ZBTB33 is mutated in clonal hematopoiesis and myelodysplastic syndromes and impacts RNA splicing.

Ellen M. Beauchamp,Matthew Leventhal,Elsa Bernard,Emma R. Hoppe,Gabriele Todisco,Maria Creignou,Anna Gallì,Cecilia A. Castellano,Marie McConkey,Akansha Tarun,Waihay J. Wong,Monica Schenone,Caroline Stanclift,Benjamin Tanenbaum,Edyta Malolepsza,Björn Nilsson,Alexander G. Bick,Joshua S. Weinstock,Mendy Miller,Abhishek Niroula,Andrew Dunford,Amaro Taylor-Weiner,Timothy R. Wood,Alex Barbera,Shankara Anand,Bruce M. Psaty,Pinkal Desai,Michael H. Cho,Andrew D. Johnson,Ruth J. F. Loos,Daniel G. MacArthur,Monkol Lek,Donna Neuberg,Kasper Lage,Steven A. Carr,Eva Hellström-Lindberg,Luca Malcovati,Elli Papaemmanuil,Chip Stewart,Gad Getz,Robert K. Bradley,Siddhartha Jaiswal,Benjamin L. Ebert

ZBTB33 is mutated in clonal hematopoiesis and myelodysplastic syndromes and impacts RNA splicing.

2021

Clonal hematopoiesis results from somatic mutations in cancer driver genes in hematopoietic stem cells. We sought to identify novel drivers of clonal expansion using an unbiased analysis of sequencing data from 84,683 persons and identified common mutations in the 5-methylcytosine reader, ZBTB33, as well as in YLPM1, SRCAP, and ZNF318. We also identified these mutations at low frequency in myelodysplastic syndrome patients. Zbtb33 edited mouse hematopoietic stem and progenitor cells exhibited a competitive advantage in vivo and increased genome-wide intron retention. ZBTB33 mutations potentially link DNA methylation and RNA splicing, the two most commonly mutated pathways in clonal hematopoiesis and MDS.

Keywords:

Biology
Stem cell
Haematopoiesis
Gene
Progenitor cell
Intron
Myelodysplastic syndromes
Genetics
RNA splicing
DNA methylation

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