| Literature DB >> 34354145 |
Alexander Mattebo1, Taha Sen1, Maria Jassinskaja2, Kristýna Pimková2, Isabel Prieto González-Albo1, Abdul Ghani Alattar1, Ramprasad Ramakrishnan3, Stefan Lang2, Marcus Järås3, Jenny Hansson2, Shamit Soneji2, Sofie Singbrant1, Emile van den Akker4, Johan Flygare5.
Abstract
The YPEL family genes are highly conserved across a diverse range of eukaryotic organisms and thus potentially involved in essential cellular processes. Ypel4, one of five YPEL family gene orthologs in mouse and human, is highly and specifically expressed in late terminal erythroid differentiation (TED). In this study, we investigated the role of Ypel4 in murine erythropoiesis, providing for the first time an in-depth description of a Ypel4-null phenotype in vivo. We demonstrated that the Ypel4-null mice displayed a secondary polycythemia with macro- and reticulocytosis. While lack of Ypel4 did not affect steady-state TED in the bone marrow or spleen, the anemia-recovering capacity of Ypel4-null cells was diminished. Furthermore, Ypel4-null red blood cells (RBC) were cleared from the circulation at an increased rate, demonstrating an intrinsic defect of RBCs. Scanning electron micrographs revealed an ovalocytic morphology of Ypel4-null RBCs and functional testing confirmed reduced deformability. Even though Band 3 protein levels were shown to be reduced in Ypel4-null RBC membranes, we could not find support for a physical interaction between YPEL4 and the Band 3 protein. In conclusion, our findings provide crucial insights into the role of Ypel4 in preserving normal red cell membrane integrity.Entities:
Year: 2021 PMID: 34354145 DOI: 10.1038/s41598-021-95291-1
Source DB: PubMed Journal: Sci Rep ISSN: 2045-2322 Impact factor: 4.379