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药物递送在优化骨形态发生蛋白在牙周再生过程中的作用方面的重要性。

The importance of drug delivery to optimize the effects of bone morphogenetic proteins during periodontal regeneration.

作者信息

King G N

机构信息

University of Texas Health Science Center, Department of Periodontics, Dental School-MSC, San Antonio 78229-3900, USA.

出版信息

Curr Pharm Biotechnol. 2001 Jun;2(2):131-42. doi: 10.2174/1389201013378716.

Abstract

Bone morphogenetic proteins (BMPs) include a large number of proteins belonging to the TGF-beta superfamily which are characterized by their ability to induce bone and cartilage formation. Since the isolation and purification of BMPs by recombinant technology, the effects of single BMPs can now be evaluated in animal models. Subcutanous placement of a single recombinant BMP, such as recombinant human (rh) BMP-2, in a rat ectopic assay shows recruitment of undifferentiated mesenchymal cells, cartilage formation, followed by replacement with bone, formation of its own bone marrow and physiological bone remodelling. The therapeutic use of recombinant BMPs in the treatment of periodontal disease (destruction of the tooth ligaments, surrounding bone and tooth cementum, the latter of which anchors the ligaments to the tooth surface from the adjacent tooth socket) has attracted considerable interest due to their potent ability to stimulate intramembranous bone formation without an endochondral intermediate. Their predictability in stimulating new bone may provide an alternative that has greater osteogenic potential than autogenous bone, other growth factors and bone substitutes. The biological processes and the potential role of growth factors involved in promoting regeneration are complicated by the involvement of different cell types each with their different growth rates and responses to various stimuli. The major cell types involved in periodontal regeneration include osteoblasts, cementoblasts and fibroblasts. Here, the formation of the new mineralized layers on the tooth and bone surfaces by cementoblasts and osteoblasts respectively are a prerequisite before periodontal ligament formation and attachment by fibroblasts can occur. In this regard, BMPs are likely candidates to stimulate periodontal regeneration because of their ability not only to promote osteogenesis but also to stimulate cementogenesis (new cementum formation). However, understanding when to manipulate each of the various cells differentiation pathway with the application of single or multiple doses of BMPs at the appropriate concentration is dependent upon a suitable delivery system that can be modified in order to optimize its effect during periodontal wound healing. Furthermore, treatment of intrabony periodontal defects with BMPs are likely to not only require appropriate temporal release of the agent, but also adaptation of a carrier that is robust enough to maintain its integrity around the coronal aspect of the root in order to provide space maintenance and support the mucoperiosteal flap. This review evaluates the effects of different delivery systems upon BMP-induced periodontal regeneration.

摘要

骨形态发生蛋白(BMPs)包括大量属于转化生长因子-β超家族的蛋白质,其特点是具有诱导骨和软骨形成的能力。自从通过重组技术分离和纯化BMPs以来,现在可以在动物模型中评估单一BMPs的作用。在大鼠异位试验中皮下植入单一重组BMP,如重组人(rh)BMP-2,可显示未分化间充质细胞的募集、软骨形成,随后被骨替代、形成自身的骨髓以及生理性骨重塑。重组BMPs在治疗牙周疾病(牙齿韧带、周围骨和牙骨质的破坏,牙骨质将韧带从相邻牙槽窝锚固到牙齿表面)中的治疗应用因其强大的刺激膜内骨形成而无软骨内中间阶段的能力而引起了相当大的兴趣。它们在刺激新骨形成方面的可预测性可能提供一种比自体骨、其他生长因子和骨替代物具有更大成骨潜力的替代方案。由于不同细胞类型的参与,每种细胞具有不同的生长速率和对各种刺激的反应,促进再生所涉及的生物学过程和生长因子的潜在作用变得复杂。参与牙周再生的主要细胞类型包括成骨细胞、成牙骨质细胞和成纤维细胞。在此,分别由成牙骨质细胞和成骨细胞在牙齿和骨表面形成新的矿化层是成纤维细胞形成牙周韧带并附着之前的先决条件。在这方面,BMPs可能是刺激牙周再生的候选者,因为它们不仅能够促进成骨,还能刺激牙骨质生成(新牙骨质形成)。然而,了解何时以适当浓度应用单剂量或多剂量BMPs来操纵各种细胞的分化途径取决于一种合适的递送系统,该系统可以进行修改以在牙周伤口愈合期间优化其效果。此外,用BMPs治疗骨内牙周缺损可能不仅需要药物的适当时间释放,还需要一种足够坚固的载体,以在牙根冠方周围维持其完整性,从而提供空间维持并支持粘骨膜瓣。本综述评估了不同递送系统对BMP诱导的牙周再生的影响。

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