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基于肽的无机纳米颗粒作为高效的细胞内递送系统

Peptide-Based Inorganic Nanoparticles as Efficient Intracellular Delivery Systems.

作者信息

Shirazi Amir Nasrolahi, Vadlapatla Rajesh, Koomer Ajoy, Nguyen Anthony, Khoury Vian, Parang Keykavous

机构信息

Department of Pharmaceutical Sciences, College of Pharmacy, Marshall B. Ketchum University, 2575 Yorba Linda Blvd., Fullerton, CA 92831, USA.

Center for Targeted Drug Delivery, Department of Biomedical and Pharmaceutical Sciences, Chapman University School of Pharmacy, Harry and Diane Rinker Health Science Campus, 9401 Jeronimo Rd, Irvine, CA 92618, USA.

出版信息

Pharmaceutics. 2025 Aug 28;17(9):1123. doi: 10.3390/pharmaceutics17091123.

DOI:10.3390/pharmaceutics17091123
PMID:41012460
Abstract

: Peptide-based inorganic nanoparticles (PINPs) have emerged as promising candidates for intracellular delivery due to their unique structural and functional attributes. These hybrid nanostructures combine the high surface area and tunable optical/magnetic properties of metal cores (e.g., Au, Ag, FeO) with the biocompatibility, targeting specificity, and responsive behavior of peptides. In particular, peptides with amphipathic or cell-penetrating features could facilitate efficient transport of molecular cargos across cellular membranes while enabling stimulus-responsive drug release in target tissues. : We review key synthesis methods (especially green, peptide-mediated one-pot approaches), functionalization strategies (e.g., thiol-gold bonds, click chemistries), and characterization techniques (TEM, DLS, FTIR, etc.) that underpin PINP design. In addition, we highlight diverse peptide classes (linear, cyclic, amphipathic, self-assembling) and their roles (targeting ligands, capping/stabilizing agents, reducing agents) in constructing multifunctional nanocarriers. : The prospects of PINPs are considerable: they enable targeted drug delivery with imaging/theranostic capability, improve drug stability and cellular uptake, and harness peptide programmability for precision nanomedicine. However, challenges such as in vivo stability, immunogenicity, and standardization of evaluation must be addressed. : Overall, PINPs represent multifunctional platforms that could significantly advance drug delivery and diagnostic applications in the future.

摘要

基于肽的无机纳米粒子(PINPs)因其独特的结构和功能特性,已成为细胞内递送的有前途的候选者。这些杂化纳米结构将金属核(如金、银、氧化铁)的高比表面积和可调谐光学/磁性特性与肽的生物相容性、靶向特异性和响应行为结合在一起。特别是,具有两亲性或细胞穿透特性的肽可以促进分子货物跨细胞膜的有效运输,同时在靶组织中实现刺激响应性药物释放。

我们综述了支撑PINP设计的关键合成方法(特别是绿色的、肽介导的一锅法)、功能化策略(如硫醇-金键、点击化学)和表征技术(透射电子显微镜、动态光散射、傅里叶变换红外光谱等)。此外,我们强调了不同类型的肽(线性、环状、两亲性、自组装)及其在构建多功能纳米载体中的作用(靶向配体、封端/稳定剂、还原剂)。

PINPs的前景十分广阔:它们能够实现具有成像/治疗诊断能力的靶向药物递送,提高药物稳定性和细胞摄取,并利用肽的可编程性实现精准纳米医学。然而,必须解决诸如体内稳定性、免疫原性和评估标准化等挑战。

总体而言,PINPs代表了多功能平台,有望在未来显著推动药物递送和诊断应用的发展。

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本文引用的文献

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Peptide-Based Nanoparticle for Tumor Therapy.用于肿瘤治疗的肽基纳米颗粒
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Impact of stereochemical replacement on activity and selectivity of membrane-active antibacterial and antifungal cyclic peptides.
立体化学取代对膜活性抗菌和抗真菌环肽的活性及选择性的影响
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In vitro localization of modified zinc oxide nanoparticles showing selective anticancer effects against colorectal carcinoma using biophysical techniques.使用生物物理技术对显示出对结直肠癌具有选择性抗癌作用的改性氧化锌纳米颗粒进行体外定位。
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Antibacterial and Antifungal Activities of Linear and Cyclic Peptides Containing Arginine, Tryptophan, and Diphenylalanine.含精氨酸、色氨酸和二苯基丙氨酸的线性及环状肽的抗菌和抗真菌活性
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