The use of recombinant human bone morphogenetic protein-2 （rhBMP-2） in maxillofacial trauma

In recent years, recombinant human bone morphogenetic protein-2 （rhBMP-2） has been introduced as a therapeutic option in the treatment of several congenital and acquired craniofacial defects. Although there have been promising clinical results, the international literature still lacks complete guidelines, including limits and indications for the use of rhBMP-2. The possible indications for rhBMP-2 in patients undergoing facial trauma are discussed in this article.

Use of recombinant human bone morphogenetic protein-2 in spine surgery

Bone morphogenetic proteins are osteoinductive factors which have gained popularity in orthopaedicsurgery and especially in spine surgery. The use of recombinant human bone morphogenetic protein-2 has been officially approved by the United States Food and Drug Administration only for single level anterior lumbar interbody fusion, nevertheless it is widely used by many surgeons with off-label indications. Despite advantages in bone formation, its use still remains a controversial issue and several complications have been described by authors who oppose their wide use.

Implantation of xenogeneic bone combined with recombinant human bone morphogenetic protein-2 into bone defect—An scanning electron microscopic study

To determine the ability of a new type of composite xenogeneic bone grafting to repair bone defect. Methods: The new type of composite xenogeneic bone was obtained by combining the chemically treated cance1lous bone with recombinant human bone morphogenetic protein-2 (rhBMP-2). It was implanted on the bone defect of rabbit. Results: There was a large amount of new bone formation within the combined material and the amount was increasing as the time elapsed. In contrast, there was a lot of fibrous tissue with a little new bone formed on the area of the bone defect when the treated cancellous bone was implanted alone. Conclusion: The results imply that the rhBMP-2 plays a very important role in new bone formation and the composite xenogeneic bone appear to be an ideal material for repair of bone defect.

CORAL AS A CARRIER FOR RECOMBINANT HUMAN BONE MORPHOGENETIC PROTEIN-2

By combining coral with recombinant human bone morphogenetic protein-2 (rhBMP-2), rhBMP-2/coral composite was obtained in this study. Following implantation of the composite into the muscle pouches of mice, cartilage growth was induced in the pores or on the surface of the implants at one week, woven bone at three week and lamellar bone with bone marrow at six week, and coral was absorbed partially. The induced formation of endochondral bone was time-related and rhBMP-2 dose-related. The results of this study indicate that the composite possesses a superior ability of osteogenesis, and coral acts as one of the most suitable rhBMP-2 slowrelease carriers currently available. The composite will be a new type of bone substitute to be used in orthopaedics and maxillofacial surgery.

Regulating the bioactivity of non-glycosylated recombinant human bone morphogenetic protein-2 to enhance bone regeneration

Recombinant human bone morphogenetic protein-2(rhBMP-2)is the predominant growth factor that effectively induces osteogenic differentiation in orthopedic procedures.However,the bioactivity and stability of rhBMP-2 are intrinsically associated with its sequence,structure,and storage conditions.In this study,we successfully determined the amino acid sequence and protein secondary structure model of non-glycosylated rhBMP-2 expressed by an E.coli expression system through X-ray crystal structure analysis.Furthermore,we observed that acidic storage conditions enhanced the proliferative and osteoinductive activity of rhBMP-2.Although the osteogenic activity of non-glycosylated rhBMP-2 is relatively weaker compared to glycosylated rhBMP-2;however,this discrepancy can be mitigated by incorporating exogenous chaperone molecules.Overall,such information is crucial for rationalizing the design of stabilization methods and enhancing the bioactivity of rhBMP-2,which may also be applicable to other growth factors.

