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用于创伤后骨关节炎的关节内白细胞介素-1受体拮抗剂(IL1-ra)微球:体外生物学活性和体内疾病修饰作用

Intra-articular interleukin-1 receptor antagonist (IL1-ra) microspheres for posttraumatic osteoarthritis: in vitro biological activity and in vivo disease modifying effect.

作者信息

Elsaid Khaled A, Ubhe Anand, Shaman Ziyad, D'Souza Gerard

机构信息

Department of Pharmaceutical Sciences, School of Pharmacy-Boston, MCPHS University, Boston, MA, USA.

Biomedical and Pharmaceutical Sciences, Chapman University School of Pharmacy, 9401 Jeronimo Road, Irvine, CA, 92618, USA.

出版信息

J Exp Orthop. 2016 Dec;3(1):18. doi: 10.1186/s40634-016-0054-4. Epub 2016 Aug 19.

Abstract

BACKGROUND

Interleukin-1 receptor antagonist (IL-1 ra) can be disease-modifying in posttraumatic osteoarthritis (PTOA). One limitation is its short joint residence time. We hypothesized that IL-1 ra encapsulation in poly (lactide-co-glycolide) (PLGA) microspheres reduces IL-1 ra systemic absorption and provides an enhanced anti-PTOA effect.

METHODS

IL-1 ra release kinetics and biological activity: IL-1 ra encapsulation into PLGA microsphere was performed using double emulsion solvent extraction. Lyophilized PLGA IL-1 ra microspheres were resuspended in PBS and supernatant IL-1 ra concentrations were assayed. The biological activity of IL-1 ra from PLGA IL-1 ra microspheres was performed using IL-1 induced lymphocyte proliferation and bovine articular cartilage degradation assays. Systemic absorption of IL-1 ra following intra-articular (IA) injection of PLGA IL-1 ra or IL-1 ra: At 1, 3, 6, 12 and 24 h following injection of 50 μl PLGA IL-1 ra (n = 6) or IL-1 ra (n = 6), serum samples were collected and IL-1 ra concentrations were determined. Anterior cruciate ligament transection (ACLT) and IA dosing: ACLT was performed in 8-10 week old male Lewis rats (n = 42). PBS (50 μl; n = 9), IL-1 ra (50 μl; 5 mg/ml; n = 13), PLGA IL-1 ra (50 μl; equivalent to 5 mg/ml IL-1 ra; n = 14) or PLGA particles (50 μl; n = 6) treatments were performed on days 7, 14, 21 and 28 following ACLT. Cartilage and synovial histopathology: On day 35, animal ACLT joints were harvested and tibial cartilage and synovial histopathology scoring was performed.

RESULTS

Percent IL-1 ra content in the supernatant at 6 h was 13.44 ± 9.27 % compared to 34.16 ± 12.04 %, 47.89 ± 12.71 %, 57.14 ± 11.71 %, and 93.90 ± 8.50 % at 12, 24, 48 and 72 h, respectively. PLGA IL-1 ra inhibited lymphocyte proliferation and cartilage degradation similar to IL-1 ra. Serum IL-1 ra levels were significantly lower at 1, 3, and 6 h following PLGA IL-1 ra injection compared to IL-1 ra. Cartilage and synovial histopathology scores were significantly lower in the PLGA IL-1 ra group compared to PBS and PLGA groups (p < 0.001).

CONCLUSIONS

IL-1 ra encapsulation in PLGA microspheres is feasible with no alteration to IL-1 ra biological activity. PLGA IL-1 ra exhibited an enhanced disease-modifying effect in a PTOA model compared to similarly dosed IL-1 ra.

摘要

背景

白细胞介素-1受体拮抗剂(IL-1ra)可改善创伤后骨关节炎(PTOA)。其局限性之一是在关节内的停留时间短。我们推测,将IL-1ra包裹于聚(丙交酯-乙交酯)(PLGA)微球中可减少IL-1ra的全身吸收,并增强抗PTOA效应。

方法

IL-1ra释放动力学及生物活性:采用复乳溶剂萃取法将IL-1ra包裹于PLGA微球中。将冻干的PLGA IL-1ra微球重悬于PBS中,测定上清液中IL-1ra的浓度。采用IL-1诱导的淋巴细胞增殖和牛关节软骨降解试验检测PLGA IL-1ra微球中IL-1ra的生物活性。关节内(IA)注射PLGA IL-1ra或IL-1ra后IL-1ra的全身吸收:注射50μl PLGA IL-1ra(n = 6)或IL-1ra(n = 6)后1、3、6、12和24小时,采集血清样本并测定IL-1ra浓度。前交叉韧带切断术(ACLT)及IA给药:对8 - 10周龄雄性Lewis大鼠(n = 42)实施ACLT。在ACLT后第7、14、21和28天,分别给予PBS(50μl;n = 9)、IL-1ra(50μl;5mg/ml;n = 13)、PLGA IL-1ra(50μl;相当于5mg/ml IL-1ra;n = 14)或PLGA颗粒(50μl;n = 6)进行治疗。软骨及滑膜组织病理学检查:在第35天,采集动物ACLT关节,对胫骨软骨和滑膜进行组织病理学评分。

结果

6小时时上清液中IL-1ra含量百分比为13.44±9.27%,而在12、24、48和72小时时分别为34.16±12.04%、47.89±12.71%、57.14±11.71%和93.90±8.50%。PLGA IL-1ra抑制淋巴细胞增殖和软骨降解的作用与IL-1ra相似。与IL-1ra相比,PLGA IL-1ra注射后1、3和6小时血清IL-1ra水平显著降低。与PBS组和PLGA组相比,PLGA IL-1ra组的软骨和滑膜组织病理学评分显著降低(p < 0.001)。

结论

将IL-1ra包裹于PLGA微球中是可行的,且不改变IL-1ra的生物活性。与同等剂量的IL-1ra相比,PLGA IL-1ra在PTOA模型中表现出更强的疾病改善作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/10be/4990523/7f4452de9355/40634_2016_54_Fig1_HTML.jpg

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