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RNA干扰针对HIV感染细胞靶点的治疗潜力。

Therapeutic potential of RNA interference against cellular targets of HIV infection.

作者信息

Zhang Jia, Wu Y O, Xiao Li, Li Kai, Chen L L, Sirois P

机构信息

Gene Core, The Genomics Institute of the Novartis Research Foundation, San Diego, CA, USA.

出版信息

Mol Biotechnol. 2007 Nov;37(3):225-36. doi: 10.1007/s12033-007-9000-0. Epub 2007 Sep 15.

Abstract

RNA interference is not only very promising in identifying new targets for drug development, siRNA/shRNA themselves may be directly used as therapeutic agents. In inhibiting viral infections by RNA interference, both viral targets and cellular proteins have been evaluated. Most of the early studies in this field had chosen viral targets for RNA interference. However, recent efforts are mainly focusing on cellular proteins for RNA silencing due to the realization that a variety of viral responses substantially minimize siRNA effects. With the application of siRNA approaching, many new cellular targets relevant to HIV infection have been identified. The value of siRNA/shRNA in the treatment of AIDS is largely dependent on better understanding of the biology of HIV replication. Efforts in the identification of cellular processes with the employment of siRNA/shRNA have shed some new lights on our understanding of how HIV infection occurs. Furthermore, the relative specific effects and simplicity of design makes siRNA/shRNA themselves to be favorable drug leads.

摘要

RNA干扰不仅在为药物开发确定新靶点方面很有前景,siRNA/shRNA本身也可直接用作治疗剂。在通过RNA干扰抑制病毒感染方面,病毒靶点和细胞蛋白都已得到评估。该领域的大多数早期研究都选择病毒靶点进行RNA干扰。然而,由于认识到多种病毒反应会大大降低siRNA的效果,最近的研究主要集中在细胞蛋白的RNA沉默上。随着siRNA应用的临近,许多与HIV感染相关的新细胞靶点已被确定。siRNA/shRNA在治疗艾滋病方面的价值很大程度上取决于对HIV复制生物学的更好理解。利用siRNA/shRNA识别细胞过程的努力为我们理解HIV感染的发生方式带来了一些新的启示。此外,相对特异性的作用和设计的简单性使siRNA/shRNA本身成为有利的药物先导物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/da3f/7091338/513638b65556/12033_2007_9000_Fig1_HTML.jpg

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