The expression of mouse CLEC-2 on leucocyte subsets varies according to their anatomical location and inflammatory state.

Kate L Lowe,Cécile Bénézech,Bernhard Nieswandt,Guillaume E Desanti,Saba Nayar,Leyre Navarro‐Núñez,Steve P Watson,Francesca Barone,Bethany L Kingston,Christopher D Buckley

doi:10.1002/eji.201445314

Abstract

Expression of mouse C‐type lectin‐like receptor 2 (CLEC‐2) has been reported on circulating CD11bhigh Gr‐1high myeloid cells and dendritic cells (DCs) under basal conditions, as well as on a variety of leucocyte subsets following inflammatory stimuli or in vitro cell culture. However, previous studies assessing CLEC‐2 expression failed to use CLEC‐2‐deficient mice as negative controls and instead relied heavily on single antibody clones. Here, we generated CLEC‐2‐deficient adult mice using two independent approaches and employed two anti‐mouse CLEC‐2 antibody clones to investigate surface expression on hematopoietic cells from peripheral blood and secondary lymphoid organs. We rule out constitutive CLEC‐2 expression on resting DCs and show that CLEC‐2 is upregulated in response to LPS‐induced systemic inflammation in a small subset of activated DCs isolated from the mesenteric lymph nodes but not the spleen. Moreover, we demonstrate for the first time that peripheral blood B lymphocytes present exogenously derived CLEC‐2 and suggest that both circulating B lymphocytes and CD11bhigh Gr‐1high myeloid cells lose CLEC‐2 following entry into secondary lymphoid organs. These results have significant implications for our understanding of CLEC‐2 physiological functions

Highlights

Many physiological functions are critically regulated by finetuned interactions between diverse subsets of hematopoietic andC 2015 The Authors
We investigated C-type lectin-like receptor 2 (CLEC-2) expression on hematopoietic cells isolated from lethally irradiated wild-type (WT) adult mice reconstituted with foetal liver (FL) cells from E14.5 Clec1b+/+ or Clec1b−/− embryos [25]
Our study confirms that CLEC-2 is constitutively expressed by mouse platelets and circulating CD11bhigh Gr-1high myeloid cells and shows for the first time that CLEC-2 is present on the surface of peripheral blood B lymphocytes

Summary

Introduction

Many physiological functions are critically regulated by finetuned interactions between diverse subsets of hematopoietic andC 2015 The Authors. Many physiological functions are critically regulated by finetuned interactions between diverse subsets of hematopoietic and. European Journal of Immunology published by WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim. Www.eji-journal.eu expression by developing thymocytes regulates medullary thymic epithelial cell maturation (for review; [1]). A similar scenario can be considered for the C-type lectin-like receptor 2 (CLEC-2) and its ligand podoplanin (PDPN), which are involved in a variety of physiological and pathophysiological processes (for review: [2]). PDPN expression is upregulated at the leading edge of tumors and in additional hematopoietic and nonhematopoietic cell types during inflammation (for review: [2]). CLEC-2/PDPN interactions play essential roles in the immune system, as they prevent blood–lymph mixing [9,10,11], are required for lymph node (LN) development [12] and maintenance of LN vascular integrity [12, 13] and contribute to the generation of optimal adaptive immune responses [12, 14, 15]

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Results

Conclusion