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YB-1 依赖性病毒疗法联合替莫唑胺作为一种多模态治疗方法,以根除恶性脑胶质瘤。

YB-1 dependent virotherapy in combination with temozolomide as a multimodal therapy approach to eradicate malignant glioma.

机构信息

Institut für Experimentelle Onkologie und Therapieforschung, Klinikum Rechts der Isar, Munich, Germany.

出版信息

Int J Cancer. 2011 Sep 1;129(5):1265-76. doi: 10.1002/ijc.25783. Epub 2011 Jan 6.

DOI:10.1002/ijc.25783
PMID:21710499
Abstract

The human Y-box binding protein 1 (YB-1) is known to be a promising target for cancer therapy. We have demonstrated that YB-1 plays an important role in the adenoviral life cycle by regulating the adenoviral E2-gene expression. Thus, we studied the oncolytic effect of the recombinant adenovirus Ad-Delo3-RGD, in which the transactivation domain CR3 of the E1A protein is ablated to enable viral replication only in YB-1 positive cancer cells. In vitro Southern Blot analysis and cytopathic effect assays demonstrate high anti-glioma potency, which was significantly increased in combination with temozolomide (TMZ), daunorubicin and cisplatin. Since vascular endothelial growth factor (VEGF) is thought to promote the hypervascular phenotype of primary, malignant brain tumors, we also tested Ad-Delo3-RGD in regard to the inhibition of VEGF expression. Indeed, we found that Ad-Delo3-RGD induced VEGF down regulation, which was even amplified under hypoxic conditions. Tumor-bearing nudemice treated with the YB-1 dependent oncolytic adenovirus showed significantly smaller tumors than untreated controls. Furthermore, combination therapy with TMZ led to a regression in all treated animals with complete tumor regression in 33 % of analyzed mice, which was verified by bioluminescence imaging and histological studies. In addition, histopathological evaluation revealed enhanced apoptosis and a reduction in tumor vessel formation, indicating that Ad-Delo3-RGD has an anti-angiogenic effect in addition to its oncolytic capacity in vivo. Hence, our results demonstrate that the combination therapy of YB-1 dependent virotherapy and TMZ is effective in a xenograft glioma mouse model and might be useful in a YB-1 based clinical setting.

摘要

人 Y 框结合蛋白 1(YB-1)已被证实是癌症治疗的一个有前途的靶点。我们已经证明,YB-1 通过调节腺病毒 E2 基因的表达,在腺病毒生命周期中发挥重要作用。因此,我们研究了重组腺病毒 Ad-Delo3-RGD 的溶瘤作用,其中 E1A 蛋白的转录激活域 CR3 被切除,以使病毒复制仅在 YB-1 阳性癌细胞中进行。体外 Southern Blot 分析和细胞病变效应试验表明,其对神经胶质瘤具有很强的杀伤作用,与替莫唑胺(TMZ)、柔红霉素和顺铂联合应用时,杀伤作用显著增强。由于血管内皮生长因子(VEGF)被认为促进了原发性恶性脑肿瘤的高血管表型,我们还测试了 Ad-Delo3-RGD 对 VEGF 表达的抑制作用。事实上,我们发现 Ad-Delo3-RGD 诱导 VEGF 下调,在缺氧条件下甚至被放大。用依赖 YB-1 的溶瘤腺病毒治疗的荷瘤裸鼠的肿瘤明显小于未治疗的对照组。此外,TMZ 联合治疗导致所有治疗动物的肿瘤消退,33%的分析小鼠完全消退,这通过生物发光成像和组织学研究得到了验证。此外,组织病理学评估显示凋亡增加和肿瘤血管形成减少,表明 Ad-Delo3-RGD 除了具有体内溶瘤能力外,还具有抗血管生成作用。因此,我们的研究结果表明,YB-1 依赖性病毒治疗和 TMZ 的联合治疗在异种移植神经胶质瘤小鼠模型中是有效的,并且在基于 YB-1 的临床环境中可能是有用的。

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