使用 Barbell Technique® 垂直骨增量手术中的自体微移植与异种无机骨。

Luiz Antonio Mazzucchelli Cosmo, Reginaldo Machado Coutinho, Luís Guilherme Scavone de Macedo, Antonio Carlos Aloise, Sérgio Jorge Jayme, João Pedro Grandini Zeferino, Antonio Graziano, Elizabeth Ferreira Martinez, Peter Karyen Moy, André Antonio Pelegrine
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引用次数: 0

摘要

简介目的:通过一项前瞻性对照研究,评估将骨膜或骨组织提取的微移植物添加到无机异种移植物中,用于上颌后牙垂直重建的再生潜力:经过临床选择和 CBCT 扫描分析后,采用 Barbell Technique® 对 19 名患者的 24 个上颌后牙部位进行了治疗。需要镶牙和嵌体重建的部位都被纳入了研究范围。对照组(CG,n = 8)在嵌体部位使用异种移植物,在镶嵌部位使用 1:1 的异种移植物和自体移植物混合体。在测试组 1(TG1,n = 8)中,嵌体和镶嵌部位都使用了与骨膜提取的微小移植物相关的异种移植物。在测试组 2(TG2,n = 8)中,内镶和外镶部位都移植了异种移植物和从骨中提取的微移植物。手术六个月后,进行 CBCT 扫描,并在植入手术中采集骨活检样本。通过测量重要矿化组织(VMT)、非重要矿化组织(NVMT)和非矿化组织(NMT)的百分比,对骨标本进行组织形态学分析。通过免疫组织化学方法,采用评分法对血管内皮生长因子的水平进行分类:组织形态学分析表明,镶嵌移植物组的 VMT、NVMT 和 NMT 无明显差异。然而,就镶嵌移植物而言,CG 的 VMT 值高于 TG2,而 NMT 值则与之相反。在这方面,CG 和 TG1 之间没有统计学差异。在免疫组化方面,CG 和 TG1 的血管内皮生长因子(VEGF)值略高于 TG2 的内镶和外镶移植物,但无统计学意义。CBCT 分析表明,所有组的骨增量水平相似,无论是内植骨还是外植骨。临床上,在总共安装的 50 个种植体中,有一个种植体(CG)出现早期失败,3 个月后被更换。所有患者均接受了种植体支持修复:这项研究表明,与从骨组织中提取的微量移植材料不同,从骨膜中提取的微量移植材料在临床应用中可能会增加嵌体重建中的骨形成。
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Use of autologous micrografts associated with xenogeneic anorganic bone in vertical bone augmentation procedures with Barbell Technique®.

Introduction: Bidirectional vertical ridge augmentation in the posterior maxilla is very challenging.

Purpose: To evaluate the regenerative potential of micrografts, derived from periosteum or bone tissue, added to an anorganic xenograft in vertical reconstruction of the posterior maxilla, by a prospective, controlled study.

Materials and methods: After clinical selection and the analysis of CBCT scans, 24 posterior maxillary sites, in 19 patients, were treated by using Barbell Technique®. Sites requiring both inlay and onlay reconstruction were enrolled in the study. In the Control Group (CG, n = 8), a xenograft was used in the inlay site and for the onlay site, a 1:1 mix of xenograft and an autograft was used. In Test Group 1 (TG1, n = 8), both inlay and onlay sites were grafted with the xenograft associated with the micrografts derived from periosteum. In Test Group 2 (TG2, n = 8), both inlay and onlay sites were grafted with the xenograft associated with the micrografts derived from bone. Six months after the procedures, CBCT scans were obtained, and bone biopsy samples were harvested during implant placement surgery. The bone specimens were analyzed histomorphometrically, by measuring the percentages of vital mineralized tissue (VMT), non vital mineralized tissue (NVMT) and non mineralized tissue (NMT). Immunohistochemically, the levels of VEGF were categorized by a score approach.

Results: Histomorphometric analysis revealed, for the inlay grafts, no significant difference among the groups for VMT, NVMT and NMT. However, for onlay grafts, CG achieved a higher amount of VMT in comparison with TG2, and the opposite occurred for NMT values. In this regard, no statistical difference was observed between CG and TG1. Concerning immunohistochemistry, the VEGF values for CG and TG1 were slightly higher than those obtained by TG2 for both inlay and onlay grafts, but without statistical significance. CBCT analysis showed a similar level of gain for all groups, for both inlay and onlay bone augmentation sites. Clinically, one implant (in CG) within a total of 50 implants installed, had early failure and was replaced after 3 months. All patients received implant supported prosthesis.

Conclusion: This study indicated that the clinical use of micrograft derived from periosteum may have some potential to increase bone formation in onlay reconstructions, unlike the micrograft derived from bone tissue.

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