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. 2013 Jun 10;8(6):e66825. doi: 10.1371/journal.pone.0066825

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© 2013 Ogbomo, et al

This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.

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M153R-mediated down-regulation of MHC I or blockade of MHC I with mAb results in enhanced NK cell-mediated killing of U87 (A) or U251 (B) target cells. For mAb blocking, mock-infected or virus-infected cells were pre-incubated with 20 µg/ml MHC class I Ab (W6/32) or isotype-matched control Ab for 30 min before co-culture with NK cells. Columns represent means of triplicate of one representative experiment. Error bars represent 95% confidence intervals. Supernatant was collected from 4 h co-cultures of NK cells and Mock- or MYXV- or vMyx-M153KO-infected U87 (C) or U251 (D) target cells, that were pre-incubated with either 20 µg/ml MHC class I Ab (W6/32) or isotype-matched control, and analyzed by ELISA for granzyme B release. Baseline NK cells granzyme B release was 1624 pg/ml. The result shown is granzyme B release in NK/glioma co-culture minus baseline granzyme B release by NK cells alone. Columns represent means of triplicate of one representative experiment. Error bars represent 95% confidence intervals.