In vivo pro-apoptotic and antitumor efficacy of a c-Raf antisense phosphorothioate oligonucleotide: relationship to tumor size.

Antisense & nucleic acid drug development Pub Date : 2002-02-01 DOI:10.1089/108729002753670229

Q. Lau, T. Achenbach, Oliver Borchers, R. Müller, E. Slater

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引用次数: 9

Abstract

Previously, we have shown that a phosphorothioate antisense oligonucleotide (ODN) targeted against c-raf RNA (ISIS5132; cRaf-AS) induces apoptosis in human tumor cells. We now show that the same ODN also efficiently triggers apoptosis in human tumor xenografts in nu/nu mice. Although cRaf-AS showed a clearly inhibitory effect on the growth of established tumors (approximately 150 mm3) compared to a mismatched control ODN (MM), tumor progression was not prevented. This correlated with a partial refractoriness of the tumor to cRaf-AS-induced cell killing, which seemed to be due to an inhomogeneous and inefficient penetration of the ODN into the tumor tissue rather than cellular resistance. In agreement with this conclusion, we found that growth of small tumors (<50 mm3) was completely inhibited concomitantly with an accumulation of the ODN throughout the tumor. These data show that the cRaf-AS is a highly efficacious antitumor agent, provided accessibility into the tumor tissue is warranted, and suggest that PS-AS-ODN treatment may be particularly useful in an adjuvant setting.

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c-Raf反义硫代寡核苷酸的体内促凋亡和抗肿瘤作用:与肿瘤大小的关系。

在此之前，我们已经证明了一种靶向c-raf RNA的硫代反义寡核苷酸(ODN) (ISIS5132;craft - as)诱导人肿瘤细胞凋亡。我们现在发现，同样的ODN也能有效地触发nu/nu小鼠的人类肿瘤异种移植物的细胞凋亡。虽然与不匹配的对照ODN (MM)相比，craft - as对已建立的肿瘤(约150 mm3)的生长有明显的抑制作用，但并没有阻止肿瘤的进展。这与肿瘤对craft - as诱导的细胞杀伤的部分难耐相关，这似乎是由于ODN进入肿瘤组织的不均匀和低效渗透，而不是细胞抵抗。与这一结论一致，我们发现小肿瘤(<50 mm3)的生长完全被抑制，同时ODN在整个肿瘤中积累。这些数据表明，只要保证能进入肿瘤组织，craft - as是一种非常有效的抗肿瘤药物，并表明PS-AS-ODN治疗在辅助治疗中可能特别有用。

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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Antisense & nucleic acid drug development

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