软骨边界润滑协同作用由透明质酸浓度、润滑蛋白4浓度和结构介导。
Cartilage boundary lubrication synergism is mediated by hyaluronan concentration and PRG4 concentration and structure.
作者信息
Ludwig Taryn E, Hunter Miles M, Schmidt Tannin A
机构信息
Biomedical Engineering Graduate Program, University of Calgary, Calgary, Canada.
Faculty of Kinesiology, University of Calgary, Calgary, Canada.
出版信息
BMC Musculoskelet Disord. 2015 Dec 14;16:386. doi: 10.1186/s12891-015-0842-5.
BACKGROUND
Proteoglycan 4 (PRG4) and hyaluronan (HA) are key synovial fluid constituents that contribute synergistically to cartilage boundary lubrication; however, the effects of their concentrations as well as their structure, both of which can be altered in osteoarthritis, on this functional synergism are unknown. The objectives of this study were to evaluate cartilage boundary lubricating ability of 1) PRG4 + HA in solution at constant HA concentration in a range of PRG4 concentrations, 2) constant PRG4 concentration in a range of HA concentrations, 3) HA + reduced/alkylated (R/A) PRG4, and 4) hylan G-F 20 + PRG4.
METHODS
Static and kinetic friction coefficients (μ(static,Neq), <μ(kinetic,Neq)>) were measured using a previously characterized cartilage-cartilage boundary mode friction test for the following concentrations of purified PRG4 and HA: Test 1: HA (1.5 MDa, 3.3 mg/mL) + PRG4 from 4.5 - 1500 μg/mL; Test 2: PRG4 (450, 150, 45 μg/mL) + HA (1.5 MDa) from 0.3 - 3.3 mg/mL. Test 3: hylan G-F 20 (3. 3 mg/mL) + PRG4 (450 μg/mL). Test 4: HA (3.3 mg/mL) + R/A PRG4 (450 μg/mL). ANOVA was used to compare lubricants within (comparing 6 lubricants of interest) and between (comparing 3 lubricants of interest) test sequences, with Tukey and Fishers post-hoc testing respectively.
RESULTS
This study demonstrates that both PRG4 and HA concentration, as well as PRG4 disulfide-bonded structure, can alter the cartilage boundary lubricating ability of PRG4 + HA solutions. The boundary lubricating ability of high MW HA + PRG4 solutions was limited by very low concentrations of PRG4. Decreased concentrations of high MW HA also limited the cartilage boundary lubricating ability of HA + PRG4 solutions, with the effect exacerbated by low PRG4 concentrations. The reduction of friction by addition of PRG4 to a cross-linked HA viscosupplement product, but not with addition of R/A PRG4 to HA, is consistent with a non-covalent mechanism of interaction where tertiary and quaternary PRG4 structure are important.
CONCLUSIONS
Collectively, these results demonstrate that deficiency of either or both PRG4 and HA, or alterations in PRG4 structure, may be detrimental to SF cartilage boundary lubricating function. This study provides further insight into the nature of cartilage boundary lubrication and advancement towards potential formulation of new intra-articular biotherapeutic treatments for osteoarthritis using PRG4 ± HA.
背景
蛋白聚糖4(PRG4)和透明质酸(HA)是滑液的关键成分,它们协同作用于软骨边界润滑;然而,它们的浓度以及结构(二者在骨关节炎中均可改变)对这种功能协同作用的影响尚不清楚。本研究的目的是评估以下几种情况的软骨边界润滑能力:1)在一系列PRG4浓度下,HA浓度恒定的溶液中的PRG4 + HA;2)在一系列HA浓度下,PRG4浓度恒定的情况;3)HA + 还原/烷基化(R/A)PRG4;4)hylan G-F 20 + PRG4。
方法
使用先前已表征的软骨 - 软骨边界模式摩擦试验,测量以下纯化的PRG4和HA浓度下的静摩擦系数和动摩擦系数(μ(static,Neq),<μ(kinetic,Neq)>):试验1:HA(1.5 MDa,3.3 mg/mL)+ 4.5 - 1500 μg/mL的PRG4;试验2:0.3 - 3.3 mg/mL的HA(1.5 MDa)+ 450、150、45 μg/mL的PRG4。试验3:hylan G-F 20(3.3 mg/mL)+ PRG4(450 μg/mL)。试验4:HA(3.3 mg/mL)+ R/A PRG4(450 μg/mL)。方差分析用于比较试验序列内(比较6种感兴趣的润滑剂)和试验序列间(比较3种感兴趣的润滑剂)的润滑剂,分别采用Tukey和Fisher事后检验。
结果
本研究表明,PRG4和HA的浓度以及PRG4的二硫键结构均可改变PRG4 + HA溶液的软骨边界润滑能力。高分子量HA + PRG4溶液的边界润滑能力受到PRG4极低浓度的限制。高分子量HA浓度的降低也限制了HA + PRG4溶液的软骨边界润滑能力,低PRG4浓度会加剧这种影响。向交联HA粘弹性补充剂产品中添加PRG4可降低摩擦,但向HA中添加R/A PRG4则不然,这与一种非共价相互作用机制一致,其中PRG4的三级和四级结构很重要。
结论
总体而言,这些结果表明PRG4和HA其中之一或两者缺乏,或PRG4结构改变,可能对滑液软骨边界润滑功能有害。本研究进一步深入了解了软骨边界润滑的本质,并朝着使用PRG4 ± HA开发治疗骨关节炎的新型关节内生物治疗制剂的潜在方向迈进。
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