Journal of Personalized Medicine (Nov 2021)

Epigenotype, Genotype, and Phenotype Analysis of Taiwanese Patients with Silver–Russell Syndrome

  • Hsiang-Yu Lin,
  • Chung-Lin Lee,
  • Sisca Fran,
  • Ru-Yi Tu,
  • Ya-Hui Chang,
  • Dau-Ming Niu,
  • Chia-Ying Chang,
  • Pao-Chin Chiu,
  • Yen-Yin Chou,
  • Hui-Pin Hsiao,
  • Meng-Che Tsai,
  • Mei-Chyn Chao,
  • Li-Ping Tsai,
  • Chia-Feng Yang,
  • Pen-Hua Su,
  • Yu-Wen Pan,
  • Chen-Hao Lee,
  • Tzu-Hung Chu,
  • Chih-Kuang Chuang,
  • Shuan-Pei Lin

DOI
https://doi.org/10.3390/jpm11111197
Journal volume & issue
Vol. 11, no. 11
p. 1197

Abstract

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Background: Silver–Russell syndrome (SRS) is a clinically and genetically heterogeneous disorder characterized by severe intrauterine growth retardation, poor postnatal growth, characteristic facial features, and body asymmetry. Hypomethylation of the imprinted genes of the chromosome 11p15.5 imprinting gene cluster and maternal uniparental disomy of chromosome 7 (mUPD7) are the major epigenetic disturbances. The aim of this study was to characterize the epigenotype, genotype, and phenotype of these patients in Taiwan. Methods: Two hundred and six subjects with clinically suspected SRS were referred for diagnostic testing, which was performed by profiling the methylation of H19-associated imprinting center (IC) 1 and the imprinted PEG1/MEST region using methylation-specific multiplex ligation-dependent probe amplification and high-resolution melting analysis with a methylation-specific polymerase chain reaction assay. We also applied a whole genome strategy to detect copy number changes and loss of heterozygosity. Clinical manifestations were recorded and analyzed according to the SRS scoring system proposed by Bartholdi et al. Results: Among the 206 referred subjects, 100 were classified as having a clinical diagnosis of SRS (score ≥ 8, maximum = 15) and 106 had an SRS score ≤ 7. Molecular lesions were detected in 45% (45/100) of the subjects with a clinical diagnosis of SRS, compared to 5% (5/106) of those with an SRS score ≤ 7. Thirty-seven subjects had IC1 hypomethylation, ten subjects had mUPD7, and three subjects had microdeletions. Several clinical features were found to be statistically different (p p < 0.001). The SRS subjects with mUPD7 seemed to have fewer typical features and lower SRS scores than those with IC1 hypomethylation. Careful clinical observation and timely molecular confirmation are important to allow for an early diagnosis and multidisciplinary management of these patients.

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