ACKR3 Regulation of Neuronal Migration Requires ACKR3 Phosphorylation, but Not β-Arrestin

Publikation: Beitrag in FachzeitschriftForschungsartikelBeigetragenBegutachtung

Beitragende

  • Friederike Saaber - , Friedrich-Schiller-Universität Jena (Autor:in)
  • Dagmar Schütz - , Friedrich-Schiller-Universität Jena (Autor:in)
  • Elke Miess - , Friedrich-Schiller-Universität Jena (Autor:in)
  • Philipp Abe - , Friedrich-Schiller-Universität Jena (Autor:in)
  • Srinidhi Desikan - , Friedrich-Schiller-Universität Jena (Autor:in)
  • Praveen Ashok Kumar - , Friedrich-Schiller-Universität Jena (Autor:in)
  • Sara Balk - , Friedrich-Schiller-Universität Jena (Autor:in)
  • Ke Huang - , Friedrich-Schiller-Universität Jena (Autor:in)
  • Jean Martin Beaulieu - , University of Toronto (Autor:in)
  • Stefan Schulz - , Friedrich-Schiller-Universität Jena (Autor:in)
  • Ralf Stumm - , Friedrich-Schiller-Universität Jena (Autor:in)

Abstract

Phosphorylation of heptahelical receptors is thought to regulate G protein signaling, receptor endocytosis, and non-canonical signaling via recruitment of β-arrestins. We investigated chemokine receptor functionality under phosphorylation-deficient and β-arrestin-deficient conditions by studying interneuron migration in the embryonic cortex. This process depends on CXCL12, CXCR4, G protein signaling and on the atypical CXCL12 receptor ACKR3. We found that phosphorylation was crucial, whereas β-arrestins were dispensable for ACKR3-mediated control of CXCL12 levels in vivo. Cortices of mice expressing phosphorylation-deficient ACKR3 exhibited a major interneuron migration defect, which was accompanied by excessive activation and loss of CXCR4. Cxcl12-overexpressing mice mimicked this phenotype. Excess CXCL12 caused lysosomal CXCR4 degradation, loss of CXCR4 responsiveness, and, ultimately, similar motility defects as Cxcl12 deficiency. By contrast, β-arrestin deficiency caused only a subtle migration defect mimicked by CXCR4 gain of function. These findings demonstrate that phosphorylation regulates atypical chemokine receptor function without β-arrestin involvement in chemokine sequestration and non-canonical signaling.

Details

OriginalspracheEnglisch
Seiten (von - bis)1473-1488.e9
FachzeitschriftCell reports
Jahrgang26
Ausgabenummer6
PublikationsstatusVeröffentlicht - 5 Feb. 2019
Peer-Review-StatusJa
Extern publiziertJa

Externe IDs

PubMed 30726732
ORCID /0000-0002-8067-1802/work/173989176

Schlagworte

ASJC Scopus Sachgebiete

Schlagwörter

  • ACKR, ACKR3, atypical chemokine receptor, CXCL12, CXCR4, CXCR7, G protein-coupled receptor kinase, GRK, internalization, interneuron, migration, phosphorylation, β-arrestin