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CK2的下调诱导癌细胞凋亡——一种潜在的癌症治疗方法。

Downregulation of CK2 induces apoptosis in cancer cells--a potential approach to cancer therapy.

作者信息

Wang Guixia, Unger Gretchen, Ahmad Kashif A, Slaton Joel W, Ahmed Khalil

机构信息

Cellular and Molecular Biochemistry Research Laboratory (151), Minneapolis Veterans Affairs Medical Center, Minneapolis, MN 55417, USA.

出版信息

Mol Cell Biochem. 2005 Jun;274(1-2):77-84. doi: 10.1007/s11010-005-3077-1.

Abstract

We have previously documented that naked antisense CK2alpha ODN can potently induce apoptosis in cancer cells in culture and in mouse xenograft human prostate cancer. The effects of the antisense CK2alpha are related to downregulation of CK2alpha message and rapid loss of the CK2 from the nuclear compartment. Here we demonstrate that downregulation of CK2 elicited by diverse methods leads to inhibition of cell growth and induction of apoptosis. The various approaches to downregulation of CK2 employed were transfection with kinase-inactive plasmid, use of CK2alpha siRNA, use of inhibitors of CK2 activity, and use of antisense CK2alpha ODN packaged in sub-50 nm nanocapsules made from tenascin. In all cases, the downregulation of CK2 is associated with loss in cell survival. We have also described preliminary observations on an approach to targeting CK2 in cancer cells. For this, sub-50 nm tenascin-based nanocapsules bearing the antisense CK2alpha ODN were employed to test that the antisense is delivered to the cancer cells in vivo. The results provide the first preliminary evidence that such an approach may be feasible for targeting CK2 in cancer cells. Together, our results suggest that CK2 is potentially a highly plausible target for cancer therapy.

摘要

我们之前已证明,裸反义CK2α寡脱氧核苷酸(ODN)可在培养的癌细胞以及小鼠异种移植人前列腺癌模型中有效诱导细胞凋亡。反义CK2α的作用与CK2α信使核糖核酸(mRNA)的下调以及CK2从细胞核区室的快速丢失有关。在此,我们证明通过多种方法引发的CK2下调会导致细胞生长抑制和细胞凋亡诱导。用于下调CK2的各种方法包括用激酶失活质粒转染、使用CK2α小干扰RNA(siRNA)、使用CK2活性抑制剂以及使用包装在由肌腱蛋白制成的50纳米以下纳米胶囊中的反义CK2α ODN。在所有情况下,CK2的下调都与细胞存活能力的丧失相关。我们还描述了一种针对癌细胞中CK2的方法的初步观察结果。为此,使用携带反义CK2α ODN的50纳米以下基于肌腱蛋白的纳米胶囊来测试反义分子在体内是否能递送至癌细胞。结果提供了首个初步证据,表明这种方法可能对于在癌细胞中靶向CK2是可行的。总之,我们的结果表明CK2可能是癌症治疗的一个非常合理的靶点。

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