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The antiviral immune response in mice devoid of immunoproteasome activity

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2011

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Kirk, Christopher J.

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http://nbn-resolving.de/urn:nbn:de:bsz:352-181342
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https://doi.org/10.4049/jimmunol.1101064
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The Journal of Immunology. 2011, 187(11), pp. 5548-5557. ISSN 0022-1767. eISSN 1550-6606. Available under: doi: 10.4049/jimmunol.1101064

Zusammenfassung

The replacement of the catalytically active proteasome subunits β1, β2, and β5 by the immunoproteasome subunits low molecular mass polypeptide (LMP) 2 (β1i), multicatalytic endopeptidase complex-like-1 (MECL-1) (β2i), and LMP7 (β5i) is required for the production of numerous class I ligands. Hitherto, investigation of the immunoproteasome was confined to the analysis of mice deficient for one or two immunosubunits. In this study, we characterized LMP2(-/-)/MECL-1(-/-) double-deficient mice and used the well-defined LMP7-selective inhibitor ONX 0914 in these mice to generate mice lacking the activity of all immunoproteasome subunits. LMP2(-/-)/MECL-1(-/-) double-deficient mice had strongly reduced numbers of CD8(+) T cells in the spleen. Nevertheless, infection with the lymphocytic choriomeningits virus induced a normal cytotoxic T cell response in these mice, although the T cell response to several class I epitopes was altered. Treatment of LMP2(-/-)/MECL-1(-/-) double-deficient mice with the LMP7-selective inhibitor ONX 0914 elicited a strong CTL response in lymphocytic choriomeningitis virus-infected mice. Thereby, the T(CD8+) response to nucleoprotein 205-212, which is barely detectable in LMP2(-/-)/MECL-1(-/-) double-deficient mice, could be reverted to normal levels by LMP7 inhibition. Additional experiments could demonstrate that the increased CTL response to the nucleoprotein 205-212 in mice lacking functional immunoproteasome is due to an altered class I presentation of this epitope. Taken together, to our knowledge, this is the first study investigating viral infection in mice lacking activity of all three immunoproteasome subunits.

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570 Biowissenschaften, Biologie

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ISO 690BASLER, Michael, Ulrike BECK, Christopher J. KIRK, Marcus GRÖTTRUP, 2011. The antiviral immune response in mice devoid of immunoproteasome activity. In: The Journal of Immunology. 2011, 187(11), pp. 5548-5557. ISSN 0022-1767. eISSN 1550-6606. Available under: doi: 10.4049/jimmunol.1101064
BibTex
@article{Basler2011-12-01antiv-18134,
  year={2011},
  doi={10.4049/jimmunol.1101064},
  title={The antiviral immune response in mice devoid of immunoproteasome activity},
  number={11},
  volume={187},
  issn={0022-1767},
  journal={The Journal of Immunology},
  pages={5548--5557},
  author={Basler, Michael and Beck, Ulrike and Kirk, Christopher J. and Gröttrup, Marcus}
}
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    <dcterms:abstract xml:lang="eng">The replacement of the catalytically active proteasome subunits β1, β2, and β5 by the immunoproteasome subunits low molecular mass polypeptide (LMP) 2 (β1i), multicatalytic endopeptidase complex-like-1 (MECL-1) (β2i), and LMP7 (β5i) is required for the production of numerous class I ligands. Hitherto, investigation of the immunoproteasome was confined to the analysis of mice deficient for one or two immunosubunits. In this study, we characterized LMP2(-/-)/MECL-1(-/-) double-deficient mice and used the well-defined LMP7-selective inhibitor ONX 0914 in these mice to generate mice lacking the activity of all immunoproteasome subunits. LMP2(-/-)/MECL-1(-/-) double-deficient mice had strongly reduced numbers of CD8(+) T cells in the spleen. Nevertheless, infection with the lymphocytic choriomeningits virus induced a normal cytotoxic T cell response in these mice, although the T cell response to several class I epitopes was altered. Treatment of LMP2(-/-)/MECL-1(-/-) double-deficient mice with the LMP7-selective inhibitor ONX 0914 elicited a strong CTL response in lymphocytic choriomeningitis virus-infected mice. Thereby, the T(CD8+) response to nucleoprotein 205-212, which is barely detectable in LMP2(-/-)/MECL-1(-/-) double-deficient mice, could be reverted to normal levels by LMP7 inhibition. Additional experiments could demonstrate that the increased CTL response to the nucleoprotein 205-212 in mice lacking functional immunoproteasome is due to an altered class I presentation of this epitope. Taken together, to our knowledge, this is the first study investigating viral infection in mice lacking activity of all three immunoproteasome subunits.</dcterms:abstract>
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