| Literature DB >> 32043463 |
Jose F Moruno-Manchon1, Pauline Lejault2, Yaoxuan Wang1, Brenna McCauley3, Pedram Honarpisheh4,5, Diego A Morales Scheihing4, Shivani Singh6, Weiwei Dang3, Nayun Kim6, Akihiko Urayama4,5, Liang Zhu7,8, David Monchaud2, Louise D McCullough4,5, Andrey S Tsvetkov1,5,9.
Abstract
Guanine-rich DNA sequences can fold into four-stranded G-quadruplex (G4-DNA) structures. G4-DNA regulates replication and transcription, at least in cancer cells. Here, we demonstrate that, in neurons, pharmacologically stabilizing G4-DNA with G4 ligands strongly downregulates the Atg7 gene. Atg7 is a critical gene for the initiation of autophagy that exhibits decreased transcription with aging. Using an in vitro assay, we show that a putative G-quadruplex-forming sequence (PQFS) in the first intron of the Atg7 gene folds into a G4. An antibody specific to G4-DNA and the G4-DNA-binding protein PC4 bind to the Atg7 PQFS. Mice treated with a G4 stabilizer develop memory deficits. Brain samples from aged mice contain G4-DNA structures that are absent in brain samples from young mice. Overexpressing the G4-DNA helicase Pif1 in neurons exposed to the G4 stabilizer improves phenotypes associated with G4-DNA stabilization. Our findings indicate that G4-DNA is a novel pathway for regulating autophagy in neurons.Entities:
Keywords: G-quadruplex; aging; autophagy; cell biology; mouse; neurodegeneration; neurons; neuroscience; rat
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Year: 2020 PMID: 32043463 PMCID: PMC7012600 DOI: 10.7554/eLife.52283
Source DB: PubMed Journal: Elife ISSN: 2050-084X Impact factor: 8.713