TET2 missense variants in human neoplasia. A proposal of structural and functional classification

Elena Bussaglia; Rosa Antón; Josep F. Nomdedéu; Pablo Fuentes‐Prior

doi:10.1002/mgg3.772

Molecular Genetics & Genomic Medicine (Jul 2019)

TET2 missense variants in human neoplasia. A proposal of structural and functional classification

Elena Bussaglia,
Rosa Antón,
Josep F. Nomdedéu,
Pablo Fuentes‐Prior

Affiliations

Elena Bussaglia: Hematology Department and Diagnostic Hematology Group Barcelona Spain
Rosa Antón: Molecular Bases of Disease The Biomedical Research Institute Sant Pau (IIB Sant Pau), Hospital de la Santa Creu i Sant Pau Barcelona Spain
Josep F. Nomdedéu: Hematology Department and Diagnostic Hematology Group Barcelona Spain
Pablo Fuentes‐Prior: Molecular Bases of Disease The Biomedical Research Institute Sant Pau (IIB Sant Pau), Hospital de la Santa Creu i Sant Pau Barcelona Spain

DOI: https://doi.org/10.1002/mgg3.772
Journal volume & issue: Vol. 7, no. 7
pp. n/a – n/a

Abstract

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Abstract Background The human TET2 gene plays a pivotal role in the epigenetic regulation of normal and malignant hematopoiesis. Somatic TET2 mutations have been repeatedly identified in age‐related clonal hematopoiesis and in myeloid neoplasms ranging from acute myeloid leukemia (AML) to myeloproliferative neoplasms. However, there have been no attempts to systematically explore the structural and functional consequences of the hundreds of TET2 missense variants reported to date. Methods We have sequenced the TET2 gene in 189 Spanish AML patients using Sanger sequencing and NGS protocols. Next, we performed a thorough bioinformatics analysis of TET2 protein and of the expected impact of all reported TET2 missense variants on protein structure and function, exploiting available structure‐and‐function information as well as 3D structure prediction tools. Results We have identified 38 TET2 allelic variants in the studied patients, including two frequent SNPs: p.G355D (10 cases) and p.I1762V (28 cases). Four of the detected mutations are reported here for the first time: c.122C>T (p.P41L), c.4535C>G (p.A1512G), c.4760A>G (p.D1587G), and c.5087A>T (p.Y1696F). We predict a complex multidomain architecture for the noncatalytic regions of TET2, and in particular the presence of well‐conserved α+β globular domains immediately preceding and following the actual catalytic unit. Further, we provide a rigorous interpretation of over 430 missense SNVs that affect the TET2 catalytic domain, and we hypothesize explanations for ~700 additional variants found within the regulatory regions of the protein. Finally, we propose a systematic classification of all missense mutants and SNPs reported to date into three major categories (severe, moderate, and mild), based on their predicted structural and functional impact. Conclusions The proposed classification of missense TET2 variants would help to assess their clinical impact on human neoplasia and may guide future structure‐and‐function investigations of TET family members.

Published in Molecular Genetics & Genomic Medicine

ISSN: 2324-9269 (Online)
Publisher: Wiley
Country of publisher: United States
LCC subjects: Science: Biology (General): Genetics
Website: https://onlinelibrary.wiley.com/journal/23249269

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