P123
mRNA-capping enzyme nsP1
     (EC 2.1.1.-)
     (EC 2.7.7.-)
     (Non-structural protein 1)
Protease/triphosphatase/NTPase/helicase nsP2
     (EC 3.4.22.-)
     (EC 3.1.3.33)
     (EC 3.6.1.15)
     (EC 3.6.1.-)
     (Non-structural protein 2)
     (nsP2)
Non-structural protein 3
     (nsP3)
RNA-directed RNA polymerase nsP4
     (EC 2.7.7.48)
     (Non-structural protein 4)
     (nsP4)

Gene name

None

From

Chikungunya virus (strain S27-African prototype) (CHIKV)

[TaxID: 371094]

Taxonomy

Viruses; ssRNA positive-strand viruses, no DNA stage; Togaviridae; Alphavirus; SFV complex.

Virus hosts

Aedes aegypti (Yellowfever mosquito) [TaxID: 7159]
Aedes albopictus (Forest day mosquito) [TaxID: 7160]
Aedes furcifer [TaxID: 299627]
Aedes polynesiensis [TaxID: 188700]
Cercopithecus [TaxID: 9533]
Homo sapiens (Human) [TaxID: 9606]
Macaca (macaques) [TaxID: 9539]
Pan troglodytes (Chimpanzee) [TaxID: 9598]
Papio (baboons) [TaxID: 9554]
Presbytis [TaxID: 9573]

Protein existence

2: Evidence at transcript level;

References

[1]

NUCLEOTIDE SEQUENCE [GENOMIC RNA].
PubMed=12466484 [NCBI, ExPASy, EBI, Israel, Japan]
Khan A.H., Morita K., Parquet Md Mdel C., Hasebe F., Mathenge E.G., Igarashi A.;
"Complete nucleotide sequence of chikungunya virus and evidence for an internal polyadenylation site.";
J. Gen. Virol. 83:3075-3084(2002).

