Cxcl12 evolution – subfunctionalization of a ligand through altered interaction with the chemokine receptor

Author:

Boldajipour Bijan12,Doitsidou Maria2,Tarbashevich Katsiaryna1,Laguri Cedric3,Yu Shuizi Rachel4,Ries Jonas5,Dumstrei Karin2,Thelen Sylvia6,Dörries Julia2,Messerschmidt Esther-Maria1,Thelen Marcus6,Schwille Petra5,Brand Michael4,Lortat-Jacob Hugues3,Raz Erez12

Affiliation:

1. Institute of Cell Biology, Center of Molecular Biology of Inflammation, University of Münster, von-Esmarch-Str. 56, 48149 Münster, Germany

2. Max-Planck Institute of Biophysical Chemistry, Am Fassberg 11, 37070 Göttingen, Germany

3. IBS, Institut de Biologie Structurale, UMR 5075 CNRS CEA UJF, 41 Rue Horowitz, F-38027 Grenoble, France

4. Biotechnology Center, and Center for Regenerative Therapies, TU Dresden, Tatzberg 47-49, 01307 Dresden, Germany

5. Biophysics, Biotechnology Center, TU Dresden, Tatzberg 47-49, 01307 Dresden, Germany

6. Institute for Research in Biomedicine, via Vela 6, CH-6500 Bellinzona, Switzerland

Abstract

The active migration of primordial germ cells (PGCs) from their site of specification towards their target is a valuable model for investigating directed cell migration within the complex environment of the developing embryo. In several vertebrates, PGC migration is guided by Cxcl12, a member of the chemokine superfamily. Interestingly, two distinct Cxcl12 paralogs are expressed in zebrafish embryos and contribute to the chemotattractive landscape. Although this offers versatility in the use of chemokine signals, it also requires a mechanism through which migrating cells prioritize the relevant cues that they encounter. Here, we show that PGCs respond preferentially to one of the paralogs and define the molecular basis for this biased behavior. We find that a single amino acid exchange switches the relative affinity of the Cxcl12 ligands for one of the duplicated Cxcr4 receptors, thereby determining the functional specialization of each chemokine that elicits a distinct function in a distinct process. This scenario represents an example of protein subfunctionalization – the specialization of two gene copies to perform complementary functions following gene duplication – which in this case is based on receptor-ligand interaction. Such specialization increases the complexity and flexibility of chemokine signaling in controlling concurrent developmental processes.

Publisher

The Company of Biologists

Subject

Developmental Biology,Molecular Biology

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