Construction and production of fluorescent papillomavirus-like particles

Peng Shiwen , Zhou Jian , Ian H. Frazer

Current Medical Science ›› 1999, Vol. 19 ›› Issue (3) : 170 -174.

PDF
Current Medical Science ›› 1999, Vol. 19 ›› Issue (3) : 170 -174. DOI: 10.1007/BF02887727
Article

Construction and production of fluorescent papillomavirus-like particles

Author information +
History +
PDF

Abstract

The green fluorescent protein (GFP) from the jellyfishAequorea victoria has attracted widespread interest since it was demonstrated to be fluorescent in vivo when expressed in other organisms. In order to investigate papillomavirus life cycle which hampered by the unavailability of conventional cell culture system, we constructed a chimeric bovine papillomavirus (BPV) type 1 virus-like particles (VLPs) containing GFP. It was found that fluorescent VLPs could be assembled from L2 protein in which GFP is inserted into the N-terminal region of L2 (aa 88). The fluorescent VLPs could also be assembled from a GFP/L2 fusion protein in which part of the L2 sequence had been deleted.In vitro, fluorescent VLPs could bind to CV-1 cells, and this VLP/cell interaction could be analyzed by FACS assay. These results demonstrated that GFP could incorporate into BPVl VLPs without disruption of the VLP structure. Fluorescent VLPs might be a useful tool for study of papillomavirus virus/cell interaction.

Keywords

papillomavirus / virus-like particles / green fluorescent protein

Cite this article

Download citation ▾
Peng Shiwen, Zhou Jian, Ian H. Frazer. Construction and production of fluorescent papillomavirus-like particles. Current Medical Science, 1999, 19(3): 170-174 DOI:10.1007/BF02887727

登录浏览全文

4963

注册一个新账户 忘记密码

References

Publishing order | Descend order by publishing year | Descend order by cited within
[1]

ZhouJ, SunX Y, StenzelD J. Expression of vaccinia recombinant HPV 16 L1 and L2 ORF proteins in epithelial cells is sufficient for assembly of HPV virion-like particles. Virology, 1991, 185: 251-251

[2]

QiY M, PengS W, HengstK. Epithelial cells display separate receptors for papillomavirus VLPs and for soluble L1 capsid protein. Virology, 1996, 216: 35-35

[3]

SchillerJ T, RodenR B. Papillomavirus-like particles. Papillomavirus Report, 1995, 6: 121-121
[4]

LiuW J, GissmannL, SunX Y, et al.. Sequence close to the N-terminus of L2 protein is displayed on the surface of bovine papillomavirus type 1 virions. Virology, 1997, 227: 474-474

[5]

CubittA B, HeimR, AdamsSR, et al.. Understanding, improving and using green fluorescent proteins. Trends Biochem Sci, 1995, 20: 448-448

[6]

ChalfieM, TuY, EuskirchenG, et al.. Green fluorescent protein as a marker for gene expression. Science, 1994, 263: 802-802

[7]

WangS, HazelriggT. Implications for bcd mRNA localization from spatial distribution of exu protein in Drosophila oogenesis. Nature, 1994, 369: 400-400

[8]

PengS W, FrazerI H, FernandoG J, et al.. Papillomavirus virus-like particles can deliver defined CTL epitopes to the MHC class I pathway. Virology, 1998, 240: 147-147

[9]

SunX Y, FrazerI, MullerM, et al.. Sequences required for the nuclear targeting and accumulation of human papillomavirus type 6B L2 protein. Virology, 1995, 213: 321-321

[10]

ZhouJ, SunX Y, LouisK, et al.. Interaction of human papillomavirus (HPV) type 16 capsid proteins with HPV DNA requires an intact L2 N-terminal sequence. J Virol, 1994, 68: 619-619

[11]

HeimR, CubittA B, TsienR Y. Improved green fluorescence [letter]. Nature, 1995, 373: 663-663

AI Summary AI Mindmap
PDF

92

Accesses

0

Citation

Detail
Sections
Recommended

AI思维导图

/