收稿日期: 2022-07-03
录用日期: 2022-11-18
网络出版日期: 2022-12-28
基金资助
国家自然科学基金(82071097);上海市浦江人才计划(2020PJD026)
Effect of transient receptor potential vanilloid 4 on traumatic heterotopic ossification around temporomandibular joint
Received date: 2022-07-03
Accepted date: 2022-11-18
Online published: 2022-12-28
Supported by
National Natural Science Foundation of China(82071097);Shanghai Pujiang Program(2020PJD026)
目的·探索瞬时受体电位香草素受体4型通道蛋白(transient receptor potential vanilloid 4,TRPV4)在创伤性颞下颌关节异位骨化(traumatic heterotopic ossification around temporomandibular joint,THO-TMJ)发生中的作用。方法·将18只8周龄雄性小鼠按单纯随机抽样方法分成2组,均行一侧髁突的一半髁突软骨切除术,建立THO-TMJ小鼠模型。实验组9只小鼠术后以灌胃方式给予TRPV4阻断剂[14 mg/(kg·d)],对照组9只小鼠给予等量生理盐水。选取术后14、30和90 d三阶段头颅样本,利用苏木精-伊红(H-E)染色、Micro CT扫描检查颞下颌关节区异位骨化的形成情况,对影像学资料进行三维重建,获取髁突的体积和表面积数据,计算异位形成的骨组织形态学指数(morphometric index,MI),并比较2组的异位骨化情况。结果·组织学染色结果显示,2组小鼠受损的髁突周围均发生活跃的软骨内成骨导致的异位骨化。Micro CT影像显示,实验组和对照组术后的TMJ区域先表现为髁突周围的组织密度逐渐升高,随后异位骨组织逐渐向髁突外增生,部分连接于关节窝,关节间隙内可见散在的骨性赘生物,但该TMJ骨性融合趋势在对照组中较明显。实验组的 MI(0.15±0.01)显著小于对照组(0.18±0.03),差异有统计学意义(P<0.05)。结论·阻断TRPV4功能有助于延缓THO-TMJ的形成和发展。
朱悦 , 顾佳颖 , 代杰文 . 瞬时受体电位香草素受体4型通道蛋白在创伤性颞下颌关节异位骨化发生中的作用[J]. 上海交通大学学报(医学版), 2022 , 42(12) : 1649 -1655 . DOI: 10.3969/j.issn.1674-8115.2022.12.001
Objective ·To investigate the effect of transient receptor potential vanilloid 4 (TRPV4) on traumatic heterotopic ossification around temporomandibular joint (THO-TMJ). Methods ·Eighteen eight-week-old male mice were divided into two groups by simple random sampling. Half right condylar cartilage was removed in every mouse. Nine mice in experimental group was administered TRPV4 blocker [14 mg/(kg·d)] via oral gavage. The same amount of saline was given to nine mice in control group. The skull samples were collected at 14, 30 and 90 d after surgery. The heterotopic ossification was evaluated by H-E staining and Micro CT scan. Three-dimensional reconstruction of the skulls was performed to measure the volume and surface area of condyles. Morphometric index (MI) was applied to indicate the degree of heterotopic ossification in both groups. Results ·H-E staining results showed that active endochondral ossification occurred around the injured condyles in both groups. Micro CT images showed that the tissue density around the condyles in both groups gradually increased in the TMJ area after operation, and then the ectopic bone tissues gradually proliferated outside the condyle, partially connecting to the joint fossa. Scattered osteophytes were seen in the joint space. The trend of TMJ bone fusion was more obvious in the control group. The morphological index of the experimental group (MI=0.15±0.01) was lower than that of the control group (MI=0.18±0.03, P<0.05). Conclusion ·Blocking TRPV4 function can help reduce the formation and progression of THO-TMJ.
