Litcius/Paper detail

Intralumenal docking of connexin 36 channels in the ER isolates mistrafficked protein

Stephan Tetenborg, Viktoria Liss, Leonhard Breitsprecher, Ksenia Timonina, Anna Kotova, Alejandra Jesús Acevedo Harnecker, Chunxu Yuan, Eyad Shihabeddin, Fatemeh Ariakia, Guoting Qin, Cai Chengzhi, Karin Dedek, Georg Zoidl, Michael Hensel, John O’Brien

2023Journal of Biological Chemistry14 citationsDOIOpen Access PDF

Abstract

The intracellular domains of connexins are essential for the assembly of gap junctions. For connexin 36 (Cx36), the major neuronal connexin, it has been shown that a dysfunctional PDZ-binding motif interferes with electrical synapse formation. However, it is still unknown how this motif coordinates the transport of Cx36. In the present study, we characterize a phenotype of Cx36 mutants that lack a functional PDZ-binding motif using HEK293T cells as an expression system. We provide evidence that an intact PDZ-binding motif is critical for proper endoplasmic reticulum (ER) export of Cx36. Removing the PDZ-binding motif of Cx36 results in ER retention and the formation of multimembrane vesicles containing gap junction-like connexin aggregates. Using a combination of site-directed mutagenesis and electron micrographs, we reveal that these vesicles consist of Cx36 channels that docked prematurely in the ER. Our data suggest a model in which ER-retained Cx36 channels reshape the ER membrane into concentric whorls that are released into the cytoplasm.

Topics & Concepts

PDZ domainConnexinGap junctionCell biologyVesicleCytoplasmMutantBinding siteBiologyDocking (animal)ChemistryBiophysicsIntracellularBiochemistryMembraneGeneNursingMedicineConnexins and lens biologyHeat shock proteins researchYersinia bacterium, plague, ectoparasites research