| Literature DB >> 22899927 |
Abstract
In the course of evolution, viruses have developed various molecular mechanisms to evade the defense reactions of the host organism. When understanding the mechanisms used by viruses to overcome manifold defense systems of the animal organism, represented by molecular factors and cells of the immune system, we would not only comprehend better but also discover new patterns of organization and function of these most important reactions directed against infectious agents. Here, study of the orthopoxviruses pathogenic for humans, such as variola (smallpox), monkeypox, cowpox, and vaccinia viruses, may be most important. Analysis of the experimental data, presented in this paper, allows to infer that variola virus and other orthopoxviruses possess an unexampled set of genes whose protein products efficiently modulate the manifold defense mechanisms of the host organisms compared with the viruses from other families.Entities:
Year: 2012 PMID: 22899927 PMCID: PMC3413996 DOI: 10.1155/2012/524743
Source DB: PubMed Journal: Adv Virol ISSN: 1687-8639
Orthopoxviral Bcl-2-like proteins.
| Protein function | VACV-COP | CPXV-GRI | MPXV-ZAI | VARV-IND | ||||
|---|---|---|---|---|---|---|---|---|
| ORF | Size, aa | ORF | Size, aa | ORF | Size, aa | ORF | Size, aa | |
| Inhibition of NF- | A46R | 214 | A49R | 240 | A47R | 240 | A52R | 240 |
| Inhibition of NF- | A52R | 190 | A55R | 190 | — | — | J6R | 71 |
| Inhibition of NF- | B15R | 149 | B13R | 149 | B13R | 149 | B14R | 149 |
| Inhibition of NF- | N1L | 117 | Q1L | 117 | P1L | 117 | P1L | 117 |
| Inhibition of NF- | K7R | 149 | M6R | 149 | C6R | 149 | C4R | 149 |
| Inhibition of IRF3 and IRF7 activation by interacting with TANK, NAP1, and SINTBAD | C6L | 151 | C14L | 156 | D11L | 153 | D9L | 156 |
| Unknown | C1L | 224 | C19L | 231 | D19L | 214 | D14L | 214 |
| Unknown | C16L | 181 | D5L | 153 | — | — | D1L | 153 |
| Unknown | N2L | 175 | Q2L | 175 | P2L | 177 | P2L | 177 |
VARV-IND: VARV strain India,1967, MPXV-ZAI: MPXV strain Zaire-I-96, CPXV-GRI: CPXV strain GRI-90, VAC-COP: VACV strain Copenhagen. ORF: open reading frame; aa: protein size in number of amino acid residues.
Figure 1A schematic of two classes of orthopoxvirus E3 ubiquitin ligases: (a) SCF E3 ligase and (b) BTB-kelch/Cul3 E3 ligase.
Orthopoxviral ankyrin-F-box-like proteins.
| VACV-COP | CPXV-GRI | MPXV-ZAI | VARV-IND | ||||
|---|---|---|---|---|---|---|---|
| ORF | Size, aa | ORF | Size, aa | ORF | Size, aa | ORF | Size, aa |
| C19L∗ | 259 |
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| None | None |
| C17L∗ | 386 |
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| None | None | None | None |
| None | None |
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| None | None | None | None |
| None | None |
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| None | None | None | None |
| None | None |
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| None | None |
| None | None |
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| None | None | None | None |
| None | None |
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| D6L | 452 |
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| D7L | 153 |
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| K1L | 284 | M1L | 284 | C1L | 284 | C1L | 66 |
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| None | None |
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| B20R | 127 |
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| B21R∗ | 91 |
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| None | None | None | None |
| None | None | None | None |
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| None | None |
| B23R∗ | 386 |
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| None | None | None | None |
| B25R∗ | 259 |
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Asterisks denote ORFs that are duplicated in left and right inverted terminal repeat regions of the viral genome. ORFs with full length are set in bold. The ORFs for the proteins with experimentally confirmed interaction with the cellular Cullin1-containing ubiquitin-protein ligase are indicated by bold italic letters.
