Pharmacological Stimulation of Nurr1 Promotes Cell Cycle Progression in Adult Hippocampal Neural Stem Cells

Moon, Haena; Jeon, Seong Gak; Kim, Jin-il; Kim, Hyeon soo; Lee, Sang-Ho; Kim, Dongok; Park, Seungjoon; Moon, Minho; Chung, Hyun Ju

doi:10.3390/ijms21010004

Cited by 8 publications

(8 citation statements)

References 115 publications

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“…CDKN1B has been reported to regulate G 1 progression and maintain the cell function in response to cell proliferation inhibition or cell differentiation [36,37]. In addition, it has been confirmed that CDKN1B can act as a key modulator in cell growth by induction of CDK2 and Cyclin E1 [38,39]. The findings were consistent to these of previous studies.…”

Section: Plos Onesupporting

confidence: 90%

Knockdown of hsa_circ_0001275 reverses dexamethasone-induced osteoblast growth inhibition via mediation of miR-377/CDKN1B axis

Sun

et al. 2021

PLoS ONE

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Background Osteoporosis affects the quality of life among middle-aged and elderly individuals. In addition, dysfunction of osteoblasts can lead to the progression of osteoporosis. Circular (circ)RNAs are involved in various types of diseases, including osteoporosis. Moreover, it has been reported that hsa_circ_0001275 expression is upregulated in osteoporosis. However, the effects of hsa_circ_0001275 on the growth of osteoblasts remain unclear. Methods In the present study, the gene and protein expression levels in hFOB1.19 cells were detected via reverse transcription-quantitative (RT-qPCR) and western blot analyses, respectively. In addition, alkaline phosphatase (ALP) activity and calcium nodules were examined by ALP and alizarin red staining, respectively. Cell proliferation was measured using the Cell Counting Kit-8 assay. Cell apoptosis and cell cycle were analyzed by flow cytometry. Furthermore, dual luciferase reporter and RNA pull-down assay were used to confirm the association among hsa_circ_0001275, microRNA (miR)-377 and CDKN1B. Results DEX-induced hFOB1.19 cell growth inhibition was significantly reversed by silencing hsa_circ_0001275. Moreover, DEX significantly increased ALP activity and calcium nodules in hFOB1.19 cells, while this effect was significantly reversed in the presence of hsa_circ_0001275 small interfering RNA. In addition, miR-377 was sponged by hsa_circ_0001275 and CDKN1B was directly targeted by miR-377 in hFOB1.19 cells. Furthermore, the therapeutic effect of hsa_circ_0001275 knockdown on osteoporosis was notably reversed by miR-377 antagomir. Conclusion The data demonstrated that knockdown of hsa_circ_0001275 reversed DEX-induced osteoblast growth inhibition via activation of the miR-377/CDKN1B axis. Therefore, this study might shed new lights on the treatment of osteoporosis.

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Section: Plos Onesupporting

confidence: 90%

Knockdown of hsa_circ_0001275 reverses dexamethasone-induced osteoblast growth inhibition via mediation of miR-377/CDKN1B axis

Sun

et al. 2021

PLoS ONE

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“…37 Particularly, it is pointed out that the inhibition of the activity of Cyclin-CDK complexes in vitro and the blocking of the cell cycle process by regulating the G 1 to S phase transition are all closely related to p57 KIP2 . 22 Our results showed that there was a notable rise in negative cell cycle regulatory factors, specifically p27 KIP1 and p57 KIP2 , for 24 h after treatment with Mn. More importantly, Nurr1 is considered to be a neuroprotective transcription regulator, which is closely related to the cell cycle.…”

Section: Discussionsupporting

confidence: 48%

Melatonin promotes cell cycle progression of neural stem cells subjected to manganese via Nurr1

