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纳米金刚石作为“人工蛋白”:使用无机纳米晶体的低纳摩尔溶液来调节细胞信号系统。

Nanodiamonds as "artificial proteins": Regulation of a cell signalling system using low nanomolar solutions of inorganic nanocrystals.

机构信息

Department of Biology, Faculty of Medicine, Masaryk University, 62500, Brno, Czech Republic.

Institute of Experimental Biology, Faculty of Sciences, Masaryk University, 62500, Brno, Czech Republic; Institute of Animal Physiology and Genetics of the CAS, 60200, Brno, Czech Republic.

出版信息

Biomaterials. 2018 Sep;176:106-121. doi: 10.1016/j.biomaterials.2018.05.030. Epub 2018 May 21.

DOI:10.1016/j.biomaterials.2018.05.030
PMID:
29879652
Abstract

The blocking of specific protein-protein interactions using nanoparticles is an emerging alternative to small molecule-based therapeutic interventions. However, the nanoparticles designed as "artificial proteins" generally require modification of their surface with (bio)organic molecules and/or polymers to ensure their selectivity and specificity of action. Here, we show that nanosized diamond crystals (nanodiamonds, NDs) without any synthetically installed (bio)organic interface enable the specific and efficient targeting of the family of extracellular signalling molecules known as fibroblast growth factors (FGFs). We found that low nanomolar solutions of detonation NDs with positive ζ-potential strongly associate with multiple FGF ligands present at sub-nanomolar concentrations and effectively neutralize the effects of FGF signalling in cells without interfering with other growth factor systems and serum proteins unrelated to FGFs. We identified an evolutionarily conserved FGF recognition motif, ∼17 amino acids long, that contributes to the selectivity of the ND-FGF interaction. In addition, we inserted this motif into a de novo constructed chimeric protein, which significantly improved its interaction with NDs. We demonstrated that the interaction of NDs, as purely inorganic nanoparticles, with proteins can mitigate pathological FGF signalling and promote the restoration of cartilage growth in a mouse limb explant model. Based on our observations, we foresee that NDs may potentially be applied as nanotherapeutics to neutralize disease-related activities of FGFs in vivo.

摘要

利用纳米颗粒阻断特定的蛋白质-蛋白质相互作用是一种新兴的替代小分子治疗干预的方法。然而,设计为“人工蛋白”的纳米颗粒通常需要用(生物)有机分子和/或聚合物对其表面进行修饰,以确保其作用的选择性和特异性。在这里,我们表明,没有任何合成安装的(生物)有机界面的纳米尺寸金刚石晶体(纳米金刚石,NDs)能够特异性和有效地靶向称为成纤维细胞生长因子(FGFs)的细胞外信号分子家族。我们发现,带正 ζ 电位的爆炸 ND 的低纳摩尔溶液强烈地与存在于亚纳摩尔浓度下的多个 FGF 配体结合,并有效地中和 FGF 信号在细胞中的作用,而不干扰其他与 FGF 无关的生长因子系统和血清蛋白。我们确定了一个进化上保守的 FGF 识别基序,长约 17 个氨基酸,它有助于 ND-FGF 相互作用的选择性。此外,我们将这个基序插入到一个新构建的嵌合蛋白中,这显著提高了它与 ND 的相互作用。我们证明了 ND 作为纯无机纳米颗粒与蛋白质的相互作用可以减轻病理性 FGF 信号,并促进在小鼠肢体外植体模型中软骨生长的恢复。基于我们的观察,我们预计 ND 可能作为纳米药物在体内中和与疾病相关的 FGF 活性。

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