Integrated DNA methylation analysis reveals a potential role for PTPRN2 in Marfan syndrome scoliosis-Reference-Cited by-同舟云学术

Integrated DNA methylation analysis reveals a potential role for PTPRN2 in Marfan syndrome scoliosis

Published:2023-05-17 Issue: Volume: Page:
ISSN:
Container-title:
language:
Short-container-title:

Author:

Zheng Zhen-zhong¹,Xu Jing-hong¹,Chen Jia-lin¹,Jiang Bin¹,Ma Hong¹,Li Lei¹,Li Ya-wei¹,Dai Yu-liang¹,Wang Bing¹

Affiliation:

1. Central South University

Abstract

Abstract Background Marfan syndrome (MFS) is a rare genetic disorder caused by mutations in the Fibrillin-1 gene (FBN1) with significant clinical features in the skeletal, cardiopulmonary, and ocular systems. To gain deeper insights into the contribution of epigenetics in the variability of phenotypes observed in MFS, we undertook the first analysis of integrating DNA methylation and gene expression profiles in whole blood from MFS and healthy controls (HCs). Methods The Illumina 850K (EPIC) DNA methylation array was used to detect DNA methylation changes on peripheral blood samples of seven patients with MFS and five HCs. Associations between methylation levels and clinical features of MFS were analyzed. Subsequently, we conducted an integrated analysis of the outcomes of the transcriptome data to analyze the correlation between differentially methylated positions (DMPs) and differentially expressed genes (DEGs) and explore the potential role of methylation regulated DEGs (MeDEGs) in MFS scoliosis. The weighted gene co‑expression network analysis (WGCNA) was used to find gene modules with the highest correlation coefficient with target MeDEGs to annotate their functions in MFS. Results Our study identified 1253 DMPs annotated to 236 genes that were primarily associated with scoliosis, cardiomyopathy, and vital capacity. These conditions are typically associated with reduced lifespan in untreated MFS. We calculated correlations between DMPs and clinical features, such as cobb angle to evaluate scoliosis and FEV1% to assess pulmonary function. Notably, cg20223687 (PTPRN2) and cg00259849 (CSMD1) exhibited an inverse correlation with cobb angle of scoliosis, potentially playing a role in ERKs inactivation and chondrocyte proliferation, respectively. Conclusions Taken together, our systems-level approach sheds light on the contribution of epigenetics to MFS and offers a plausible explanation for the complex phenotypes that are linked to reduced lifespan in untreated MFS patients.

Publisher

Research Square Platform LLC

Reference65 articles.

1. 1. Wright IH, Gaylard DG. Marfan's syndrome. Anaesthesia. 1985;40:206.

2. 2. Dietz HC, Cutting GR, Pyeritz RE, Maslen CL, Sakai LY, Corson GM, et al. Marfan syndrome caused by a recurrent de novo missense mutation in the fibrillin gene. Nature. 1991;352:337-9.

3. 3. Milewicz DM, Braverman AC, De Backer J, Morris SA, Boileau C, Maumenee IH, et al. Marfan syndrome. Nature reviews Disease primers. 2021;7:64.

4. 4. Ruiz G, Torres-Lugo NJ, Marrero-Ortiz P, Guzmán H, Olivella G, Ramírez N. Early-onset scoliosis: a narrative review. EFORT Open Rev. 2022;7:599–610.

5. 5. Lin Y, Shen J, Chen L, Yuan W, Cong H, Luo J, et al. Cardiopulmonary Function in Patients with Congenital Scoliosis: An Observational Study. The Journal of bone and joint surgery American volume. 2019;101:1109-18.