Bone grafts,bone substitutes and orthobiologics

The biology of fracture healing is better understood than ever before, with advancements such as the locking screw leading to more predictable and less eventful osseous healing. However, at times one’s intrinsic biological response, and even concurrent surgical stabilization, is inadequate. In hopes of facilitating osseous union, bone grafts, bone substitutes and orthobiologics are being relied on more than ever before. The osteoinductive, osteoconductive and osteogenic properties of these substrates have been elucidated in the basic science literature and validated in clinical orthopaedic practice. Furthermore, an industry built around these items is more successful and in demand than ever before. This review provides a comprehensive overview of the basic science, clinical utility and economics of bone grafts, bone substitutes and orthobiologics.     

Implanting Glass Spinal Cord Windows in Adult Mice with Experimental Autoimmune Encephalomyelitis

Experimental autoimmune encephalomyelitis (EAE) in adult rodents is the standard experimental model for studying autonomic demyelinating diseases such as multiple sclerosis. Here we present a low-cost and reproducible glass window implantation protocol that is suitable for intravital microscopy and studying the dynamics of spinal cord cytoarchitecture with subcellular resolution in live adult mice with EAE. Briefly, we surgically expose the vertebrae T12-L2 and construct a chamber around the exposed vertebrae using a combination of cyanoacrylate and dental cement. A laminectomy is performed from T13 to L1, and a thin layer of transparent silicone elastomer is applied to the dorsal surface of the exposed spinal cord. A modified glass cover slip is implanted over the exposed spinal cord taking care that the glass does not directly contact the spinal cord. To reduce the infiltration of inflammatory cells between the window and spinal cord, anti-inflammatory treatment is administered every 2 days (as recommended by ethics committee) for the first 10 days after implantation. EAE is induced only 2-3 weeks after the cessation of anti-inflammatory treatment.Using this approach we successfully induced EAE in 87% of animals with implanted windows and, using Thy1-CFP-23 mice (blue axons in dorsal spinal cord), quantified axonal loss throughout EAE progression. Taken together, this protocol may be useful for studying the recruitment of various cell populations as well as their interaction dynamics, with subcellular resolution and for extended periods of time. This intravital imaging modality represents a valuable tool for developing therapeutic strategies to treat autoimmune demyelinating diseases such as EAE.     

羊水直接PCR法快速诊断脊肌萎缩症的实验研究

目的：建立一种快速、简便的产前诊断脊肌萎缩症的检测方法。方法：基于运动神经元生存基因SMNc和SMNt的两个同源拷贝碱基的差异,对SMNt基因第7、8外显子进行缺失分析,抽取孕妇羊水后用作者自行研制的“HpH—Buffer”,以离心后羊水沉淀中的胎儿细胞为模板直接进行PCR扩增,扩增产物进行酶切限制性片断长度多态性分析,对2例有脊肌萎缩症患儿生育史的孕妇怀有的胎儿进行产前基因诊断。同时,为考察羊水直接扩增方法的效率,对羊水样本直接扩增和对羊水样本中提取的基因组DNA扩增进行了平行实验。结果：2例胎儿均有SMNt基因第7、8外显子缺失;以羊水为模板和以基因组DNA为模板进行扩增的效率相似。结论：应用“HpHBuffer”直接对羊水样本中SMN基因上外显子7、8进行扩增,结合限制性片断长度多态性分析SMNt上是否发生缺失,可缩短诊断时间,节约诊断成本,减少检测过程中可能出现的样本交叉污染,有望成为临床上产前诊断脊肌萎缩症的新方法。     

Enhancement of thermal stability of chondroitinase ABC I by site-directed mutagenesis: An insight from Ramachandran plot

The application of chondroitinase ABC I (cABC I) in damaged nervous tissue is believed to prune glycosaminoglycan chains of proteoglycans, thereby facilitates axon regeneration. However, the utilization of cABC I as therapeutics is notably restricted due to its thermal instability. In the present study, we have explored the possibility of thermostabilization of cABC I through release of its conformational strain using Ramachandran plot information. In this regard, Gln140 with non-optimal φ and ψ values were replaced with Gly, Ala and Asn. The results indicated that Q140G and Q140A mutants were able to improve both activity and thermal stability of the enzyme while Q140N variant reduced the enzyme activity and destabilized it. Moreover, the two former variants displayed a remarkable resistance to trypsin degradation. Structural analysis of all mutants showed an increase in intrinsic fluorescence intensity and secondary structure content of Q140G and Q140A compared to the wild type which indicated more compact structure upon mutation. This investigation demonstrated that relief of conformational tension can be considered as a possible approach to increase the stability of the protein.     

