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Heterologous Prime-Boost Enhances the Antitumor Immune Response Elicited by Plant-Virus-Based Cancer Vaccine

机译:异源性初级增强增强植物病毒癌疫苗引发的抗肿瘤免疫应答

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摘要

New cancer vaccine strategies are required to vanquish the self-tolerance and elicit robust immune responses against tumor-associated antigens and/or neoantigens. Contemporary approaches in nanomedicine center on the use of a single nanocarrier modified with multiple copies of multiple different functional domains, e.g., epitopes for vaccines. Therefore, we set out to develop a combinatorial approach toward the next-generation concept of epitope delivery: a prime-boost strategy in which the same epitope is delivered using different nanocarriers. We tested this concept in the setting of HER2(+) breast cancer. We synthesized HER2-based cancer vaccines using three icosahedral plant viruses as carriers and evaluated the immune response as a result of repetitive, homologous immunization using BALB/c mice. Two of the vaccines induced a Th2-predominant response and the other a Th1-predominant response. To enhance the immunogenicity of the vaccines, we developed a heterologous prime-boost strategy with each of the vaccines administered only once, yielding higher titers of HER2-specific immunoglobulins and increasing the toxicity of the antisera toward cancer cells. The prime-boost also induced a Th1-predominant response. An in vivo tumor challenge showed that the prime-boost regimen reduced tumor growth and improved survival in mice. This novel strategy to elicit robust immune responses against weakly immunogenic antigens in principle could be broadly applicable to cancers and other diseases.
机译:需要新的癌症疫苗策略来突然耐受对肿瘤相关抗原和/或新抗原的自我容忍和促进肥力的免疫应答。纳米美床中心在使用多个不同功能域的多个拷贝的单个纳米载体中使用的当代方法,例如疫苗的表位。因此,我们旨在开发一种朝向表位递送的下一代概念的组合方法:使用不同的纳米载体递送相同表位的初始促进策略。我们在HER2(+)乳腺癌的设置中测试了这一概念。我们使用三个icosahral植物病毒作为载体来合成HER2的癌症疫苗,并根据使用BALB / C小鼠的重复,同源免疫的结果评估免疫应答。两个疫苗诱导Th2-主要反应,另一个疫苗和其他Th1主要反应。为了增强疫苗的免疫原性,我们开发了一种仅施用一次疫苗的异源性初级促进策略,从而产生高于HER2特异性免疫球蛋白的滴度,并增加抗血清对癌细胞的毒性。 Prime-Boost还诱导了Th1主要的反应。体内肿瘤挑战表明,素升压方案降低了肿瘤生长和改善小鼠的存活。这种新的策略以原则上引出弱免疫原性抗原的强大免疫反应可以广泛适用于癌症和其他疾病。

著录项

  • 来源
    《Journal of the American Chemical Society》 |2019年第16期|6509-6518|共10页
  • 作者单位

    Univ Calif San Diego Dept NanoEngn La Jolla CA 92093 USA|Case Western Reserve Univ Dept Biomed Engn 10900 Euclid Ave Cleveland OH 44106 USA;

    Univ Calif San Diego Dept NanoEngn La Jolla CA 92093 USA|Case Western Reserve Univ Dept Biomed Engn 10900 Euclid Ave Cleveland OH 44106 USA;

    Univ Calif San Diego Dept NanoEngn La Jolla CA 92093 USA|Case Western Reserve Univ Dept Biomed Engn 10900 Euclid Ave Cleveland OH 44106 USA;

    Sri Venkateswara Univ Dept Virol Tirupati 517502 Andhra Pradesh India;

    Univ Calif San Diego Dept NanoEngn La Jolla CA 92093 USA|Univ Calif San Diego Dept Radiol La Jolla CA 92093 USA|Univ Calif San Diego Dept Bioengn La Jolla CA 92093 USA|Univ Calif San Diego Moores Canc Ctr La Jolla CA 92093 USA|Case Western Reserve Univ Dept Biomed Engn 10900 Euclid Ave Cleveland OH 44106 USA;

  • 收录信息 美国《科学引文索引》(SCI);美国《工程索引》(EI);美国《生物学医学文摘》(MEDLINE);美国《化学文摘》(CA);
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  • 正文语种 eng
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