Exploring the impact of dexamethasone on gene regulation in myeloma cells-Reference-Cited by-同舟云学术

Exploring the impact of dexamethasone on gene regulation in myeloma cells

Published:2023-07-31 Issue:9 Volume:6 Page:e202302195
ISSN:2575-1077
Container-title:Life Science Alliance
language:en
Short-container-title:Life Sci. Alliance

Author:

Bessonneau-Gaborit Victor¹²,Cruard Jonathan¹,Guerin-Charbonnel Catherine¹³^ORCID,Derrien Jennifer¹,Alberge Jean-Baptiste¹,Douillard Elise¹²,Devic Magali¹²^ORCID,Deshayes Sophie¹,Campion Loïc¹³,Westermann Frank⁴⁵^ORCID,Moreau Phillipe¹²,Herrmann Carl⁶,Bourdon Jérémie⁷^ORCID,Magrangeas Florence¹²^ORCID,Minvielle Stéphane¹²^ORCID

Affiliation:

1. Université de Nantes, CNRS, INSERM, Centre de Recherche en Cancérologie et Immunologie Intégrée Nantes Angers, France

2. Centre Hospitalier Universitaire, Nantes, France

3. Institut de Cancérologie de l’Ouest, Nantes, France

4. Hopp Children’s Cancer Center Heidelberg, KITZ, Heidelberg, Germany

5. Division of Neuroblastoma Genomics, German Cancer Research Center, Heidelberg, Germany

6. Health Data Science Unit, Medical Faculty Heidelberg and BioQuant, Heidelberg, Germany

7. Université de Nantes, LS2N, CNRS, Nantes, France

Abstract

Among glucocorticoids (GCs), dexamethasone (Dex) is widely used in treatment of multiple myelomas. However, despite a definite benefit, all patients relapse. Moreover, the molecular basis of glucocorticoid efficacy remains elusive. To determine genomic response to Dex in myeloma cells, we generated bulk and single-cell multi-omics data and high-resolution contact maps of active enhancers and target genes. We show that a minority of glucocorticoid receptor-binding sites are associated with enhancer activity gains, increased interaction loops, and transcriptional activity. We identified and characterized a predominant enhancer enriched in cohesin (RAD21) and more accessible upon Dex exposure. Analysis of four gene-specific networks revealed the importance of the CTCF–cohesin couple and the synchronization of regulatory sequence openings for efficient transcription in response to Dex. Notably, these epigenomic changes are associated with cell-to-cell transcriptional heterogeneity, in particular, lineage-specific genes. As consequences,BCL2L11-encoding BIM critical for Dex-induced apoptosis andCXCR4protective from chemotherapy-induced apoptosis are rather up-regulated in different cells. In summary, our work provides new insights into the molecular mechanisms involved in Dex escape.

Funder

Fondation Française Pour la Recherche Contre le Myélome et les Gammapathies Monoclonales

Programme d’investissement d’Avenir ISITE-NexT

SIRIC ILIAD

Publisher

Life Science Alliance, LLC

Subject

Health, Toxicology and Mutagenesis,Plant Science,Biochemistry, Genetics and Molecular Biology (miscellaneous),Ecology

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