Orthopoxviral BTB-kelch-like proteins.
| VACV-COP | CPXV-GRI | MPXV-ZAI | VARV-IND | ||||
|---|---|---|---|---|---|---|---|
| ORF | Size, aa | ORF | Size, aa | ORF | Size, aa | ORF | Size, aa |
| None | None |
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| None | None | None | None |
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| D18L | 107 | None | None |
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| C7L | 179 |
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| None | None | J7R | 71 |
| B10R | 166 |
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| None | None | None | None |
| None | None |
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| B18R | 70 | B22R | 70 |
ORFs with full length are set in bold. The ORFs for the proteins with experimentally confirmed interaction with the cellular Cullin 3-containing ubiquitin-protein ligase are indicated by bold italic letters.
Orthopoxviral proteins modulating defense reactions of mammals.
| Protein function | VACV-COP | CPXV-GRI | MPXV-ZAI | VARV-IND | ||||
|---|---|---|---|---|---|---|---|---|
| ORF | Size, aa | ORF | Size, aa | ORF | Size, aa | ORF | Size, aa | |
| Apoptosis inhibitor, caspase-1 and caspase-8 inhibitor, SPI-2 |
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| B12R | 345 | B12R | 344 | B13R | 344 |
| Apoptosis inhibitor, SPI-1 | C12L | 353 | B20R | 375 | B19R | 357 | B25R | 372 |
| Apoptosis inhibitor, Bcl-2-like | N1L | 117 | Q1L | 117 | P1L | 117 | P1L | 117 |
| Mitochondria-associated apoptosis inhibitor, caspase-9 inhibitor | F1L | 226 | G1L | 238 | C7L | 219 | C5L | 251 |
| Apoptosis inhibitor, transmembrane protein of Golgi apparatus |
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| T1R | 210 |
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| Apoptosis inhibitor, RING-domain containing E3 ubiquitin ligase |
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| C7R | 242 | D5R | 242 | D4R | 242 |
| Apoptosis inhibitor, dsRNA-binding, interferon resistance | E3L | 190 | F3L | 190 |
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| E3L | 190 |
| eIF-2 | K3L | 88 | M3L | 88 |
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| C3L | 88 |
| Phosphatase, dephosphorylation of Stat 1 | H1L | 171 | J1L | 171 | H1L | 171 | I1L | 171 |
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| B8R | 272 | B7R | 271 | B9R | 267 | B9R | 266 |
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| B19R | 353 | B17R | 351 | B16R | 352 | B20R | 354 |
| IL-1 |
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| C8L | 124 | D6L | 126 | D5L | 126 |
| IL-18-binding |
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| B14R | 326 | B14R | 326 |
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| Complement binding | C3L | 263 | C17L | 259 |
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| D12L | 263 |
| TNF- and chemokine-binding, CrmB |
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| H4R | 351 | J2R | 348 | G2R | 349 |
| TNF-binding, CrmC |
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| A56R | 186 |
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| TNF- and chemokine-binding, CrmD |
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| K2R | 322 |
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| TNF-binding, CrmE |
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| K3R | 167 |
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| CC-chemokine-binding |
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| I5R | 255 | J3R | 246 | G3R | 253 |
| CC- | A41L | 219 | A43L | 219 | A41L | 221 | A46L | 218 |
| Inhibitor of NK-mediated NKG2D-dependent lysis of infected cells |
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| C2L | 178 | N3R | 176 |
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| Inhibitor of MHC class II antigen presentation | A35R | 176 | A36R | 176 | A37R | 176 |
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| Inhibitor of MHC class I complexes release from the PLC |
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| D10L | 96 |
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| Inhibitor of the intracellular trafficking of MHC class I molecules |
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| B8R | 221 | B10R | 221 |
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ORFs that are altered/nonfunctional as compared with a CPXV-GRI counterpart are set in bold.