| Literature DB >> 32795391 |
Jaroslaw Cendrowski1, Marta Kaczmarek1, Michał Mazur1, Katarzyna Kuzmicz-Kowalska1, Kamil Jastrzebski1, Marta Brewinska-Olchowik2, Agata Kominek2, Katarzyna Piwocka2, Marta Miaczynska1.
Abstract
Intracellular transport undergoes remodeling upon cell differentiation, which involves cell type-specific regulators. Bone morphogenetic protein 2-inducible kinase (BMP2K) has been potentially implicated in endocytosis and cell differentiation but its molecular functions remained unknown. We discovered that its longer (L) and shorter (S) splicing variants regulate erythroid differentiation in a manner unexplainable by their involvement in AP-2 adaptor phosphorylation and endocytosis. However, both variants interact with SEC16A and could localize to the juxtanuclear secretory compartment. Variant-specific depletion approach showed that BMP2K isoforms constitute a BMP2K-L/S regulatory system that controls the distribution of SEC16A and SEC24B as well as SEC31A abundance at COPII assemblies. Finally, we found L to promote and S to restrict autophagic degradation and erythroid differentiation. Hence, we propose that BMP2K-L and BMP2K-S differentially regulate abundance and distribution of COPII assemblies as well as autophagy, possibly thereby fine-tuning erythroid differentiation.Entities:
Keywords: autophagy; cell biology; copii trafficking; endocytosis; erythroid differentiation; human; mouse; splicing variants
Year: 2020 PMID: 32795391 PMCID: PMC7473771 DOI: 10.7554/eLife.58504
Source DB: PubMed Journal: Elife ISSN: 2050-084X Impact factor: 8.140