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急性海马切片中针对二异丙基氟磷酸酯的神经保护作用

Neuroprotection Against Diisopropylfluorophosphate in Acute Hippocampal Slices.

作者信息

Ferchmin P A, Pérez Dinely, Cuadrado Brenda L, Carrasco Marimée, Martins Antonio H, Eterović Vesna A

机构信息

Department of Biochemistry, Universidad Central Del Caribe, School of Medicine, Ave. Laurel, Santa Juanita, Bayamón, PR, 00956, USA.

, PO BOX 60327, Bayamón, PR, 00960-6032, USA.

出版信息

Neurochem Res. 2015 Oct;40(10):2143-51. doi: 10.1007/s11064-015-1729-4. Epub 2015 Oct 5.

Abstract

Diisopropylfluorophosphate (DFP) is an irreversible inhibitor of acetylcholine esterase and a surrogate of the organophosphorus (OP) nerve agent sarin. The neurotoxicity of DFP was assessed as a reduction of population spike (PS) area elicited by synaptic stimulation in acute hippocampal slices. Two classical antidotes, atropine, and pralidoxime, and two novel antidotes, 4R-cembranotriene-diol (4R) and a caspase nine inhibitor, were tested. Atropine, pralidoxime, and 4R significantly protected when applied 30 min after DFP. The caspase inhibitor was neuroprotective when applied 5-10 min before or after DFP, suggesting that early synaptic apoptosis is responsible for the loss of PSs. It is likely that apoptosis starts at the synapses and, if antidotes are not applied, descends to the cell bodies, causing death. The acute slice is a reliable tool for mechanistic studies, and the assessment of neurotoxicity and neuroprotection with PS areas is, in general, pharmacologically congruent with in vivo results and predicts the effect of drugs in vivo. 4R was first found to be neuroprotective in slices and later we demonstrated that 4R is neuroprotective in vivo. The mechanism of neurotoxicity of OPs is not well understood, and there is a need for novel antidotes that could be discovered using acute slices.

摘要

二异丙基氟磷酸酯(DFP)是乙酰胆碱酯酶的不可逆抑制剂,也是有机磷(OP)神经毒剂沙林的替代物。通过急性海马脑片中突触刺激引发的群体峰电位(PS)面积减少来评估DFP的神经毒性。测试了两种经典解毒剂阿托品和氯解磷定,以及两种新型解毒剂4R-西松三烯二醇(4R)和一种半胱天冬酶9抑制剂。DFP作用30分钟后应用阿托品、氯解磷定和4R可显著起到保护作用。半胱天冬酶抑制剂在DFP作用前5 - 10分钟或作用后应用具有神经保护作用,这表明早期突触凋亡是PS丧失的原因。凋亡可能始于突触,如果不应用解毒剂,会向下蔓延至细胞体,导致死亡。急性脑片是进行机制研究的可靠工具,用PS面积评估神经毒性和神经保护作用,总体上在药理学上与体内结果一致,并能预测药物在体内的作用。4R最初是在脑片中被发现具有神经保护作用,后来我们证明4R在体内也具有神经保护作用。OPs神经毒性的机制尚未完全了解,需要利用急性脑片发现新型解毒剂。

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