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将肿瘤归巢和线粒体靶向肽结构域杂交,以设计用于治疗诊断应用的新型双成像自组装肽纳米颗粒。

Hybridization of tumor homing and mitochondria-targeting peptide domains to design novel dual-imaging self-assembled peptide nanoparticles for theranostic applications.

作者信息

Rizvi Syed Faheem Askari, Shahid Samiah, Mu Shuai, Zhang Haixia

机构信息

College of Chemistry and Chemical Engineering, Gansu Province, Lanzhou University, Lanzhou-730000, People's Republic of China.

Institute of Molecular Biology and Biotechnology (IMBB), The University of Lahore, Lahore-54000, Punjab, Pakistan.

出版信息

Drug Deliv Transl Res. 2022 Jul;12(7):1774-1785. doi: 10.1007/s13346-021-01066-6. Epub 2021 Sep 17.

Abstract

A novel hybridized dual-targeting peptide-based nanoprobe was successfully designed by using the cyclic heptapeptide. This peptide has Arg-Gly-Asp-Lys-Leu-Ala-Lys sequence, in which the RGD homing motif and KALK mitochondria-targeting motif were linked via amide bond. The designed peptide probe was further modified through covalent linkage to induce dual-imaging functionality, and self-assembled to form spherical nanoparticles. The novel Cy5.5-SAPD-Tc nanoparticles were tested for in vitro cytotoxicity, cellular uptake, and apoptosis-inducing functionalities. The cellular internalization, enhanced cytotoxicity and selective receptor binding capabilities against U87MG cells, excellent dual-imaging potential, improved apoptosis-inducing feature by damaging mitochondria, and in vivo preclinical investigations suggested that our newly designed novel hybridized peptide-based dual-imaging nanoparticles may serve as an admirable theranostic probe to treat brain tumor glioblastoma multiforme. This study describes the development of dual-targeting self-assembled peptide nanoparticles followed by modifications using NIRF dye and radiolabeled with Tc for dual-imaging and enhanced therapeutic efficacy against brain tumor.

摘要

通过使用环七肽成功设计了一种新型的基于双靶向肽的纳米探针。该肽具有Arg-Gly-Asp-Lys-Leu-Ala-Lys序列,其中RGD归巢基序和KALK线粒体靶向基序通过酰胺键相连。设计的肽探针通过共价连接进一步修饰以诱导双成像功能,并自组装形成球形纳米颗粒。对新型Cy5.5-SAPD-Tc纳米颗粒进行了体外细胞毒性、细胞摄取和诱导凋亡功能的测试。细胞内化、增强的细胞毒性和对U87MG细胞的选择性受体结合能力、出色的双成像潜力、通过损伤线粒体改善的诱导凋亡特性以及体内临床前研究表明,我们新设计的基于新型杂交肽的双成像纳米颗粒可能作为一种令人钦佩的治疗诊断探针来治疗多形性胶质母细胞瘤。本研究描述了双靶向自组装肽纳米颗粒的开发,随后使用近红外荧光染料进行修饰并用Tc进行放射性标记,用于双成像并增强对脑肿瘤的治疗效果。

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