| Literature DB >> 34528509 |
Susu Pan1,2, Kaili Yin1,2, Zhiwei Tang3, Shuren Wang4, Zhuo Chen1,2, Yirong Wang3, Hongxia Zhu4, Yunyun Han2,5, Mei Liu4, Man Jiang3, Ningzhi Xu4, Guo Zhang1,2.
Abstract
Emerging evidence suggests that the nervous system is involved in tumor development in the periphery, however, the role of the central nervous system remains largely unknown. Here, by combining genetic, chemogenetic, pharmacological, and electrophysiological approaches, we show that hypothalamic oxytocin (Oxt)-producing neurons modulate colitis-associated cancer (CAC) progression in mice. Depletion or activation of Oxt neurons could augment or suppress CAC progression. Importantly, brain treatment with celastrol, a pentacyclic triterpenoid, excites Oxt neurons and inhibits CAC progression, and this anti-tumor effect was significantly attenuated in Oxt neuron-lesioned mice. Furthermore, brain treatment with celastrol suppresses sympathetic neuronal activity in the celiac-superior mesenteric ganglion (CG-SMG), and activation of β2 adrenergic receptor abolishes the anti-tumor effect of Oxt neuron activation or centrally administered celastrol. Taken together, these findings demonstrate that hypothalamic Oxt neurons regulate CAC progression by modulating the neuronal activity in the CG-SMG. Stimulation of Oxt neurons using chemicals, for example, celastrol, might be a novel strategy for colorectal cancer treatment.Entities:
Keywords: cancer biology; colorectal cancer; hypothalamus; mouse; neuroscience; oxytocin neuron; tumor progression
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Year: 2021 PMID: 34528509 PMCID: PMC8536257 DOI: 10.7554/eLife.67535
Source DB: PubMed Journal: Elife ISSN: 2050-084X Impact factor: 8.140