| Literature DB >> 35336933 |
Ashley E Strother1, Jill K Thompson2, Steven G Widen2, Alan D T Barrett1,3.
Abstract
The disease yellow fever was prevented by two live attenuated vaccines, strains 17D and French neurotropic vaccine (FNV), derived by serial passage of wild-type (WT) strains Asibi and French Viscerotropic virus (FVV), respectively. Both 17D and FNV displayed decreased genetic diversity and resistance to the antiviral Ribavirin compared to their WT parental strains, which are thought to contribute to their attenuated phenotypes. Subsequent studies found that only a few passages of WT strain FVV in HeLa cells resulted in an attenuated virus. In the current study, the genome sequence of FVV following five passages in HeLa cells (FVV HeLa p5) was determined through Next Generation Sequencing (NGS) with the aim to investigate the molecular basis of viral attenuation. It was found that WT FVV and FVV HeLa p5 virus differed by five amino acid substitutions: E-D155A, E-K331R, E-I412V, NS2A-T105A, and NS4B-V98I. Surprisingly, the genetic diversity and Ribavirin resistance of the FVV HeLa p5 virus were not statistically different to WT parent FVV. These findings suggest that while FVV HeLa p5 is attenuated, this is not dependent on a high-fidelity replication complex, characterized by reduced genetic diversity or increased Ribavirin stability, as seen with FNV and 17D vaccines.Entities:
Keywords: attenuation; flavivirus; genetic diversity; genome; yellow fever virus
Mesh:
Substances:
Year: 2022 PMID: 35336933 PMCID: PMC8949127 DOI: 10.3390/v14030527
Source DB: PubMed Journal: Viruses ISSN: 1999-4915 Impact factor: 5.048
Coding Changes between FVV, FNV, and FVV HeLa p5.
| Nucleotide | FVV | FVV HeLa p5 | FNV | NT in Codon | Residue | FVV | FVV HeLa p5 | FNV |
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| 239 | T | T | C | 2nd | C-80 |
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| 268 | A | A | G | 1st | C-90 |
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| 436 | G | G | A | 1st | prM-25 |
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| 736 | C | C | T | 1st | M-36 |
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| 882 | C | T | C | 3rd | E-9 |
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| 1016 | C | C | T | 2nd | E-54 |
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| 1319 | A | C | A | 2nd | E-155 |
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| 1454 | C | C | A | 2nd | E-200 |
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| 1600 | A | A | G | 1st | E-249 |
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| 1847 | A | G | G | 2nd | E-331 |
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| 2089 | A | G | A | 1st | E-412 |
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| 3634 | A | A | G | 1st | NS2A-82 |
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| 3703 | A | G | G | 1st | NS2A-105 |
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| 4240 | T | T | T | 1st | NS2B-60 |
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| 5027 | T | T | A | 2nd | NS3-192 |
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| 6409 | T | T | C | 3rd | NS4A-29 |
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| 6725 | A | A | T | 2nd | NS4A-135 |
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| 7053 | A | A | G | 3rd | NS4B-95 |
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| 7060 | G | A | A | 1st | NS4B-98 |
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| 7262 | C | C | T | 2nd | NS4B-165 |
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| 8291 | T | T | C | 2nd | NS5-258 |
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| 8522 | G | G | A | 2nd | NS5-335 |
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| 8799 | C | T | C | 3rd | NS5-427 |
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| 9109 | T | T | C | 1st | NS5-531 |
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Figure 1Shannon Entropy Values for FVV HeLa p5 (A) and FVV (B). FVV HeLa P5 displays statistically similar levels of Shannon Entropy compared to FVV.
Single nucleotide variants (SNVs) for FVV and FVV Hela p5 virus. A: SNVs in FVV HeLa p5. Red denotes residue distinguishing FVV and FNV. Blue denotes residue distinguishing Asibi and Asibi HeLa p6. B: SNVs in FVV.
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| CDS Position | HeLa P5 | Variant | NT in Codon | Residue | HeLa P5 | Variant | % |
| 1117 | C | A | 1st | E-373 | G | R | 7.07 |
| 1319 |
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| 1.34 |
| 1727 | C | A | 2nd | E-291 | T | K | 2.41 |
| 1823 | A | G | 2nd | E-323 | K | R | 17.66 |
| 1924 | T | A | 1st | E-357 | S | T | 5.78 |
| 3703 |
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| 7060 |
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| 1.01 |
| 9852 | A | G | 3rd | NS5-778 | L | L | 1.30 |
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| CDS Position | FVV | Variant | NT in Codon | Residue | FVV | Variant | % |
| 174 | A | G | 3rd | C-58 | G | G | 11.41 |
| 5490 | T | G | 3rd | NS3-346 | S | R | 2.50 |
| 5562 | T | C | 3rd | NS3-370 | I | I | 15.91 |
| 5895 | T | C | 3rd | NS3-481 | P | P | 12.54 |
| 8320 | A | G | 1st | NS5-268 | T | A | 1.84 |
| 10137 | T | C | 3rd | NS5-873 | R | R | 11.70 |
| 10142 | G | A | 2nd | NS5-875 | R | Q | 11.87 |
| 10276 | G | C | N/A | 3′UTR | N/A | N/A | 1.83 |
| 10314 | T | C | N/A | 3′UTR | N/A | N/A | 1.46 |
Figure 2Ribavirin sensitivity curve for FVV HeLa p5 in Vero cells. FVV is in burgundy (0.20 µM, R2 = 0.96), FVV HeLa p5 (0.45 µM, R2 = 0.93) is in yellow, and FNV (17.31 µM, R2 = 0.79) is in purple.