Beydoun Talal, Deloche Catherine, Perino Julien, Kirwan Bridget-Anne, Combette Jean-Marc, Behar-Cohen Francine
1 Department of Ophthalmology, AP-HP Hôtel-Dieu, Paris, France .
J Ocul Pharmacol Ther. 2015 Mar;31(2):93-9. doi: 10.1089/jop.2013.0247. Epub 2014 Oct 27.
We aimed to investigate the safety, tolerability, and systemic diffusion of a single escalating dose of XG-102 (a 31-D-amino-acid peptide inhibiting JNK pathway activation), administered subconjunctivally in the treatment of post-surgery or post-trauma intraocular inflammation.
This is a dose-escalating, tolerance Phase Ib study. Twenty patients with post-surgery or post-traumatic intraocular inflammation were assigned to 1 of the 4 dose escalating (45, 90, 450, or 900 μg XG-102) groups of 5 patients each. Patients were evaluated at 24, 48 h, 8, and 28 days following the administration of XG-102, including laboratory tests, standard eye examinations, vital signs, and occurrence of adverse events. A single plasma quantification of XG-102 was performed 30 min after administration, according to previous pharmacokinetics studies performed on volunteers.
A total of 17 non-serious adverse events, considered unrelated to the study treatment, were reported for 10 patients. The adverse event incidence was not related to the drug dose. All patients experienced a decrease in intraocular inflammation as of 24 h post-administration and this decrease was sustained up to 28 days thereafter. No patient required local injection or systemic administration of corticoids following the administration of XG-102. XG-102 was undetectable in the first 3 dose groups. In the fourth-dose group (900 μg) the XG-102 plasma levels were above the limit of detection for 3 patients and above the limit of quantification for 1 patient.
In this first clinical trial using XG-102, administered as a single subconjunctival injection as adjunct therapy, in patients with recent post-surgery or post-trauma intraocular inflammation is safe and well tolerated. Further studies are required to evaluate its efficacy.
我们旨在研究单次递增剂量的XG-102(一种抑制JNK通路激活的31个氨基酸的D型肽)结膜下给药治疗手术后或创伤后眼内炎症的安全性、耐受性及全身扩散情况。
这是一项剂量递增的耐受性Ib期研究。20例手术后或创伤后眼内炎症患者被分为4个剂量递增组(每组5例),分别给予45、90、450或900μg XG-102。在给予XG-102后的24、48小时、8天和28天对患者进行评估,包括实验室检查、标准眼科检查、生命体征及不良事件的发生情况。根据之前对志愿者进行的药代动力学研究,在给药30分钟后对XG-102进行单次血浆定量。
共报告了10例患者的17起非严重不良事件,认为与研究治疗无关。不良事件发生率与药物剂量无关。所有患者在给药后24小时眼内炎症均减轻,且此后持续减轻至28天。给予XG-102后,没有患者需要局部注射或全身使用皮质类固醇。在前3个剂量组中未检测到XG-102。在第四剂量组(900μg)中,3例患者的XG-102血浆水平高于检测限,1例患者高于定量限。
在这项首次使用XG-102的临床试验中,作为单次结膜下注射作为辅助治疗,对于近期手术后或创伤后眼内炎症患者是安全且耐受性良好的。需要进一步研究来评估其疗效。
