Introduction: The α -thalassemia 44.6 kb or Chiang Rai (-- ) deletion has been reported in northern Thailand and is capable of causing hemoglobin (Hb) H disease and a lethal α-thalassemia genotype, Hb Bart's hydrops fetalis, in this region. However, there are no current data regarding the frequency of -- nationwide due to a lack of effective diagnostic assay. Therefore, this study aimed to develop a reliable platform for simultaneous genotyping of -- and two common α -thalassemias in Thailand (-- and -- ) and investigate the frequency of -- across Thailand.

Methods: Multiplex gap-PCR assay and five renewable plasmid DNA controls for -- , -- , -- , α2-globin (HBA2), and β-actin (ACTB) were newly developed and validated with reference methods. The developed assay was further tested on 1046 unrelated individuals with a reduced mean corpuscular volume (MCV) of less than 75 fl for investigating genotypic and allelic spectrum of -- .

Results: Our developed assay showed 100% concordance with reference methods. The results were valid and reproducible throughout hundreds of reactions. Comparison of the genotypic and allelic spectra revealed that heterozygous -- (-- /αα) and -- alleles were dominant with the frequency of 22.85% (239/1046) and 13.34% (279/2092), respectively. Of these, -- and -- were relatively rare in this population and comparable to each other with the allelic frequency of 0.14% (3/2092).

Conclusion: This study successfully established a reliable molecular diagnostic platform for genotyping of -- , -- , and -- in a single reaction. Additionally, we demonstrated the frequency of -- in Thailand for the first time and provided knowledge basis for the planning of severe α-thalassemia prevention and control programs in Thailand, where thalassemia is endemic.

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http://dx.doi.org/10.1111/ahg.12496DOI Listing

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