BMC Medical Genetics (May 2019)

Molecular analysis of a large novel deletion causing α+-thalassemia

  • Jianlong Zhuang,
  • Jie Tian,
  • Jitao Wei,
  • Yu Zheng,
  • Qianmei Zhuang,
  • Yuanbai Wang,
  • Qingyue Xie,
  • Shuhong Zeng,
  • Geng Wang,
  • Yanchao Pan,
  • Yuying Jiang

DOI
https://doi.org/10.1186/s12881-019-0797-8
Journal volume & issue
Vol. 20, no. 1
pp. 1 – 6

Abstract

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Abstract Background α-thalassaemia is an inherited blood disorder caused by mutations in the α-globin gene cluster. Recognizing the pathogenic α-globin gene mutations associated with α-Thalassemia is of significant importance to thalassaemia’s diagnosis and management. Methods A family with α-thalassaemia from Fujian, China was recruited for this study. The phenotype was confirmed through haematological analysis. Commercially available Gap-PCR genotypic methods were employed to identify the known deletions causing α-thalassemia. MLPA analysis was used to study the novel mutations; this was then confirmed through DNA sequencing and bioinformatics analysis. Results The proband of the family belonged to Southeast Asian type (--SEA) thalassaemia. None of the known mutations associated with α-thalassaemia were detected in this family’s genetics, whereas a novel 6.9 kb deletion (16p13.3 g.29,785-36,746) covering the α2 gene on the globin gene cluster was identified with MLPA and confirmed through Sanger Sequencing. This data led us to propose a novel pathogenic deletion associated with α-thalassemia: -α6.9 /--SEA. Conclusions A novel α-thalassaemia deletion was identified in members of a Chinese family and subsequently analyzed. This finding has helped broaden the spectrum of pathogenic mutations leading to the development of α-thalassaemia, paving the way for improved disease diagnosis and management.

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