Literature DB >> 18453625

Antigen sensitivity of CD22-specific chimeric TCR is modulated by target epitope distance from the cell membrane.

Scott E James1, Philip D Greenberg, Michael C Jensen, Yukang Lin, Jinjuan Wang, Brian G Till, Andrew A Raubitschek, Stephen J Forman, Oliver W Press.   

Abstract

We have targeted CD22 as a novel tumor-associated Ag for recognition by human CTL genetically modified to express chimeric TCR (cTCR) recognizing this surface molecule. CD22-specific cTCR targeting different epitopes of the CD22 molecule promoted efficient lysis of target cells expressing high levels of CD22 with a maximum lytic potential that appeared to decrease as the distance of the target epitope from the target cell membrane increased. Targeting membrane-distal CD22 epitopes with cTCR(+) CTL revealed defects in both degranulation and lytic granule targeting. CD22-specific cTCR(+) CTL exhibited lower levels of maximum lysis and lower Ag sensitivity than CTL targeting CD20, which has a shorter extracellular domain than CD22. This diminished sensitivity was not a result of reduced avidity of Ag engagement, but instead reflected weaker signaling per triggered cTCR molecule when targeting membrane-distal epitopes of CD22. Both of these parameters were restored by targeting a ligand expressing the same epitope, but constructed as a truncated CD22 molecule to approximate the length of a TCR:peptide-MHC complex. The reduced sensitivity of CD22-specific cTCR(+) CTL for Ag-induced triggering of effector functions has potential therapeutic applications, because such cells selectively lysed B cell lymphoma lines expressing high levels of CD22, but demonstrated minimal activity against autologous normal B cells, which express lower levels of CD22. Thus, our results demonstrate that cTCR signal strength, and consequently Ag sensitivity, can be modulated by differential choice of target epitopes with respect to distance from the cell membrane, allowing discrimination between targets with disparate Ag density.

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Year:  2008        PMID: 18453625      PMCID: PMC2585549          DOI: 10.4049/jimmunol.180.10.7028

Source DB:  PubMed          Journal:  J Immunol        ISSN: 0022-1767            Impact factor:   5.422


  63 in total

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Journal:  J Immunol       Date:  2007-04-01       Impact factor: 5.422

4.  T cell receptor binding kinetics required for T cell activation depend on the density of cognate ligand on the antigen-presenting cell.

Authors:  Pablo A González; Leandro J Carreño; Daniel Coombs; Jorge E Mora; Edith Palmieri; Byron Goldstein; Stanley G Nathenson; Alexis M Kalergis
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5.  Autocrine activation of PDGFRalpha promotes the progression of ovarian cancer.

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6.  Cutting edge: dueling TCRs: peptide antagonism of CD4+ T cells with dual antigen specificities.

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Journal:  Leukemia       Date:  2005-01       Impact factor: 11.528

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  107 in total

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Review 3.  Recent advances and discoveries in the mechanisms and functions of CAR T cells.

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6.  CAR T Cells with Enhanced Sensitivity to B Cell Maturation Antigen for the Targeting of B Cell Non-Hodgkin's Lymphoma and Multiple Myeloma.

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Review 8.  Bispecific T-Cell Redirection versus Chimeric Antigen Receptor (CAR)-T Cells as Approaches to Kill Cancer Cells.

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Review 9.  Chimeric antigen receptor-engineered T cells for immunotherapy of cancer.

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10.  Antibody-mediated B-cell depletion before adoptive immunotherapy with T cells expressing CD20-specific chimeric T-cell receptors facilitates eradication of leukemia in immunocompetent mice.

Authors:  Scott E James; Nural N Orgun; Thomas F Tedder; Mark J Shlomchik; Michael C Jensen; Yukang Lin; Philip D Greenberg; Oliver W Press
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