罗哌卡因抑制脊髓胶质细胞的激活而减轻CCI大鼠的神经病理性疼痛

目的:通过硬膜外注射局麻药罗哌卡因,评价其对神经病理性疼痛模型大鼠的作用及其机制.方法:在坐骨神经损伤神经病理性疼痛大鼠模型(CCI)术后7d,进行硬膜外置管手术,在术后8d和11d由硬膜外导管注入罗哌卡因,观测CCI大鼠机械痛阈(PWT)和脊髓后角纤维酸性蛋白(GFAP)的变化.结果:硬膜外注射罗哌卡因能够升高CCI大鼠患肢的机械痛阈,降低脊髓后角GFAP的表达.结论:在CCI大鼠模型硬膜外注射罗哌卡因可以较长时间抑制脊髓胶质细胞的激活,从而减轻神经病理性疼痛.     

Toll-like Receptor 2 Mediates Peripheral Nerve Injury-induced NADPH Oxidase 2 Expression in Spinal Cord Microglia

We have previously reported that NADPH oxidase 2 (Nox2) is up-regulated in spinal cord microglia after spinal nerve injury, demonstrating that it is critical for microglia activation and subsequent pain hypersensitivity. However, the mechanisms and molecules involved in Nox2 induction have not been elucidated. Previous studies have shown that Toll-like receptors (TLRs) are involved in nerve injury-induced spinal cord microglia activation. In this study, we investigated the role of TLR in Nox2 expression in spinal cord microglia after peripheral nerve injury. Studies using TLR knock-out mice have shown that nerve injury-induced microglial Nox2 up-regulation is abrogated in TLR2 but not in TLR3 or -4 knock-out mice. Intrathecal injection of lipoteichoic acid, a TLR2 agonist, induced Nox2 expression in spinal cord microglia both at the mRNA and protein levels. Similarly, lipoteichoic acid stimulation induced Nox2 expression and reactive oxygen species production in primary spinal cord glial cells in vitro. Studies on intracellular signaling pathways indicate that NF-κB and p38 MAP kinase activation is required for TLR2-induced Nox2 expression in glial cells. Conclusively, our data show that TLR2 mediates nerve injury-induced Nox2 gene expression in spinal cord microglia via NF-κB and p38 activation and thereby may contribute to spinal cord microglia activation.     

跟骨骨折手术治疗并发症原因分析及预防

目的:探讨手术内固定治疗跟骨骨折发生并发症的原因及预防.方法:2007年5月～2010年9月应用切开复位跟骨钛板和闭合橇拔复位斯氏针内固定术治疗的64例跟骨骨折患者中,对出现并发症的患者进行回顾性分析,探讨其发生并发症的可能原因.结果:其中2例切口感染浅表坏死,1例腓肠神经损伤,腓骨长短肌腱断裂1例,腓骨肌腱炎4例,创伤性关节炎5例,复位丢失3例.结论:应根据骨折类型选择恰当的治疗方案,正确把握手术时机、规范操作,可有效减少并发症,获得满意的疗效.     

