CD4+ T cells reactive to enteric bacterial antigens in spontaneously colitic C3H/HeJBir mice: increased T helper cell type 1 response and ability to transfer disease. - Wikidata - awgldk - TriplyDB

CD4+ T cells reactive to enteric bacterial antigens in spontaneously colitic C3H/HeJBir mice: increased T helper cell type 1 response and ability to transfer disease.

CD4+ T cells reactive to enteric bacterial antigens in spontaneously colitic C3H/HeJBir mice: increased T helper cell type 1 response and ability to transfer disease.

http://www.wikidata.org/entity/Q36400483

about

Rhinosinusitis derived Staphylococcal enterotoxin B possibly associates with pathogenesis of ulcerative colitis.Effector and memory T cell responses to commensal bacteria Central role of gimap5 in maintaining peripheral tolerance and T cell homeostasis in the gut Mechanisms of Natural Tolerance in the Intestine Inflammatory bowel disease Th1-type responses mediate spontaneous ileitis in a novel murine model of Crohn's disease.Immune therapy in inflammatory bowel disease and models of colitis.Colonic bacteria express an ulcerative colitis pANCA-related protein epitope Temporal and spatial analysis of clinical and molecular parameters in dextran sodium sulfate induced colitis.CD103-CD11b+ dendritic cells regulate the sensitivity of CD4 T-cell responses to bacterial flagellin.The role of IL-10 in inflammatory bowel disease: "of mice and men".Colitis in transgenic and knockout animals as models of human inflammatory bowel disease.Helicobacter hepaticus triggers colitis in specific-pathogen-free interleukin-10 (IL-10)-deficient mice through an IL-12- and gamma interferon-dependent mechanism The C3H/HeJBir mouse model: a high susceptibility phenotype for colitis.Microbiota innate stimulation is a prerequisite for T cell spontaneous proliferation and induction of experimental colitis Probiotics and inflammatory bowel disease: is there a scientific rationale?A major quantitative trait locus on chromosome 3 controls colitis severity in IL-10-deficient mice.Segmented filamentous bacteria are potent stimuli of a physiologically normal state of the murine gut mucosal immune system Differential induction of colitis and gastritis in HLA-B27 transgenic rats selectively colonized with Bacteroides vulgatus or Escherichia coli.Identification of a novel mycobacterial histone H1 homologue (HupB) as an antigenic target of pANCA monoclonal antibody and serum immunoglobulin A from patients with Crohn's disease.Different subsets of enteric bacteria induce and perpetuate experimental colitis in rats and mice.Molecular cloning of a Bacteroides caccae TonB-linked outer membrane protein identified by an inflammatory bowel disease marker antibody.The gastrointestinal ecosystem: a precarious alliance among epithelium, immunity and microbiota.Association between chronic liver and colon inflammation during the development of murine syngeneic graft-versus-host disease The SAMP1/Yit mouse: another step closer to modeling human inflammatory bowel disease.Recent advances in inflammatory bowel disease.Bin1 attenuation suppresses experimental colitis by enforcing intestinal barrier function.Crucial role for CD69 in the pathogenesis of dextran sulphate sodium-induced colitis.Induction of colitis by a CD4+ T cell clone specific for a bacterial epitope Relevance of commensal microbiota in the treatment and prevention of inflammatory bowel disease.Probiotics and inflammatory bowel disease: from fads and fantasy to facts and future.Accumulation of CD4+ T cells in the colon of CsA-treated mice following myeloablative conditioning and bone marrow transplantation.Microbiota regulation of inflammatory bowel disease and colorectal cancer.Gamma interferon augments the intracellular pathway for lipopolysaccharide (LPS) recognition in human intestinal epithelial cells through coordinated up-regulation of LPS uptake and expression of the intracellular Toll-like receptor 4-MD-2 complex.Immune networks in animal models of inflammatory bowel disease.Immunology of inflammatory bowel disease and molecular targets for biologics.Diversion of intestinal flow decreases the numbers of interleukin 4 secreting and interferon gamma secreting T lymphocytes in small bowel mucosa.Characterisation of mucosal lymphoid aggregates in ulcerative colitis: immune cell phenotype and TcR-gammadelta expression.Increased rectal mucosal enteroendocrine cells, T lymphocytes, and increased gut permeability following acute Campylobacter enteritis and in post-dysenteric irritable bowel syndrome Interleukin (IL)-21 promotes intestinal IgA response to microbiota.

