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在帕金森病的6-羟基多巴胺损伤大鼠模型中观察到,A2A/NR2B受体拮抗剂联合使用具有前所未有的治疗潜力。

Unprecedented therapeutic potential with a combination of A2A/NR2B receptor antagonists as observed in the 6-OHDA lesioned rat model of Parkinson's disease.

作者信息

Michel Anne, Downey Patrick, Nicolas Jean-Marie, Scheller Dieter

机构信息

Neurosciences TA Biology, UCB BioPharma SPRL, Braine l'Alleud, Belgium.

Non-Clinical Development, UCB BioPharma SPRL, Braine l'Alleud, Belgium.

出版信息

PLoS One. 2014 Dec 16;9(12):e114086. doi: 10.1371/journal.pone.0114086. eCollection 2014.

Abstract

In Parkinson's disease, the long-term use of dopamine replacing agents is associated with the development of motor complications; therefore, there is a need for non-dopaminergic drugs. This study evaluated the potential therapeutic impact of six different NR2B and A2A receptor antagonists given either alone or in combination in unilateral 6-OHDA-lesioned rats without (monotherapy) or with (add-on therapy) the co-administration of L-Dopa: Sch-58261+ Merck 22; Sch-58261+Co-101244; Preladenant + Merck 22; Preladenant + Radiprodil; Tozadenant + Radiprodil; Istradefylline + Co-101244. Animals given monotherapy were assessed on distance traveled and rearing, whereas those given add-on therapy were assessed on contralateral rotations. Three-way mixed ANOVA were conducted to assess the main effect of each drug separately and to determine whether any interaction between two drugs was additive or synergistic. Additional post hoc analyses were conducted to compare the effect of the combination with the effect of the drugs alone. Motor activity improved significantly and was sustained for longer when the drugs were given in combination than when administered separately at the same dose. Similarly, when tested as add-on treatment to L-Dopa, the combinations resulted in higher levels of contralateral rotation in comparison to the single drugs. Of special interest, the activity observed with some combinations could not be described by a simplistic additive effect and involved more subtle synergistic pharmacological interactions. The combined administration of A2A/NR2B-receptor antagonists improved motor behaviour in 6-OHDA rats. Given the proven translatability of this model such a combination may be expected to be effective in improving motor symptoms in patients.

摘要

在帕金森病中,长期使用多巴胺替代药物与运动并发症的发生有关;因此,需要非多巴胺能药物。本研究评估了六种不同的NR2B和A2A受体拮抗剂单独或联合使用对单侧6-OHDA损伤大鼠的潜在治疗作用,这些大鼠未联合使用左旋多巴(单药治疗)或联合使用左旋多巴(附加治疗):SCH-58261+默克22;SCH-58261+Co-101244;普雷拉登特+默克22;普雷拉登特+拉地普地尔;托扎登特+拉地普地尔;异他林+Co-101244。接受单药治疗的动物通过行进距离和竖毛行为进行评估,而接受附加治疗的动物通过对侧旋转进行评估。进行三因素混合方差分析以分别评估每种药物的主要作用,并确定两种药物之间的任何相互作用是相加还是协同作用。进行了额外的事后分析以比较联合用药与单药的效果。与以相同剂量单独给药相比,联合给药时运动活性显著改善且持续时间更长。同样,当作为左旋多巴的附加治疗进行测试时,联合用药导致的对侧旋转水平高于单一药物。特别值得注意的是,一些联合用药观察到的活性不能用简单的相加效应来描述,而是涉及更微妙的协同药理相互作用。A2A/NR2B受体拮抗剂联合给药改善了6-OHDA大鼠的运动行为。鉴于该模型已被证实具有可转化性,预计这种联合用药在改善患者运动症状方面可能有效。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/15de/4267740/aa52391036a3/pone.0114086.g002.jpg

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