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首页> 外文期刊>Regulatory Toxicology and Pharmacology: RTP >Implications of retinal effects observed in chronic toxicity studies on the clinical development of a CNS-active drug candidate
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Implications of retinal effects observed in chronic toxicity studies on the clinical development of a CNS-active drug candidate

机译:慢性毒性研究中观察到的视网膜效应对中枢神经系统活性药物候选物临床发展的影响

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The development path described for JNJ-26489112 provides perspectives on interpretation of retinal effects observed in nonclinical studies and their implications for clinical development. JNJ-26489112 is a CNS-active investigational drug that has potential as a novel treatment for treatment-resistant and bipolar depression, epilepsy, and neuropathic/inflammatory pain. In a 6-month toxicity study in albino rats, retinal atrophy was observed at supratherapeutic exposures to JNJ-26489112. The histopathological changes and topography of the lesions were characteristic of light-induced damage specific to albino rats. The species/strain specificity is supported by an absence of any ocular effects in dogs and in pigmented and albino rats, housed under standard and reduced lighting, respectively. To further evaluate its potential to cause ocular effects, in vivo functional and structural ocular analyses were included in a 9-month monkey toxicity study. Reductions in rod- and cone-mediated electroretinograms were observed at supratherapeutic exposures but without any histopathologic changes. These data suggested that the effects of JNJ-26489112 in monkeys were neuromodulatory and not neurotoxic. Taken together, data related to the light-induced atrophy in albino rats and reversible neuromodulatory effects in monkeys, supported the safe evaluation of JNJ-26489112 in a clinical proof-of-concept study that included comprehensive functional and structural ocular monitoring.
机译:针对JNJ-26489112所述的开发路径为非临床研究中观察到的视网膜效应及其对临床发展的意义提供了解释。 JNJ-26489112是一种具有CNS活性的研究药物,具有潜在的治疗耐药性和躁郁症,癫痫病和神经性/炎性疼痛的新疗法的潜力。在一项针对白化病大鼠的为期6个月的毒性研究中,超治疗暴露于JNJ-26489112时观察到了视网膜萎缩。病变的组织病理学变化和形貌是白化大鼠特有的光诱导损伤的特征。分别在标准和减少光照下饲养的狗和有色和白化病大鼠中没有任何眼睛作用,从而支持了物种/菌株特异性。为了进一步评估其引起眼部影响的潜力,在9个月的猴子毒性研究中进行了体内功能和结构性眼部分析。在治疗上暴露时观察到杆和锥介导的视网膜电图减少,但没有任何组织病理学改变。这些数据表明,JNJ-26489112对猴子的作用具有神经调节作用,而没有神经毒性。综上所述,与白化病大鼠中的光致萎缩和猴子中可逆的神经调节作用有关的数据,在临床概念验证研究中支持对JNJ-26489112的安全评估,该研究包括全面的功能和结构眼部监测。

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