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Targeting Localized Immune Suppression Within the Tumor Through Repeat Cycles of Immune Cell-oncolytic Virus Combination Therapy

机译:通过重复周期的免疫细胞溶瘤病毒联合治疗靶向靶向肿瘤内的局部免疫抑制。

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摘要

A major limitation to the use of immunotherapy in the treatment of cancer has been the localized immune suppressive environment within the tumor. Although there is evidence that tumor-selective (oncolytic) viruses may help to overcome this immune suppression, a primary limitation to their use has been limited systemic delivery potential, especially in the face of antiviral immunity. We recently demonstrated that tumor-trafficking immune cells can efficiently deliver oncolytic viral therapies to their tumor targets. These cells act as both a therapeutic agent and also a carrier vehicle for the oncolytic virus. Here, we demonstrate that such delivery is also possible in the face of pre-existing antiviral immunity, so overcoming the limited systemic delivery of naked, cell-free virus. It was also found that treatment of previously immunized mice or repeat treatments leading to immunization resulted in a switch from a primarily oncolytic to an immunotherapeutic mechanism of action. Furthermore, repeat cycles of treatment with combination immune cell-viral therapy resulted in increased tumor infiltration of effector T-cells and a general reduction in the levels of known immune suppressive lymphocyte populations. This therefore represents a novel and effective means to overcome localized immune suppression within the tumor micoenvironment.
机译:在癌症的治疗中使用免疫疗法的主要限制是肿瘤内的局部免疫抑制环境。尽管有证据表明肿瘤选择性(溶瘤性)病毒可能有助于克服这种免疫抑制,但其使用的主要限制是全身递送潜力有限,尤其是面对抗病毒免疫时。我们最近证明,贩运肿瘤的免疫细胞可以有效地将溶瘤性病毒疗法传递给其肿瘤靶标。这些细胞既是溶瘤病毒的治疗剂又是载体。在这里,我们证明面对已有的抗病毒免疫,这种递送也是可能的,因此克服了裸露,无细胞病毒的有限全身递送。还发现对先前免疫的小鼠的治疗或导致免疫的重复治疗导致从最初的溶瘤作用向免疫治疗作用机制的转变。此外,用免疫细胞-病毒联合治疗的重复周期导致效应T细胞的肿瘤浸润增加,并且已知免疫抑制性淋巴细胞群体的水平普遍降低。因此,这代表了克服肿瘤微环境内局部免疫抑制的新颖有效的手段。

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