Pizzoccaro Marie-Alix, Nikel Ondrej, Sene Saad, Philippe Coralie, Mutin P Hubert, Bégu Sylvie, Vashishth Deepak, Laurencin Danielle
Institut Charles Gerhardt de Montpellier, UMR 5253, CNRS-UM-ENSCM, Place E. Bataillon, CC1701, 34095 Montpellier cedex 05, France.
Institut Charles Gerhardt de Montpellier, UMR 5253, CNRS-UM-ENSCM, Place E. Bataillon, CC1701, 34095 Montpellier cedex 05, France; Department of Biomedical Engineering, Center for Biotechnology and Interdisciplinary Studies, Rensselaer Polytechnic Institute, Troy, NY 12180, United States.
Acta Biomater. 2016 Sep 1;41:342-50. doi: 10.1016/j.actbio.2016.06.008. Epub 2016 Jun 6.
Benzoxaboroles are a family of molecules that are finding an increasing number of applications in the biomedical field, particularly as a "privileged scaffold" for the design of new drugs. Here, for the first time, we determine the interaction of these molecules with hydroxyapatites, in view of establishing (i) how benzoxaborole drugs may adsorb onto biological apatites, as this could impact on their bioavailability, and (ii) how apatite-based materials can be used for their formulation. Studies on the adsorption of the benzoxaborole motif (C7H7BO2, referred to as BBzx) on two different apatite phases were thus performed, using a ceramic hydroxyapatite (HAceram) and a nanocrystalline hydroxyapatite (HAnano), the latter having a structure and composition more similar to the one found in bone mineral. In both cases, the grafting kinetics and mechanism were studied, and demonstration of the surface attachment of the benzoxaborole under the form of a tetrahedral benzoxaborolate anion was established using (11)B solid state NMR (including (11)B-(31)P correlation experiments). Irrespective of the apatite used, the grafting density of the benzoxaborolates was found to be low, and more generally, these anions demonstrated a poor affinity for apatite surfaces, notably in comparison with other anions commonly found in biological media, such as carboxylates and (organo)phosphates. The study was then extended to the adsorption of a molecule with antimicrobial and antifungal properties (3-piperazine-bis(benzoxaborole)), showing, on a more general perspective, how hydroxyapatites can be used for the development of novel formulations of benzoxaborole drugs.
Benzoxaboroles are an emerging family of molecules which have attracted much attention in the biomedical field, notably for the design of new drugs. However, the way in which these molecules, once introduced in the body, may interact with bone mineral is still unknown, and the possibility of associating benzoxaboroles to calcium phosphates for drug-formulation purposes has not been looked into. Here, we describe the first study of the adsorption of benzoxaboroles on hydroxyapatite, which is the main mineral phase present in bone. We describe the mode of grafting of benzoxaboroles on this material, and show that they only weakly bind to its surface, especially in comparison to other ionic species commonly found in physiological media, such as phosphates and carboxylates. This demonstrates that administered benzoxaborole drugs are unlikely to remain adsorbed on hydroxyapatite surfaces for long periods of time, which means that their biodistribution will not be affected by such phenomena. Moreover, this work shows that the formulation of benzoxaborole drugs by association to calcium phosphates like hydroxyapatite will lead to a rapid release of the molecules.
苯并硼唑是一类分子,在生物医学领域有越来越多的应用,特别是作为新药设计的“特权支架”。在此,我们首次确定了这些分子与羟基磷灰石的相互作用,目的是确定:(i)苯并硼唑药物如何吸附到生物磷灰石上,因为这可能影响其生物利用度;(ii)基于磷灰石的材料如何用于其制剂。因此,使用陶瓷羟基磷灰石(HAceram)和纳米晶羟基磷灰石(HAnano)对苯并硼唑基序(C7H7BO2,简称BBzx)在两种不同磷灰石相上的吸附进行了研究,后者的结构和组成与骨矿物质中发现的更相似。在这两种情况下,都研究了接枝动力学和机理,并使用(11)B固态核磁共振(包括(11)B-(31)P相关实验)确定了苯并硼唑以四面体苯并硼酸盐阴离子形式在表面的附着。无论使用哪种磷灰石,发现苯并硼酸盐的接枝密度都很低,更一般地说,这些阴离子对磷灰石表面的亲和力较差,特别是与生物介质中常见的其他阴离子(如羧酸盐和(有机)磷酸盐)相比。然后将研究扩展到具有抗菌和抗真菌特性的分子(3-哌嗪-双(苯并硼唑))的吸附,从更一般的角度表明羟基磷灰石如何用于开发苯并硼唑药物的新型制剂。
苯并硼唑是一类新兴分子,在生物医学领域备受关注,特别是在新药设计方面。然而,这些分子一旦引入体内与骨矿物质相互作用的方式仍然未知,并且尚未研究将苯并硼唑与磷酸钙结合用于药物制剂的可能性。在此,我们描述了对苯并硼唑在羟基磷灰石上吸附的首次研究,羟基磷灰石是骨中存在的主要矿物相。我们描述了苯并硼唑在这种材料上的接枝模式,并表明它们仅微弱地结合到其表面,特别是与生理介质中常见的其他离子物种(如磷酸盐和羧酸盐)相比。这表明给药的苯并硼唑药物不太可能长时间吸附在羟基磷灰石表面,这意味着它们的生物分布不会受此类现象影响。此外,这项工作表明将苯并硼唑药物与羟基磷灰石等磷酸钙结合制剂会导致分子快速释放。