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Feasibility of Applying Helper-Dependent Adenoviral Vectors for Cancer Immunotherapy

机译:应用辅助依赖型腺病毒载体进行癌症免疫治疗的可行性

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摘要

Adenoviruses (Ads) infect a broad range of tissue types, and derived vectors have been extensively used for gene therapy. Helper-dependent Ad vectors (HDAds), devoid of viral coding sequences, allow for insertion of large or multiple transgenes in a single vector and have been preclinically used for the study of genetic disorders. However, the clinical application of Ad vectors including HDAds for genetic disorders has been hampered by an acute toxic response. This characteristic, while disadvantageous for gene replacement therapy, could be strategically advantageous for the activation of an immune response if HDAds were used as an adjunct treatment in cancer. Cancer treatments including immunotherapy are frequently limited by the inhibitory environment produced by both tumors and their stroma, each of which express numerous inhibitory molecules. Hence, multiple inhibitory mechanisms must be overcome for development of anti-tumor immunity. The large coding capacity of HDAds can accommodate multiple immune modulating transgenes that could produce a combined effect to overcome tumor-derived inhibition and ensure intratumoral effector T-cell proliferation and function. In this review, we discuss the potential advantages of HDAds to cancer immunotherapy based on potent host immune responses to Ads.
机译:腺病毒(Ads)感染广泛的组织类型,并且衍生的载体已广泛用于基因治疗。缺乏病毒编码序列的辅助依赖型Ad载体(HDAds)可在单个载体中插入较大或多个转基因,并且已在临床上用于遗传疾病的研究。然而,包括HDAds在内的Ad载体在遗传疾病中的临床应用受到急性毒性反应的阻碍。如果将HDAds用作癌症的辅助治疗,则该特征尽管不利于基因替代疗法,但对于激活免疫应答可能在策略上有利。包括免疫疗法在内的癌症治疗常常受到肿瘤及其间质产生的抑制环境的限制,它们各自表达许多抑制分子。因此,必须克服多种抑制机制才能发展抗肿瘤免疫力。 HDAds的高编码能力可以容纳多个免疫调节转基因,这些转基因可以产生组合效应,从而克服肿瘤衍生的抑制作用并确保肿瘤内效应子T细胞增殖和功能。在这篇综述中,我们将基于对Ads的强大宿主免疫反应,讨论HDAds在癌症免疫治疗中的潜在优势。

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