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Nanoencapsulated anti-CK2 small molecule drug or siRNA specifically targets malignant cancer but not benign cells.

机译：纳米囊化的抗CK2小分子药物或siRNA专门针对恶性肿瘤，但不针对良性细胞。

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CK2, a pleiotropic Ser/Thr kinase, is an important target for cancer therapy. We tested our novel tenfibgen-based nanocapsule for delivery of the inhibitor 2-dimethylamino-4,5,6,7-tetrabromo-1H-benzimidazole (DMAT) and an siRNA directed against both CK2?? and ??' catalytic subunits to prostate cancer cells. We present data on the TBG nanocapsule itself and on CK2 inhibition or downregulation in treated cells, including effects on Nuclear Factor-kappa B (NF-??B) p65. By direct comparison of two CK2-directed cargos, our data provide proof that the TBG encapsulation design for delivery of drugs specifically to cancer cells has strong potential for small molecule- and nucleic acid-based cancer therapy.

机译：CK2是一种多效性Ser / Thr激酶，是癌症治疗的重要靶标。我们测试了我们新的基于tenfibgen的纳米胶囊对抑制剂2-二甲氨基-4,5,6,7-四溴-1H-苯并咪唑（DMAT）和针对CK2α2的siRNA的递送。和??前列腺癌细胞的催化亚基。我们提供了有关TBG纳米胶囊本身以及处理细胞中CK2抑制或下调的数据，包括对核因子-κB（NF-κB）p65的影响。通过直接比较两种由CK2操纵的货物，我们的数据提供了证据，证明专门用于向癌细胞输送药物的TBG封装设计具有强大的潜力，可用于基于小分子和核酸的癌症治疗。

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Trembley JH; Unger GM; Korman VL; Tobolt DK; Kazimierczuk Z; Pinna LA; Kren BT; Ahmed K;
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年度 2012
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正文语种 eng
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1. Nanoencapsulated anti-CK2 small molecule drug or siRNA specifically targets malignant cancer but not benign cells [J] . TrembleyJ.H., UngerG.M., KormanV.L., Cancer letters . 2012,第1期

机译：纳米封装的抗CK2小分子药物或siRNA专门针对恶性肿瘤，但不针对良性细胞
2. Metabonomics by Proton Nuclear Magnetic Resonance in Human Pleural Effusions: A Route to Discriminate Between Benign and Malignant Pleural Effusions and to Target Small Molecules as Potential Cancer Biomarkers [J] . Zennaro Lucio, Vanzani Paola, Nicole Lorenzo, Cancer: A Journal of the American Cancer Society . 2017,第5期

机译：通过质子核磁共振在人类胸膜沸腾中的代谢学：一种辨别良性和恶性胸腔积液的途径和将小分子靶向潜在的癌症生物标志物
3. Immunohistochemical expression of mitochondrial membrane complexes (MMCs) I, III, IV and V in malignant and benign periampullary epithelium: a potential target for drug therapy of periampullary cancer? [J] . Mark M Aloysius, Abed M Zaitoun, Timothy E Bates, BMC Cancer . 2010,第1期

机译：线粒体膜复合物（MMCs）I，III，IV和V在恶性和良性壶腹周围上皮中的免疫组织化学表达：壶腹周围癌药物治疗的潜在目标？
4. Single Molecule Tracking of siRNA Dynamics in Living Cells. [C] . Svitlana Berezhna, Ashok A. Deniz, Arkady Voloshin SEM Annual Conference and Exposition on Experimental and Applied Mechanics . 2009

机译：活细胞中siRNA动力学的单分子跟踪。
5. Targeted siRNA-directed Therapy to Increase Chemosensitivity In Drug Resistant Bladder Cancer Cells [D] . Trejo, Jerry 2013

机译：靶向siRNA定向疗法可提高耐药性膀胱癌细胞的化学敏感性
6. Nanoencapsulated anti-CK2 small molecule drug or siRNA specifically targets malignant cancer but not benign cells [O] . Janeen H. Trembley, Gretchen M. Unger, Vicci L. Korman, -1

机译：纳米封闭的抗CK2小分子药物或siRNA特异性靶向恶性癌症但不是良性细胞
7. Metabonomics by proton nuclear magnetic resonance in human pleural effusions: A route to discriminate between benign and malignant pleural effusions and to target small molecules as potential cancer biomarkers [O] . Lucio Zennaro, Paola Vanzani, Lorenzo Nicolè, 2017

机译：通过质子核磁共振在人胸膜血液中的代谢学：一种辨别良性和恶性胸腔积液的途径，并将小分子靶向潜在的癌症生物标志物

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Nanoencapsulated anti-CK2 small molecule drug or siRNA specifically targets malignant cancer but not benign cells.

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