Affiliation:
1. Cancer Research Campaign Institute for Cancer Studies, The Medical School, University of Birmingham, United Kingdom.
Abstract
The function of the human papillomavirus (HPV) E4 proteins is unknown. In cultured epithelial cells the proteins associate with the keratin intermediate filaments (IFs) and, for some E4 types, e.g., HPV type 16 (HPV-16), induce collapse of the keratin networks. An N-terminal leucine-rich motif (LLXLL) is a conserved feature of many E4 proteins. In a previous study we showed that deletion of this region from the HPV-1 and -16 E4 proteins abrogated the localization of the mutant proteins to the keratin cytoskeleton in a simian virus 40-transformed human keratinocyte cell line (S. Roberts, I. Ashmole, L. J. Gibson, S. M. Rookes, G. J. Barton, and P. H. Gallimore, J. Virol. 68:6432-6445, 1994). The E4 proteins of HPV-1 and -16 have little sequence homology except at the N terminus. Therefore, to establish the role of sequences other than those at the N terminus, we have performed a mutational analysis of the HPV-16 E4 protein. The results of the analysis were as follows: (i) similar to findings for the HPV-1 protein, no mutation of HPV-16 E4 sequences (other than the N-terminal leucine motif) results in a mutant protein which fails to colocalize to the keratin IFs; (ii) the C-terminal domain (residues 61 to 92) is not essential for association with the cytoskeleton; and (iii) deletion of C-terminal sequences (residues 84 to 92; LTVIVTLHP) corresponding to part of a domain conserved between mucosal E4 proteins affects the ability of the mutant protein to induce cytoskeletal collapse, despite colocalization with the keratin IFs. Further analysis of this region showed that conserved hydrophobic residues valines 86 and 88 are important. In addition, we show that the HPV-16 E4 protein is detergent insoluble and exists as several disulfide-linked, high-molecular-weight complexes which could represent homo-oligomers. The C-terminal sequences (residues 84 to 92), in particular valines 86 and 88, are important in the formation of these insoluble complexes. The results of this study support our postulate that the E4 proteins include functional domains at the N terminus and the C terminus, with the intervening sequences possibly acting as a flexible hinge.
Publisher
American Society for Microbiology
Subject
Virology,Insect Science,Immunology,Microbiology
Reference52 articles.
1. Ashmole I. P. H. Gallimore and S. Roberts. The identification and characterisation of hydrophobic C-terminal residues of the human papillomavirus type 1 E1 ∧ E4 protein necessary for oligomerisation. Submitted for publication.
2. Breitburd F. O. Croissant and G. Orth. 1987. Expression of human papillomavirus type 1 E4 gene products in warts p. 115-122. In B. M. Steinberg J. L. Brandsma and L. B. Taichman (ed.) Papillomaviruses: cancer cells. Cold Spring Harbor Laboratory Press Cold Spring Harbor N.Y.
3. The adenovirus L3 23- kilodalton proteinase cleaves the amino-terminal head domain from cytokeratin 18 and disrupts the cytokeratin network of HeLa cells;Chen P. H.;J. Virol.,1993
4. Viral E1 and E2 proteins support replication of homologous and heterologous papillomavirus origins;Chiang C.;Proc. Natl. Acad. Sci. USA,1992
5. Human papillomavirus types 6 and 11 mRNAs from genital condylomata acuminata;Chow L. T.;J. Virol.,1987
Cited by
42 articles.
订阅此论文施引文献
订阅此论文施引文献,注册后可以免费订阅5篇论文的施引文献,订阅后可以查看论文全部施引文献