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Correction to: Protein Cell https://doi.org/10.1007/s13238-019-00672-y
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A similar study from Chao Lu group was published online on 5 September 2019 in Nature, entitled “The histone mark H3K36me2 recruits DNMT3A and shapes the intergenic DNA methylation landscape” (Weinberg et al., 2019). Although both studies reported the preferential recognition of H3K36me2 by DNMT3A PWWP, ours in addition uncovered a stimulation function by such interaction on the activity of DNMT3A. On the disease connections, we used a NSD2 gain-of-function model which led to the discovery of potential therapeutic implication of DNA inhibitors in the related cancers, while the other study only used NSD1 and DNMT3A loss-of-function models.
References
Weinberg DN, Papillon-Cavanagh S, Chen H, Yue Y, Chen X, Rajagopalan KN, Horth C, McGuire JT, Xu X, Nikbakht H et al (2019) The histone mark H3K36me2 recruits DNMT3A and shapes the intergenic DNA methylation landscape. Nature 573:281–286
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Xu, W., Li, J., Rong, B. et al. Correction to: DNMT3A reads and connects histone H3K36me2 to DNA methylation. Protein Cell 11, 230 (2020). https://doi.org/10.1007/s13238-019-00678-6
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DOI: https://doi.org/10.1007/s13238-019-00678-6