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Distinct CD16a features on human NK cells observed by flow cytometry correlate with increased ADCC.


ABSTRACT: Natural killer (NK) cells destroy tissue that have been opsonized with antibodies. Strategies to generate or identify cells with increased potency are expected to enhance NK cell-based immunotherapies. We previously generated NK cells with increased antibody-dependent cell mediated cytotoxicity (ADCC) following treatment with kifunensine, an inhibitor targeting mannosidases early in the N-glycan processing pathway. Kifunensine treatment also increased the antibody-binding affinity of Fc γ receptor IIIa/CD16a. Here we demonstrate that inhibiting NK cell N-glycan processing increased ADCC. We reduced N-glycan processing with the CRIPSR-CAS9 knockdown of MGAT1, another early-stage N-glycan processing enzyme, and showed that these cells likewise increased antibody binding affinity and ADCC. These experiments led to the observation that NK cells with diminished N-glycan processing capability also revealed a clear phenotype in flow cytometry experiments using the B73.1 and 3G8 antibodies binding two distinct CD16a epitopes. We evaluated this "affinity profiling" approach using primary NK cells and identified a distinct shift and differentiated populations by flow cytometry that correlated with increased ADCC.

SUBMITTER: Benavente MCR 

PROVIDER: S-EPMC10995120 | biostudies-literature | 2024 Apr

REPOSITORIES: biostudies-literature

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Distinct CD16a features on human NK cells observed by flow cytometry correlate with increased ADCC.

Benavente Maria C Rodriguez MCR   Hakeem Zainab A ZA   Davis Alexander R AR   Murray Nathan B NB   Azadi Parastoo P   Mace Emily M EM   Barb Adam W AW  

Scientific reports 20240404 1


Natural killer (NK) cells destroy tissue that have been opsonized with antibodies. Strategies to generate or identify cells with increased potency are expected to enhance NK cell-based immunotherapies. We previously generated NK cells with increased antibody-dependent cell mediated cytotoxicity (ADCC) following treatment with kifunensine, an inhibitor targeting mannosidases early in the N-glycan processing pathway. Kifunensine treatment also increased the antibody-binding affinity of Fc γ recept  ...[more]

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