P2860

Q24814625-CCC7A992-1EFA-4DC7-8A1C-1415E8A03004 Q27024742-E9C7BC28-52E0-442F-8948-D870896C2C4F Q27025911-7404C592-551D-407B-B64A-76197EFA8A18 Q29031968-D5D9FFA3-7054-4168-916F-BCC62CA37249 Q29615500-D1678F7C-B063-431E-B599-12E9525D5077 Q30307038-88A4FBCD-333B-49E9-B3D6-C0227621F1DE Q30774968-4E0CC5BC-9046-4950-9EC0-23DED94531C3 Q31518042-0262DD2A-547A-4B5A-A836-FAFDEB607BD5 Q33475620-9B7C2A3F-9F02-4172-8218-0995205DF8BC Q33654093-FCF67B92-569D-4A1E-AD8A-BFE5C5A2FBE3 Q33657725-285F1236-6C9A-4FF4-AF62-482803844C86 Q33713331-BE071326-DF10-402C-A62E-3C0110F13BB2 Q33767365-5CD6ED0E-636F-4F6D-AC64-DA154D95CE94 Q33867170-2FC0ABD8-6CEA-4AC3-A940-5845633225A1 Q33902387-D25A582C-D6E6-445D-816F-A487B6EC048E Q33930749-F3169D72-4227-4504-92B9-126BF3DD90BB Q33950098-3A188021-BC33-4D4B-87D8-2BB7AD858E6F Q34000988-A8091A93-B69A-4D1E-83E0-65833519CD9C Q34001149-2A18B8DA-C6BF-4D44-8468-6532AAB45CBE Q34002778-3BAAF020-6F81-4D8C-A4EB-5A205BF7131F Q34006798-01BD0369-6619-4FEF-8BCA-B67094147146 Q34009198-345C67ED-E935-401E-A146-75BAB0D83F07 Q34156291-CF72B85B-63E7-4805-826A-591FF5CF9859 Q34178879-07EA08AA-F008-4C99-ABF3-85ACC88FADB7 Q34187186-6CF00362-3802-4625-ABDA-A4858814720B Q34188405-9F3E1786-7FBC-466B-A23A-D1B06EF91CB8 Q34270337-A22EC6C8-C52F-46D8-8CAD-C9BA32607D69 Q34778713-0A87B8B5-9504-406D-B704-B4D879920B60 Q34792169-548A08C3-C50B-47BC-AB2A-ADAEEB6AB24B Q34813567-0DC1360A-EB6D-4B54-8F9B-58B034CCB3A8 Q34820458-AA303F5E-4B20-41A8-A855-31DA219BD51C Q34979948-E2D1E644-0AA4-4CF4-A579-1880B6664CFE Q35000300-E0C76961-4BD3-4C84-9501-BF368EBC1BD3 Q35011477-15891E85-34E0-458C-867B-EAE7CB220D29 Q35193871-588BF8B9-B092-483C-955A-6E244C37A2D8 Q35222593-8CE835AB-3134-4E6C-93BE-1D05AA19EDF4 Q35358504-60DB2326-1920-46B8-A69A-63A29D03F0D2 Q35361010-4D1692E7-9652-44CD-8DAF-72CDA05EE384 Q35362266-8972D95B-8AA7-4D5D-A5F0-10DBE735E3AA Q35542428-8375E6E2-9E77-402C-9EA6-4511BD551D58

P2860

CD4+ T cells reactive to enteric bacterial antigens in spontaneously colitic C3H/HeJBir mice: increased T helper cell type 1 response and ability to transfer disease.

http://www.wikidata.org/entity/Q36400483

description

1998 nî lūn-bûn

@nan

1998年の論文

@ja

1998年学术文章

@wuu

1998年学术文章

@zh-cn

1998年学术文章

@zh-hans

1998年学术文章

@zh-my

1998年学术文章

@zh-sg

1998年學術文章

@yue

1998年學術文章

@zh

1998年學術文章

@zh-hant

name

CD4+ T cells reactive to enter ...... d ability to transfer disease.

@ast

CD4+ T cells reactive to enter ...... d ability to transfer disease.

@en

type

label

CD4+ T cells reactive to enter ...... d ability to transfer disease.

@ast

CD4+ T cells reactive to enter ...... d ability to transfer disease.

@en

prefLabel

CD4+ T cells reactive to enter ...... d ability to transfer disease.

@ast

CD4+ T cells reactive to enter ...... d ability to transfer disease.

