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肿瘤微环境触发的金属-有机框架杂化物的离子交换用于肿瘤的多模式成像和协同治疗。

Tumor-Microenvironment-Triggered Ion Exchange of a Metal-Organic Framework Hybrid for Multimodal Imaging and Synergistic Therapy of Tumors.

机构信息

Key Laboratory of Biomedical Polymers of Ministry of Education, and Department of Chemistry, Wuhan University, Wuhan, 430072, P. R. China.

出版信息

Adv Mater. 2020 Jun;32(24):e2001452. doi: 10.1002/adma.202001452. Epub 2020 May 6.

Abstract

Nanotheranostic agents (NTAs) that integrate diagnostic capabilities and therapeutic functions have great potential for personalized medicine, yet poor tumor specificity severely restricts further clinical applications of NTAs. Here, a pro-NTA (precursor of nanotheranostic agent) activation strategy is reported for in situ NTA synthesis at tumor tissues to enhance the specificity of tumor therapy. This pro-NTA, also called PBAM, is composed of an MIL-100 (Fe)-coated Prussian blue (PB) analogue (K Mn[Fe(CN) ]) with negligible absorption in the near-infrared region and spatial confinement of Mn ions. In a mildly acidic tumor microenvironment (TME), PBAM can be specifically activated to synthesize the photothermal agent PB nanoparticles, with release of free Mn ions due to the internal fast ion exchange, resulting in the "ON" state of both T -weighted magnetic resonance imaging and photoacoustic signals. In addition, the combined Mn -mediated chemodynamic therapy in the TME and PB-mediated photothermal therapy guarantee a more efficient therapeutic performance compared to monotherapy. In vivo data further show that the pro-NTA activation strategy could selectively brighten solid tumors and detect invisible lymph node metastases with high specificity.

摘要

纳米诊疗试剂(Nanotheranostic agents,NTAs)集诊断功能和治疗功能于一体,在个性化医疗方面具有巨大的潜力,但肿瘤特异性差严重限制了 NTAs 的进一步临床应用。在此,报道了一种前体纳米诊疗试剂(pro-NTA)激活策略,用于在肿瘤组织原位合成 NTA,以增强肿瘤治疗的特异性。这种前体纳米诊疗试剂也称为 PBAM,由 MIL-100(Fe)包覆的普鲁士蓝(PB)类似物(KMn[Fe(CN)6])组成,在近红外区域几乎没有吸收,并且 Mn 离子被空间限制。在轻度酸性的肿瘤微环境(TME)中,PBAM 可以被特异性激活,合成光热剂 PB 纳米颗粒,由于内部快速离子交换,释放游离的 Mn 离子,导致 T1 加权磁共振成像和光声信号的“ON”状态。此外,TME 中 Mn 介导的化学动力学治疗与 PB 介导的光热治疗相结合,保证了比单一疗法更有效的治疗效果。体内数据进一步表明,该前体纳米诊疗试剂激活策略可以选择性地使实体瘤显影,并以高特异性检测不可见的淋巴结转移。

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