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當(dāng)前位置:首頁(yè) > 新聞中心 > 中國(guó)藥科大學(xué)使用IPHASE產(chǎn)品發(fā)表高質(zhì)量文章(IF=14.6)

中國(guó)藥科大學(xué)使用IPHASE產(chǎn)品發(fā)表高質(zhì)量文章(IF=14.6)

更新時(shí)間:2025-12-17      點(diǎn)擊次數(shù):29

近日,中國(guó)藥科大學(xué)韓超課題組趙雨老師,使用IPHASE品牌產(chǎn)品:人CD4+T細(xì)胞、人pbmc、小鼠CD4+T細(xì)胞在《Acta Pharmaceutica Sinica B》權(quán)-威期刊上發(fā)表文章《LSD1 inhibition sensitizes anti-PD1 blockade immunotherapy by inhibiting the long-range attack of tumor-derived extracellular vesicles》,影響因子14.6!


摘要

Platinum-based drugs (Pt drugs) are widely used in cancer chemotherapy, yet their genome-wide binding patterns remain incompletely understood. Here, we present Pt sequencing (Pt-seq), an antibody-assisted, genomewide method for mapping Pt-DNA adducts at single-base resolution. By using exo- and endonucleases to remove background, Pt-seq enables robust and sensitive profiling of binding sites for cisplatin, oxaliplatin, lobaplatin, and a Pt(IV) complex. Using Pt-seq, we identified tens to hundreds of binding clusters that are 10 to 20 kilobases in median length and highly consistent among different drugs, predominantly localizing to centromeric and ribosomal DNA regions. In cisplatin-resistant cells, we found significantly reduced binding within these regions. Moreover, we found that mutations in cancer cells can generate previously unidentified binding sites. On this basis, we demonstrated that ICR-191, an acridine orange compound capable of inducing G insertions, enhances cisplatinDNA binding and sensitizes

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