| Literature DB >> 31578203 |
Sascha Geue1, Katja Aurbach2,3, Mailin-Christin Manke1, Georgi Manukjan3, Patrick Münzer1, David Stegner2,3, Caroline Brähler3, Britta Walker-Allgaier1, Melanie Märklin4, Carla E Borst5, Leticia Quintanilla-Fend6, Dominik Rath1, Tobias Geisler1, Helmut R Salih4, Peter Seizer1, Florian Lang1,7, Bernhard Nieswandt2,3, Meinrad Gawaz1, Harald Schulze3, Irina Pleines2,3, Oliver Borst1.
Abstract
During thrombopoiesis, megakaryocytes (MKs) form proplatelets within the bone marrow (BM) and release platelets into BM sinusoids. Phosphoinositide-dependent protein kinase-1 (PDK1) is required for Ca2+-dependent platelet activation, but its role in MK development and regulation of platelet production remained elusive. The present study explored the role of PDK1 in the regulation of MK maturation and polarization during thrombopoiesis using a MK/platelet-specific knockout approach. Pdk1-deficient mice (Pdk1-/-) developed a significant macrothrombocytopenia as compared with wild-type mice (Pdk1fl/fl). Pdk1 deficiency further dramatically increased the number of MKs without sinusoidal contact within the BM hematopoietic compartment, resulting in a pronounced MK hyperplasia and a significantly increased extramedullary thrombopoiesis. Cultured Pdk1-/- BM-MKs showed impaired spreading on collagen, associated with an altered actin cytoskeleton structure with less filamentous actin (F-actin) and diminished podosome formation, whereas the tubulin cytoskeleton remained unaffected. This phenotype was associated with abrogated phosphorylation of p21-activated kinase (PAK) as well as its substrates LIM domain kinase and cofilin, supporting the hypothesis that the defective F-actin assembly results from increased cofilin activity in Pdk1-deficient MKs. Pdk1-/- BM-MKs developed increased ploidy and exhibited an abnormal ultrastructure with disrupted demarcation membrane system (DMS). Strikingly, Pdk1-/- BM-MKs displayed a pronounced defect in DMS polarization and produced significantly less proplatelets, indicating that PDK1 is critically required for proplatelet formation. In human MKs, genetic PDK1 knockdown resulted in increased maturity but reduced platelet-like particles formation. The present observations reveal a pivotal role of PDK1 in the regulation of MK cytoskeletal dynamics and polarization, proplatelet formation, and thrombopoiesis.Entities:
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Year: 2019 PMID: 31578203 DOI: 10.1182/blood.2019000185
Source DB: PubMed Journal: Blood ISSN: 0006-4971 Impact factor: 22.113