Comments

FUNCTION: P123 is short-lived polyproteins, accumulating during early stage of infection. It localizes the viral replication complex to the cytoplasmic surface of modified endosomes and lysosomes. By interacting with nsP4, it starts viral genome replication into antigenome. After these early events, P123 is cleaved sequentially into nsP1, nsP2 and nsP3. This sequence of delayed processing would allow correct assembly and membrane association of the RNA polymerase complex (By similarity).
FUNCTION: nsP1 is a cytoplasmic capping enzyme. This function is necessary since all viral RNAs are synthesized in the cytoplasm, and host capping enzymes are restricted to the nucleus. The enzymatic reaction involves a covalent link between 7-methyl-GMP and nsP1, whereas eukaryotic capping enzymes form a covalent complex only with GMP. nsP1 capping would consist in the following reactions: GTP is first methylated and then forms the m7GMp-nsP1 complex, from which 7-methyl-GMP complex is transferred to the mRNA to create the cap structure. Palmitoylated nsP1 is remodeling host cell cytoskeleton, and induces filopodium-like structure formation at the surface of the host cell (By similarity).
FUNCTION: nsP2 has two separate domain with different biological activities. The N-terminal section is part of the RNA polymerase complex and has RNA trisphosphatase and RNA helicase activity. The C-terminal section harbors a protease that specifically cleaves and releases the four mature proteins (By similarity).
FUNCTION: nsP3 is essential for minus strand and subgenomic 26S mRNA synthesis (By similarity).
FUNCTION: nsP4 is a RNA dependent RNA polymerase. It replicates genomic and antigenomic RNA by recognizing replications specific signals. Transcribes also a 26S subgenomic mRNA by initiating RNA synthesis internally on antigenomic RNA. This 26S mRNA encodes for structural proteins (By similarity).
CATALYTIC ACTIVITY: S-adenosyl-L-methionine + GTP = m₇GTP.
CATALYTIC ACTIVITY: m₇GTP + (5')pp-Pur-mRNA = diphosphate + m₇G(5')ppp-Pur-mRNA.
CATALYTIC ACTIVITY: (5')ppp-mRNA + H₂O = (5')pp-mRNA + phosphate.
CATALYTIC ACTIVITY: A 5'-phosphopolynucleotide + H₂O = a polynucleotide + phosphate.
CATALYTIC ACTIVITY: NTP + H₂O = NDP + phosphate.
CATALYTIC ACTIVITY: Nucleoside triphosphate + RNA(n) = diphosphate + RNA(n+1).
SUBUNIT: P123 interacts with nsP4; nsP1, nsP2, nsP3 and nsP4 interact with each other, and with uncharacterized host factors (By similarity).
SUBCELLULAR LOCATION: Non-structural polyprotein: Endosome membrane; Peripheral membrane protein; Cytoplasmic side (By similarity). Lysosome membrane; Peripheral membrane protein; Cytoplasmic side (By similarity). Note=Located on the cytoplasmic surface of modified endosomes and lysosomes, also called cytopathic vacuoles type I (CPVI). These vacuoles contain numerous small circular invaginations (spherules) which may be the sites of RNA synthesis.
SUBCELLULAR LOCATION: P123: Endosome membrane; Peripheral membrane protein; Cytoplasmic side (By similarity). Lysosome membrane; Peripheral membrane protein; Cytoplasmic side (By similarity).
SUBCELLULAR LOCATION: mRNA-capping enzyme nsP1: Endosome membrane; Peripheral membrane protein; Cytoplasmic side (By similarity). Lysosome membrane; Peripheral membrane protein; Cytoplasmic side (By similarity). Cell membrane; Peripheral membrane protein; Cytoplasmic side (By similarity). Note=In the late phase of infection, the polyprotein is quickly cleaved before localization to cellular membranes. Then a fraction of nsP1 localizes to the inner surface of the plasma membrane and its filopodial extensions (By similarity).
SUBCELLULAR LOCATION: Protease/triphosphatase/NTPase/helicase nsP2: Endosome membrane; Peripheral membrane protein; Cytoplasmic side (By similarity). Lysosome membrane; Peripheral membrane protein; Cytoplasmic side (By similarity). Nucleus (By similarity). Note=In the late phase of infection, the polyprotein is quickly cleaved before localization to cellular membranes. Then approximately half of nsP2 is found in the nucleus (By similarity).
SUBCELLULAR LOCATION: Non-structural protein 3: Endosome membrane; Peripheral membrane protein; Cytoplasmic side (By similarity). Lysosome membrane; Peripheral membrane protein; Cytoplasmic side (By similarity). Cytoplasm (By similarity). Note=In the late phase of infection, the polyprotein is quickly cleaved before localization to cellular membranes. Then nsP3 and nsP3' seems to aggregate in cytoplasm (By similarity).
SUBCELLULAR LOCATION: RNA-directed RNA polymerase nsP4: Endosome membrane; Peripheral membrane protein; Cytoplasmic side (By similarity). Lysosome membrane; Peripheral membrane protein; Cytoplasmic side (By similarity).
INDUCTION: Viral replication produces dsRNA in the late phsae of infection, resulting in a strong activation of host EIF2AK2/PKR, leading to almost complete phosphorylation of EIF2A. This inactivates completely cellular translation initiation, resulting in a dramatic shutoff of proteins synthesis. Translation of viral non-structural polyprotein and all cellular proteins are stopped in infected cell between 2 and 4 hours post infection. Only the 26S mRNA is still translated into viral structural proteins, presumably through a unique mechanism of enhancer element which counteract the translation inhibition mediated by EIF2A. By doing this, the virus uses the cellular defense for its own advantage: shutoff of cellular translation allows to produce big amounts of structural proteins needed for the virus to bud out of the doomed cell.
PTM: Specific enzymatic cleavages in vivo yield mature proteins. The polyprotein is synthesized as P1234 by stop codon readthrough. This polyprotein is processed differently depending on the stage of infection. In early stages, P1234 is first cleaved in trans, through its nsP2 protease activity, releasing P123 and nsP4. P123 and nsP4 start to replicate the viral genome into its antigenome. After these early events, nsP1 is cleaved in cis by nsP2 protease, releasing P23 polyprotein. Cleavage of nsP1 exposes an 'activator' at the N-terminus of P23 which induces its cleavage into nsP2 and nsP3 by the viral protease. This sequence of delayed processing would allow correct assembly and membrane association of the RNA-polymerase complex. In the late stage of infection, the presence of free nsP2 in the cytoplasm cleaves P1234 quickly into P12 and P34, then into the four nsP (By similarity).
PTM: nsP1 is palmitoylated by host (By similarity).
PTM: nsP4 is ubiquitinated; targets the protein for rapid degradation via the ubiquitin system (By similarity).
SIMILARITY: Contains 1 Macro domain.
SIMILARITY: Contains 1 peptidase C9 domain [view classification].
SIMILARITY: Contains 1 RdRp catalytic domain.
CAUTION: There is no stop codon readthrough before nsP4.

