| Literature DB >> 18275613 |
Abstract
BACKGROUND: Flaviviruses include the mosquito-borne dengue, Japanese encephalitis, yellow fever and West Nile and the tick-borne encephalitis viruses. They are responsible for considerable world-wide morbidity and mortality. Viral entry is mediated by a conserved fusion peptide containing 16 amino acids located in domain II of the envelope protein E. Highly orchestrated conformational changes initiated by exposure to acidic pH accompany the fusion process and are important factors limiting amino acid changes in the fusion peptide that still permit fusion with host cell membranes in both arthropod and vertebrate hosts. The cell-fusing related agents, growing only in mosquitoes or insect cell lines, possess a different homologous peptide.Entities:
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Year: 2008 PMID: 18275613 PMCID: PMC2275255 DOI: 10.1186/1743-422X-5-27
Source DB: PubMed Journal: Virol J ISSN: 1743-422X Impact factor: 4.099
Wild-type fusion peptide sequences in pathogenic arthropod-borne flaviviruses
| Flavivirus | Wild-type sequencea |
| Mosquito-borne except dengueb | DRGWGNGCGLFGKGSI |
| Dengue type 1 | DRGWGNGCGLFGKGS |
| Dengue type 2 | DRGWGNGCGLFGKG |
| Dengue type 3 | DRGWGNGCGLFGKG |
| Dengue type 4 | DRGWGNGCGLFGKG |
| Tick-bornec except Powassan | DRGW |
| Powassan including deer tick | DRGW |
aChanges from the amino acids in the most common mosquito-borne sequence are in bold
bJEV, YFV, WNV including Kunjin, Murray Valley encephalitis and SLEV viruses
cTBEV, Langat, louping ill, Omsk hemorrhagic fever virus, Kyasanur Forest disease virus including Alkhurma, Royal Farm virus, Karshi, Gadgets Gully, Spanish sheep encephalomyelitis and Turkish sheep encephalitis viruses.
Wild-type fusion peptide sequences in other flaviviruses
| Flavivirus | Vector | Wild-type sequencea |
| Additional mosquito-borne not in Table 1b | Mosquito | DRGWGNGCGLFGKGSI |
| Viruses with variations only in amino acid 16c | Mosquito | DRGWGNGCGLFGKGS |
| Iguape virus | Mosquito | DRGW |
| Bussuquara | Mosquito | |
| Seabird tick-borne virusesd | Tick | DRGWGN |
| Kadam virus | Tick | DRGWGN |
| Some NKVe | None known | DRGWGNGCGLFGKGSI |
| Modoc virus | None known | DRGWGNGC |
| Tamana bat virusf | None known | DRGW |
| Cell fusing agent (CFAV) | No known vertebrate host | |
| CFA Puerto Rico (CFAV) | No known vertebrate host | |
| Culex flavivirus (CXFV) | No known vertebrate host | |
| Kamiti River virus (KRV) | No known vertebrate host |
aChanges from the amino acids in the most common mosquito-borne sequence are in bold.
bIncluding Usutu, Sepik and Entebbe bat, Ilheus, Bagaza and Yokose viruses
cKokobera, Rocio, Kédougou and Zika viruses in which amino acid 16, X, = M, L, Y and L respectively
dTyuleniy, Meaban and Saumarez Reef viruses
eRio Bravo, Apoi and Montana myotis leukoencephalitis viruses
fA new genus has been proposed for this virus.
Figure 1Distribution of conserved cysteines in arthropod-borne and CFRV flavivirus protein E. The disulfide linkages and their domains are indicated for the arthropod-borne flaviviruses. The figure demonstrates that 4 of the CFRV conserved cysteine residues (257, 309, 312 and 352) are not homologous to the arthropod-borne flaviviruses.
Frequency of nonsynonymous mutations in flavivirus fusion peptides
| Flavivirus | Wild-type fusion peptide sequence | # of mutant sequences | Total # of sequences | % with mutations |
| Dengue 1 | DRGWGNGCGLFGKGSL | 12 | 428 | 2.8 |
| Dengue 2 | DRGWGNGCGLFGKGGI | 14 | 413 | 3.4 |
| Dengue 3 | DRGWGNGCGLFGKGSL | 2 | 240 | 0.8 |
| Dengue 4 | DRGWGNGCGLFGKGGV | 9 | 171 | 5.3 |
| West Nile including Kunjin | DRGWGNGCGLFGKGSI | 6 | 303 | 2.0 |
| Japanese encephalitis | DRGWGNGCGLFGKGSI | 18 | 243 | 7.4 |
| Yellow fever | DRGWGNGCGLFGKGSI | 47 | 177 | 26.6 |
| St. Louis encephalitis | DRGWGNGCGLFGKGSI | 0 | 97 | 0.0 |
| Tick-borne encephalitis | DRGWGNHCGLFGKGSI | 4 | 151 | 2.6 |
| Powassan including deer tick | DRGWGNHCGFFGKGSI | 1 | 22 | 4.6 |
| Total | 113 | 2,245 | 5.0 |
Figure 2Comparison of fusion peptide mutations in yellow fever virus with other pathogenic flaviviruses. aThe mosquito-borne sequence is shown. In tick-borne viruses G is replaced by H as the 7th amino acid. In Powassan, a tick-borne virus, the 10th amino acid is F in lieu of L. Amino acids 15 and 16 are SL, GI, SL and GV in DENV1–4, respectively instead of SI.
Figure 3Phylogenetic tree of yellow fever viruses with a G100S E protein mutation. The nearest neighbor-joining tree was developed from sequences in the prM/E region (nucleotides 643–1308). Similar results were obtained using maximum parsimony. Selected strains with G100S mutations indicated by red circles were supplemented with strains with the wild-type codon to indicate additional branching patterns.