Expression of mature peptide of human bone morphogenetic protein-2 in Escherichia coli

To express die mature peptide of human bone morphogenetic protein-2 in Escherichia coil. Methods: TheDNA fragment encoding the mature peptide of human bone morphogenetic protein-2 (hBMP-2m) was inserted into expression vectorpDH in which foreign gene was controlled by PRPL promoters. E. coli DH5a transformed with recombinant plasmid pDHB2m wasinduced at 42℃to express the target protein. The expressed product was partially purified and refolded, and then implanted intorat thigh muscles to assay its bone inductive activity. Results: After induction, a protein band on SDS-PAGE gel with an apparentmol. wt. of 13kD was observed to anticipate in the strain carrying pDHB2m, but not in the control. The expressed hBMP-2m accounted for 45%-60% of the total bacterial protein. The expressed product existed in a form of inclusion body. After partially purified and refolded, rhBMP-2m could induce the formation of cartilage and bone tissue heterotopically. Conclusion: The maturepeptide of human bone morphogenetic protein-2 has ben successfully expressed in E. coli and the product has ectopic bone inductive activity.

含重组人碱性成纤维细胞生长因子和重组人骨形态发生蛋白-2骨水泥在骨质疏松性腰椎压缩性骨折治疗的应用价值

目的:探讨含重组人碱性成纤维细胞生长因子(recombinant human basic fibroblast growth factor,rhbFGF)和重组人骨形态发生蛋白-2(recombinant human bone morphogenetic protein-2,rhBMP-2)骨水泥在骨质疏松性腰椎压缩性骨折(osteoporotic vertebral compression fracture,OVCF)患者经皮椎体后凸成形术(percutaneous kyphoplasty,PKP)治疗的应用价值。方法:回顾性分析2018年1月至2021年1月收治的103例行PKP手术治疗的OVCF患者,男40例,女63例;年龄61~78(65.72±3.29)岁。受伤原因:滑倒33例,跌倒42例,提重物受伤28例。根据填充骨水泥不同分为3组:磷酸钙组34例,男14例,女20例,年龄(65.1±3.3)岁,填充磷酸钙骨水泥;rhBMP-2组34例,男12例,女22例,年龄(64.8±3.2)岁,填充含rhBMP-2的骨水泥;rhbFGF+rhBMP-2组35例,男14例,女21例,年龄(65.1±3.6)岁,填充含rhbFGF和rhBMP-2的骨水泥。比较3组Oswestry功能障碍指数(Oswestry dysfunction index,ODI)、骨密度、椎体前缘丢失高度、伤椎前缘压缩率、疼痛视觉模拟评分(visual simulation score,VAS)及再骨折发生率。结果:所有患者获得12个月随访。3组术后ODI、VAS呈下降(P<0.001),骨密度增高(P<0.001),椎体前缘丢失高度、伤椎前缘压缩率呈先下降后缓慢上升趋势(P<0.001),rhbFGF+rhBMP-2组术后第1、6、12个月ODI、VAS均低于rhBMP-2组和磷酸钙组(P<0.05),术后第6、12个月骨密度大于rhBMP-2组和磷酸钙组(P<0.05)。rhbFGF+rhBMP-2组术后第6、12个月椎体前缘丢失高度、伤椎前缘压缩率均低于rhBMP-2组和磷酸钙组(P<0.05)。3组再骨折发生率比较差异无统计学意义(P>0.05)。结论:含rhbFGF和rhBMP-2骨水泥可更有效地增加OVCF患者骨密度,获得术后满意的临床和放射学效果,显著改善临床症状。

重组人骨形态发生蛋白-2用于骨壁缺损拔牙位点保存的效果

目的:评价重组人骨形态发生蛋白-2(recombinant bone morphogenetic proteinrh-2,rhBMP-2)用于骨壁缺损拔牙位点保存的临床效果。方法:2019年2月~2023年1月将符合条件的142例患者随机分组,A组使用rhBMP-2+胶原蛋白海绵填充拔牙窝,B组使用胶原蛋白海绵,C组不使用移植物。于拔牙后18周、24周开展种植手术,并编为A1、A2;B1、B2;C1、C2组,种植术中发现有牙槽嵴顶骨缺损的病例测量牙槽嵴缺损的最大近远中径(L)、颊舌径(W)及深度(H),计算体积(V)值(V=L×W×H);无牙槽骨顶骨缺损的病例取种植窝骨块进行组织学分析。结果:A1、A2组牙槽嵴顶骨缺损的发生频率分别为:0.32、0.14;B1、B2组分别为:0.75、0.43;C1、C2组分别为:0.72、0.37。A1B1组间、A2B2组间、A1C1组间及A2C2组间V值差异有统计学意义(P<0.05)。A1B1组间及A1C1组间新生骨占比差异有统计学意义(P<0.05)。结论:rhBMP-2用于骨壁缺损的拔牙位点保存可缩短成骨时间(18周),减少不良愈合的发生,为后期种植手术的开展创造更有利的骨条件。

