Prevalence and genotype-phenotype correlation study of ASXL1 variants c.1773C>G(Tyr591Ter) and c.1282C>Tp.(Gln428Ter) in a Sri Lankan Myeloproliferative Neoplasm cohort

dc.contributor.authorManamperi, S.T.
dc.contributor.authorKarunatilake, S.T.
dc.contributor.authorCostha, N.N.H.
dc.contributor.authorAmarasinghe, N.
dc.contributor.authorCosta, Y.J.
dc.contributor.authorGoonasekara, H.W.W.
dc.date.accessioned2026-05-14T09:25:07Z
dc.date.issued2025
dc.description.abstractMolecular insights into ASXL1 gene variants are valuable for the diagnosis and prognosis of myeloproliferative neoplasms (MPNs). Their prevalence varies across ethnicities, with limited data available for South Asian populations. This study investigated two Asian-specific ASXL1 variants c.1773C>G (p.Tyr591Ter) and c.1282C>T (p.Gln428Ter) and assessed genotype phenotype correlations in a Sri Lankan MPN cohort. Fifty patients from a tertiary care hospital in North Colombo were recruited following ethical approval (EC-24-150). Variant selection was based on Genome Aggregation and VarSome databases. Detection was performed using Tetra-primer ARMS-PCR, with a modified touchdown PCR protocol for the c.1282C>T variant. Results were validated through Sanger sequencing and analyzed using IBM SPSS Statistics 19. Of the cohort (PV: 82%, ET: 10%, PMF: 8%; male:female ratio 2.3:1; mean age 56 years), the c.1773C>G variant was identified in 12% (n=6, all heterozygous) and was present across all MPN subtypes. The c.1282C>T variant was not detected in any patient. ARMS-PCR results were consistent with Sanger sequencing. No statistically significant genotype phenotype correlations were observed, though trends included lower hemoglobin and higher platelet counts in variant-positive patients. This is the first report of the c.1773C>G variant in Sri Lankan MPNs. The absence of the c.1282C>T variant may reflect its rarity or post-treatment clonal loss. The development and validation of cost-effective ARMS-PCR protocols for ASXL1 variant screening represent a significant step toward personalized MPN management in South Asia. Larger studies are warranted to confirm these findings.
dc.identifier.citationManamperi, S. T., Karunatilake, S. T., Costha, N. N. H., Amarasinghe, N., Costa, Y. J., & Goonasekara, H. W. W. (2025). Prevalence and genotype-phenotype correlation study of ASXL1 variants c.1773C>G (Tyr591Ter) and c.1282C>T p.(Gln428Ter) in a Sri Lankan myeloproliferative neoplasm cohort. Proceedings of the Annual Research Symposium-2025, University of Colombo, Sri Lanka, p.57.
dc.identifier.urihttps://archive.cmb.ac.lk/handle/70130/8819
dc.identifier.urihttps://doi.org/10.66281/70130/8819
dc.language.isoen
dc.publisherUniversity of Colombo
dc.subjectSri Lankan Myeloproliferative Neoplasms
dc.subjectASXL1c.1773C>G(Tyr591Ter)
dc.subjectASXL1c.1282C>T(Gln428Ter)
dc.subjectTetra-primer ARMS-PCR
dc.subjectTouchdown-PCR
dc.titlePrevalence and genotype-phenotype correlation study of ASXL1 variants c.1773C>G(Tyr591Ter) and c.1282C>Tp.(Gln428Ter) in a Sri Lankan Myeloproliferative Neoplasm cohort
dc.typeArticle

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