Modulation of SETDB1 activity by APQ ameliorates heterochromatin condensation, motor function, and neuropathology in a Huntington's disease mouse model

Authors
Hwang, Yu JinHyeon, Seung JaeKim, YoungheeLim, SungsuLee, Min YoungKim, JieunASHWINI, MACHHINDRA LONDHEGotina, LizavetaKim, YunhaPae, Ae NimCho, Yong SeoSeong, JihyeSeo, HyemyungKim, Yun KyungChoo, HyunahRyu, HoonMin, Sun-Joon
Issue Date
2021-01
Publisher
Taylor & Francis
Citation
Journal of Enzyme Inhibition and Medicinal Chemistry, v.36, no.1, pp.856 - 868
Abstract
The present study describes evaluation of epigenetic regulation by a small molecule as the therapeutic potential for treatment of Huntington's disease (HD). We identified 5-allyloxy-2-(pyrrolidin-1-yl)quinoline (APQ) as a novel SETDB1/ESET inhibitor using a combined in silico and in vitro cell based screening system. APQ reduced SETDB1 activity and H3K9me3 levels in a HD cell line model. In particular, not only APQ reduced H3K9me3 levels in the striatum but it also improved motor function and neuropathological symptoms such as neuronal size and activity in HD transgenic (YAC128) mice with minimal toxicity. Using H3K9me3-ChIP and genome-wide sequencing, we also confirmed that APQ modulates H3K9me3-landscaped epigenomes in YAC128 mice. These data provide that APQ, a novel small molecule SETDB1 inhibitor, coordinates H3K9me-dependent heterochromatin remodelling and can be an epigenetic drug for treating HD, leading with hope in clinical trials of HD.
Keywords
SETDB1; Huntington’ s disease; medium spiny neuron; motor function
ISSN
1475-6366
URI
https://pubs.kist.re.kr/handle/201004/117620
DOI
10.1080/14756366.2021.1900160
Appears in Collections:
KIST Article > 2021
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