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利用刺激响应型材料克服实体瘤的间质和肿瘤内屏障实现药物传递和治疗一体化。

Intertumoral and intratumoral barriers as approaches for drug delivery and theranostics to solid tumors using stimuli-responsive materials.

机构信息

Department of Chemistry, Iran University of Science and Technology, Tehran, P.O. Box 16846-13114, Iran.

Department of Physics, Iran University of Science and Technology, Tehran, P.O. Box 16846-13114, Iran.

出版信息

Mikrochim Acta. 2024 Aug 16;191(9):541. doi: 10.1007/s00604-024-06583-y.

Abstract

The solid tumors provide a series of biological barriers in cellular microenvironment for designing drug delivery methods based on advanced stimuli-responsive materials. These intertumoral and intratumoral barriers consist of perforated endotheliums, tumor cell crowding, vascularity, lymphatic drainage blocking effect, extracellular matrix (ECM) proteins, hypoxia, and acidosis. Triggering opportunities have been drawn for solid tumor therapies based on single and dual stimuli-responsive drug delivery systems (DDSs) that not only improved drug targeting in deeper sites of the tumor microenvironments, but also facilitated the antitumor drug release efficiency. Single and dual stimuli-responsive materials which are known for their lowest side effects can be categorized in 17 main groups which involve to internal and external stimuli anticancer drug carriers in proportion to microenvironments of targeted solid tumors. Development of such drug carriers can circumvent barriers in clinical trial studies based on their superior capabilities in penetrating into more inaccessible sites of the tumor tissues. In recent designs, key characteristics of these DDSs such as fast response to intracellular and extracellular factors, effective cytotoxicity with minimum side effect, efficient permeability, and rate and location of drug release have been discussed as core concerns of designing paradigms of these materials.

摘要

实体瘤在细胞微环境中提供了一系列生物屏障,可用于设计基于先进刺激响应材料的药物输送方法。这些肿瘤间和肿瘤内的屏障包括有孔的内皮细胞、肿瘤细胞拥挤、血管生成、淋巴引流阻断效应、细胞外基质 (ECM) 蛋白、缺氧和酸中毒。基于单一和双重刺激响应药物输送系统 (DDS) 的实体瘤治疗已经有了触发机会,这些系统不仅提高了药物在肿瘤微环境深层部位的靶向性,还提高了抗肿瘤药物的释放效率。单一和双重刺激响应材料因其副作用最低而被分类为 17 个主要组别,这些组别涉及到内部和外部刺激抗癌药物载体,以匹配靶向实体瘤的微环境。这些药物载体的开发可以避免临床试验研究中的障碍,因为它们具有优越的穿透能力,可以进入肿瘤组织更难以到达的部位。在最近的设计中,这些 DDS 的关键特性,如对细胞内和细胞外因素的快速响应、最小副作用的有效细胞毒性、高效渗透性以及药物释放的速度和位置,已被视为设计这些材料范式的核心关注点。

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