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Induction of melanoma cell apoptosis and inhibition of tumor growth using a cell-permeable Survivin antagonist.使用一种可穿透细胞的Survivin拮抗剂诱导黑色素瘤细胞凋亡并抑制肿瘤生长。
Oncogene. 2006 Nov 2;25(52):6968-74. doi: 10.1038/sj.onc.1209676. Epub 2006 May 15.
2
Construction, expression, and purification of HIV-TAT-survivin (T34A) mutant: a pro-apoptosis protein in Escherichia coli.HIV-TAT-生存素(T34A)突变体在大肠杆菌中的构建、表达及纯化:一种促凋亡蛋白
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High-level expression, purification and pro-apoptosis activity of HIV-TAT-survivin (T34A) mutant to cancer cells in vitro.HIV-TAT-生存素(T34A)突变体在体外对癌细胞的高表达、纯化及促凋亡活性
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Extracellular, cell-permeable survivin inhibits apoptosis while promoting proliferative and metastatic potential.细胞外、可透过细胞膜的生存素可抑制细胞凋亡,同时促进增殖和转移潜能。
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A single amino acid change (Asp 53 --> Ala53) converts Survivin from anti-apoptotic to pro-apoptotic.单个氨基酸变化(天冬氨酸53位→丙氨酸53位)可使生存素由抗凋亡转变为促凋亡。
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[Preparation of recombinant HIV-TATm-survivin (T34A) protein and its pro-apoptosis activity to cancer cells in vitro].重组HIV-TATm-生存素(T34A)蛋白的制备及其对癌细胞的体外促凋亡活性
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Survivin-responsive conditionally replicating adenovirus kills rhabdomyosarcoma stem cells more efficiently than their progeny.Survivin 反应性条件复制腺病毒比其后代更有效地杀死横纹肌肉瘤干细胞。
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The Ectopic Expression of SurvivinT34A and FilC Can Enhance the Oncolytic Effects of Vaccinia Virus in Murine Gastric Cancer.生存素T34A和FilC的异位表达可增强痘苗病毒对小鼠胃癌的溶瘤作用。
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Targeting survivin in cancer: novel drug development approaches.靶向生存素治疗癌症:新型药物研发方法。
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The Antitumor Activity of Antrodia camphorata in Melanoma Cells: Modulation of Wnt/β-Catenin Signaling Pathways.樟芝抗肿瘤活性的研究进展:对 Wnt/β-连环蛋白信号通路的调控。
Evid Based Complement Alternat Med. 2012;2012:197309. doi: 10.1155/2012/197309. Epub 2012 Sep 25.
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Survivin inhibition by an interacting recombinant peptide, derived from the human ferritin heavy chain, impedes tumor cell growth.来源于人铁蛋白重链的相互作用重组肽抑制生存素可阻碍肿瘤细胞生长。
J Cancer Res Clin Oncol. 2012 Jul;138(7):1205-20. doi: 10.1007/s00432-012-1195-1. Epub 2012 Mar 18.
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Survivin-T34A: molecular mechanism and therapeutic potential.生存素-T34A:分子机制与治疗潜力
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The potential role of vitamin D in the progression of benign and malignant melanocytic neoplasms.维生素 D 在良性和恶性黑色素细胞肿瘤进展中的潜在作用。
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本文引用的文献

1
Chromosome alignment and segregation regulated by ubiquitination of survivin.生存素的泛素化调控染色体排列与分离。
Science. 2005 Dec 2;310(5753):1499-504. doi: 10.1126/science.1120160.
2
Survivin expression by metastatic melanoma predicts poor disease outcome in patients receiving adjuvant polyvalent vaccine.转移性黑色素瘤中Survivin的表达预示着接受辅助多价疫苗治疗的患者疾病预后不良。
Int J Cancer. 2005 Dec 20;117(6):1032-8. doi: 10.1002/ijc.21267.
3
Rational design of shepherdin, a novel anticancer agent.新型抗癌药物希普丁的合理设计
Cancer Cell. 2005 May;7(5):457-68. doi: 10.1016/j.ccr.2005.03.035.
4
Survivin splice variants regulate the balance between proliferation and cell death.生存素剪接变体调节细胞增殖与细胞死亡之间的平衡。
Oncogene. 2005 Mar 17;24(12):1994-2007. doi: 10.1038/sj.onc.1208350.
5
Silencing of antiapoptotic survivin gene by multiple approaches of RNA interference technology.通过RNA干扰技术的多种方法使抗凋亡生存素基因沉默。
Biotechniques. 2004 Mar;36(3):450-4, 456-60. doi: 10.2144/04363RR01.
6
Rapid induction of mitochondrial events and caspase-independent apoptosis in Survivin-targeted melanoma cells.Survivin靶向的黑色素瘤细胞中线粒体事件和非半胱天冬酶依赖性凋亡的快速诱导。
Oncogene. 2004 Jan 8;23(1):39-48. doi: 10.1038/sj.onc.1206978.
7
Survivin, versatile modulation of cell division and apoptosis in cancer.存活素,癌症中细胞分裂与凋亡的多功能调控
Oncogene. 2003 Nov 24;22(53):8581-9. doi: 10.1038/sj.onc.1207113.
8
Regulation of survivin function by Hsp90.热休克蛋白90对生存素功能的调控
Proc Natl Acad Sci U S A. 2003 Nov 25;100(24):13791-6. doi: 10.1073/pnas.2434345100. Epub 2003 Nov 12.
9
Acute ablation of survivin uncovers p53-dependent mitotic checkpoint functions and control of mitochondrial apoptosis.生存素的急性消融揭示了p53依赖的有丝分裂检查点功能和线粒体凋亡的调控。
J Biol Chem. 2004 Jan 16;279(3):2077-84. doi: 10.1074/jbc.M309479200. Epub 2003 Oct 27.
10
Constitutive mitogen-activated protein kinase activation in melanoma is mediated by both BRAF mutations and autocrine growth factor stimulation.黑色素瘤中组成型丝裂原活化蛋白激酶的激活是由BRAF突变和自分泌生长因子刺激共同介导的。
Cancer Res. 2003 Feb 15;63(4):756-9.

