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Neoantigen enriched biomimetic nanovaccine for personalized cancer immunotherapy

Nature Communications. 2025-05; 
Yuwei Li, Maoxin Fang, Haotian Yu, Xianglei Wang, Shiyao Xue, Zeze Jiang, Zixuan Huang, Shaoqin Rong, Xiaoli Wei, Zhigang Lu, Min Luo Institute of Pediatrics of Children's Hospital of Fudan University, the Shanghai Key Laboratory of Medical Epigenetics, the International Co-laboratory of Medical Epigenetics and Metabolism, Ministry of Science and Technology, Institutes of Biomedical Sciences, Fudan University, Shanghai, China.
Products/Services Used Details Operation
Peptide Synthesis OVA257–264 peptide was purchased from Genscript (Nanjing, China). Gp70423-431(AH1, SPSYVYHQF), Gp10021–41 (VGALEGSRNQDWLGVPRQLVT), Trp1214–237 (SHEGPAF LTWHRYHLLQLERDMQE), Trp2173–196 (QPQIANCSVYDFFVWLHYYSVRDT), B16-M27(REGVELCPGNKYEMRRHGTTHSLVIHD), B16-M33 (DSGSPFPAAVILRDALH MARGLKYLHQ), Rpl18115-132 (KAGGKILTFDRLALESPK), AdpgkR304M (GIPVHLELA SMTNMELMSSIVHQQVFPT), and CT26-M19 (QAIVRGCSMPGPWRSGRLLVSRR WSVE) were synthesised by Genscript (Nanjing, China). Get A Quote

摘要

Personalized cancer vaccines elicit robust T cell immunity and anti-tumour potency, but identifying tumour-specific antigens remains challenging, severely constraining the therapeutic window. Biomimetic nanovaccines employing cancer cell membranes display inherent biocompatibility and stimulate T-cell responses against diverse tumour antigens, though tumours develop multiple mechanisms to reduce antigen presentation. Here we demonstrate a rapid and general strategy to fabricate personalized nanovaccines based on Antigen-Enriched tumor Cell Membranes (AECM) for early intervention. Interferon-γ potently stimulates antigen presentation across a broad range of cancer cell types. By coupling the generated AECM with... More

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