| 1 | YAN Y B, LIANG S X, SHEN J, et al. Current concepts in the pathogenesis of traumatic temporomandibular joint ankylosis[J]. Head Face Med, 2014, 10: 35. |
| 2 | RANGANATHAN K, LODER S, AGARWAL S, et al. Heterotopic ossification: basic-science principles and clinical correlates [J]. J Bone Joint Surg Am, 2015, 97(13): 1101-1111. |
| 3 | BEDI A, ZBEDA R M, BUENO V F, et al. The incidence of heterotopic ossification after hip arthroscopy [J]. Am J Sports Med, 2012, 40(4): 854-863. |
| 4 | ZHENG L, HWANG J M, HWANG D S, et al. Incidence and location of heterotopic ossification following hip arthroscopy[J]. BMC Musculoskelet Disord, 2020, 21(1): 132. |
| 5 | REICHEL L M, SALISBURY E, MOUSTOUKAS M J, et al. Molecular mechanisms of heterotopic ossification[J]. J Hand Surg Am, 2014, 39(3): 563-566. |
| 6 | EVERAERTS W, NILIUS B, OWSIANIK G. The vanilloid transient receptor potential channel TRPV4: from structure to disease[J]. Prog Biophys Mol Biol, 2010, 103(1): 2-17. |
| 7 | PHAN M N, LEDDY H A, VOTTA B J, et al. Functional characterization of TRPV4 as an osmotically sensitive ion channel in porcine articular chondrocytes[J]. Arthritis Rheum, 2009, 60(10): 3028-3037. |
| 8 | ZHAO Y, OUYANG N, CHEN L, et al. Stimulating factors and origins of precursor cells in traumatic heterotopic ossification around the temporomandibular joint in mice[J]. Front Cell Dev Biol, 2020, 8: 445. |
| 9 | SACCUCCI M, D'ATTILIO M, RODOLFINO D, et al. Condylar volume and condylar area in class I, class II and class III young adult subjects[J]. Head Face Med, 2012, 8: 34. |
| 10 | CHALMERS J, GRAY D H, RUSH J. Observations on the induction of bone in soft tissues[J]. J Bone Joint Surg Br, 1975, 57(1): 36-45. |
| 11 | AGARWAL S, LODER S J, CHOLOK D, et al. Scleraxis-lineage cells contribute to ectopic bone formation in muscle and tendon[J]. Stem Cells, 2016, 35(3): 705-710. |
| 12 | DAI J, OUYANG N, ZHU X, et al. Injured condylar cartilage leads to traumatic temporomandibular joint ankylosis [J]. J Craniomaxillofac Surg, 2016, 44(3): 294-300. |
| 13 | HUANG Y, WANG X, LIN H. The hypoxic microenvironment: a driving force for heterotopic ossification progression [J]. Cell Commun Signal, 2020, 18(1): 20. |
| 14 | YAN Y B, LI J M, XIAO E, et al. A pilot trial on the molecular pathophysiology of traumatic temporomandibular joint bony ankylosis in a sheep model. Part Ⅱ: the differential gene expression among fibrous ankylosis, bony ankylosis and condylar fracture [J]. J Craniomaxillofac Surg, 2014, 42(2): e23-28. |
| 15 | O'CONOR C J, LEDDY H A, BENEFIELD H C, et al. TRPV4-mediated mechanotransduction regulates the metabolic response of chondrocytes to dynamic loading[J]. PNAS, 2014, 111(4): 1316-1321. |
| 16 | KUPCSIK L, STODDART M J, LI Z, et al. Improving chondrogenesis: potential and limitations of SOX9 gene transfer and mechanical stimulation for cartilage tissue engineering[J]. Tissue Eng Part A, 2010, 16(6): 1845-1855. |
| 17 | 汪淑华,徐高丽,吴枝武,等. 兔盘前移颞下颌关节的髁突软骨细胞中SOX9和MMP12的表达[J]. 口腔颌面外科杂志, 2015(6): 407-411. |
| 17 | WANG S H, XU G L, WU Z W, et al. Expression of Sox9 and MMP12 in the condylar chondrocyte in a rabbit model of temporomandibular joint internal derangement [J]. J Oral Maxil Surg, 2015(6): 407-411. |
| 18 | ROSENBERG N M, BULL A M J. Application of a mechanobiological algorithm to investigate mechanical mediation of heterotopic bone in trans-femoral amputees[J]. Sci Rep, 2018, 8(1): 14196. |
| 19 | SHANNON A H, ELDER C T, LU G, et al. Pharmacologic inhibition of transient receptor channel vanilloid 4 attenuates abdominal aortic aneurysm formation[J]. FASEB J, 2020, 34(7): 9787-9801. |
