Characterization of a potent non-cytotoxic shRNA directed to the HIV-1 co-receptor CCR5.

Saki Shimizu, Masakazu Kamata, Panyamol Kittipongdaja, Kevin N Chen, Sanggu Kim, Shen Pang, Joshua Boyer, F Xiao-Feng Qin, Dong Sung An, Irvin Sy Chen
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引用次数: 41

Abstract

Background: The use of shRNAs to downregulate the expression of specific genes is now relatively routine in experimentation but still hypothetical for clinical application. A potential therapeutic approach for HIV-1 disease is shRNA mediated downregulation of the HIV-1 co-receptor, CCR5. It is increasingly recognized that siRNAs and shRNAs can have unintended consequences such as cytotoxicities in cells, particularly when used for long term therapeutic purposes. For the clinical use of shRNAs, it is crucial to identify a shRNA that can potently inhibit CCR5 expression without inducing unintended cytotoxicities.

Results: Previous shRNAs to CCR5 identified using conventional commercial algorithms showed cytotoxicity when expressed using the highly active U6 pol III promoter in primary human peripheral blood derived mononuclear cells. Expression using the lower activity H1 promoter significantly reduced toxicity, but all shRNAs also reduced RNAi activity. In an effort to identify shRNAs that were both potent and non-cytotoxic, we created a shRNA library representing all potential CCR5 20 to 22-nucleotide shRNA sequences expressed using an H1 promoter and screened this library for downregulation of CCR5. We identified one potent CCR5 shRNA that was also non-cytotoxic when expressed at a low level with the H1 promoter. We characterized this shRNA in regards to its function and structure. This shRNA was unique that the use of commercial and published algorithms to predict effective siRNA sequences did not result in identification of the same shRNA. We found that this shRNA could induce sequence specific reduction of CCR5 at post transcriptional level, consistent with the RNA interference mechanism. Importantly, this shRNA showed no obvious cytotoxicity and was effective at downregulating CCR5 in primary human peripheral blood derived mononuclear cells.

Conclusion: We report on the characterization of a rare shRNA with atypical structural features having potent RNAi activity specific to CCR5. These results have implications for the application of RNAi technology for therapeutic purposes.

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靶向HIV-1共受体CCR5的强效非细胞毒性shRNA的表征
背景:利用shrna下调特定基因的表达目前在实验中是相对常规的,但在临床应用中仍是假设的。shRNA介导的下调HIV-1共受体CCR5是HIV-1疾病的一种潜在治疗方法。越来越多的人认识到sirna和shrna可以产生意想不到的后果,如细胞毒性,特别是当用于长期治疗目的时。对于shRNA的临床应用,鉴定一种能够有效抑制CCR5表达而不诱导意外细胞毒性的shRNA至关重要。结果:先前使用传统商业算法鉴定的CCR5的shrna在原代人外周血源性单核细胞中使用高活性U6 pol III启动子表达时显示细胞毒性。使用活性较低的H1启动子表达可显著降低毒性,但所有shrna也会降低RNAi活性。为了鉴定既有效又无细胞毒性的shRNA,我们创建了一个shRNA文库,代表所有使用H1启动子表达的潜在CCR5 20至22核苷酸shRNA序列,并筛选该文库中CCR5的下调。我们发现了一种有效的CCR5 shRNA,当与H1启动子低水平表达时,它也是非细胞毒性的。我们根据它的功能和结构来描述这个shRNA。该shRNA的独特之处在于,使用商业和已发表的算法来预测有效的siRNA序列不会导致鉴定相同的shRNA。我们发现该shRNA可以在转录后水平诱导CCR5序列特异性减少,符合RNA干扰机制。重要的是,该shRNA没有表现出明显的细胞毒性,并且在原代人外周血源性单核细胞中有效下调CCR5。结论:我们报道了一种罕见的具有非典型结构特征的shRNA的特征,该shRNA具有针对CCR5的强效RNAi活性。这些结果对RNAi技术在治疗中的应用具有启示意义。
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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