Bone Regeneration Enhanced by Antigen-Extracted Xenogeneic Cancellous Bone Graft with rhBMP-2 in Rabbits Mandibular Defect Repair

The effects of large piece xenogeneic bone which was separated from healthy pigs as a scaffold on repair of mandibular defect was investigated and the applicability of antigen-extracted xenogeneic cancellous bone (AXCB) soaked with rhBMP-2 in bone defect repair was assessed. Mandibular defects were created in 48 New Zealand Rabbits, and then randomly divided into 4 groups, which was grafted in the mandibular defects with AXCB, AXCB soaked with rhBMP-2, autograft bone, or blank. Equal number of animals from each group was classified into three time points (4, 8, and 12 weeks) after operation for gross pathological observation, hematoxylin and eosin (H & E) staining, radiographic examination, and bone density measurement. H & E staining revealed that the area percentage of bone regeneration in the group of AXCB/rhBMP-2 graft was 27.72 ± 4.68, 53.90 ± 21.92, and 77.35 ± 9.83 when at 4, 8, and 12 weeks, which was better than that of auto bone graft, prompting that the group of AXCB/rhBMP-2 graft had commendable osteogenic effect. And comparing with the AXCB without rhBMP-2, of which the area percentage of bone regeneration was only 14.03 ± 5.02, 28.49 ± 11.35, and 53.90 ± 21.92, the osteogenic effect of AXCB/rhBMP-2 graft was demonstrated to be much better. In the group of AXCB/rhBMP-2 graft, the area percentage of bone regeneration increased, and the implanted materials were gradually degraded and replaced by autogenous bone regeneration over time. We concluded that antigen-extracted xenogeneic cancellous bone (AXCB) graft soaked with rhBMP-2 had shown excellent osteogenic effect in repair of bone defects, with good biocompability.

携载rhBMP-2微球的新型可注射自凝固复合人工骨的制备及特性研究

[目的]制备一种具有良好降解性和成骨活性、可注射的自凝固新型骨修复材料。[方法]制备携载rh-BMP-2的聚乳酸与聚乙醇酸共聚物(PLGA)微球,并将其与rhBMP-2/磷酸钙骨水泥(CPC)复合,制备出rhBMP-2/PLGA微球/CPC复合人工骨。探讨了材料的特性,包括形貌、固化时间、抗压强度及反映材料体外降解速度的指标—体外降解液Ca、P浓度变化,测定复合材料rhBMP-2的释药速度及体外诱导MSCs细胞成骨分化的能力。[结果]与单纯CPC-rhBMP-2相比,复合材料的固化时间少量增加,抗压强度下降明显。体外降解速度及体外释药明显提高,释放的rhBMP-2具有骨诱导活性。[结论]rhBMP-2/PLGA微球/磷酸钙骨水泥新型复合人工骨是具有良好应用前景的骨修复材料。

