Grundman Michael, Morgan Roger, Lickliter Jason D, Schneider Lon S, DeKosky Steven, Izzo Nicholas J, Guttendorf Robert, Higgin Michelle, Pribyl Julie, Mozzoni Kelsie, Safferstein Hank, Catalano Susan M
Global R&D Partners, San Diego, CA, USA.
University of California San Diego, San Diego, CA, USA.
Alzheimers Dement (N Y). 2019 Jan 23;5:20-26. doi: 10.1016/j.trci.2018.11.001. eCollection 2019.
Elayta (CT1812) is a novel allosteric antagonist of the sigma-2 receptor complex that prevents and displaces binding of Aβ oligomers to neurons. By stopping a key initiating event in Alzheimer's disease, this first-in-class drug candidate mitigates downstream synaptotoxicity and restores cognitive function in aged transgenic mouse models of Alzheimer's disease.
A phase 1, two-part single and multiple ascending dose study was conducted in 7 and 4 cohorts of healthy human subjects, respectively. In part A, healthy, young subjects (<65 years old) received CT1812 doses ranging from 10 to 1120 mg (6:2 active to placebo [A:P] per cohort). In part B, subjects were administered 280, 560, and 840 mg once daily for 14 days (8:2 A:P per cohort). An elderly cohort, aged 65-75 years, was dosed at 560 mg once daily for 14 days (7:2 A:P). Serum concentrations of CT1812 in part B were measured on day 3 and 14 and cerebrospinal fluid concentrations on day 7 or 9. Cognitive testing was performed in the healthy elderly cohort at baseline and at day 14 of treatment.
Treatment with CT1812 was well tolerated in all cohorts. Adverse events were mild to moderate in severity and included headache and GI tract symptoms. Plasma concentrations of drug were dose proportional across two orders of magnitude with minimal accumulation over 14 days. Cognitive scores in the healthy elderly cohort were similar before and after treatment.
CT1812 was well tolerated with single dose administration up to 1120 mg and with multiple dose administration up to 840 mg and 560 mg in healthy young and healthy elderly subjects, respectively. CT1812 is currently being studied in early phase 2 trials in patients with Alzheimer's disease.
伊莱塔(CT1812)是一种新型的σ-2受体复合物变构拮抗剂,可阻止并取代Aβ寡聚体与神经元的结合。通过阻止阿尔茨海默病中的一个关键起始事件,这种同类首创的候选药物可减轻下游突触毒性,并在老年阿尔茨海默病转基因小鼠模型中恢复认知功能。
分别在7组和4组健康人类受试者中进行了一项1期、两部分的单剂量和多剂量递增研究。在A部分,健康的年轻受试者(<65岁)接受了10至1120毫克的CT1812剂量(每组活性药物与安慰剂比例为6:2)。在B部分,受试者每天服用一次280、560和840毫克,持续14天(每组活性药物与安慰剂比例为8:2)。一个65至75岁的老年组每天服用560毫克,持续14天(活性药物与安慰剂比例为7:2)。在第3天和第14天测量B部分中CT1812的血清浓度,在第7天或第9天测量脑脊液浓度。在健康老年组的基线和治疗第14天进行认知测试。
所有组中CT1812治疗的耐受性良好。不良事件的严重程度为轻度至中度,包括头痛和胃肠道症状。药物的血浆浓度在两个数量级上与剂量成正比,在14天内积累极少。健康老年组治疗前后的认知评分相似。
在健康年轻受试者中,CT1812单剂量给药高达1120毫克,在健康老年受试者中多剂量给药高达840毫克和560毫克时耐受性良好。CT1812目前正在阿尔茨海默病患者中进行2期早期试验研究。
