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Efficient antitumor effects of a novel oncolytic adenovirus fully composed of species B adenovirus serotype 35

机译:高效抗肿瘤患者含有物种B腺病毒血清型35的新型糖尿病腺病毒

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Oncolytic adenoviruses (OAds) are among the most promising oncolytic viruses. Almost all oncolytic adenoviruses are composed of human adenovirus serotype 5 (Ad5) (OAd5). However, expression of the primary infection receptor for Ad5, coxsackievirus-adenovirus receptor (CAR), often declines on malignant tumor cells, resulting in inefficient infection in CAR-negative tumor cells. In addition, at least 80% of adults have neutralizing antibodies against Ad5. In this study, we developed a novel OAd fully composed of OAd35. OAd35 recognizes CD46, which is ubiquitously expressed on almost all human cells and is often upregulated on malignant tumor cells, as an infection receptor. Moreover, 20% or fewer adults have neutralizing antibodies against Ad35. OAd35 mediated efficient cell lysis activities at levels similar to OAd5 in CAR-positive tumor cells, while OAd35 showed higher levels of cell lysis activities than OAd5 in CAR-negative tumor cells. Anti-Ad5 serum significantly inhibited in?vitro tumor cell lysis activities of OAd5, whereas OAd35 exhibited comparable levels of in?vitro tumor cell lysis activities in the presence of anti-Ad5 and naive serum. OAd35 significantly suppressed growth of the subcutaneous CAR-positive and CAR-negative tumors following intratumoral administration. These results indicated that OAd35 is a promising alternative oncolytic virus for OAd5.
机译:溶瘤腺病毒(OADS)是最有前途的溶解病毒之一。几乎所有葡萄酒腺病毒由人腺病毒血清型5(AD5)(OAD5)组成。然而,AD5的主要感染受体的表达,Coxsackievirus-腺病毒受体(轿车)经常在恶性肿瘤细胞上下降,导致车载阴性肿瘤细胞中的效率低下。此外,至少80%的成年人已经对AD5中和抗体。在这项研究中,我们开发了一种完全由OAD35组成的新型OAD。 OAD35识别CD46,其在几乎所有人体细胞上普遍地表达,并且通常对恶性肿瘤细胞进行上调,作为感染受体。此外,20%或更少的成年人对AD35的中和抗体进行了中和。 OAD35介导的高效细胞裂解活性与OAD5在汽车阳性肿瘤细胞中的水平,而OAD35在车载阴性肿瘤细胞中显示出比OAD5更高水平的细胞裂解活性。抗AD5血清在OAD5的体外肿瘤细胞裂解活性中显着抑制,而OAD35在抗AD5和幼稚血清存在下表现出体外肿瘤细胞裂解活性的相当水平。 OAD35在肿瘤内给药后显着抑制了皮下汽车阳性和尸体肿瘤的生长。这些结果表明OAD35是OAD5的有希望的溶解病毒。

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