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The protective role of DOT1L in UV-induced melanomagenesis

Authors :: Jay L. Hess
Peilin Ma
Colin R. Goding
Min Liu
Nicholas K. Hayward
Changpeng Han
Yujiang Shi
Xiumei Gao
Zhenyu Xuan
Shuyang Chen
Jie Zhang
Christine G. Lian
Chengqian Yin
Zhao-Qian Liu
Dali Liu
Jingxuan Pan
Zhi-Xiang Xu
Xiaoyang Zhang
Hongshen Wang
Zhi Wei
Xiang Chen
Lixin Wan
Yongjun Wang
Rutao Cui
Cong Peng
Bo Zhu
Jun Zhou
Sharon Prince
Tao Wang
Wenyi Wei
Source :: Nature Communications, Nature Communications, Vol 9, Iss 1, Pp 1-13 (2018)
Publication Year :: 2018
Publisher :: Springer Science and Business Media LLC, 2018.
Abstract: The DOT1L histone H3 lysine 79 (H3K79) methyltransferase plays an oncogenic role in MLL-rearranged leukemogenesis. Here, we demonstrate that, in contrast to MLL-rearranged leukemia, DOT1L plays a protective role in ultraviolet radiation (UVR)-induced melanoma development. Specifically, the DOT1L gene is located in a frequently deleted region and undergoes somatic mutation in human melanoma. Specific mutations functionally compromise DOT1L methyltransferase enzyme activity leading to reduced H3K79 methylation. Importantly, in the absence of DOT1L, UVR-induced DNA damage is inefficiently repaired, so that DOT1L loss promotes melanoma development in mice after exposure to UVR. Mechanistically, DOT1L facilitates DNA damage repair, with DOT1L-methylated H3K79 involvement in binding and recruiting XPC to the DNA damage site for nucleotide excision repair (NER). This study indicates that DOT1L plays a protective role in UVR-induced melanomagenesis.<br />The interaction of DOT1L with MLL oncogenic fusion proteins has been implicated in leukemogenesis. Here, the authors show a contrasting role for DOT1L in protecting UVR-induced melanomagenesis by facilitating DNA repair through interaction with XPC.