The cancer-associated CTCFL/BORIS protein targets multiple classes of genomic repeats, with a distinct binding and functional preference for humanoid-specific SVA transposable elements.
Elena M PugachevaEvgeny TeplyakovQiongfang WuJingjing LiCheng ChenChengcheng MengJian LiuSusan RobinsonDmitry LoukinovAbdelhalim BoukabaAndrew Paul HutchinsVictor LobanenkovAlexander V StrunnikovPublished in: Epigenetics & chromatin (2016)
Thus, BORIS directly binds to, and regulates SVA repeats, which are essentially movable CpG islands, via clusters of BORIS binding sites. This finding uncovers a new function of the global germline-specific transcriptional regulator BORIS in regulating and repressing the newest class of transposable elements that are actively transposed in human genome when activated. This function of BORIS in cancer cells is likely a reflection of its roles in the germline.