snRNA-seq analysis in multinucleated myogenic FSHD cells identifies heterogeneous FSHD transcriptome signatures associated with embryonic-like program activation and oxidative stress-induced apoptosis

Author:

Zheng Dongxu1,Wondergem Annelot1,Kloet Susan1,Willemsen Iris1,Balog Judit1,Tapscott Stephen J2,Mahfouz Ahmed13,van den Heuvel Anita1,van der Maarel Silvère M1

Affiliation:

1. Department of Human Genetics, Leiden University Medical Center , Einthovenweg 20, 2333 ZC, Leiden , The Netherlands

2. Division of Human Biology, Fred Hutchinson Cancer Research Center , 1100 Fairview Ave N, Seattle, WA 98109 , USA

3. Delft Bioinformatics Lab, Delft University of Technology , Van Mourik Broekmanweg 2628 XE, Delft , The Netherlands

Abstract

Abstract The sporadic nature of DUX4 expression in FSHD muscle challenges comparative transcriptome analyses between FSHD and control samples. A variety of DUX4 and FSHD-associated transcriptional changes have been identified, but bulk RNA-seq strategies prohibit comprehensive analysis of their spatiotemporal relation, interdependence and role in the disease process. In this study, we used single-nucleus RNA-sequencing of nuclei isolated from patient- and control-derived multinucleated primary myotubes to investigate the cellular heterogeneity in FSHD. Taking advantage of the increased resolution in snRNA-sequencing of fully differentiated myotubes, two distinct populations of DUX4-affected nuclei could be defined by their transcriptional profiles. Our data provides insights into the differences between these two populations and suggests heterogeneity in two well-known FSHD-associated transcriptional aberrations: increased oxidative stress and inhibition of myogenic differentiation. Additionally, we provide evidence that DUX4-affected nuclei share transcriptome features with early embryonic cells beyond the well-described cleavage stage, progressing into the 8-cell and blastocyst stages. Altogether, our data suggests that the FSHD transcriptional profile is defined by a mixture of individual and sometimes mutually exclusive DUX4-induced responses and cellular state-dependent downstream effects.

Funder

Prinses Beatrix Spierfonds

Publisher

Oxford University Press (OUP)

Subject

Genetics (clinical),Genetics,Molecular Biology,General Medicine

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