Combining Sclerostin Neutralization with Tissue Engineering: An Improved Strategy for Craniofacial Bone Repair

BioRN: Regeneration (Topic) Pub Date : 2021-12-01 DOI:10.2139/ssrn.3919746

Sophie Maillard, L. Sicard, Caroline Andrique, Coralie Torrens, J. Lesieur, B. Baroukh, T. Coradin, A. Poliard, L. Slimani, C. Chaussain

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引用次数: 3

Abstract

Scaffolds associated with different types of mesenchymal stromal stem cells (MSC) are extensively studied for the development of novel therapies for large bone defects. Moreover, monoclonal antibodies have been recently introduced for the treatment of cancer-associated bone loss and other skeletal pathologies. In particular, antibodies against sclerostin, a key player in bone remodeling regulation, have demonstrated a real benefit for treating osteoporosis but their contribution to bone tissue-engineering remains uncharted. Here, we show that combining implantation of dense collagen hydrogels hosting wild-type (WT) murine dental pulp stem cells (mDPSC) with weekly systemic injections of a sclerostin antibody (Scl-Ab) leads to increased bone regeneration within critical size calvarial defects performed in WT mice. Furthermore, we show that bone formation is equivalent in calvarial defects in WT mice implanted with Sost knock-out (KO) mDPSC and in Sost KO mice, suggesting that the implantation of sclerostin-deficient MSC similarly promotes new bone formation than complete sclerostin deficiency. Altogether, our data demonstrate that an antibody-based therapy can potentialize tissue-engineering strategies for large craniofacial bone defects and urges the need to conduct research for antibody-enabled local inhibition of sclerostin. STATEMENT OF SIGNIFICANCE: : The use of monoclonal antibodies is nowadays broadly spread for the treatment of several conditions including skeletal bone diseases. However, their use to potentialize tissue engineering constructs for bone repair remains unmet. Here, we demonstrate that the neutralization of sclerostin, through either a systemic inhibition by a monoclonal antibody or the implantation of sclerostin-deficient mesenchymal stromal stem cells (MSC) directly within the defect, improves the outcome of a tissue engineering approach, combining dense collagen hydrogels and MSC derived from the dental pulp, for the treatment of large craniofacial bone defects.

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结合硬化蛋白中和与组织工程:颅面骨修复的改进策略

不同类型间充质基质干细胞(MSC)相关的支架被广泛研究，用于开发大型骨缺损的新疗法。此外，单克隆抗体最近已被引入治疗癌症相关的骨质流失和其他骨骼病理。特别是，针对硬化蛋白的抗体，在骨重塑调节中的关键角色，已经证明对治疗骨质疏松症有真正的好处，但它们对骨组织工程的贡献仍然未知。在本研究中，我们发现将携带野生型(WT)小鼠牙髓干细胞(mDPSC)的致密胶原水凝胶与每周全身注射硬化蛋白抗体(Scl-Ab)相结合，可以增加WT小鼠临界尺寸颅骨缺损内的骨再生。此外，我们发现骨形成在植入Sost敲除(KO) mDPSC的WT小鼠和Sost KO小鼠的颅骨缺陷中是相同的，这表明植入缺乏硬化蛋白的MSC与完全缺乏硬化蛋白类似地促进新骨形成。总之，我们的数据表明，基于抗体的治疗可以潜在地用于大颅面骨缺损的组织工程策略，并敦促需要进行抗体激活的局部抑制硬化蛋白的研究。意义说明:*目前，单克隆抗体广泛用于治疗包括骨骼疾病在内的几种疾病。然而，它们在潜在的骨修复组织工程构建中的应用仍未得到满足。在这里，我们证明了通过单克隆抗体的系统抑制或直接在缺损内植入缺乏硬化蛋白的间充质间质干细胞(MSC)来中和硬化蛋白，可以改善组织工程方法的结果，将致密胶原水凝胶和来自牙髓的间充质间质干细胞结合起来，用于治疗大颅面骨缺损。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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BioRN: Regeneration (Topic)

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