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A critical evaluation of behavioral rodent models of motor impairment used for screening of antiparkinsonian activity: The case of adenosine A2A receptor antagonists

机译:用于筛选抗帕金森病活性的运动障碍行为啮齿动物模型的关键评估:腺苷A2A受体拮抗剂的案例

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Animal models of motor dysfunction constitute the basis for the screening of new drugs with potential efficacy in diseases characterized by motor impairment, such as Parkinson's Disease (PD). Taking adenosine A2A receptor antagonists as an example of a new class of drugs for PD, the review will examine the most utilized rodent models of motor impairment and the results reported in the literature with this class of drugs. The results obtained so far in rodent models of PD suggested that A2A receptor antagonists might have symptomatic therapeutic efficacy in PD. They may ameliorate initiation of movement, gait and muscle rigidity, sensorimotor integration deficits, and tremor. Moreover, A2A receptor antagonists when administered with a low sub-threshold dose of L-DOPA potentiated its efficacy. However, the clinical trials so far performed have evaluated their efficacy in the "ON/OFF" of PD patients with motor complications, showing a limited efficacy of this class of drug. Therefore, on one hand, animal models of PD might have a limited validity; on the other hand, clinical trials should explore the efficacy of A2A receptor antagonists on a broader range of parkinsonian conditions.
机译:运动功能障碍的动物模型构成了筛选新药的基础,这些新药在以运动障碍为特征的疾病(如帕金森氏病(PD))中具有潜在功效。以腺苷A2A受体拮抗剂为一类新的PD药物为例,该综述将研究运动障碍最常用的啮齿动物模型,以及该类药物在文献中报道的结果。到目前为止,在PD的啮齿动物模型中获得的结果表明,A2A受体拮抗剂可能在PD中具有对症治疗功效。它们可以改善运动的开始,步态和肌肉的僵硬,感觉运动整合缺陷和震颤。此外,当与亚阈值以下剂量的L-DOPA一起给药时,A2A受体拮抗剂可增强其疗效。然而,迄今为止进行的临床试验已经评估了它们在具有运动并发症的PD患者的“开/关”中的功效,显示出这类药物的功效有限。因此,一方面,PD的动物模型可能具有有限的有效性。另一方面,临床试验应探讨A2A受体拮抗剂在更广泛的帕金森病中的疗效。

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