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用肽偶联吗啉代寡聚物在细胞培养物中抑制传染性造血坏死病毒

Inhibition of infectious haematopoietic necrosis virus in cell cultures with peptide-conjugated morpholino oligomers.

作者信息

Alonso M, Stein D A, Thomann E, Moulton H M, Leong J C, Iversen P, Mourich D V

机构信息

Department of Microbiology and Center for Fish Disease Research, Oregon State University, Corvallis, OR, USA.

出版信息

J Fish Dis. 2005 Jul;28(7):399-410. doi: 10.1111/j.1365-2761.2005.00641.x.

Abstract

Delivery of phosphorodiamidate morpholino oligomers (PMO) into fish cells in vitro and tissues in vivo was examined. Uptake was evaluated by fluorescence microscopy and flow cytometry after treating cultured cells or live rainbow trout with 3' fluorescein-tagged PMO. Arginine-rich peptide conjugated to the 5' end of the PMO markedly enhanced cellular uptake in culture by 8- to 20-fold compared with non-peptide-conjugated PMO as determined by flow cytometry. Enhanced uptake of PMO conjugated to peptide was also observed in tissues of fish treated by immersion. The efficacy of PMO as inhibitors of infectious haematopoietic necrosis virus (IHNV) replication was determined in vitro. Peptide-conjugated PMOs targeting sequences within the IHNV genomic RNA (negative polarity) or antigenomic RNA (positive polarity) significantly inhibited replication in a dose-dependent and sequence-specific manner. A PMO complementary to sequence near the 5' end of IHNV genomic RNA was the most effective, diminishing titre by 97%, as measured by plaque assay and Western blot. These data demonstrate that replication of a negative-stranded non-segmented RNA virus can be inhibited by antisense compounds that target positive polarity viral RNA, or by a compound that targets negative polarity viral RNA.

摘要

研究了磷酰二胺吗啉代寡聚物(PMO)在体外进入鱼类细胞以及在体内进入组织的情况。在用3'荧光素标记的PMO处理培养细胞或活虹鳟后,通过荧光显微镜和流式细胞术评估摄取情况。与非肽缀合的PMO相比,与PMO 5'端缀合的富含精氨酸的肽通过流式细胞术测定,在培养中显著增强细胞摄取8至20倍。在通过浸泡处理的鱼的组织中也观察到肽缀合的PMO摄取增强。在体外确定了PMO作为传染性造血坏死病毒(IHNV)复制抑制剂的功效。靶向IHNV基因组RNA(负链)或反基因组RNA(正链)内序列的肽缀合PMO以剂量依赖性和序列特异性方式显著抑制复制。通过噬斑测定和蛋白质印迹法测量,与IHNV基因组RNA 5'端附近序列互补的PMO最有效,使滴度降低97%。这些数据表明,负链非节段RNA病毒的复制可以被靶向正链病毒RNA的反义化合物或靶向负链病毒RNA的化合物抑制。

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