使用一种可穿透细胞的Survivin拮抗剂诱导黑色素瘤细胞凋亡并抑制肿瘤生长。

Induction of melanoma cell apoptosis and inhibition of tumor growth using a cell-permeable Survivin antagonist.

作者信息

Yan H, Thomas J, Liu T, Raj D, London N, Tandeski T, Leachman S A, Lee R M, Grossman D

机构信息

Huntsman Cancer Institute, University of Utah, Salt Lake City, UT 84112, USA.

出版信息

Oncogene. 2006 Nov 2;25(52):6968-74. doi: 10.1038/sj.onc.1209676. Epub 2006 May 15.

DOI:10.1038/sj.onc.1209676
PMID:16702945
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2292411/
Abstract

The inhibitor of apoptosis gene family member Survivin is highly expressed in most tumors, and appears to be a promising target for cancer therapy. Although a variety of Survivin antagonists have been shown to induce apoptosis in malignant cells, the potential utility of these agents is limited by inefficient delivery and cell impermeability. We generated recombinant fusion proteins containing the TAT protein transduction domain and either wild-type Survivin (TAT-Surv-WT) or a dominant-negative mutant (TAT-Surv-T34A). The TAT-Surv proteins were purified by sequential affinity and ion-exchange chromatography, and at 30 nM concentration demonstrated rapid entry into cells at 30 min. Whereas TAT-Surv-WT had minimal effect on YUSAC2 or WM793 melanoma cells, TAT-Surv-T34A induced cell detachment, DNA fragmentation, caspase-3 activation and mitochondrial release of apoptosis-inducing factor at low microM concentrations. Intraperitoneal (i.p.) injection of mice bearing subcutaneous YUSAC2 xenografts with TAT-Surv-T34A (10 mg/kg) was associated with rapid tumor accumulation at 1 h, and increased tumor cell apoptosis and aberrant nuclei formation in situ. Repeated i.p. injection of TAT-Surv-T34A resulted in a 40-50% reduction in growth and mass of established tumors, compared to those similarly injected with saline buffer or TAT-Surv-WT. These studies demonstrate the feasibility of systemic tumor treatment using a cell-permeable Survivin antagonist.

摘要

凋亡抑制基因家族成员Survivin在大多数肿瘤中高表达,似乎是癌症治疗的一个有前景的靶点。尽管多种Survivin拮抗剂已被证明可诱导恶性细胞凋亡,但这些药物的潜在效用受到递送效率低下和细胞不透性的限制。我们生成了包含TAT蛋白转导结构域和野生型Survivin(TAT-Surv-WT)或显性负性突变体(TAT-Surv-T34A)的重组融合蛋白。TAT-Surv蛋白通过顺序亲和和离子交换色谱法纯化,在30 nM浓度下30分钟内即可快速进入细胞。虽然TAT-Surv-WT对YUSAC2或WM793黑色素瘤细胞影响极小,但TAT-Surv-T34A在低微摩尔浓度下可诱导细胞脱离、DNA片段化、caspase-3激活以及凋亡诱导因子的线粒体释放。给携带皮下YUSAC2异种移植瘤的小鼠腹腔注射(i.p.)TAT-Surv-T34A(10 mg/kg),1小时时肿瘤迅速聚集,原位肿瘤细胞凋亡增加且出现异常核形成。与注射生理盐水缓冲液或TAT-Surv-WT的小鼠相比,重复腹腔注射TAT-Surv-T34A可使已形成肿瘤的生长和质量降低40-50%。这些研究证明了使用细胞可渗透的Survivin拮抗剂进行全身肿瘤治疗的可行性。