Molecular Genetics and Metabolism Reports (Jan 2014)

A rapid screening with direct sequencing from blood samples for the diagnosis of Leigh syndrome

  • Hiroko Shimbo,
  • Mariko Takagi,
  • Mitsuko Okuda,
  • Yu Tsuyusaki,
  • Kyoko Takano,
  • Mizue Iai,
  • Sumimasa Yamashita,
  • Kei Murayama,
  • Akira Ohtake,
  • Yu-ichi Goto,
  • Noriko Aida,
  • Hitoshi Osaka

DOI
https://doi.org/10.1016/j.ymgmr.2014.02.006
Journal volume & issue
Vol. 1, no. C
pp. 133 – 138

Abstract

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Large numbers of genes are responsible for Leigh syndrome (LS), making genetic confirmation of LS difficult. We screened our patients with LS using a limited set of 21 primers encompassing the frequently reported gene for the respiratory chain complexes I (ND1–ND6, and ND4L), IV(SURF1), and V(ATP6) and the pyruvate dehydrogenase E1α-subunit. Of 18 LS patients, we identified mutations in 11 patients, including 7 in mDNA (two with ATP6), 4 in nuclear (three with SURF1). Overall, we identified mutations in 61% of LS patients (11/18 individuals) in this cohort. Sanger sequencing with our limited set of primers allowed us a rapid genetic confirmation of more than half of the LS patients and it appears to be efficient as a primary genetic screening in this cohort.

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