@en

P1433

Q36400483-95324273-AFCE-4A86-9DD4-C388D3D9088B

P1476

Q36400483-7DDA4276-2BE1-4682-8AC0-3B01C09B7C37

P2093

Q36400483-03BC942E-6AC6-49EF-8F1D-7246632BD8BA

Q36400483-22CC8A72-D988-459E-874E-B006403CE819

Q36400483-6B49FD31-5012-412C-ACFD-4C776016167C

Q36400483-71BE11F8-F9A0-4DC8-8218-FBB2E034215D

Q36400483-BEF96B06-26DD-401C-ACD4-65D08F7B192F

Q36400483-E8F47E7C-CB83-4638-8297-5B5C47B43FD8

Q36400483-FF259F85-5B3F-4DC5-932F-E0D1235169A5

P2860

Q36400483-0D37F940-92F2-4B02-B16C-1112999B8911

Q36400483-0DFB6A53-7C10-4D0C-BF64-9F798EA39F27

Q36400483-12E4CCAF-5008-4CE1-99E6-210522CC5F70

Q36400483-1A4B2F61-5C21-4590-A94E-E940522430FA

Q36400483-23A2E5FF-38DD-436D-8338-2AC3014D80F2

Q36400483-288F4225-E480-401E-A134-ADAD24C97924

Q36400483-3D1D2263-CBDD-43F0-AD7A-3FF7DD003F0A

Q36400483-4DBA2C12-F7CD-4AC3-94B2-075CC60CDF4E

Q36400483-5AA31E1E-4FAA-4139-87DB-2A9007DA14A8

Q36400483-6168F3E8-46C4-417E-8CED-208AC653FF1E

P304

Q36400483-790D2136-FA96-491B-BDC9-82A4330F4E55

P31

Q36400483-C8D450D7-F28F-4659-8257-431B3B51457D

P356

Q36400483-BEE8A8D5-827C-47CA-846C-50B5704435A4

P407

Q36400483-B9088384-80D1-4CBB-B70B-43878C21666F

P433

Q36400483-90752BB5-F995-4F31-A528-7B42B89FA84F

P478

Q36400483-D481F558-3FE7-42C0-82B7-7FD08498B301

P577

Q36400483-11A8AFFF-537F-42C5-B410-5435E523232C

P5875

Q36400483-92EB7BF2-31A4-4410-9DE0-E9A6DA754626

P698

Q36400483-7464198E-6AF9-47DF-877F-2E86364C4084

P932

Q36400483-86CED67D-0699-4E89-B5E8-7AD0E45C448C

P356

P1433

Journal of Experimental Medicine

P1476

CD4+ T cells reactive to enter ...... d ability to transfer disease.

@en

P2093

A Lazenby

http://www.w3.org/2001/XMLSchema#string

C O Elson

http://www.w3.org/2001/XMLSchema#string

E H Birkenmeier

http://www.w3.org/2001/XMLSchema#string

J P Sundberg

http://www.w3.org/2001/XMLSchema#string

R P McCabe

http://www.w3.org/2001/XMLSchema#string

S L Brandwein

http://www.w3.org/2001/XMLSchema#string

Y Cong

http://www.w3.org/2001/XMLSchema#string

P2860

Enterocolitis and colon cancer in interleukin-10-deficient mice are associated with aberrant cytokine production and CD4(+) TH1-like responses

Ulcerative colitis-like disease in mice with a disrupted interleukin-2 gene

Interleukin-10-deficient mice develop chronic enterocolitis

Responses of the Peyer's Patches in Germ-Free Mice to Antigenic Stimulation

Inhibition of Th1 responses prevents inflammatory bowel disease in scid mice reconstituted with CD45RBhi CD4+ T cells.

The gastrointestinal epithelium and its autochthonous bacterial flora.

CD4+ T cells that express high levels of CD45RB induce wasting disease when transferred into congenic severe combined immunodeficient mice. Disease development is prevented by cotransfer of purified CD4+ T cells.

The germfree state prevents development of gut and joint inflammatory disease in HLA-B27 transgenic rats

A rapid method for the isolation of functional thymus-derived murine lymphocytes

Normal luminal bacteria, especially Bacteroides species, mediate chronic colitis, gastritis, and arthritis in HLA-B27/human beta2 microglobulin transgenic rats.

P304

855-864

http://www.w3.org/2001/XMLSchema#string

P31

scholarly article

P356

10.1084/JEM.187.6.855

http://www.w3.org/2001/XMLSchema#string

P407

P433

6

http://www.w3.org/2001/XMLSchema#string

P478

187

http://www.w3.org/2001/XMLSchema#string

P577

1998-03-01T00:00:00Z

http://www.w3.org/2001/XMLSchema#dateTime

P5875

51298526

http://www.w3.org/2001/XMLSchema#string

P698

9500788

http://www.w3.org/2001/XMLSchema#string

P932

2212186

http://www.w3.org/2001/XMLSchema#string