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通过多种预测算法设计酪氨酸酶小干扰RNA并评估其抗黑色素生成作用

Designing Tyrosinase siRNAs by Multiple Prediction Algorithms and Evaluation of Their Anti-Melanogenic Effects.

作者信息

Kwon Ok-Seon, Kwon Soo-Jung, Kim Jin Sang, Lee Gunbong, Maeng Han-Joo, Lee Jeongmi, Hwang Gwi Seo, Cha Hyuk-Jin, Chun Kwang-Hoon

机构信息

Department of Life Sciences, Sogang University, Seoul 04107, Republic of Korea.

Leaders Cosmetics Co., Ltd., Anseong 17599, Republic of Korea.

出版信息

Biomol Ther (Seoul). 2018 May 1;26(3):282-289. doi: 10.4062/biomolther.2017.115.

Abstract

Melanin is a pigment produced from tyrosine in melanocytes. Although melanin has a protective role against UVB radiation-induced damage, it is also associated with the development of melanoma and darker skin tone. Tyrosinase is a key enzyme in melanin synthesis, which regulates the rate-limiting step during conversion of tyrosine into DOPA and dopaquinone. To develop effective RNA interference therapeutics, we designed a melanin siRNA pool by applying multiple prediction programs to reduce human tyrosinase levels. First, 272 siRNAs passed the target accessibility evaluation using the program. Then we selected 34 siRNA sequences with ΔG ≥-34.6 kcal/mol, value ≥65, and ≤30. siRNAs were designed as 19-bp RNA duplexes with an asymmetric 3' overhang at the 3' end of the antisense strand. We tested if these siRNAs effectively reduced tyrosinase gene expression using qRT-PCR and found that 17 siRNA sequences were more effective than commercially available siRNA. Three siRNAs further tested showed an effective visual color change in MNT-1 human cells without cytotoxic effects, indicating these sequences are anti-melanogenic. Our study revealed that human tyrosinase siRNAs could be efficiently designed using multiple prediction algorithms.

摘要

黑色素是由黑素细胞中的酪氨酸产生的一种色素。尽管黑色素对紫外线B辐射诱导的损伤具有保护作用,但它也与黑色素瘤的发生和较深的肤色有关。酪氨酸酶是黑色素合成中的关键酶,它在酪氨酸转化为多巴和多巴醌的过程中调节限速步骤。为了开发有效的RNA干扰疗法,我们通过应用多个预测程序设计了一个黑色素小干扰RNA(siRNA)池,以降低人类酪氨酸酶水平。首先,使用该程序,272个小干扰RNA通过了靶标可及性评估。然后我们选择了34个小干扰RNA序列,其ΔG≥-34.6千卡/摩尔, 值≥65,且 ≤30。小干扰RNA被设计为19个碱基对的RNA双链体,在反义链的3'端有一个不对称的3'突出端。我们使用定量逆转录聚合酶链反应(qRT-PCR)测试了这些小干扰RNA是否能有效降低酪氨酸酶基因表达,发现17个小干扰RNA序列比市售小干扰RNA更有效。进一步测试的三个小干扰RNA在MNT-1人类细胞中显示出有效的视觉颜色变化,且无细胞毒性作用,表明这些序列具有抗黑色素生成作用。我们的研究表明,使用多个预测算法可以有效地设计人类酪氨酸酶小干扰RNA。

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