| 20 | YIN J, MICHALICK L, TANG C, et al. Role of transient receptor potential vanilloid 4 in neutrophil activation and acute lung injury[J]. Am J Respir Cell Mol Biol, 2016, 54(3): 370-383. |
| 21 | THORNELOE K S, CHEUNG M, BAO W, et al. An orally active TRPV4 channel blocker prevents and resolves pulmonary edema induced by heart failure[J]. Sci Transl Med, 2012, 4(159): 159ra148. |
| 22 | KANG S S, SHIN S H, AUH C K, et al. Human skeletal dysplasia caused by a constitutive activated transient receptor potential vanilloid 4 (TRPV4) cation channel mutation[J]. Exp Mol Med, 2012, 44(12): 707-722. |
| 23 | LAMANDé S R, YUAN Y, GRESSHOFF I L, et al. Mutations in TRPV4 cause an inherited arthropathy of hands and feet[J]. Nat Genet, 2011, 43(11): 1142-1146. |
| 24 | CLARK A L, VOTTA B J, KUMAR S, et al. Chondroprotective role of the osmotically sensitive ion channel transient receptor potential vanilloid 4: age- and sex-dependent progression of osteoarthritis in Trpv4-deficient mice[J]. Arthritis Rheum, 2010, 62(10): 2973-2983. |
| 25 | O'CONOR C J, RAMALINGAM S, ZELENSKI N A, et al. Cartilage-specific knockout of the mechanosensory ion channel TRPV4 decreases age-related osteoarthritis[J]. Sci Rep, 2016, 6: 29053. |
| 26 | 杜根来. 力学微环境对膝关节软骨细胞力敏感离子通道的影响[D]. 太原:太原理工大学, 2018. |
| 26 | DU G L. Effects of mechanical microenvironment on Mechano-sensitive ion channels of knee chondrocytes [D]. Taiyuan:Taiyuan University of Technology, 2018. |
| 27 | LEE W, LEDDY H A, CHEN Y, et al. Synergy between Piezo1 and Piezo2 channels confers high-strain mechanosensitivity to articular cartilage[J]. PNAS, 2014, 111(47): E5114-E5122. |
| 28 | 危振元, 仲飙. 创伤性异位骨化发病机制及治疗的研究进展[J]. 国际骨科学杂志, 2020, 41(2): 82-86. |
| 28 | WEI Z Y, ZHONG B. Research progress on pathogenesis and treatment of traumatic heterotopic ossification [J]. Int J Orthop, 2020, 41(2): 82-86. |
| 29 | YEUNG M, JAMSHIDI S, HORNER N, et al. Efficacy of nonsteroidal anti-inflammatory drug prophylaxis for heterotrophic ossification in hip arthroscopy: a systematic review[J]. Arthroscopy, 2016, 32(3): 519-525. |
| 30 | SHEHAB D, ELGAZZAR A H, COLLIER B D. Heterotopic ossification[J]. J Nucl Med, 2002, 43(3): 346-353. |
| 31 | 张玉辉, 吕银娟. 选择性COX-2抑制剂与非甾体抗炎药在预防肘部骨折术后异位骨化的效果比较[J].川北医学院学报, 2019, 34(6): 776-778,824. |
| 31 | ZHANG Y H, Lü Y J. Comparison of the effects of selective COX-2 inhibitors and non-steroidal anti-inflammatory drugs on prevention of heterotopic ossification after el-bow fracture [J]. J North Sichuan Med Coll, 2019, 34(6): 776-778,824. |
| 32 | 居家宝, 寇玉辉, 张殿英, 等. 肘关节异位骨化发病因素及诊治进展[J]. 中华肩肘外科电子杂志, 2019, 7(2): 174-177. |
| 32 | JU J B, KOU Y H, ZHANG D Y, et al. Pathogenesis factors, diagnosis and treatment progress of heterotopic ossification of elbow joint [J]. Chin J Shoulder Elbow, 2019, 7(2): 174-177. |
| 33 | 张弛, 纪方. SMAD7调控内皮间质转化可预防跟腱损伤后的异位骨化[J]. 中国组织工程研究, 2017, 21(8): 1178-1185. |
| 33 | ZHANG C, JI F. SMAD7 prevents heterotopic ossification by regulating endothelial-mesenchymal transition after Achilles tendon injury [J]. J Clin Rehabil Tis Eng Res, 2017, 21(8): 1178-1185. |
| 34 | LIN L, CHEN L, WANG H, et al. Adenovirus-mediated transfer of siRNA against Runx2/Cbfa1 inhibits the formation of heterotopic ossification in animal model[J]. Biochem Biophys Res Commun, 2006, 349(2): 564-572. |
| 35 | 丁纳, 卢海妹, 刘亚坤, 等. 异位骨化的预防与治疗[J]. 基础医学与临床, 2018, 38(8): 1153-1157. |
| 35 | DING N, LU H M, LIU Y K. Prevention and treatment of heterotopic ossification [J]. Basic Clin Med, 2018, 38(8): 1153-1157. |
/
| 〈 |
|
〉 |