Huang Su-Hua, Lien Jin-Cherng, Chen Chao-Jung, Liu Yu-Ching, Wang Ching-Ying, Ping Chia-Fong, Lin Yu-Fong, Huang An-Cheng, Lin Cheng-Wen
Department of Biotechnology, Asia University, Wufeng, Taichung 413, Taiwan.
School of Pharmacy, China Medical University, Taichung 404, Taiwan.
Int J Mol Sci. 2016 Aug 24;17(9):1386. doi: 10.3390/ijms17091386.
Japanese encephalitis virus (JEV), a mosquito-borne flavivirus, has five genotypes (I, II, III, IV, and V). JEV genotype I circulates widely in some Asian countries. However, current JEV vaccines based on genotype III strains show low neutralizing capacities against genotype I variants. In addition, JE has no specific treatment, except a few supportive treatments. Compound CW-33, an intermediate synthesized derivative of furoquinolines, was investigated for its antiviral activities against JEV in this study. CW-33 exhibited the less cytotoxicity to Syrian baby hamster kidney (BHK-21) and human medulloblastoma (TE761) cells. CW-33 dose-dependently reduced the cytopathic effect and apoptosis of JEV-infected cells. Supernatant virus yield assay pinpointed CW-33 as having potential anti-JEV activity with IC50 values ranging from 12.7 to 38.5 μM. Time-of-addition assay with CW-33 indicated that simultaneous and post-treatment had no plaque reduction activity, but continuous and simultaneous treatments proved to have highly effective antiviral activity, with IC50 values of 32.7 and 48.5 μM, respectively. CW-33 significantly moderated JEV-triggered Ca(2+) overload, which correlated with the recovery of mitochondria membrane potential as well as the activation of Akt/mTOR and Jak/STAT1 signals in treated infected cells. Phosphopeptide profiling by LC-MS/MS revealed that CW-33 upregulated proteins from the enzyme modulator category, such as protein phosphatase inhibitor 2 (I-2), Rho GTPase-activating protein 35, ARF GTPase-activating protein GIT2, and putative 3-phosphoinositide-dependent protein kinase 2. These enzyme modulators identified were associated with the activation of Akt/mTOR and Jak/STAT1 signals. Meanwhile, I-2 treatment substantially inhibited the apoptosis of JEV-infected cells. The results demonstrated that CW-33 exhibited a significant potential in the development of anti-JEV agents.
日本脑炎病毒(JEV)是一种由蚊子传播的黄病毒,有五种基因型(I、II、III、IV和V)。JEV基因型I在一些亚洲国家广泛传播。然而,目前基于基因型III毒株的JEV疫苗对基因型I变异株的中和能力较低。此外,除了一些支持性治疗外,日本脑炎没有特效治疗方法。在本研究中,对呋喃喹啉的中间合成衍生物化合物CW-33进行了抗JEV抗病毒活性研究。CW-33对叙利亚幼仓鼠肾(BHK-21)细胞和人髓母细胞瘤(TE761)细胞的细胞毒性较小。CW-33剂量依赖性地降低了JEV感染细胞的细胞病变效应和凋亡。上清液病毒产量测定表明CW-33具有潜在的抗JEV活性,IC50值范围为12.7至38.5μM。用CW-33进行的添加时间试验表明,同时添加和后处理没有噬斑减少活性,但持续添加和同时添加处理被证明具有高效的抗病毒活性,IC50值分别为32.7和48.5μM。CW-33显著减轻了JEV引发的Ca(2+)过载,这与处理后的感染细胞中线粒体膜电位的恢复以及Akt/mTOR和Jak/STAT1信号的激活相关。通过LC-MS/MS进行的磷酸肽谱分析显示,CW-33上调了来自酶调节剂类别的蛋白质,如蛋白磷酸酶抑制剂2(I-2)、Rho GTP酶激活蛋白35、ARF GTP酶激活蛋白GIT2和假定的3-磷酸肌醇依赖性蛋白激酶2。鉴定出的这些酶调节剂与Akt/mTOR和Jak/STAT1信号的激活有关。同时,I-2处理显著抑制了JEV感染细胞的凋亡。结果表明,CW-33在抗JEV药物的开发中具有显著潜力。
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