The adhesion molecule L1 regulates transendothelial migration and trafficking of dendritic cells

Author:

Maddaluno Luigi12,Verbrugge Sue Ellen12,Martinoli Chiara32,Matteoli Gianluca32,Chiavelli Andrea32,Zeng Yiping4,Williams Elizabeth D.4,Rescigno Maria32,Cavallaro Ugo12

Affiliation:

1. The FIRC Institute of Molecular Oncology (IFOM), 20139 Milan, Italy

2. IFOM-IEO Campus, 20139 Milan, Italy

3. Department of Experimental Oncology, European Institute of Oncology, 20141 Milan, Italy

4. Centre for Cancer Research, Monash Institute for Medical Research, Monash University, Victoria 3800, Australia

Abstract

The adhesion molecule L1, which is extensively characterized in the nervous system, is also expressed in dendritic cells (DCs), but its function there has remained elusive. To address this issue, we ablated L1 expression in DCs of conditional knockout mice. L1-deficient DCs were impaired in adhesion to and transmigration through monolayers of either lymphatic or blood vessel endothelial cells, implicating L1 in transendothelial migration of DCs. In agreement with these findings, L1 was expressed in cutaneous DCs that migrated to draining lymph nodes, and its ablation reduced DC trafficking in vivo. Within the skin, L1 was found in Langerhans cells but not in dermal DCs, and L1 deficiency impaired Langerhans cell migration. Under inflammatory conditions, L1 also became expressed in vascular endothelium and enhanced transmigration of DCs, likely through L1 homophilic interactions. Our results implicate L1 in the regulation of DC trafficking and shed light on novel mechanisms underlying transendothelial migration of DCs. These observations might offer novel therapeutic perspectives for the treatment of certain immunological disorders.

Publisher

Rockefeller University Press

Subject

Immunology,Immunology and Allergy

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