TGF-β增强rhBMP-2诱导成骨中Ⅰ、Ⅱ型胶原mRNA及碱性磷酸酶的表达

目的 :对TGF β增强rhBMP 2诱导成骨中CollagenⅠ、ⅡmRNA及碱性磷酸酶 (ALP)的表达进行研究。方法 :BALB/c小鼠 110只随机分 2组 ,每组 5 5只。rhBMP 2 /TGF β为实验组 ,rhBMP 2为对照组 ,于术后 3～2 1d 8个时间点取材 ,用原位杂交方法对新生骨组织中的Ⅰ、Ⅱ型胶原mRNA进行检测 ;对ALP活性进行定量分析 ,观察 2组在诱导成骨中CollageⅠ、ⅡmRNA及ALP的表达情况。结果 :(1)Ⅱ型胶原mRNA的出现是和成软骨、软骨细胞的出现相伴随的 ;(2 )做为成骨细胞成熟标志物的Ⅰ型胶原mRNA、ALP在软骨形成期即有表达 ,随着成骨细胞的出现 ,骨组织的形成Ⅰ型胶原mRNA仍表现为高表达 ,而ALP的表达则呈下降趋势 ;(3 )实验组CollagenⅠ、ⅡmRNA及ALP的表达早于对照组。结论 :TGF β增强了rhBMP 2诱导成骨中CollagenⅠ、ⅡmRNA及ALP的表达。

bFGF增强rhBMP-2诱导成骨中Ⅰ、Ⅱ型胶原及碱性磷酸酶的表达

目的 :对bFGF增强rhBMP 2诱导成骨中CollagenⅠ、Ⅱ及碱性磷酸酶 (ALP)的表达进行研究。方法 :110只BALB/c小鼠随机分为 2组 ,每组 5 5只 ,rhBMP 2 /bFGF为实验组 ,rhBMP 2为对照组 ,分别于术后 3～ 2 1d 8个时间点取材 ,用免疫组化法对新生骨组织中的Ⅰ、Ⅱ型胶原进行检测 ;对ALP活性进行定量分析 ,观察 2组在诱导成骨中CollagenⅠ、Ⅱ及ALP的表达情况。结果 :( 1)Ⅱ型胶原和成软骨、软骨细胞的出现相伴随 ,但肥大、变性的软骨细胞并不表达Ⅱ型胶原。 ( 2 )作为成骨细胞成熟标志物的Ⅰ型胶原 ,ALP在软骨形成期即有表达 ,但随着成骨细胞的出现 ,骨组织的形成Ⅰ型胶原表现为高表达 ,而ALP的表达则呈下降趋势。 ( 3)实验组CollagenⅠ、Ⅱ及ALP的表达早于对照组。结论 :bFGF增强了rhBMP 2诱导成骨中CollagenⅠ。

rhBMP-2对兔骨髓基质细胞VEGF表达及成骨潜能的影响

目的 :观察经不同剂量重组人骨形态发生蛋白 2 (recombinanthumanbonemorphogeneticpro tein 2 ,rhBMP 2 )刺激后的兔骨髓基质细胞 (marrowstromalcell,MSC) ,其血管内皮生长因子 (vascularendothelialgrowthfactor ,VEGF)表达及成骨潜能变化的情况。方法 :取兔双侧股骨骨髓基质细胞体外培养 ,分别以不同剂量rhBMP 2刺激细胞 ,并设立空白对照组。培养 5d后 ,进行细胞形态 (HE染色 )、增殖情况 (细胞记数法与MTT法 )、碱性磷酸酶 (组化染色与活性测定 )、钙化结节 (图像分析 )、VEGF阳性细胞率 (免疫组化染色 )等项目的检测。结果 :不同剂量组间在碱性磷酸酶活性、矿化面积百分率、VEGF阳性细胞率三项观测指标上差异显著 ,rhBMP 2剂量为 10 0ng/ml左右时效果最佳 ;在细胞记数与MTT检测上各组差别不显著。结论 :应用rhBMP 2在促进基质细胞成骨潜能的同时 ,还可促进VEGF的表达 ,其应用剂量与效果之间存在明显相关关系 ,应用剂量为 10 0ng/ml左右时 ,其促进VEGF表达及成骨潜能作用同时达到最佳效果 ,超过此应用剂量 ,两者则有下降趋势。应用rhBMP

