# Profiling Translational Control of Gene Expression and Nascent Proteomic Responses in Erythropoietic Progression and Ribosomopathies

> **NIH NIH K08** · UNIVERSITY OF COLORADO DENVER · 2022 · $84,230

## Abstract

SCIENTIFIC ABSTRACT
Erythropoiesis is guided by a complex interplay of signaling cues triggering expression of gene networks
necessary for production of mature red blood cells. Rapid response to these signals in erythroid precursors
temporally orchestrate functions required for erythroid differentiation. Timely and appropriate selection of mRNAs
for translation by the ribosome is essential for maintaining the balance between maintaining erythroid precursors
differentiation. This concept, known as translational control governs efficiency of mRNA translation and thus
plays a crucial role in regulating responses to extracellular cues such as anemia and hypoxia. Failure of the
ribosomal machinery to regulate this process underlies the ribosomopathies, a set of human diseases resulting
from ribosomal mutations leading to profound consequences for hematopoietic maturation. This proposal
focuses on outstanding, fundamental questions in how translational control 1.) directs mRNA selection in normal
erythropoiesis and 2.) is impaired in ribosomopathies in response to signaling cues. Aim 1 will explore how
eIF4E, a key factor in translation initiation is repressed in a dynamic, cell-intrinsic manner to direct translation of
a specific set of transcripts. Failure to repress eIF4E activity in maturing erythroblasts leads to inappropriate
expression of genes necessary for maintenance of early erythroid precursors and impaired differentiation. This
aim will mechanistically decipher motifs in target mRNA and decipher how eIF4E specifically recognizes these
transcripts for ribosomal recruitment. Dependence of tight regulation of eIF4E on erythropoiesis will be tested
in vivo employing a novel mouse model utilizing doxycycline-responsive expression of eIF4E localized to specific
phases of hematopoietic maturation. A paradigm example of ribosomopathies, Diamond Blackfan Anemia (DBA)
results in erythroid aplasia and failure to respond to erythropoietin (Epo), a key signal in differentiation of early
erythroid precursors. However, why hematopoietic precursors in DBA fail to generate the appropriate nascent
gene expression response to these cues is still poorly understood. Aim 2 will use employ a universally-applicable,
mass spectrometry-based method (OPP-ID) pioneered by Dr. Forester to characterize the nascent proteomic
landscape in healthy and DBA-derived iPSCs in response to erythropoietin. Identification of impaired proteomic
responses in DBA iPSCs will give insight into how specific ribosomal mutations prevent translation of key genes
crucial in early differentiation. This technology will be applied to understand how dexamethasone, a known
mediator of hematopoietic rescue of unclear mechanism, remodels the erythroid proteome in response to Epo.
Successful completion will result in both a unique contribution into the fields of translational control and
erythropoiesis as well as a novel approach to understanding how the nascent translatome is impaired in
ribosomo...

## Key facts

- **NIH application ID:** 10668587
- **Project number:** 3K08DK119561-05S1
- **Recipient organization:** UNIVERSITY OF COLORADO DENVER
- **Principal Investigator:** CRAIG M. FORESTER
- **Activity code:** K08 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2022
- **Award amount:** $84,230
- **Award type:** 3
- **Project period:** 2020-03-01 → 2023-08-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/10668587

## Citation

> US National Institutes of Health, RePORTER application 10668587, Profiling Translational Control of Gene Expression and Nascent Proteomic Responses in Erythropoietic Progression and Ribosomopathies (3K08DK119561-05S1). Retrieved via AI Analytics 2026-05-22 from https://api.ai-analytics.org/grant/nih/10668587. Licensed CC0.

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