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http://dx.doi.org/10.4110/in.2011.11.2.100

Characterization of CTL Clones Specific for Single Antigen, H60 Minor Histocompatibility Antigen  

Jeon, Ji-Yeong (Department of Biomedical Sciences, Seoul National University College of Medicine)
Jung, Kyung-Min (Graduate Program of Immunology, Seoul National University College of Medicine)
Chang, Jun (Division of Life and Pharmaceutical Sciences, Ewha Womans University)
Choi, Eun-Young (Department of Biomedical Sciences, Seoul National University College of Medicine)
Publication Information
IMMUNE NETWORK / v.11, no.2, 2011 , pp. 100-106 More about this Journal
Abstract
Background: Disparities of Minor H antigens can induce graft rejection after MHC-matched transplantation. H60 has been characterized as a dominant antigen expressed on hematopoietic cells and considered to be an ideal model antigen for study on graft-versus-leukemia effect. Methods: Splenocytes from C57BL/6 mice immunized with H60 congenic splenocytes were used for establishment of H60-specific CTL clones. Then the clones were characterized for proliferation capacity and cytotoxicity after stimulation with H60. Clone #14, #15, and #23 were tested for the TCR binding avidity to H60-peptide/$H-2K^b$ and analyzed for TCR sequences. Results: H60-specific CTL clones showed different levels of proliferation capacity and cytotoxic activity to H60-stimulation. Clones #14, #15, and #23 showed high proliferation activity, high cytotoxicity, and low activities on both aspects, respectively, and have TCRs with different binding avidities to H60-peptide/$H-2K^b$ with $t_{1/2}$ values of 4.87, 6.92, and 13.03 minutes, respectively. The TCR usages were $V{\alpha}12D-3-01+J{\alpha}11-01$ and $V{\beta}12-1-01+D{\beta}1-01+J2-7-01$ for clone #14, $V{\alpha}13D-1-02+J{\alpha}34-02$ and $V{\beta}13-1-02+D{\beta}2-01+J{\beta}2-7-01$ for clone #15, and $V{\alpha}16D+J{\alpha}45-01$ and $V{\beta}12-1-01+D{\beta}1-01+J{\beta}2-5-01$ for clone #23. Conclusion: The results will be useful for modeling GVL and generation TCR transgenic mouse.
Keywords
CTL clone; Proliferation; Cytotoxicity; Avidity; TCR usage;
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