PLGA-Ⅱ型胶原复合rhBMP-2/bFGF修复兔膝关节软骨的缺损

目的:探讨经Ⅱ型胶原涂层改性后的聚丙交酯-乙交酯(PLGA)材料(PLGA-Ⅱ型胶原)用作生长因子重组人骨形态发生蛋白2(rhBMP-2)和碱性成纤维生长因子(bFGF)载体来修复兔膝关节软骨缺损的可行性和有效性。初步探讨生长因子rhBMP-2和bFGF之间在修复兔膝关节软骨缺损中的协同作用机制。方法:将45只成年新西兰兔随机分成A^E 5组,每组9只,用在兔右侧膝关节内侧髁钻孔的方式建立软骨缺损模型,A组植入PLGA-Ⅱ型胶原/rhBMP-2+bFGF复合物,B组植入PLGA-Ⅱ型胶原/rhBMP-2复合物,C组植入PLGA-Ⅱ型胶原/bFGF复合物,D组植入单纯PLGA-Ⅱ型胶原支架材料,E组未植入任何材料。将A、B、C组统称为实验组,D、E组统称为对照组。分别于术后4周,8周,12周处死动物,取材进行大体、组织学观察。结果:实验组的复合材料对软骨缺损的修复都有不同程度的促进作用,其中A组的效果最佳,对照组的软骨缺损的修复不明显,实验组总评分与对照组相比差异有显著性意义(P<0.05)。结论:3种带生长因子的复合体材料对兔软骨缺损的修复都有明显的促进作用。PLGA-Ⅱ型胶原复合物可用作生长因子rhBMP-2和bFGF的载体材料。生长因子rhBMP-2、bFGF对软骨缺损的修复均有促进作用,并且在剂量比为0.5 mg∶50 ng时存在着协同作用。

LASP1下调和ferritin上调在rhBMP-2诱导的比格犬BMSCs成骨分化中起重要作用

目的建立稳定的比格犬骨髓间充质干细胞(BMSCs)诱导成骨分化模型;鉴定参与比格犬BMSCs细胞成骨分化过调控的蛋白质,探讨其可能的调控机制。方法分离培养比格犬BMSCs细胞,rhBMP-2诱导细胞成骨分化7 d,基于蛋白质双向凝胶电泳的蛋白质组学分析成骨分化组与对照组差异表达的蛋白质,对感兴趣的蛋白质LASP1、ferritin轻链和重链表达情况用Q-PCR、Western blot进行验证。结果成功诱导比格犬BMSCs成骨分化;蛋白质组学分析获得rhBMP-2诱导上调的蛋白质9个,下调的蛋白质11个。荧光定量PCR技术和Western blot对LASP1和ferritin表达情况进行了验证,发现rhBMP-2诱导7 d后,LASP1显著下调而ferritin显著上调,与蛋白质组学结果一致。结论 LASP1在调节细胞骨架活性方面发挥重要功能,而ferritin是细胞铁离子稳态维持的重要分子,提示这两种蛋白质在rhBMP-2诱导的比格犬BMSCs成骨分化过程中发挥重要作用。

rhBMP-2在体内诱导成骨中Ⅰ、Ⅱ型胶原mRNA及碱性磷酸酶的表达

目的 :研究rhBMP 2在体内诱导成骨中CollagenⅠ、ⅡmRNA及碱性磷酸酶 (ALP)的表达。方法 :将含rhBMP 2 0 .5mg的松质骨载体植入BALB/c小鼠的右股部肌袋内 ,于术后 3～ 2 1d间 8个时间点取材 ,用原位杂交法对新生骨组织中的Ⅰ、Ⅱ型胶原mRNA进行检测 ;定量分析ALP活性 ,观察rhBMP 2在诱导成骨中CollagenⅠ、ⅡmRNA及ALP的表达。结果 :( 1)Ⅱ型胶原mRNA的出现是和成软骨、软骨细胞的出现相伴随。肥大、变性的软骨细胞并不表达Ⅱ型胶原mRNA。 ( 2 )作为成骨细胞成熟标志物的Ⅰ型胶原mRNA、ALP在软骨形成期即有表达 ,随着成骨细胞的出现 ,骨组织的形成 ,Ⅰ型胶原mRNA仍表现为高表达 ,而ALP的表达则呈下降趋势。结论 :在体内诱导成骨中rhBMP 2促进了CollagenⅠ。

