Functional evolution of the Colony Stimulating Factor 1 Receptor (CSF1R) and its ligands in birds

CARLA GARCIA MORALES; Maria Weronika Gutowska; David Humes; Adebabay Kebede Belew; oladeji bamidele; Adriana Vallejo Trujillo; Jacqueline Smith

Please use this identifier to cite or link to this item: http://ri.uaemex.mx/handle20.500.11799/105860

Title:	Functional evolution of the Colony Stimulating Factor 1 Receptor (CSF1R) and its ligands in birds
Keywords:	Macrophage;CSF1;Evolution;info:eu-repo/classification/cti/2
Publisher:	Journal of Leukocyte Biology
Project:	107 2020 2 https://doi.org/10.1002/JLB.6MA0519-172R
Description:	Macrophage colony‐stimulating factor (CSF1 or M‐CSF) and interleukin 34 (IL34) are secreted cytokines that control macrophage survival and differentiation. Both act through the CSF1 receptor (CSF1R), a type III transmembrane receptor tyrosine kinase. The functions of CSF1R and both ligands are conserved in birds. We have analyzed protein‐coding sequence divergence among avian species. The intracellular tyrosine kinase domain of CSF1R was highly conserved in bird species as in mammals but the extracellular domain of avian CSF1R was more divergent in birds with multiple positively selected amino acids. Based upon crystal structures of the mammalian CSF1/IL34 receptor‐ligand interfaces and structure‐based alignments, we identified amino acids involved in avian receptor‐ligand interactions. The contact amino acids in both CSF1 and CSF1R diverged among avian species. Ligand‐binding domain swaps between chicken and zebra finch CSF1 confirmed the function of variants that confer species specificity on the interaction of CSF1 with CSF1R. Based upon genomic sequence analysis, we identified prevalent amino acid changes in the extracellular domain of CSF1R even within the chicken species that distinguished commercial broilers and layers and tropically adapted breeds. The rapid evolution in the extracellular domain of avian CSF1R suggests that at least in birds this ligand‐receptor interaction is subjected to pathogen selection. We discuss this finding in the context of expression of CSF1R in antigen‐sampling and antigen‐presenting cells. UK Government's Department for International Development. Grant Number: OPP1127286
URI:	http://ri.uaemex.mx/handle20.500.11799/105860
Other Identifiers:	http://hdl.handle.net/20.500.11799/105860
Rights:	info:eu-repo/semantics/openAccess http://creativecommons.org/licenses/by-nc-nd/4.0
Appears in Collections:	Producción

Show full item record

Google Scholar^TM

Check

DSpace CRIS

Es una versión "extendida" de DSpace, con un modelo de datos potente y flexible para describir no sólo las publicaciones, sino también todas las entidades del entorno de investigación y sus enlaces significativos.

Creado en 2009 en la Universidad de Hong Kong

Google Scholar^TM

DSpace CRIS

Es una versión "extendida" de DSpace, con un modelo de datos potente y flexible para describir no sólo las publicaciones, sino también todas las entidades del entorno de investigación y sus enlaces significativos.Creado en 2009 en la Universidad de Hong Kong

Google ScholarTM

Es una versión "extendida" de DSpace, con un modelo de datos potente y flexible para describir no sólo las publicaciones, sino también todas las entidades del entorno de investigación y sus enlaces significativos.

Creado en 2009 en la Universidad de Hong Kong

Google Scholar^TM