Colec12 and Trail signaling confine cranial neural crest cell trajectories and promote collective cell migration

Author:

McLennan Rebecca12,Giniunaite Rasa345,Hildebrand Katie6,Teddy Jessica M.1,Kasemeier‐Kulesa Jennifer C.1,Bolanos Lizbeth1,Baker Ruth E.3,Maini Philip K.3,Kulesa Paul M.16ORCID

Affiliation:

1. Stowers Institute for Medical Research Kansas City Missouri USA

2. Childrens Mercy Kansas City Kansas City Missouri USA

3. Wolfson Centre for Mathematical Biology University of Oxford Oxford UK

4. Faculty of Mathematics and Informatics Vilnius University Vilnius Lithuania

5. Faculty of Mathematics and Natural sciences Kaunas University of Technology Kaunas Lithuania

6. University of Kansas School of Medicine Kansas City Kansas USA

Abstract

AbstractBackgroundCollective and discrete neural crest cell (NCC) migratory streams are crucial to vertebrate head patterning. However, the factors that confine NCC trajectories and promote collective cell migration remain unclear.ResultsComputational simulations predicted that confinement is required only along the initial one‐third of the cranial NCC migratory pathway. This guided our study of Colec12 (Collectin‐12, a transmembrane scavenger receptor C‐type lectin) and Trail (tumor necrosis factor‐related apoptosis‐inducing ligand, CD253) which we show expressed in chick cranial NCC‐free zones. NCC trajectories are confined by Colec12 or Trail protein stripes in vitro and show significant and distinct changes in cell morphology and dynamic migratory characteristics when cocultured with either protein. Gain‐ or loss‐of‐function of either factor or in combination enhanced NCC confinement or diverted cell trajectories as observed in vivo with three‐dimensional confocal microscopy, respectively, resulting in disrupted collective migration.ConclusionsThese data provide evidence for Colec12 and Trail as novel NCC microenvironmental factors playing a role to confine cranial NCC trajectories and promote collective cell migration.

Funder

Eunice Kennedy Shriver National Institute of Child Health and Human Development

Publisher

Wiley

Subject

Developmental Biology

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