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Tumor-Targeting Anti-CD20 Antibodies Mediate Expansion of Memory Natural Killer Cells: Impact of CD16 Affinity Ligation Conditions and Priming. | LitMetric

AI Article Synopsis

  • Natural killer (NK) cells are crucial for the body's natural immune response against tumors, and their effectiveness can be influenced by environmental factors like viral infections, particularly human cytomegalovirus (HCMV), which helps form a long-lived "memory" NK cell subset.
  • The study highlights how anti-CD20 therapeutic monoclonal antibodies (mAbs) can promote the growth of these memory NK cells and shows that both the HCMV status of the donor and the method of CD16 activation play crucial roles in this process.
  • Findings reveal that low-affinity interactions from rituximab induce greater NK cell proliferation, while high-affinity interactions from glycoengineered obinutuzumab enhance their functional responses, providing insights

Article Abstract

Natural killer (NK) cells represent a pivotal player of innate anti-tumor immune responses. The impact of environmental factors in shaping the representativity of different NK cell subsets is increasingly appreciated. Human cytomegalovirus (HCMV) infection profoundly affects NK cell compartment, as documented by the presence of a CD94/NKG2CFcεRIγ long-lived "memory" NK cell subset, endowed with enhanced CD16-dependent functional capabilities, in a fraction of HCMV-seropositive subjects. However, the requirements for memory NK cell pool establishment/maintenance and activation have not been fully characterized yet. Here, we describe the capability of anti-CD20 tumor-targeting therapeutic monoclonal antibodies (mAbs) to drive the selective expansion of memory NK cells and we show the impact of donor' HCMV serostatus and CD16 affinity ligation conditions on this event. expanded memory NK cells maintain the phenotypic and functional signature of their freshly isolated counterpart; furthermore, our data demonstrate that CD16 affinity ligation conditions differently affect memory NK cell proliferation and functional activation, as rituximab-mediated low-affinity ligation represents a superior proliferative stimulus, while high-affinity aggregation mediated by glycoengineered obinutuzumab results in improved multifunctional responses. Our work also expands the molecular and functional characterization of memory NK cells, and investigates the possible impact of CD16 functional allelic variants on their and expansions. These results reveal new insights in Ab-driven memory NK cell responses in a therapeutic setting and may ultimately inspire new NK cell-based intervention strategies against cancer, in which the enhanced responsiveness to mAb-bound target could significantly impact therapeutic efficacy.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5958227PMC
http://dx.doi.org/10.3389/fimmu.2018.01031DOI Listing

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