An arginase 2 promoter transgenic line illuminates immune cell polarisation in zebrafish

Author:

Hammond Ffion R.12,Lewis Amy12,Speirs Zoë C.12,Anderson Holly E.12,Sipka Tamara3,Williams Lewis G.12,Nguyen-Chi Mai3,Meijer Annemarie H.4ORCID,Wiegertjes Geert F.56,Elks Philip M.12ORCID

Affiliation:

1. The Bateson Centre 1 , Department of Infection and Immunity and Cardiovascular Disease , , Sheffield S10 2TN , UK

2. University of Sheffield, Western Bank 1 , Department of Infection and Immunity and Cardiovascular Disease , , Sheffield S10 2TN , UK

3. LPHI, University of Montpellier, CNRS 2 , 34090 Montpellier , France

4. Institute of Biology Leiden, Leiden University 3 , Einsteinweg 55, 2333 CC Leiden , The Netherlands

5. Aquaculture and Fisheries Group 4 , Department of Animal Sciences , , 6700 AH Wageningen , The Netherlands

6. Wageningen University & Research 4 , Department of Animal Sciences , , 6700 AH Wageningen , The Netherlands

Abstract

ABSTRACT Innate immune responses to inflammation and infection are complex and represent major challenges for developing much needed new treatments for chronic inflammatory diseases and drug-resistant infections. To be ultimately successful, the immune response must be balanced to allow pathogen clearance without excess tissue damage, processes controlled by pro- and anti-inflammatory signals. The roles of anti-inflammatory signalling in raising an appropriate immune response are underappreciated, representing overlooked potential drug targets. This is especially true in neutrophils, a difficult cell type to study ex vivo owing to a short lifespan, dogmatically seen as being highly pro-inflammatory. Here, we have generated and describe the first zebrafish transgenic line [TgBAC(arg2:eGFP)sh571] that labels expression of the anti-inflammatory gene arginase 2 (arg2) and show that a subpopulation of neutrophils upregulate arginase soon after immune challenge with injury and infection. At wound-healing stages, arg2:GFP is expressed in subsets of neutrophils and macrophages, potentially representing anti-inflammatory, polarised immune cell populations. Our findings identify nuanced responses to immune challenge in vivo, responses that represent new opportunities for therapeutic interventions during inflammation and infection.

Funder

Wellcome Trust

Royal Society

University of Sheffield

National Centre for the Replacement, Refinement and Reduction of Animals in Research

Wolfson Foundation

Publisher

The Company of Biologists

Subject

General Biochemistry, Genetics and Molecular Biology,Immunology and Microbiology (miscellaneous),Medicine (miscellaneous),Neuroscience (miscellaneous)

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