Accueil Kevin Rouault-Pierre’s team – Stress Integration in Normal and Malignant Hematopoietic Stem Cells

Kevin Rouault-Pierre’s team – Stress Integration in Normal and Malignant Hematopoietic Stem Cells

Kevin Rouault-Pierre

Team leader

Institut de recherche Saint-Louis

Pubmed : https://www.ncbi.nlm.nih.gov/myncbi/14M2DQoPpOx57/bibliography/public/

ORCID : https://orcid.org/0000-0001-7671-7364

Google Scholar : https://scholar.google.com/citations?user=HU9UcHYAAAAJ&hl=en&oi=ao

Linkedin : https://www.linkedin.com/in/kevin-rouault-pierre-2382489a/

X / BlueSky : @kevinrouault.bsky.social

Research themes

The laboratory’s research program aims to identify and exploit vulnerabilities induced by splicing dysregulation in order to develop precision therapeutic strategies for patients with MDS.

Research areas

Programme 1 – Aberrant splicing: from molecular mechanisms to precision therapy

In this program, we aim to identify and characterise aberrant splicing events that act as functional drivers of myelodysplastic syndromes (MDS), particularly in hematopoietic stem and progenitor cells.

Building on splicing profiles generated from primary cells of patients harboring SF3B1 or SRSF2 mutations, we have identified several hundred specifically aberrant isoforms that are absent in normal hematopoietic cells.

Based on these human-derived signatures, we are developing a targeted screen of mis-spliced genes in MDS to identify novel key regulators of hematopoietic stem cell self-renewal, differentiation, and proliferation.

The most relevant candidates are then functionally validated in human cellular models, patient-derived xenografts, and conditional murine models.

This integrated approach enables us to link specific splicing alterations to actionable biological vulnerabilities and to pave the way for precision therapeutic strategies based on mechanisms directly derived from patient cells.

For instance, building on our findings on COASY, we are currently running a clinical trial (B5ForMDS), in which patients with SF3B1-mutant MDS will receive high doses of vitamin B5 to restore ineffective erythropoiesis. Link1 ; Link2.

Programme 2 – Proteostasis and stress adaptation in normal and malignant stem cells

Aberrant splicing in MDS leads to the continuous production of abnormal transcripts and proteins, generating chronic proteotoxic stress. However, the mechanisms by which hematopoietic stem cells harboring splicing mutations tolerate and adapt to this stress remain poorly understood.

This program investigates how proteostasis networks are remodeled in normal and mutant hematopoietic stem cells. Building on previous work, from our lab and others, demonstrating the sensitivity of hematopoietic stem and progenitor cells to endoplasmic reticulum stress, it integrates RNA splicing analyses with functional approaches in primary human cells.

This approach enables the identification of stress adaptation pathways that are specifically required by mutant clones while remaining dispensable for normal stem cells. It thereby defines therapeutically exploitable proteostasis vulnerabilities and provides a mechanistic framework to understand inter-patient heterogeneity in disease progression and treatment responses.

Programme 3 – Nonsense mRNA decay, proteotoxic overload, and synthetic lethality in MDS

This program explores how the high burden of transcripts sensitive to nonsense-mediated decay (NMD) in MDS with splicing factor mutations can be exploited to induce synthetic lethality. It builds on the observation that modulating the translation of these aberrant transcripts exacerbates proteotoxic stress and disrupts protein quality control systems in mutant cells.

By combining functional approaches with integrated genomic analyses in both mutant and non-mutant myeloid models, this program aims to identify specific molecular dependencies that emerge under conditions of heightened protein stress.

These studies will define selective vulnerabilities of clones harboring splicing alterations while sparing normal cells. Ultimately, this work provides a rational framework for the development of combination therapeutic strategies that preferentially target mutant cells and supports the emergence of new preclinical approaches in MDS and other diseases associated with splicing factor mutations.

Kevin Rouault-Pierre's team members

Jimena Castorena	Postdoc (Paris team)
Marjorie Delahaye	Postdoc (Paris team)
Andrea Martisova	Postdoc (Paris team)
Arantxa Leon Carrasco	Postdoc (London team)
Daniel Mouzo Calzadilla	Postdoc (London team)
Shoshana Burke	Clinical Research Fellow (London team)

Alumni

Celine Philippe	Postdoc
Fadimana Kaya	PhD student
Faika Laz Banti	PhD student
Doriana Di Bella	PhD
Wei Wei Tang	PhD
Evens Bousiquot	Technician
Pantelitsa Protopapa	Technician
Sophie Louise Katsiavriades	Technician
Beatriz Galvao	Technician
Pramiksha Bagale	Technician