Literature DB >> 21972290

Allo-HLA-reactive T cells inducing graft-versus-host disease are single peptide specific.

Avital L Amir1, Dirk M van der Steen, Renate S Hagedoorn, Michel G D Kester, Cornelis A M van Bergen, Jan W Drijfhout, Arnoud H de Ru, J H Frederik Falkenburg, Peter A van Veelen, Mirjam H M Heemskerk.   

Abstract

T-cell alloreactivity directed against non-self-HLA molecules has been assumed to be less peptide specific than conventional T-cell reactivity. A large variation in degree of peptide specificity has previously been reported, including single peptide specificity, polyspecificity, and peptide degeneracy. Peptide polyspecificity was illustrated using synthetic peptide-loaded target cells, but in the absence of confirmation against endogenously processed peptides this may represent low-avidity T-cell reactivity. Peptide degeneracy was concluded based on recognition of Ag-processing defective cells. In addition, because most investigated alloreactive T cells were in vitro activated and expanded, the previously determined specificities may have not been representative for alloreactivity in vivo. To study the biologically relevant peptide specificity and avidity of alloreactivity, we investigated the degree of peptide specificity of 50 different allo-HLA-reactive T-cell clones which were activated and expanded in vivo during GVHD. All but one of the alloreactive T-cell clones, including those reactive against Ag-processing defective T2 cells, recognized a single peptide allo-HLA complex, unique for each clone. Down-regulation of the expression of the recognized Ags using silencing shRNAs confirmed single peptide specificity. Based on these results, we conclude that biologically relevant alloreactivity selected during in vivo immune response is peptide specific.

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Year:  2011        PMID: 21972290     DOI: 10.1182/blood-2011-05-354787

Source DB:  PubMed          Journal:  Blood        ISSN: 0006-4971            Impact factor:   22.113


  28 in total

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8.  Incidence, risk factors, and outcomes of sclerosis in patients with chronic graft-versus-host disease.

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Review 9.  Allo-reactive T cells for the treatment of hematological malignancies.

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10.  Targeting B-cell neoplasia with T-cell receptors recognizing a CD20-derived peptide on patient-specific HLA.

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