肥大细胞稳定剂富马酸酮替芬对创伤后关节挛缩的剂量反应效应:兔模型的体内研究
The Dose-Response Effect of the Mast Cell Stabilizer Ketotifen Fumarate on Posttraumatic Joint Contracture: An in Vivo Study in a Rabbit Model.
作者信息
Schneider Prism S, Johal Herman, Befus A Dean, Salo Paul T, Hart David A, Hildebrand Kevin A
机构信息
McCaig Institute for Bone and Joint Health, University of Calgary, Calgary, Alberta, Canada.
McMaster University, Hamilton, Ontario, Canada.
出版信息
JB JS Open Access. 2021 Mar 26;6(1). doi: 10.2106/JBJS.OA.20.00057. eCollection 2021 Jan-Mar.
UNLABELLED
Posttraumatic joint contracture is a debilitating complication following an acute fracture or intra-articular injury that can lead to loss of motion and an inability to complete activities of daily living. In prior studies using an established in vivo model, we found that ketotifen fumarate (KF), a mast cell stabilizer, was associated with a significant reduction in the severity of posttraumatic joint contracture. Our primary research question in the current study was to determine whether a dose-response relationship exists between KF and posttraumatic joint contracture reduction.
METHODS
A standardized operative method to create posttraumatic joint contracture in a knee was performed on skeletally mature New Zealand White rabbits. The animals were randomly assigned to 1 of 5 groups (n = 10 per group): a nonoperative control group, an operative control group, or 1 of 3 experimental KF groups (0.01 mg/kg [the KF 0.01 group], 0.1 mg/kg [KF 0.1], or 5.0 mg/kg [KF 5.0]). Flexion contractures were measured following 8 weeks of knee immobilization using a hydraulic material-testing machine. The posterior knee joint capsules were then harvested for quantification of myofibroblast and mast cell numbers with immunohistochemistry analysis.
RESULTS
Forty-five rabbits were used in the final analysis. Contracture severity was significantly reduced in the KF 0.1 group (p = 0.016) and the KF 5.0 group (p = 0.001) compared with the operative control group. When converted to a percent response, posttraumatic joint contracture reduction was 13%, 45%, and 63% for the KF 0.01, KF 0.1, and KF 5.0 groups, respectively. A half-maximal effective concentration (EC) for KF of 0.22 mg/kg was established. There was also a decrease in myofibroblasts, mast cells, and substance P-containing nerve fiber counts with increasing doses of KF.
CONCLUSIONS
Using a preclinical, rabbit in vivo model of posttraumatic joint contracture, increasing doses of KF were associated with decreasing biomechanical estimates of knee posttraumatic joint contracture as well as decreasing numbers of myofibroblasts, mast cells, and substance P-containing nerve fibers.
CLINICAL RELEVANCE
KF has been used safely in humans for more than 40 years and, to our knowledge, is the first and only agent ready to be potentially translated into an effective treatment for posttraumatic joint contracture.
未标注
创伤后关节挛缩是急性骨折或关节内损伤后一种使人衰弱的并发症,可导致活动丧失及无法完成日常生活活动。在先前使用已建立的体内模型的研究中,我们发现肥大细胞稳定剂富马酸酮替芬(KF)与创伤后关节挛缩严重程度的显著降低有关。我们在当前研究中的主要研究问题是确定KF与创伤后关节挛缩减轻之间是否存在剂量反应关系。
方法
对骨骼成熟的新西兰白兔采用标准化手术方法造成膝关节创伤后关节挛缩。将动物随机分为5组中的1组(每组n = 10):非手术对照组、手术对照组或3个实验性KF组之一(0.01 mg/kg [KF 0.01组]、0.1 mg/kg [KF 0.1]或5.0 mg/kg [KF 5.0])。在膝关节固定8周后,使用液压材料试验机测量屈曲挛缩。然后收获膝关节后关节囊,通过免疫组织化学分析对肌成纤维细胞和肥大细胞数量进行定量。
结果
最终分析使用了45只兔子。与手术对照组相比,KF 0.1组(p = 0.016)和KF 5.0组(p = 0.001)的挛缩严重程度显著降低。换算为百分比反应后,KF 0.01、KF 0.1和KF 5.0组的创伤后关节挛缩减轻分别为13%、45%和63%。确定KF的半数最大有效浓度(EC)为0.22 mg/kg。随着KF剂量增加,肌成纤维细胞、肥大细胞和含P物质神经纤维数量也减少。
结论
使用创伤后关节挛缩的临床前兔体内模型,增加KF剂量与膝关节创伤后关节挛缩的生物力学评估降低以及肌成纤维细胞、肥大细胞和含P物质神经纤维数量减少有关。
临床意义
KF已在人类中安全使用40多年,据我们所知,它是第一种也是唯一一种有望转化为创伤后关节挛缩有效治疗方法的药物。
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