Effective, Long-Term, Neutrophil Depletion Using a Murinized Anti-Ly-6G 1A8 Antibody

Publication date

2022-11

Authors

Olofsen, Patricia AORCID 0000-0002-6100-9290
Stip, Marjolein
Jansen, J H Marco
Chan, Chilam
Nederend, MaaikeISNI 0000000387532079
Tieland, Ralph G.
Tsioumpekou, Maria
Leusen, JeanetteORCID 0000-0003-4982-6914ISNI 0000000390807686

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Abstract

Neutrophils are crucial innate immune cells but also play key roles in various diseases, such as cancer, where they can perform both pro- and anti-tumorigenic functions. To study the function of neutrophils in vivo, these cells are often depleted using Ly-6G or Gr-1 depleting antibodies or genetic “knockout” models. However, these methods have several limitations, being only partially effective, effective for a short term, and lacking specificity or the ability to conditionally deplete neutrophils. Here, we describe the use of a novel murinized Ly-6G (1A8) antibody. The murinized Ly-6G antibody is of the mouse IgG2a isotype, which is the only isotype that can bind all murine Fcγ receptors and C1q and is, therefore, able to activate antibody-dependent cellular cytotoxicity (ADCC), antibody-dependent phagocytosis (ADCP) and complement-dependent cytotoxicity (CDC) pathways. We show that this mouse-Ly-6G antibody shows efficient, long-term, and near-complete (>90%) neutrophil depletion in the peripheral blood of C57Bl6/J, Balb/c, NXG and SCID mice for up to at least four weeks, using a standardized neutrophil depletion strategy. In addition, we show that neutrophils are efficiently depleted in the blood and tumor tissue of IMR32 tumor-bearing SCID mice, analyzed six weeks after the start of the treatment.

Keywords

cancer, immunotherapy, in vivo neutrophil targeting, neutrophil depletion, neutrophils, General Biochemistry,Genetics and Molecular Biology

Citation

Olofsen, P A, Stip, M C, Jansen, J H M, Chan, C, Nederend, M, Tieland, R G, Tsioumpekou, M & Leusen, J H W 2022, 'Effective, Long-Term, Neutrophil Depletion Using a Murinized Anti-Ly-6G 1A8 Antibody', Cells, vol. 11, no. 21, 3406. https://doi.org/10.3390/cells11213406