Scientific Reports (Dec 2024)

Comprehensive copy number analysis of spinal muscular atrophy among the Iranian population

  • Ali Khanbazi,
  • Maryam Beheshtian,
  • Maryam Azad,
  • Masoumeh Akbari Kelishomi,
  • Fariba Afroozan,
  • Fatemeh Fatehi,
  • Khadijeh Noudehi,
  • Shima Zamanian Najafabadi,
  • Mohammadamin Omrani,
  • Haleh Habibi,
  • Maryam Taghdiri,
  • Isa Abdi Rad,
  • Shahriar Nafissi,
  • Aria Jankhah,
  • Hilda Yazdan,
  • Parvaneh Daneshmand,
  • Seyed Hosseinali Saberi,
  • Kimia Kahrizi,
  • Ariana Kariminejad,
  • Hossein Najmabadi

DOI
https://doi.org/10.1038/s41598-024-76815-x
Journal volume & issue
Vol. 14, no. 1
pp. 1 – 11

Abstract

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Abstract Copy number variations in the SMN1 gene on chromosome 5 are the primary cause of Spinal Muscular Atrophy (SMA) disease, characterized by muscle weakness and degeneration due to impaired alpha motor neurons in the spinal cord. To obtain a comprehensive molecular understanding of the SMA, including carriers, silent carriers, and patients in the Iranian population, we analyzed data from 5224 individuals referred to Kariminejad - Najmabadi Pathology & Genetics Center, Tehran, Iran, between 2006 and 2023 using MLPA and quantitative RT-PCR methods. The carrier frequency of SMA was estimated to be 5.55%. Furthermore, 3.06% of SMA parents (n = 24) had two copies of the SMN1 gene. Among 725 patients, those with an earlier onset of SMA were more likely to have two copies of the SMN2 gene (46.45%) and no copies of the NAIP gene (49.36%). Among the 654 fetal samples screened for SMA, 22.33% were found to be affected, while 3.46% of their parents tested normal. These findings are valuable for genetic counseling, carrier screening, and prenatal diagnosis of SMA in Iran. Furthermore, they underscore the importance of CNV analysis of SMN1, SMN2, and NAIP genes for accurate diagnosis and prognosis of SMA.

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