provide further insights into the biology of IL-22 in human disease and highlight its function in the regulation of pathogenic immune pathways, including neutrophil chemotaxis. The transcriptional networks regulated by IL-22 are functionally and clinically important in UC, impacting patient trajectories and responsiveness to biological intervention.
Mechanisms of non-response to ustekinumab, a biologic targeting IL-23, are currently unclear. Here, the authors show that the transcriptional program regulated by IL-22, an IL-23 responsive cytokine, is enriched in patients with ulcerative colitis unresponsive to ustekinumab and associated with higher colon neutrophil recruitment and activation of upstream IL-22 regulators.
Publisher
Nature Publishing Group UK,Nature Publishing Group,Nature Portfolio
Subject
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