锁定加压钢板和动力加压钢板治疗肱骨中下段骨折的临床比较研究

目的:对比锁定加压钢板与动力加压钢板治疗肱骨中下段骨折患者的临床疗效。方法:抽取我院2010年8月~2013年12月收治的肱骨中下段骨折患者76例,按照随机数字表法分为锁定组(锁定加压钢板治疗)与动力组(动力加压钢板治疗),每组38例,随访1年。对比两组患者临床指标,治疗效果及并发症发生率。结果:锁定组患者手术时间、骨折愈合时间及住院时间均小于动力组,差异均有统计学意义(P0.05);锁定组患者优良率为89.47%,显著高于动力组的71.05%,差异有统计学意义(P0.05);锁定组的并发症发生率为10.53%,显著低于动力组的31.58%,差异有统计学意义(P0.05)。结论:锁定加压钢板应用于治疗肱骨中下段骨折患者疗效优于动力加压钢板治疗,它具有创伤小、恢复快的优点,且并发症发生率较低,值得推广。     

后路减压内固定融合矫形治疗退变性腰椎侧凸伴椎管狭窄的临床研究

目的:探讨后路减压内固定融合矫形治疗退变性腰椎侧凸伴椎管狭窄的临床疗效。方法:将我院2009年1月~2015年1月收治的退变性腰椎侧凸伴椎管狭窄患者按照手术方法分为两组,实验组进行后路减压内固定融合矫形术治疗,对照组进行单纯后路减压固定矫形术治疗,对比两组患者术前、术后6个月和18个月的Cobb角、腰椎前凸角、日本骨科学会(JOA)评分、疼痛视觉模拟量表(VAS)情况,SRS-22国际标准量表评分情况以及出血量情况。结果:实验组术后18个月的Cobb角、腰椎前凸角分别为(16.8±5.16)°和(36.8±5.82)°,均分别低于对照组的(20.2±6.61)°和(41.2±5.67)°,且均低于术前(P0.05),而术前及术后6个月时两组比较无差异(P0.05);两组患者术后6个月和18个月的JOA评分、VAS评分比较均较术前明显改善(P0.05),且组间比较显示,术后18月两组比较均存在显著差异(P0.05);SRS-22国际标准评估量表显示,术后18个月两组患者的自理能力、自我评价、精神状态方面无显著差异(P0.05),而疼痛情况存在显著差异(P0.05)。两组术中出血量比较无统计学差异(P0.05)。结论:后路减压内固定融合矫形术治疗退变性腰椎侧凸伴椎管狭窄疗效显著,且后路减压内固定融合矫形术在改善患者的腰椎侧凸程度、功能障碍及疼痛程度方面优于单纯后路减压矫形内固定术,值得临床推广。     

不同磁共振腰骶丛神经成像序列的临床研究

目的:比较周围神经背景信号抑制弥散加权成像(diffusion-weighted neuroimag ing with background signal suppression,DWIBS)、选择性激励技术(principle of selective excitation technique,PROSET)及三维短时反转恢复(3D Short Term Inversion Recovery,3D STIR)序列在腰骶部脊神经成像中的不同表现,探讨其对腰骶部病变的临床应用价值。方法:对29名正常志愿者及42例腰骶丛病变损伤患者行磁共振腰骶丛神经成像,包括DWIBS序列,PROSET及3D STIR序列。对DWIBS及3D STIR原始图像行最大信号强度投影(MIP)后处理重建,对志愿者组及病变组所得图像质量分级并分别进行统计分析,评价三种高场强磁共振腰骶丛神经成像序列在正常组及病变组的显示效果。结果:在正常志愿者组中,三种高场强磁共振腰骶丛神经成像序列均可显示脊神经根、神经节等解剖细节,对于腰4、5脊神经的显示,三者的图像分级差异不具有统计学意义。在腰2、3脊神经成像中,三者图像质量分级的差异具有统计学意义(P0.05)。在病例组中,经秩和检验三组组间显示效果不完全相同,P0.05,差异有统计学意义。进行两两比较,DWIBS与3D SITR序列,其差异具有统计学意义(P0.01)。PROSET与3D STIR序列,差异具有统计学意义(P0.01)。而DWIBS与PROSET图像质量分级差异无明显统计学差异。结论:DWIBS、PROSET、3DSTIR序列作为常规序列的补充,均可完整的显示腰骶神经的解剖细节,而DWIBS及PROSET序列对背景组织的抑制更加充分,更利于观察神经的走行变化、判断神经受损部位及范围。DWIBS序列MIP后处理图像实现了对腰骶神经的多方位多角度旋转观察,为术前制定手术方案提供可靠的影像学依据,弥补了常规磁共振序列的不足。