"A novel DNMT3B splice variant expressed in tumor and pluripotent cells" by Suhasni Gopalakrishnan, Beth O Van Emburgh et al.

NSU-MD Faculty Articles

Title

A novel DNMT3B splice variant expressed in tumor and pluripotent cells modulates genomic DNA methylation patterns and displays altered DNA binding.

Authors

Suhasni Gopalakrishnan
Beth O Van Emburgh
Jixiu Shan
Zhen Su
C Robert Fields
Johannes Vieweg, Nova Southeastern UniversityFollow
Takashi Hamazaki
Philip H Schwartz
Naohiro Terada
Keith D Robertson

Publication Title

Molecular cancer research : MCR

Volume

Issue

Publication Date / Copyright Date

10-1-2009

First Page

1622

Last Page

1634

Publisher

American Association for Cancer Research

DOI Number

10.1158/1541-7786.MCR-09-0018

Abstract

DNA methylation is an epigenetic mark essential for mammalian development, genomic stability, and imprinting. DNA methylation patterns are established and maintained by three DNA methyltransferases: DNMT1, DNMT3A, and DNMT3B. Interestingly, all three DNMTs make use of alternative splicing. DNMT3B has nearly 40 known splice variants expressed in a tissue- and disease-specific manner, but very little is known about the role of these splice variants in modulating DNMT3B function. We describe here the identification and characterization of a novel alternatively spliced form of DNMT3B lacking exon 5 within the NH(2)-terminal regulatory domain. This variant, which we term DNMT3B3Delta5 because it is closely related in structure to the ubiquitously expressed DNMT3B3 isoform, is highly expressed in pluripotent cells and brain tissue, is downregulated during differentiation, and is conserved in the mouse. Creation of pluripotent iPS cells from fibroblasts results in marked induction of DNMT3B3Delta5. DNMT3B3Delta5 expression is also altered in human disease, with tumor cell lines displaying elevated or reduced expression depending on their tissue of origin. We then compared the DNA binding and subcellular localization of DNMT3B3Delta5 versus DNMT3B3, revealing that DNMT3B3Delta5 possessed significantly enhanced DNA binding affinity and displayed an altered nuclear distribution. Finally, ectopic overexpression of DNMT3B3Delta5 resulted in repetitive element hypomethylation and enhanced cell growth in a colony formation assay. Taken together, these results show that DNMT3B3Delta5 may play an important role in stem cell maintenance or differentiation and suggest that sequences encoded by exon 5 influence the functional properties of DNMT3B.

Disciplines

Medicine and Health Sciences

Keywords

Alternative Splicing, Animals, Base Sequence, Cell Line, Tumor, Cell Nucleus, Cell Proliferation, DNA (Cytosine-5-)-Methyltransferases, DNA Methylation, DNA-Binding Proteins, Epigenesis, Genetic, Exons, Genomic Instability, Humans, Mice, Neoplasms, Pluripotent Stem Cells, Protein Isoforms, Protein Structure, Tertiary, Tumor Stem Cell Assay

NSUWorks Citation

Gopalakrishnan, Suhasni; Van Emburgh, Beth O; Shan, Jixiu; Su, Zhen; Fields, C Robert; Vieweg, Johannes; Hamazaki, Takashi; Schwartz, Philip H; Terada, Naohiro; and Robertson, Keith D, "A novel DNMT3B splice variant expressed in tumor and pluripotent cells modulates genomic DNA methylation patterns and displays altered DNA binding." (2009). NSU-MD Faculty Articles. 52.
https://nsuworks.nova.edu/hpd_md_facarticles/52

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