Molecular Genetics and Metabolism Reports (Jan 2014)

Expanding the spectrum of HEXA mutations in Indian patients with Tay–Sachs disease

  • Jayesh Sheth,
  • Mehul Mistri,
  • Chaitanya Datar,
  • Umesh Kalane,
  • Shekhar Patil,
  • Mahesh Kamate,
  • Harshuti Shah,
  • Sheela Nampoothiri,
  • Sarita Gupta,
  • Frenny Sheth

DOI
https://doi.org/10.1016/j.ymgmr.2014.09.004
Journal volume & issue
Vol. 1, no. C
pp. 425 – 430

Abstract

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Tay–Sachs disease is an autosomal recessive neurodegenerative disorder occurring due to impaired activity of β-hexosaminidase-A (EC 3.2.1.52), resulting from the mutation in HEXA gene. Very little is known about the molecular pathology of TSD in Indian children except for a few mutations identified by us. The present study is aimed to determine additional mutations leading to Tay–Sachs disease in nine patients confirmed by the deficiency of β-hexosaminidase-A (C (D175A) and c.805G>C (p.G269R) in one case; and one small 1 bp deletion c.426delT (p.F142LfsX57) and one splice site mutation c.459+4A>C in the other two cases respectively. None of these mutations were detected in 100 chromosomes from healthy individuals of the same ethnic group. Three previously reported missense mutations, (i) c.532C>T (p.R178C), (ii) c.964G>T (p.D322Y), and (iii) c.1385A>T (p.E462V); two nonsense mutations (i) c.709C>T (p.Q237X) and (ii) c.1528C>T (p.R510X), one 4 bp insertion c.1277_1278insTATC (p.Y427IfsX5) and one splice site mutation c.459+5G>A were also identified in six cases. We observe from this study that novel mutations are more frequently observed in Indian patients with Tay–Sachs disease with clustering of ~73% of disease causing mutations in exons 5 to 12. This database can be used for a carrier rate screening in the larger population of the country.

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