Chen,

Zhou,

et al. 2024

Environmental Toxicology

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Excessive exposure to manganese (Mn) through drinking water and food during pregnancy significantly heightens the likelihood of neurodevelopmental damage in offspring. Multiple studies have indicated that melatonin (Mel) may help to relieve neurodevelopmental disorders caused by Mn, but potential mechanisms underlying this effect require further exploration. Here, we utilized primary neural stem cells (NSCs) as a model to elucidate the molecular mechanism underlying the protective function of Mel on Mn‐induced cell proliferation dysfunction and cycle arrest. Our results showed that Mn disrupted the cell cycle in NSCs by suppressing positive regulatory proteins (CDK2, Cyclin A, Cyclin D1, and E2F1) and enhancing negative ones (p27KIP1 and p57KIP2), leading to cell proliferation dysfunction. Mel inhibited the Mn‐dependent changes to these proteins and the cell cycle through nuclear receptor‐related protein 1 (Nurr1), thus alleviating the proliferation dysfunction. Knockdown of Nurr1 using lentivirus‐expressed shRNA in NSCs resulted in a diminished protective effect of Mel. We concluded that Mel mitigated Mn‐induced proliferation dysfunction and cycle arrest in NSCs through Nurr1.

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“…First, Nurr1 activation by AQ has been linked to neuroprotection. Activation of Nurr1 by AQ leads to the generation of neurons from cortical [ 42 ] and hippocampal [ 42 , 47 , 48 ] neural precursor cells, enhances short-and long-term memory, and improves cognitive deficits in mouse models of Parkinson’s [ 49 , 50 ] and Alzheimer’s disease [ 51 ]. Second, AQ is known to be a selective agonist for Nurr1 with no effect on other members of the NR4A family (Nur77 and NOR1) [ 49 ].…”

Section: Discussionmentioning

confidence: 99%

Nurr1 Is Not an Essential Regulator of BDNF in Mouse Cortical Neurons

Abdollahi

Fahnestock

2022

IJMS

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Nurr1 and brain-derived neurotrophic factor (BDNF) play major roles in cognition. Nurr1 regulates BDNF in midbrain dopaminergic neurons and cerebellar granule cells. Nurr1 and BDNF are also highly expressed in the cerebral cortex, a brain area important in cognition. Due to Nurr1 and BDNF tissue specificity, the regulatory effect of Nurr1 on BDNF in different brain areas cannot be generalized. The relationship between Nurr1 and BDNF in the cortex has not been investigated previously. Therefore, we examined Nurr1-mediated BDNF regulation in cortical neurons in activity-dependent and activity-independent states. Mouse primary cortical neurons were treated with the Nurr1 agonist, amodiaquine (AQ). Membrane depolarization was induced by KCl or veratridine and reversed by nimodipine. AQ and membrane depolarization significantly increased Nurr1 (p < 0.001) and BDNF (pAQ < 0.001, pKCl < 0.01) as assessed by real-time qRT-PCR. However, Nurr1 knockdown did not affect BDNF gene expression in resting or depolarized neurons. Accordingly, the positive correlation between Nurr1 and BDNF expression in AQ and membrane depolarization experiments does not imply co-regulation because Nurr1 knockdown did not affect BDNF gene expression in resting or depolarized cortical neurons. Therefore, in contrast to midbrain dopaminergic neurons and cerebellar granule cells, Nurr1 does not regulate BDNF in cortical neurons.

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Pharmacological Stimulation of Nurr1 Promotes Cell Cycle Progression in Adult Hippocampal Neural Stem Cells

Cited by 8 publications

References 115 publications

Knockdown of hsa_circ_0001275 reverses dexamethasone-induced osteoblast growth inhibition via mediation of miR-377/CDKN1B axis

Knockdown of hsa_circ_0001275 reverses dexamethasone-induced osteoblast growth inhibition via mediation of miR-377/CDKN1B axis

Melatonin promotes cell cycle progression of neural stem cells subjected to manganese via Nurr1

Nurr1 Is Not an Essential Regulator of BDNF in Mouse Cortical Neurons

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