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双室药代动力学模型描述了 rhprg4 在 Yucatan 小型猪 ACL 切断后在关节内的输送和保留。

Two compartment pharmacokinetic model describes the intra-articular delivery and retention of rhprg4 following ACL transection in the Yucatan mini pig.

机构信息

Ontario Veterinary College, University of Guelph, Guelph, Ontario, Canada.

Department of Pharmaceutical Sciences, Massachusetts College of Pharmacy and Health Sciences, Boston, Massachusetts.

出版信息

J Orthop Res. 2019 Feb;37(2):386-396. doi: 10.1002/jor.24191. Epub 2018 Dec 17.

Abstract

Treatment of the injured joint with rhPRG4 is based on recent observations that inflammation diminishes expression of native PRG4. Re-establishing lubrication between pressurized and sliding cartilage surfaces during locomotion promotes the nascent expression of PRG4 and thus intra-articular (IA) treatment strategies should be supported by pharmacokinetic evidence establishing the residence time of rhPRG4. A total of 21 Yucatan minipigs weighing ∼55 kg each received 4 mg of I-rhPRG4 delivered by IA injection 5 days following surgical ACL transection. Animals were sequentially euthanized following IA rhPRG4 at 10 min (time zero), 24, 72 h, 6, 13 and 20 days later. The decay of the I-rhPRG4 was measured relative to a non-injected aliquot and normalized to the weight of cartilage samples, menisci and synovium, and known cartilage volumes from each compartment surface obtained from representative Yucatan minipig knees. Decay of I-rhPRG4 from joint tissues best fit a two-compartment model with an α half-life (t ) of 11.28 h and β half-life (t ) of 4.81 days. The tibial and femoral cartilage, meniscii, and synovium retained 7.7% of dose at 24 h. High concentrations of rhPRG4 were found in synovial fluid (SF) that was non-aspiratable and resided on the articular surfaces, removable by irrigation, at 10 min following I-rhPRG4 injection. Synovial fluid K21 exceeded K12 and SF t was 28 days indicating SF is the reservoir for rhPRG4 following IA injection. Clinical Significance: rhPRG4 following IA delivery in a traumatized joint populates articular surfaces for a considerable period and may promote the native expression of PRG4. © 2018 Orthopaedic Research Society. Published by Wiley Periodicals, Inc. J Orthop Res 37:386-396, 2019.

摘要

治疗受伤关节的 rhPRG4 基于最近的观察结果,即炎症会降低天然 PRG4 的表达。在运动过程中重新建立受压和滑动软骨表面之间的润滑作用会促进 PRG4 的新生表达,因此,关节内 (IA) 治疗策略应该得到药代动力学证据的支持,该证据可以确定 rhPRG4 的驻留时间。总共 21 只体重约 55kg 的 Yucatan 小型猪在手术 ACL 横断后 5 天通过 IA 注射接受了 4mg 的 I-rhPRG4。IA rhPRG4 后 10min(零时)、24、72h、6、13 和 20 天后,动物被依次安乐死。通过与非注射等分试样相比,测量 I-rhPRG4 的衰减,并将其归一化为软骨样本、半月板和滑膜的重量,以及从每个 Yucatan 小型猪膝关节的代表性关节表面获得的已知软骨体积。IA 关节组织中 I-rhPRG4 的衰减最符合具有 α 半衰期 (t1/2) 的两室模型) 为 11.28h,β 半衰期 (t1/2) 为 4.81 天。胫骨和股骨软骨、半月板和滑膜在 24h 时保留了 7.7%的剂量。高浓度的 rhPRG4 存在于不能抽吸的滑液 (SF) 中,并且在 IA-rhPRG4 注射后 10min 位于关节表面,可通过冲洗去除。滑膜液 K21 超过 K12,SF t 为 28 天,表明 SF 是 IA 注射后 rhPRG4 的储库。临床意义:IA 递送至受伤关节后,rhPRG4 会在关节表面大量存在,并可能促进 PRG4 的天然表达。版权所有 © 2018 矫形研究协会。由 Wiley Periodicals, Inc. 出版。J Orthop Res 37:386-396, 2019.

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