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Epigenetic regulation of plastin 3 expression by the macrosatellite DXZ4 and the transcriptional regulator CHD4.

Authors :
Strathmann, Eike A.
Hölker, Irmgard
Tschernoster, Nikolai
Hosseinibarkooie, Seyyedmohsen
Come, Julien
Martinat, Cecile
Altmüller, Janine
Wirth, Brunhilde
Source :
American Journal of Human Genetics. Mar2023, Vol. 110 Issue 3, p442-459. 18p.
Publication Year :
2023

Abstract

Dysregulated Plastin 3 (PLS3) levels associate with a wide range of skeletal and neuromuscular disorders and the most common types of solid and hematopoietic cancer. Most importantly, PLS3 overexpression protects against spinal muscular atrophy. Despite its crucial role in F-actin dynamics in healthy cells and its involvement in many diseases, the mechanisms that regulate PLS3 expression are unknown. Interestingly, PLS3 is an X-linked gene and all asymptomatic SMN1 -deleted individuals in SMA-discordant families who exhibit PLS3 upregulation are female, suggesting that PLS3 may escape X chromosome inactivation. To elucidate mechanisms contributing to PLS3 regulation, we performed a multi-omics analysis in two SMA-discordant families using lymphoblastoid cell lines and iPSC-derived spinal motor neurons originated from fibroblasts. We show that PLS3 tissue-specifically escapes X-inactivation. PLS3 is located ∼500 kb proximal to the DXZ4 macrosatellite, which is essential for X chromosome inactivation. By applying molecular combing in a total of 25 lymphoblastoid cell lines (asymptomatic individuals, individuals with SMA, control subjects) with variable PLS3 expression, we found a significant correlation between the copy number of DXZ4 monomers and PLS3 levels. Additionally, we identified chromodomain helicase DNA binding protein 4 (CHD4) as an epigenetic transcriptional regulator of PLS3 and validated co-regulation of the two genes by siRNA-mediated knock-down and overexpression of CHD4. We show that CHD4 binds the PLS3 promoter by performing chromatin immunoprecipitation and that CHD4/NuRD activates the transcription of PLS3 by dual-luciferase promoter assays. Thus, we provide evidence for a multilevel epigenetic regulation of PLS3 that may help to understand the protective or disease-associated PLS3 dysregulation. Dysregulated PLS3 levels associate with various genetic diseases, PLS3 upregulation protects against spinal muscular atrophy and is a biomarker of cancer. A high copy number of DXZ4 macrosatellite facilitates the escape of PLS3 from X-inactivation in women. Moreover, independent of sex, PLS3 expression is epigenetically regulated by the CHD4/NuRD complex. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
00029297
Volume :
110
Issue :
3
Database :
Academic Search Index
Journal :
American Journal of Human Genetics
Publication Type :
Academic Journal
Accession number :
162130645
Full Text :
https://doi.org/10.1016/j.ajhg.2023.02.004