4.7 Article

Complexes assembled from TMV-derived spherical particles and entire virions of heterogeneous nature

期刊

JOURNAL OF BIOMOLECULAR STRUCTURE & DYNAMICS
卷 32, 期 8, 页码 1193-1201

出版社

TAYLOR & FRANCIS INC
DOI: 10.1080/07391102.2013.816868

关键词

immunogenic compositions; tobacco mosaic virus; spherical particles; isometric viruses; platforms

资金

  1. Federal Program Scientific and scientific-educational personnel of innovative Russia [8564]
  2. Russian Foundation for Basic Research [13-04-00543-a]
  3. Russian Ministry of Education and Science [11.519.11.2010]
  4. M.V. Lomonosov Moscow State University Program of Development

向作者/读者索取更多资源

Previously, we described some structural features of spherical particles (SPs) generated by thermal remodelling of the tobacco mosaic virus. The SPs represent a universal platform that could bind various proteins. Here, we report that entire isometric virions of heterogeneous nature bind non-specifically to the SPs. Formaldehyde (FA) was used for covalent binding of a virus to the SPs surface for stabilizing the SP-virus complexes. Transmission and high resolution scanning electron microscopy showed that the SPs surface was covered with virus particles. The architecture of SP-virion complexes was examined by immunologic methods. Mean diameters of SPs and SP-human enterovirus C and SP-cauliflower mosaic virus (CaMV) compositions were determined by nanoparticle tracking analysis (NTA) in liquid. Significantly, neither free SPs nor individual virions were detected by NTA in either FA-crosslinked or FA-untreated compositions. Entirely, all virions were bound to the SPs surface and the SP sites within the SP-CaMV complexes were inaccessible for anti-SP antibodies. Likewise, the SPs immunogenicity within the FA-treated SPs-CaMV compositions was negligible. Apparently, the SP antigenic sites were hidden and masked by virions within the compositions. Previously, we reported that the SPs exhibited adjuvant activity when foreign proteins/epitopes were mixed with or crosslinked to SPs. We found that immunogenicity of entire CaMV crosslinked to SP was rather low which could be due to the above-mentioned masking of the SPs booster. Contrastingly, immunogenicity of the FA-untreated compositions increased significantly, presumably, due to partial release of virions and unmasking of some SPs-buster sites after animals immunization.

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