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可注射双尺度介孔二氧化硅癌症疫苗,能够将负载抗原/佐剂的纳米颗粒有效递送至在局部大孔支架中募集的树突状细胞。

Injectable dual-scale mesoporous silica cancer vaccine enabling efficient delivery of antigen/adjuvant-loaded nanoparticles to dendritic cells recruited in local macroporous scaffold.

作者信息

Nguyen Thanh Loc, Cha Bong Geun, Choi Youngjin, Im Jihye, Kim Jaeyun

机构信息

School of Chemical Engineering, Sungkyunkwan University (SKKU), Suwon, 16419, Republic of Korea.

School of Chemical Engineering, Sungkyunkwan University (SKKU), Suwon, 16419, Republic of Korea; Department of Health Sciences and Technology, Samsung Advanced Institute for Health Science & Technology (SAIHST), Sungkyunkwan University (SKKU), Suwon, 16419, Republic of Korea; Biomedical Institute for Convergence at SKKU (BICS), Sungkyunkwan University (SKKU), Suwon, 16419, Republic of Korea; Institute of Quantum Biophysics (IQB), Sungkyunkwan University (SKKU), Suwon, 16419, Republic of Korea.

出版信息

Biomaterials. 2020 May;239:119859. doi: 10.1016/j.biomaterials.2020.119859. Epub 2020 Feb 10.

DOI:10.1016/j.biomaterials.2020.119859
PMID:32070828
Abstract

Despite the potential of nanoparticle-based vaccines, their therapeutic efficacy for cancer immunotherapy is limited. To elicit robust antigen-specific adaptive immune responses, antigen-loaded nanoparticles are employed for transport into host dendritic cells (DCs); however, only a minority of the nanoparticles can be engulfed by host DCs. Herein, an injectable dual-scale mesoporous silica vaccine consisting of mesoporous silica microrods (MSRs) coupled with mesoporous silica nanoparticles (MSNs) is introduced. The MSRs form a three-dimensional macroporous scaffold after injection, and the subsequent release of DC-recruiting chemokine loaded in the mesopores of MSRs leads to the recruitment of numerous DCs into the scaffold. Subsequently, MSNs co-loaded with an antigen and Toll-like receptor 9 agonist, which exist in interparticle space of the MSR scaffold, are internalized by the recruited DCs, leading to the generation of antigen-presenting activated DCs. Strikingly, the MSR-MSN dual-scale vaccine generates a significantly larger number of antigen-specific T cells and inhibits melanoma growth to a greater extent compared with a single MSR or MSN vaccine. Moreover, the dual-scale vaccine is synergized with an immune checkpoint inhibitor to inhibit tumor growth in tumor-bearing mice. The findings suggest that the MSR is a novel platform for delivering nanoparticle vaccines for the enhancement of cancer immunotherapy.

摘要

尽管基于纳米颗粒的疫苗具有潜力,但其在癌症免疫治疗中的疗效有限。为了引发强大的抗原特异性适应性免疫反应,负载抗原的纳米颗粒被用于运输到宿主树突状细胞(DCs)中;然而,只有少数纳米颗粒能够被宿主DCs吞噬。在此,介绍一种由介孔二氧化硅微棒(MSRs)与介孔二氧化硅纳米颗粒(MSNs)偶联而成的可注射双尺度介孔二氧化硅疫苗。注射后,MSRs形成三维大孔支架,随后负载在MSRs介孔中的DC招募趋化因子的释放导致大量DCs被招募到支架中。随后,与抗原和Toll样受体9激动剂共同负载的MSNs存在于MSR支架的颗粒间空间中,被招募的DCs内化,导致产生抗原呈递活化的DCs。令人惊讶的是,与单一的MSR或MSN疫苗相比,MSR-MSN双尺度疫苗产生的抗原特异性T细胞数量显著更多,并且在更大程度上抑制黑色素瘤生长。此外,双尺度疫苗与免疫检查点抑制剂协同作用,以抑制荷瘤小鼠的肿瘤生长。这些发现表明,MSR是一种用于递送纳米颗粒疫苗以增强癌症免疫治疗的新型平台。

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