首页> 美国卫生研究院文献>PLoS Clinical Trials >CD40-Activated B Cell Cancer Vaccine Improves Second Clinical Remission and Survival in Privately Owned Dogs with Non-Hodgkin's Lymphoma
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CD40-Activated B Cell Cancer Vaccine Improves Second Clinical Remission and Survival in Privately Owned Dogs with Non-Hodgkin's Lymphoma

机译:CD40激活的B细胞癌疫苗可改善非霍奇金淋巴瘤私人犬的第二次临床缓解和生存率。

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摘要

Cell-based active immunotherapy for cancer is a promising novel strategy, with the first dendritic cell (DC) vaccine achieving regulatory approval for clinical use last year. Manufacturing remains arduous, especially for DC vaccines, and the prospect of using cell-based immunotherapy in the adjuvant setting or in combination with chemotherapy remains largely untested. Here, we used a comparative oncology approach to test the safety and potential efficacy of tumor RNA-loaded, CD40-activated B cells in privately owned dogs presenting with non-Hodgkin's lymphoma (NHL), a clinical scenario that represents not only a major problem in veterinary medicine but also a bona fide spontaneous animal model for the human condition. When administered to NHL dogs in remission after induction chemotherapy, CD40-B cells electroporated ex vivo with autologous tumor RNA safely stimulated immunity in vivo. Although chemotherapy plus CD40-B vaccination did not improve time-to-progression or lymphoma-specific survival compared to dogs treated with chemotherapy alone, vaccination potentiated the effects of salvage therapy and improved the rate of durable second remissions as well as subsequent lymphoma-specific survival following salvage therapy. Several of these relapsed dogs are now long-term survivors and free of disease for more than a year. Overall, these clinical and immunological results suggest that cell-based CD40 cancer vaccination is safe and synergizes with chemotherapy to improve clinical outcome in canine NHL. More broadly, our findings underscore the unique value of clinical investigations in tumor-bearing companion animals.
机译:基于细胞的癌症主动免疫疗法是一种有前途的新策略,去年首款树突状细胞(DC)疫苗获得了监管部门的批准,可用于临床。制造仍然是艰巨的,特别是对于DC疫苗,并且在佐剂环境中或与化学疗法结合使用基于细胞的免疫疗法的前景仍然未经测试。在这里,我们使用了比较肿瘤学的方法来测试患有非霍奇金淋巴瘤(NHL)的私人狗中荷有肿瘤RNA的CD40激活的B细胞的安全性和潜在疗效,这种临床情况不仅代表主要问题在兽医学上也是人类真正的自发自然动物模型。当对NHL犬进行诱导化疗后缓解时,用自体肿瘤RNA体外电穿孔的CD40-B细胞可安全地刺激体内免疫力。尽管与单独用化学疗法治疗的狗相比,化学疗法加上CD40-B疫苗接种并未改善进展时间或特定于淋巴瘤的存活率,但接种疫苗增强了挽救疗法的效果,并提高了持久性第二次缓解率以及随后的淋巴瘤特异性抢救治疗后的生存率。这些复发的狗中有几只现在是长期幸存者,并且一年以上没有疾病。总体而言,这些临床和免疫学结果表明,基于细胞的CD40癌症疫苗接种是安全的,并且与化学疗法协同作用可改善犬NHL的临床结局。更广泛地说,我们的发现强调了在荷瘤伴侣动物中进行临床研究的独特价值。

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