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可调谐金纳米棒/NAO 缀合物用于线粒体靶向癌症治疗中的选择性药物递送。

Tunable gold nanorod/NAO conjugates for selective drug delivery in mitochondria-targeted cancer therapy.

机构信息

Departamento Química Física, Universidad Complutense de Madrid, Avda. Complutense s/n, 28040 Madrid, Spain.

Instituto de Investigación Hospital Doce de Octubre (imas12), Avenida de Córdoba s/n, 28041 Madrid, Spain.

出版信息

Nanoscale. 2022 Jun 9;14(22):8028-8040. doi: 10.1039/d2nr02353a.

DOI:10.1039/d2nr02353a
PMID:35616261
Abstract

Nonyl acridine orange (NAO) is a lipophilic and positively charged molecule widely used as a mitochondrial fluorescent probe. NAO is cytotoxic at micromolar concentration and might be potentially used as a mitochondria-targeted drug for cancer therapy. However, the use of NAO under conditions would be compromised by the unspecific interactions with off-target cells and negatively charged proteins present in the bloodstream. To tackle this limitation, we have synthesized NAO analogues carrying an imidazole group for their specific binding to nitrilotriacetic (NTA) functionalized gold nanorods (AuNRs). We demonstrate that AuNRs provide 10 binding sites and a controlled delivery under acidic conditions. Upon incubation with mouse embryonic fibroblasts, the endosomal acidic environment releases the NAO analogues from AuNRs, as visualized through the staining of the mitochondrial network. The addition of the monoclonal antibody Cetuximab to the conjugates enhanced their uptake within lung cancer cells and the conjugates were cytotoxic at subnanomolar concentrations ( ≈ 0.06 nM). Moreover, the specific interactions of Cetuximab with the epidermal growth factor receptor (EGFR) provided a specific targeting of EGFR-expressing lung cancer cells. After intravenous administration in patient-derived xenografts (PDX) mouse models, the conjugates reduced the progression of EGFR-positive tumors. Overall, the NAO-AuNRs provide a promising strategy to realize membrane mitochondria-targeted conjugates for lung cancer therapy.

摘要

壬基吖啶橙(NAO)是一种亲脂性的带正电荷的分子,广泛用作线粒体荧光探针。NAO 在微摩尔浓度下具有细胞毒性,可能被潜在地用作癌症治疗的靶向线粒体药物。然而,在条件下使用 NAO 会受到与非靶细胞和血液中带负电荷的蛋白质的非特异性相互作用的影响。为了解决这个限制,我们合成了携带咪唑基团的 NAO 类似物,用于与氮三乙酸(NTA)功能化的金纳米棒(AuNRs)特异性结合。我们证明 AuNRs 提供了 10 个结合位点,并在酸性条件下提供了受控的释放。与小鼠胚胎成纤维细胞孵育后,内体酸性环境将 NAO 类似物从 AuNRs 中释放出来,这可以通过线粒体网络的染色来观察到。将单克隆抗体西妥昔单抗添加到缀合物中增强了它们在肺癌细胞中的摄取,并且缀合物在亚纳摩尔浓度(约 0.06 nM)下具有细胞毒性。此外,西妥昔单抗与表皮生长因子受体(EGFR)的特异性相互作用为表达 EGFR 的肺癌细胞提供了特异性靶向。在患者来源的异种移植(PDX)小鼠模型中静脉给药后,缀合物减少了 EGFR 阳性肿瘤的进展。总体而言,NAO-AuNRs 为实现针对肺癌治疗的膜靶向线粒体缀合物提供了一种有前途的策略。

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