Macrophage Delivered HSV1716 Is Active against Triple Negative Breast Cancer

A. Kwan, Faith H N Howard, Natalie Winder, E. Atkinson, Ameera B A Jailani, Priya B. Patel, Richard Allen, P. Ottewell, G. Shaw, J. Conner, Caroline Wilson, S. Srivastava, S. Danson, Claire Lewis, Janet E Brown, M. Muthana
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Abstract

Oncolytic viruses (OV) promote anti-tumour responses through the initiation of immunogenic cancer cell death which activates the host’s systemic anti-tumour immunity. We have previously shown that intravenously administered HSV1716 is an effective treatment for mammary cancer. However, intravenous administration of a virus has the potential to result in neutralization and sequestration of the virus which may reduce efficacy. Here, we show that the oncolytic virus HSV1716 can be administered within a cellular carrier (macrophages). PyMT and 4T1 murine mammary cancer cell lines were implanted into immuno-competent murine models (orthotopic primary, early metastatic and brain metastasis models). HSV1716 or macrophages armed with HSV1716 (M-HSV1716) were administered intravenously, and tumour size was quantified using caliper measurement or bioluminescence imaging. Administration of M-HSV1716 led to tumour shrinkage and increased the survival of animals. Furthermore, these results were achieved with a 100-fold lower viral load, which has the potential for decreased toxicity. Our results demonstrate that M-HSV1716 is associated with activity against murine mammary cancers and provides an alternative platform for the systemic delivery of OV.
巨噬细胞传递的HSV1716对三阴性乳腺癌有活性
溶瘤病毒(OV)通过启动免疫原性癌细胞死亡来促进抗肿瘤反应,从而激活宿主的全身抗肿瘤免疫。我们之前已经证明静脉注射HSV1716是一种有效的治疗乳腺癌的方法。然而,静脉注射病毒有可能导致病毒的中和和隔离,从而降低疗效。在这里,我们证明溶瘤病毒HSV1716可以在细胞载体(巨噬细胞)内施用。将PyMT和4T1小鼠乳腺癌细胞系植入免疫功能小鼠模型(原位原发、早期转移和脑转移模型)。静脉注射HSV1716或携带HSV1716的巨噬细胞(M-HSV1716),用卡尺测量或生物发光成像定量肿瘤大小。M-HSV1716可导致肿瘤缩小,提高动物存活率。此外,这些结果是在病毒载量降低100倍的情况下实现的,这有可能降低毒性。我们的研究结果表明,M-HSV1716与抗小鼠乳腺癌的活性有关,并为OV的全身递送提供了另一种平台。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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