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Biomaterial nanoparticles redistribute therapeutic antibodies to lymph node-resident cells to enhance cancer immunotherapy via checkpoint inhibition

机译:生物材料纳米颗粒将治疗性抗体重新分配至淋巴结驻留细胞,以通过检查点抑制增强癌症免疫疗法

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We have demonstrated the ability to conjugate mAbs to lymphatic draining synthetic polymer NPs using a solvent- and denaturation-free disulfide displacement chemistry. NP conjugation enhances IgG accumulation within LNs draining the skin site of injection and lowers levels of IgG accumulation in off-target tissues. We have demonstrated the ability to reduce melanoma tumor growth using aCTLA4-NPs. These data suggest the potential of mAbs-NPs to increase the efficacy of checkpoint blockade for the treatment of advanced cancers through enhanced tumor retention and sentinel lymph node drug targeting.
机译:我们已经证明了使用无溶剂和无变性的二硫键置换化学方法将单克隆抗体与淋巴引流合成聚合物NPs缀合的能力。 NP缀合增强了LN内的IgG积累,从而耗尽了注射的皮肤部位,并降低了脱靶组织中IgG的积累水平。我们已经证明了使用aCTLA4-NP减少黑色素瘤肿瘤生长的能力。这些数据表明mAbs-NPs通过增强的肿瘤保留和前哨淋巴结药物靶向来提高检查点封锁治疗晚期癌症的功效。

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