Proteomic Analysis of Protective Effects of Dl-3-n-Butylphthalide against mpp + -Induced Toxicity via downregulating P53 pathway in N2A Cells

Abstract: Background Dl-3-n-butylphthalide (NBP) is an important medial therapy for acute ischemic stroke in China. Recent studied have revealed that NBP not only rescued the loss of dopaminergic neurons in cellular and animal models of Parkinson's disease (PD), but also could improve motor symptoms in PD patients. However, the protective mechanism is not fully understood. P53 is a multifunctional protein implicated in numerous cellular processes, including apoptosis, DNA repair, mitochondrial functions,… Show more

“…Quercetin, [ 350 ] Dl‐3‐n‐butylphthalide, [ 109 , 351 ] β ‐hydroxybutyric acid, [ 352 ] thonningianin A, [ 112 ] GW501516 (a specific PPAR δ agonist), [ 111 ] hinokitiol, [ 113 ] paeoniflorin, [ 125 ] α ‐Lipoicacid, [ 114 ] iron chelator deferoxamine (DFO), [ 353 ] SK4/DFO, [ 354 ] clioquinol, [ 115 ] apoferritin, [ 126 ] ferrostatin‐1, [ 110 , 355 ] SK4/DFO, [ 354 ] and idebenone [ 356 ] alleviate PD through inhibiting ferroptosis (Table 1 ).…”

Pharmacological Inhibition of Ferroptosis as a Therapeutic Target for Neurodegenerative Diseases and Strokes

“…Quercetin, [ 350 ] Dl‐3‐n‐butylphthalide, [ 109 , 351 ] β ‐hydroxybutyric acid, [ 352 ] thonningianin A, [ 112 ] GW501516 (a specific PPAR δ agonist), [ 111 ] hinokitiol, [ 113 ] paeoniflorin, [ 125 ] α ‐Lipoicacid, [ 114 ] iron chelator deferoxamine (DFO), [ 353 ] SK4/DFO, [ 354 ] clioquinol, [ 115 ] apoferritin, [ 126 ] ferrostatin‐1, [ 110 , 355 ] SK4/DFO, [ 354 ] and idebenone [ 356 ] alleviate PD through inhibiting ferroptosis (Table 1 ).…”

Pharmacological Inhibition of Ferroptosis as a Therapeutic Target for Neurodegenerative Diseases and Strokes

Research progress in the molecular mechanism of ferroptosis in Parkinson's disease and regulation by natural plant products

The molecular mechanism of ferroptosis and its relationship with Parkinson's disease