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用原代猪骨髓来源细胞分离猪圆环病毒 3。

Isolation of porcine circovirus 3 using primary porcine bone marrow-derived cells.

机构信息

General Incorporated Foundation Nippon Institute for Biological Science, 9-2221-1 Shin-machi, Ome, Tokyo, 198-0024, Japan.

Laboratory of Comparative Immunology, Department of Veterinary Medicine, College of Bioresource Sciences, Nihon University, 1866 Kameino, Fujisawa, Kanagawa, 252-0880, Japan.

出版信息

Virol J. 2024 Aug 12;21(1):184. doi: 10.1186/s12985-024-02463-2.

Abstract

Porcine circovirus 3 (PCV3) was first reported in the United States in 2016; this virus is considered to be involved in diverse pathologies, such as multisystem inflammation, porcine dermatitis and nephropathy syndrome, and reproductive disorders. However, successful isolation of PCV3 using cultured cells has been rare. In this study, we aimed to isolate PCV3 using primary porcine bone marrow-derived cells. Mononuclear cells were isolated from the femur bones of clinically healthy pigs. These primary cells were cultured for 6-10 days post-seeding and infected with PCV3-containing tissue homogenates. The cells were cultured for up to 37 days, and the culture medium was changed every 3-4 days. The growth curve of PCV3 in porcine bone marrow cells revealed a decline in growth during the first 10 days post-infection, followed by an increase leading to > 10 genomic copies/mL of the cell culture supernatant; moreover, the virus was capable of passaging. The indirect fluorescent antibody assay for PCV3 infection revealed the presence of PCV3 capsid protein in the cytoplasm and nuclei of infected cells. Bone marrow cells were passaged for more than 20 generations (over 5 months), and PCV3 persistently infected the cells. PCV3-infected bone marrow cells expressed mesenchymal markers. These results reflect that primary porcine bone marrow-derived mesenchymal cells are permissive to PCV3 and continuously replicate a high copy number of the PCV3 genome. These findings regarding the high replication rate of PCV3 in bone marrow-derived mesenchymal cells could enhance our understanding of PCV3 pathogenicity.

摘要

猪圆环病毒 3 型(PCV3)于 2016 年首次在美国报道;该病毒被认为与多种病理学有关,如多系统炎症、猪皮炎和肾病综合征以及生殖障碍。然而,利用细胞培养成功分离 PCV3 较为罕见。本研究旨在利用原代猪骨髓源性细胞分离 PCV3。从临床健康猪的股骨中分离出单核细胞。接种后,这些原代细胞培养 6-10 天,并感染含 PCV3 的组织匀浆。细胞培养最多可达 37 天,每隔 3-4 天更换一次培养基。PCV3 在猪骨髓细胞中的生长曲线显示,感染后前 10 天病毒生长下降,随后增加导致细胞培养上清液中超过 10 个基因组拷贝/ml;此外,该病毒能够传代。用于 PCV3 感染的间接荧光抗体检测显示,感染细胞的细胞质和核内存在 PCV3 衣壳蛋白。骨髓细胞传代超过 20 代(超过 5 个月),PCV3 持续感染细胞。PCV3 感染的骨髓细胞表达间充质标志物。这些结果表明,原代猪骨髓源性间充质细胞对 PCV3 具有易感性,并持续复制大量 PCV3 基因组。这些关于 PCV3 在骨髓源性间充质细胞中高复制率的发现,可能有助于我们加深对 PCV3 致病性的理解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d0f8/11318261/00e612fd518f/12985_2024_2463_Fig1_HTML.jpg

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