| Literature DB >> 17786195 |
Morgane Rolland1, David C Nickle, Wenjie Deng, Nicole Frahm, Christian Brander, Gerald H Learn, David Heckerman, Nebosja Jojic, Vladimir Jojic, Bruce D Walker, James I Mullins.
Abstract
BACKGROUND: While human immunodeficiency virus type 1 (HIV-1)-specific cytotoxic T lymphocytes preferentially target specific regions of the viral proteome, HIV-1 features that contribute to immune recognition are not well understood. One hypothesis is that similarities between HIV and human proteins influence the host immune response, i.e., resemblance between viral and host peptides could preclude reactivity against certain HIV epitopes. METHODOLOGY/PRINCIPALEntities:
Mesh:
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Year: 2007 PMID: 17786195 PMCID: PMC1952107 DOI: 10.1371/journal.pone.0000823
Source DB: PubMed Journal: PLoS One ISSN: 1932-6203 Impact factor: 3.240
HIV-1 nonamers with high similarities to human proteins.
| Significant 9-mers consensus 2001 | Human Protein sequence | Human protein | HIV database seq. corresponding to human prot. seq. | HIV-I B consensus 2001 position | Identities (Positives) |
| LHPVHAGPI | L | PTPRE | Gag 215–223 | 9/10 (10/10) | |
| LHP | T cell leukemia Homeobox 1 | LHP | 8/10 | ||
| EPFRDYVDRF |
| COPINE 5 | AAV71076 | Gag 291–300 | 8/9 |
| PFRDYVDR | AAV53244 | 8/9 | |||
| PDCKTILKA | HPDCKTI | DELTEX 4 homolog | AAV49378 | Gag 328–336 | 7/7 |
| NTPVFAIKKK | SP | HERV | P | Pol 209–221 | 11/13 |
| MTKILEPFR | MTKILEP | Piwi-like 2 | AAM74596 | Pol 319–327 | 7/8 |
|
| SON DNA Binding P. | AAK35877 | 6/9 (7/9) | ||
| FKNLKTGKY | FKN | Str Spe Recognition P. | FKN | Pol 501–508 | 6/7 |
| VNIVTDSQYA | VNI | HERV | VNI | Pol 648–657 | 9/10 |
| VN | Thrombospondin 3 precursor | VNI | 7/10 | ||
| YIEAEVIPA | GYIEA | unnamed P. | Pol 798–806 | 10/11 | |
| EIEAEV | p53 inducibleP. | AAV49469 | 6/6 | ||
| NWRSELYKY |
| peroxysomal acylcoA thioestherase | CAA64162 | Env 469–477 | 7/8 |
| AAG…TVW | 35/37 | Cancer associated RAK | Env 516–572 | 35/37 | |
| DQGPQREPY | qRP–DQGPQR | carcinoma ass. P. | DQGPQR | Vpr 7–15 | 9/13 (10/13) |
| DQGPQR | proline rich | 7/8 | |||
| PKTACTNCY | SQPK | Zn finger P. | SQPK | Tat 18–26 | 9/11 (10/11) |
| LAIVALVVA | ALVALVVA | Trypsin-domain P. | ALVALVVA | Vpu 7–15 | 9/10 |
| LAIVAL | small inducible cytokine 28 | 7/8 | |||
| EELLKTVRL | EELLK | nucleolar RNA associated P. | EELLK | Rev10–18 | 8/9 |
| LLKTVRL | LLKTVRL | 10/11 | |||
| TVRERMRRA | TTVR | Rhomboid P. | Nef 15–23 | 9/10 | |
| IYSQKRQDI | TYSQK | Ig heavy chain variable region | TYSQK | Nef 101–109 | 8/9 |
The level of similarity to host proteins for these HIV nonamers differed by 3 standard deviations from the level of similarity found with randomized nonamers. Amino acid changes are in bold italics and lower case.
Figure 1Frequency of recognition of HIV-1 B consensus 2001 peptides as a function of their similarity to human proteins.
410 peptides spanning the HIV-1 B consensus 2001 proteome were tested by ELISpot using PBMC from a cohort of 314 HIV-1 infected individuals. The vertical axis corresponds to the percentage of individuals who recognized a given peptide. The horizontal axis corresponds to the number of matches to the human proteome for each peptide. Matches were derived by dissecting the 410 peptides into overlapping 6-mers offset by one residue, and then scored against the RefSeq protein sequence database. Matches were normalized to account for the length of the starting peptide (ranging from 15–20 AA in length).
Figure 2Magnitude of the ELISpot responses elicited by HIV-1 B Nef peptides as a function of their similarity to human peptides.
The vertical axis corresponds to the mean number of spot-forming cells counted in ELISpot assays. The horizontal axis corresponds to Nef peptides that have 2, 3 or 4 differences with their closest human peptides.
Figure 3Frequency of recognition of HIV-1 B consensus 2001 peptides as a function of their intrinsic disorder prediction score.
The vertical axis corresponds to the percentage of HIV-1 infected individuals that recognized each of the 410 peptides spanning the HIV-1 B consensus 2001 proteome. The horizontal axis corresponds to the disorder prediction score for each peptide, calculated using predictions of order/disorder made with the VSL1 predictor (PONDR®).