Accelerated turnover of MHC class II molecules in nonobese diabetic mice is developmentally and environmentally regulated in vivo and dispensable for autoimmunity. - Wikidata - awgldk - TriplyDB

Accelerated turnover of MHC class II molecules in nonobese diabetic mice is developmentally and environmentally regulated in vivo and dispensable for autoimmunity.

Accelerated turnover of MHC class II molecules in nonobese diabetic mice is developmentally and environmentally regulated in vivo and dispensable for autoimmunity.

http://www.wikidata.org/entity/Q37202316

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Genetic Analysis of Substrain Divergence in Non-Obese Diabetic (NOD) Mice Allele-Independent Turnover of Human Leukocyte Antigen (HLA) Class Ia Molecules Ubiquitin-mediated fluctuations in MHC class II facilitate efficient germinal center B cell responses.MHC Class II Protein Turnover In vivo and Its Relevance for Autoimmunity in Non-Obese Diabetic Mice.Regulation of type 1 diabetes development and B-cell activation in nonobese diabetic mice by early life exposure to a diabetogenic environment.

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Accelerated turnover of MHC class II molecules in nonobese diabetic mice is developmentally and environmentally regulated in vivo and dispensable for autoimmunity.

http://www.wikidata.org/entity/Q37202316

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article científic

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article scientifique

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articolo scientifico

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artigo científico

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bilimsel makale

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scientific article published on 15 May 2013

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vedecký článok

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vetenskaplig artikel

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videnskabelig artikel

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vědecký článek

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name

Accelerated turnover of MHC cl ...... dispensable for autoimmunity.

@en

Accelerated turnover of MHC cl ...... dispensable for autoimmunity.

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type

label

Accelerated turnover of MHC cl ...... dispensable for autoimmunity.

@en

Accelerated turnover of MHC cl ...... dispensable for autoimmunity.

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prefLabel

Accelerated turnover of MHC cl ...... dispensable for autoimmunity.

@en

Accelerated turnover of MHC cl ...... dispensable for autoimmunity.

@nl

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JIMMUNOL.1300551

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Journal of Immunology

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Accelerated turnover of MHC cl ...... dispensable for autoimmunity.

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Alessandra De Riva

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

Anne Cooke

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Leslie J Bluck

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Mark C Varley

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Michael J Deery

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

Robert Busch

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

P2860

Interaction of HLA-DR with an acidic face of HLA-DM disrupts sequence-dependent interactions with peptides

Breeding of a non-obese, diabetic strain of mice

A correlation between the relative predisposition of MHC class II alleles to type 1 diabetes and the structure of their proteins.

The I-Ag7 MHC class II molecule linked to murine diabetes is a promiscuous peptide binder.

Autoreactivity of T cells from nonobese diabetic mice: an I-Ag7-dependent reaction.

Natural peptides selected by diabetogenic DQ8 and murine I-A(g7) molecules show common sequence specificity.

Measuring proteome dynamics in vivo: as easy as adding water?

Mass isotopomer distribution analysis at eight years: theoretical, analytic, and experimental considerations.

Measurement of protein synthesis using heavy water labeling and peptide mass spectrometry: Discrimination between major histocompatibility complex allotypes.

Homeostatic expansion of T cells during immune insufficiency generates autoimmunity.

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5961-5971

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scholarly article

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10.4049/JIMMUNOL.1300551

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12

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190

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2013-05-15T00:00:00Z

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23677470

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3785126

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