碱性成纤维细胞生长因子促进rhBMP-2诱导成骨的载体

目的 研究碱性成纤维细胞生长因子 (b FGF)在诱导成骨中的适宜载体 .方法 BAL B/c小鼠 140只随机分为 4组 ,每组 35只 .设立 rh BMP- 2 /b FGF/PVP为实验组 ,rh BMP- 2 /b FGF,rh BMP- 2 /PVP和 rh BMP- 2 3组为对照组 ,分别于术后 3～ 2 1d共 6个时间点取材 ,进行组织学、X线分析以及钙含量测定 ,观察 4组诱导成骨情况 .结果 rh BMP-2 /b FGF/PVP组在诱导间充质细胞增殖、分化、软骨及新生骨形成方面均早于对照组 ,成骨量优于对照组 ,其组织钙含量明显高于对照组 .结论 PVP是可溶性 b

rhBMP-2/hTGF-β_1/胶原复合材料的初步研究

目的合成rhBMP-2/hTGF-β1/胶原复合材料,检测其生物相容性和活性。方法用胶原复合rhBMP-2/hTGF-β1形成复合材料,通过兔眼结膜刺激试验和溶血试验对其生物相容性进行检测,观察复合材料对Beagle犬骨髓基质细胞(MSC)生长及增殖的影响,通过细胞计数(MTT法),碱性磷酸酶(ALP)活性检测,对复合材料的活性进行检测。结果rhBMP-2/hTGF-β1/胶原复合材料呈白色棉絮状或团块状。对兔眼结膜无刺激作用,对兔血也无溶血作用。复合材料明显影响体外培养的Beagle犬骨髓基质细胞(MSC)的增殖和碱性磷酸酶水平。结论按以上方法合成的rhBMP-2/hTGF-β/胶原复合材料具有良好的生物相容性和生物学活性。

rhBMP-2/CHA修复甲状软骨缺损的实验研究

目的寻找一种修复甲状软骨缺损的新支架材料。方法以重组人骨形态发生蛋白2（rhBMP-2）、I型胶原-羟基磷灰石（CHA）为材料，运用计算机辅助设计／计算机辅助制造（CAD／CAM）技术和快速成型技术，采用泡沫凝胶注模法制备不同羟基磷灰石（HA）含量（60％、50％、40％体积分数）的甲状软骨支架，检测其孔隙率，扫描电镜观察其孔隙大小。选取27只新西兰大白兔，随机分为3组，切除一侧甲状软骨板，A组为缺损区植入rhBMP－2／cHA复合支架，B组为缺损区植入CHA支架，C组为缺损区填塞明胶海绵作空白对照。分别于术后1、3、7周各组随机抽取3只兔取材行大体观察和组织病理学检查。结果HA体积分数为50％的支架孔隙率为（50．54±3．02）％，其抗压强度为（2．50±0．24）MPa，孔隙结构主要以100～200μm的内部联通的球状孔洞为基本特征。术后3周，3组材料均完全降解，A组可见少量半透明状的骨性结节，B组见较多纤维结缔组织生成而末见骨样组织形成；术后7周，A组缺损区有块状骨性组织生成，切面呈黄白色，质地较硬，新生骨质与对侧未切除甲状软骨边缘紧密结合，B组缺损区仍只见纤维结缔组织覆盖。组织病理学检查显示：A组7周术区软骨母细胞增生伴成软骨区域形成，可见软骨细胞增生及软骨骨质形成；B组、C组术区见成熟的纤维细胞增生，均未见软骨细胞及成熟骨细胞生成。结论HA体积分数为50％的支架与rhBMP2及I型胶原复合的材料具有良好的组织相容性和骨诱导作用，为甲状软骨缺损的修复和重建提供了一种新的支架材料。