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A novel aptamer-based small RNA delivery platform and its application to cancer therapy
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作者 Toshihiko Tanno Peng Zhang +5 位作者 Christopher Bailey Yin Wang Wannaporn Ittiprasert Martin Devenport Pan Zheng Yang Liu 《Genes & Diseases》 SCIE CSCD 2023年第3期1075-1089,共15页
Major challenges such as nuclease degradation, rapid renal clearance, non-specific delivery, poor cellular uptake and inflammatory response have limited the clinical application of small RNA-mediated gene silencing. T... Major challenges such as nuclease degradation, rapid renal clearance, non-specific delivery, poor cellular uptake and inflammatory response have limited the clinical application of small RNA-mediated gene silencing. To overcome these challenges, we designed a novel targeting small RNA delivery platform comprising of three oligonucleotides: (1) a guide RNA sequence, (2) part of a passenger sequence linked to a DNA aptamer via a PEG linker, and (3) another passenger sequence conjugated to cholesterol, which assemble through complementary base pair annealing. Remarkably, in the presence of magnesium, this molecule self-assembled into a nanoparticle with a hydrophobic cholesterol core, hydrophilic RNA oligonucleotide shell and PEG-linked DNA aptamer flare. The nanoparticles conferred protection to the RNA oligonucleotides against nuclease degradation, which increased bioavailability, and reduced systemic inflammatory responses. The aptamer allowed targeted delivery of RNA therapeutics through cell-specific surface markers, and once inside the cell, the nanoparticles induced lysosomal leakage that released the RNA oligonucleotides into the cytosol to achieve gene silencing. We created a c-Kit-targeting miR-26a delivery particle that specifically accumulated in c-Kit^(+) breast cancer, significantly increased T cell recruitment, and inhibited tumor growth. Regression of large established tumors were achieved when the nanoparticle was used in combination with anti-CTLA-4 monoclonal antibody. 展开更多
关键词 APTAMER Cancer Micellar nanoparticle miRNA Tar get delivery
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CD24Fc ameliorates immune-related adverse events while preserving anti-tumor therapeutic effect
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作者 Mingyue Liu Xu Wang +7 位作者 Xuexiang Du Yan Zhang Chunxia Ai Siwen Hu-Lieskovan Tianhong Li Martin Devenport Yang Liu Pan Zheng 《Signal Transduction and Targeted Therapy》 SCIE CSCD 2022年第8期2701-2703,共3页
Dear Editor,In combination,anti-CTLA-4 and anti-PD-1 mAb provide the most effective immunotherapy,although severe immune-related adverse events(irAEs)also occur at high frequency.1 It is urgent to develop strategies t... Dear Editor,In combination,anti-CTLA-4 and anti-PD-1 mAb provide the most effective immunotherapy,although severe immune-related adverse events(irAEs)also occur at high frequency.1 It is urgent to develop strategies to reduce irAEs for wide-spread adoption of immune checkpoint inhibitors(ICIs). 展开更多
关键词 PRESERVING CD24 URGENT
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