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A chemical screening approach to identify novel key mediators of erythroid enucleation

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posted on 2024-07-26, 14:08 authored by Christina B. Wölwer, Luke B. Pase, Helen B. Pearson, Nathan J. Gödde, Kurt Lackovic, David C. S. Huang, Sarah RussellSarah Russell, Patrick O. Humbert
Erythroid enucleation is critical for terminal differentiation of red blood cells, and involves extrusion of the nucleus by orthochromatic erythroblasts to produce reticulocytes. Due to the difficulty of synchronizing erythroblasts, the molecular mechanisms underlying the enucleation process remain poorly understood. To elucidate the cellular program governing enucleation, we utilized a novel chemical screening approach whereby orthochromatic cells primed for enucleation were enriched ex vivo and subjected to a functional drug screen using a 324 compound library consisting of structurally diverse, medicinally active and cell permeable drugs. Using this approach, we have confirmed the role of HDACs, proteasomal regulators and MAPK in erythroid enucleation and introduce a new role for Cyclin-dependent kinases, in particular CDK9, in this process. Importantly, we demonstrate that when coupled with imaging analysis, this approach provides a powerful means to identify and characterize rate limiting steps involved in the erythroid enucleation process.

Funding

Targeting mechanisms that promote cancer cell survival: genetic and chemical approaches to unravel the molecular mechanisms that drive tumour formation, develop novel molecular and chemical probes, and discover new therapeutics

National Health and Medical Research Council

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ISSN

1932-6203

Journal title

PLoS ONE

Volume

10

Issue

11

Article number

article no. e0142655

Pagination

11 pp

Publisher

Public Library of Science

Copyright statement

Copyright © 2015 Woelwer et al. This an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.

Language

eng

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