左旋多巴/卡比多巴持续皮下输注的药代动力学:来自ND0612临床开发项目的研究结果。
The pharmacokinetics of continuous subcutaneous levodopa/carbidopa infusion: Findings from the ND0612 clinical development program.
作者信息
LeWitt Peter A, Stocchi Fabrizio, Arkadir David, Caraco Yoseph, Adar Liat, Perlstein Itay, Case Ryan, Giladi Nir
机构信息
Department of Neurology, Wayne State University School of Medicine and Henry Ford Hospital, Detroit, MI, United States.
Department of Neurology, University and Institute for Research and Medical Care Istituto di Ricovero e Cura a Carattere Scientifico (IRCCS) San Raffaele, Rome, Italy.
出版信息
Front Neurol. 2022 Nov 10;13:1036068. doi: 10.3389/fneur.2022.1036068. eCollection 2022.
BACKGROUND
While treatment with levodopa remains the cornerstone of Parkinson's disease (PD) management, chronic oral therapy is often associated with the development of motor complications, that correlate to fluctuating levodopa plasma concentrations, limiting its clinical utility. Continuous infusion is considered to be the optimal delivery route for treating PD patients with motor fluctuations, but current infusion systems require invasive surgery. Subcutaneous infusion of (SC) levodopa has the potential to provide a better tolerated and more convenient route of continuous levodopa delivery. ND0612 is in development as a combination product providing continuous levodopa/carbidopa a minimally invasive, subcutaneous delivery system for PD patients experiencing motor response fluctuations. We present pharmacokinetic results from a series of studies that analyzed plasma concentrations after SC levodopa delivery with ND0612 to inform the clinical development program.
METHODS
We performed a series of six Phase I and II studies to characterize the pharmacokinetics of levodopa and carbidopa derived from ND0612 infusion with/without adjunct oral therapy of the same ingredients. These studies were conducted in healthy volunteers and in PD patients experiencing motor response fluctuations while on their current levodopa therapy regimen.
RESULTS
Taken together, the results demonstrate dose-proportionality dependent on rate of subcutaneous levodopa infusion leading to stable and sustained plasma concentrations of levodopa. Subcutaneous infusion of ND0612 administered with oral levodopa/carbidopa maintained near-constant, therapeutic levodopa plasma concentrations, thereby avoiding the troughs in levodopa plasma concentrations that are associated with OFF time in PD. The data generated in this series of studies also confirmed that a levodopa/carbidopa dose ratio of 8:1 would be the most reasonable choice for ND0612 development.
CONCLUSIONS
This series of clinical pharmacokinetic studies have demonstrated that ND0612, administered continuously with a levodopa concentration of 60 mg/ml combined with carbidopa 7.5 mg/ml, and complemented with oral levodopa/carbidopa, is suitable for 24 h continuous administration in patients with PD. The stable plasma concentrations of levodopa achieved predict utility of ND0612 as a parenteral formulation for achieving clinically useful delivery of levodopa for PD patients.
背景
虽然左旋多巴治疗仍是帕金森病(PD)管理的基石,但长期口服治疗常与运动并发症的发生相关,这些并发症与左旋多巴血浆浓度波动有关,限制了其临床应用。持续输注被认为是治疗有运动波动的PD患者的最佳给药途径,但目前的输注系统需要进行侵入性手术。皮下注射(SC)左旋多巴有可能提供一种耐受性更好、更方便的持续左旋多巴给药途径。ND0612正在开发中,作为一种组合产品,为经历运动反应波动的PD患者提供持续的左旋多巴/卡比多巴,采用微创皮下给药系统。我们展示了一系列研究的药代动力学结果,这些研究分析了使用ND0612进行皮下注射左旋多巴后的血浆浓度,以为临床开发项目提供信息。
方法
我们进行了一系列六项I期和II期研究,以表征来自ND0612输注的左旋多巴和卡比多巴的药代动力学,同时使用或不使用相同成分的辅助口服治疗。这些研究在健康志愿者和正在接受当前左旋多巴治疗方案且经历运动反应波动的PD患者中进行。
结果
总体而言,结果表明剂量比例取决于皮下左旋多巴输注速率,从而导致左旋多巴血浆浓度稳定且持续。与口服左旋多巴/卡比多巴联合给药时,皮下注射ND0612可维持近乎恒定的治疗性左旋多巴血浆浓度,从而避免了与PD患者“关”期相关的左旋多巴血浆浓度低谷。这一系列研究产生的数据还证实,左旋多巴/卡比多巴剂量比为8:1将是ND0612开发的最合理选择。
结论
这一系列临床药代动力学研究表明,ND0612以60mg/ml的左旋多巴浓度与7.5mg/ml的卡比多巴持续联合给药,并辅以口服左旋多巴/卡比多巴,适用于PD患者的24小时持续给药。所实现的左旋多巴稳定血浆浓度预示着ND0612作为一种肠胃外制剂可有效为PD患者实现临床上有用的左旋多巴给药。
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