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首页> 美国卫生研究院文献>Journal of Biomedical Research >Antitumor efficacy of multi-target in situ vaccinations with CpG oligodeoxynucleotides anti-OX40 anti-PD1 antibodies and aptamers
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Antitumor efficacy of multi-target in situ vaccinations with CpG oligodeoxynucleotides anti-OX40 anti-PD1 antibodies and aptamers

机译:使用 CpG 寡脱氧核苷酸、抗 OX40、抗 PD1 抗体和适配子进行多靶点原位疫苗接种的抗肿瘤疗效

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To overcome immune tolerance to cancer, the immune system needs to be exposed to a multi-target action intervention. Here, we investigated the activating effect of CpG oligodeoxynucleotides (ODNs), mesyl phosphoramidate CpG ODNs, anti-OX40 antibodies, and OX40 RNA aptamers on major populations of immunocompetent cells ex vivo. Comparative analysis of the antitumor effects of in situ vaccination with CpG ODNs and anti-OX40 antibodies, as well as several other combinations, such as mesyl phosphoramidate CpG ODNs and OX40 RNA aptamers, was conducted. Antibodies against programmed death 1 (PD1) checkpoint inhibitors or their corresponding PD1 DNA aptamers were also added to vaccination regimens for analytical purposes. Four scenarios were considered: a weakly immunogenic Krebs-2 carcinoma grafted in CBA mice; a moderately immunogenic Lewis carcinoma grafted in C57Black/6 mice; and an immunogenic A20 B cell lymphoma or an Ehrlich carcinoma grafted in BALB/c mice. Adding anti-PD1 antibodies (CpG+αOX40+αPD1) to in situ vaccinations boosts the antitumor effect. When to be used instead of antibodies, aptamers also possess antitumor activity, although this effect was less pronounced. The strongest effect across all the tumors was observed in highly immunogenic A20 B cell lymphoma and Ehrlich carcinoma.
机译:为了克服对癌症的免疫耐受,免疫系统需要接受多靶点作用干预。在这里,我们研究了 CpG 寡脱氧核苷酸 (ODN)、甲基磷酸盐 CpG ODN、抗 OX40 抗体和 OX40 RNA 适配体对体外免疫活性细胞主要群体的激活作用。对 CpG ODNs 和抗 OX40 抗体以及其他几种组合(如甲基磷酰胺 CpG ODNs 和 OX40 RNA 适配体)原位疫苗接种的抗肿瘤效果进行了比较分析。针对程序性死亡 1 (PD1) 检查点抑制剂或其相应的 PD1 DNA 适配体的抗体也被添加到疫苗接种方案中用于分析目的。考虑了四种情况:CBA 小鼠移植的弱免疫原性 Krebs-2 癌;移植到 C57Black/6 小鼠中的中度免疫原性 Lewis 癌;以及 BALB/c 小鼠移植的免疫原性 A20 B 细胞淋巴瘤或 Ehrlich 癌。在原位疫苗接种中添加抗 PD1 抗体 (CpG+αOX40+αPD1) 可增强抗肿瘤效果。当使用适配体代替抗体时,适配体也具有抗肿瘤活性,尽管这种效果不太明显。在所有肿瘤中观察到最强的效果是在高免疫原性 A20 B 细胞淋巴瘤和 Ehrlich 癌中观察到的。

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