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Post-translational polymodification of β1-tubulin regulates motor protein localization in platelet production and function

Abdullah O. Khan, Alexandre Slater, Annabel Maclachlan, Phillip L.R. Nicolson, Jeremy A. Pike, Jasmeet S. Reyat, Jack Yule, Rachel J. Stapley, Julie Rayes, Steven G. Thomas, Neil V. Morgan

2020Haematologica26 citationsDOIOpen Access PDF

Abstract

In specialised cells, the expression of specific tubulin isoforms and their subsequent post-translational modifications drive and coordinate unique morphologies and behaviours. The mechanisms by which β1-tubulin, the platelet and megakaryocyte (MK) lineage restricted tubulin isoform, drives platelet production and function remains poorly understood. We investigated the roles of two key post-translational tubulin polymodifications (polyglutamylation and polyglycylation) on these processes using a cohort of thrombocytopenic patients, human induced pluripotent stem cell (iPSC) derived MKs, and healthy human donor platelets. We find distinct patterns of polymodification in MKs and platelets, mediated by the antagonistic activities of the cell specific expression of Tubulin Tyrosine Ligase Like (TTLLs) and Cytosolic Carboxypeptidase (CCP) enzymes. The resulting microtubule patterning spatially regulates motor proteins to drive proplatelet formation in megakaryocytes, and the cytoskeletal reorganisation required for thrombus formation. This work is the first to show a reversible system of polymodification by which different cell specific functions are achieved.

Topics & Concepts

TubulinCell biologyMicrotubuleMegakaryocyteGene isoformBiologyPlateletCytoskeletonThrombopoiesisCellHaematopoiesisBiochemistryStem cellGeneImmunologyPlatelet Disorders and TreatmentsCarbohydrate Chemistry and SynthesisComplement system in diseases
Post-translational polymodification of β1-tubulin regulates motor protein localization in platelet production and function | Litcius