Anoxia and Glucose Supplementation Preserve Neutrophil Viability and Function

Overview

Journal Blood

Publisher Elsevier

Specialty Hematology

Date 2016 Jul 13

PMID 27402974

Citations 26

Authors

Valerie Monceaux

Clarisse Chiche-Lapierre

Catherine Chaput

Veronique Witko-Sarsat

Marie-Christine Prevost

Cormac T Taylor

Marie-Noelle Ungeheuer

Philippe J Sansonetti

Benoit S Marteyn

Affiliations

Soon will be listed here.

Abstract

Functional studies of human neutrophils and their transfusion for clinical purposes have been hampered by their short life span after isolation. Here, we demonstrate that neutrophil viability is maintained for 20 hours in culture media at 37°C under anoxic conditions with 3 mM glucose and 32 μg/mL dimethyloxalylglycine supplementation, as evidenced by stabilization of Mcl-1, proliferating cell nuclear antigen (PCNA), and pro-caspase-3. Notably, neutrophil morphology (nucleus shape and cell-surface markers) and functions (phagocytosis, degranulation, calcium release, chemotaxis, and reactive oxygen species production) were comparable to blood circulating neutrophils. The observed extension in neutrophil viability was reversed upon exposure to oxygen. Extending neutrophil life span allowed efficient transfection of plasmids (40% transfection efficiency) and short interfering RNA (interleukin-8, PCNA, and Bax), as a validation of effective and functional genetic manipulation of neutrophils both in vitro and in vivo. In vivo, transfusion of conditioned neutrophils in a neutropenic guinea pig model increased bacterial clearance of Shigella flexneri upon colonic infection, strongly suggesting that these conditioned neutrophils might be suitable for transfusion purposes. In summary, such conditioning of neutrophils in vitro should facilitate their study and offer new opportunities for genetic manipulation and therapeutic use.

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