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奎纳克林对映体对朊病毒增殖的差异性抑制作用

Differential inhibition of prion propagation by enantiomers of quinacrine.

作者信息

Ryou Chongsuk, Legname Giuseppe, Peretz David, Craig John C, Baldwin Michael A, Prusiner Stanley B

机构信息

Institute for Neurodegenerative Diseases, University of California, San Francisco, California 94143-0518, USA.

出版信息

Lab Invest. 2003 Jun;83(6):837-43. doi: 10.1097/01.lab.0000074919.08232.a2.

Abstract

Prion diseases are fatal neurologic disorders caused by accumulation of a pathogenic isoform (PrP(Sc)) of the prion protein (PrP). The recent discovery of the inhibitory action of quinacrine on PrP(Sc) formation in scrapie-infected neuroblastoma (ScN2a) cells raised the possibility of a treatment for patients with prion disease. To investigate the efficacy of quinacrine enantiomers, we measured the inhibitory effect of these isomers on PrP(Sc) formation in ScN2a cells. (S)-quinacrine exhibited superior antiprion activity compared with (R)-quinacrine and two generic quinacrines that appear to be racemates. Treatment with these various forms of quinacrine did not induce adverse changes affecting cell survival and the expression of marker proteins over a range of potentially therapeutic concentrations. Thus, quinacrine enantiomers demonstrated stereoselectivity on prion elimination but not cytotoxicity in ScN2a cells. Our results raise the possibility that in vivo treatment using one enantiomer of quinacrine may be superior to a racemic mixture, which is the form that is generally used when quinacrine is employed to treat parasitic diseases.

摘要

朊病毒病是由朊病毒蛋白(PrP)的致病性异构体(PrP(Sc))积累引起的致命性神经疾病。最近发现奎纳克林对感染瘙痒病的神经母细胞瘤(ScN2a)细胞中PrP(Sc)形成具有抑制作用,这为朊病毒病患者的治疗带来了可能性。为了研究奎纳克林对映体的疗效,我们测量了这些异构体对ScN2a细胞中PrP(Sc)形成的抑制作用。与(R)-奎纳克林和两种似乎是外消旋体的普通奎纳克林相比,(S)-奎纳克林表现出更强的抗朊病毒活性。在一系列潜在治疗浓度范围内,用这些不同形式的奎纳克林处理不会诱导影响细胞存活和标记蛋白表达的不良变化。因此,奎纳克林对映体在ScN2a细胞中对朊病毒清除表现出立体选择性,但无细胞毒性。我们的结果表明,使用奎纳克林的一种对映体进行体内治疗可能优于外消旋混合物,而外消旋混合物是奎纳克林用于治疗寄生虫病时通常使用的形式。

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