Copyright

Copyrighted by the UniProt Consortium, see http://www.uniprot.org/terms. Distributed under the Creative Commons Attribution-NoDerivs License.

Cross-references

Sequence databases

EMBL

AF369024; AAN05101.1; -; Genomic_RNA.

[EMBL / GenBank / DDBJ] [CoDingSequence]

RefSeq

NP_690588.1; -.

3D structure databases

HSSP

P08411; 1FW5. [HSSP ENTRY / PDB]

ModBase

Q8JUX6.

Protein family/group databases

MEROPS

C09.001; -.

Ontologies

GO:0005765;	Cellular component: lysosomal membrane (inferred from electronic annotation from UniProtKB-SubCell).
GO:0005886;	Cellular component: plasma membrane (inferred from electronic annotation from UniProtKB-SubCell).
GO:0017111;	Molecular function: nucleoside-triphosphatase activity (inferred from electronic annotation from EC).
GO:0004651;	Molecular function: polynucleotide 5'-phosphatase activity (inferred from electronic annotation from EC).
QuickGo view.

Family and domain databases

InterPro

IPR002589; A1pp.
IPR002588; MeTrfase_vir.
IPR002620; Peptidase_C9.
IPR001788; RNA-dep_RNA_pol_vir-typ.
IPR000606; RNA_helicase1_vir.
IPR007094; RNA_pol_PSvir.
Graphical view of domain structure.

Pfam

PF01661; A1pp; 1.
PF01707; Peptidase_C9; 1.
PF00978; RdRP_2; 1.
PF01443; Viral_helicase1; 1.
PF01660; Vmethyltransf; 1.
Pfam graphical view of domain structure.

SMART

SM00506; A1pp; 1.
SMART graphical view of domain structure.

PROSITE

PS51154; MACRO; 1.
PS50507; RDRP_SSRNA_POS; 1.
PROSITE graphical view of domain structure (profiles).

BLOCKS

Q8JUX6.

Genome annotation databases

GeneID

956309; -.

Other

ProtoNet

Q8JUX6.

UniRef

View cluster of proteins with at least 50% / 90% / 100% identity.

Keywords

ATP-binding; Cell membrane; Cytoplasm; Endosome; Helicase; Hydrolase; Lipoprotein; Lysosome; Membrane; Methyltransferase; mRNA capping; mRNA processing; Multifunctional enzyme; Nucleotide-binding; Nucleotidyltransferase; Nucleus; Palmitate; Phosphoprotein; Protease; RNA replication; RNA-binding; RNA-directed RNA polymerase; Thiol protease; Transferase; Ubl conjugation.

Features

Feature table viewer

Feature aligner

`Key`	`From To`	`Length`	`Description`	`FTId`
`CHAIN`	`1 2474`	`2474`	`Non-structural polyprotein.`	`PRO_0000308395`
`CHAIN`	`1 1863`	`1863`	`P123 (By similarity).`	`PRO_0000227760`
`CHAIN`	`1 535`	`535`	`mRNA-capping enzyme nsP1 (By similarity).`	`PRO_0000227761`
`CHAIN`	`536 1333`	`798`	`Protease/triphosphatase/NTPase/helicase nsP2 (By similarity).`	`PRO_0000227762`
`CHAIN`	`1334 1863`	`530`	`Non-structural protein 3 (By similarity).`	`PRO_0000227763`
`CHAIN`	`1864 2474`	`611`	`RNA-directed RNA polymerase nsP4 (By similarity).`	`PRO_0000227764`
`DOMAIN`	`964 1165`	`202`	`Peptidase C9.`
`DOMAIN`	`1334 1493`	`160`	`Macro.`
`DOMAIN`	`2228 2343`	`116`	`RdRp catalytic.`
`NP_BIND`	`721 728`	`8`	`ATP (Potential).`
`REGION`	`244 263`	`20`	`nsP1 membrane-binding (By similarity).`
`REGION`	`1005 1024`	`20`	`Nucleolus localization signal (By similarity).`
`MOTIF`	`1182 1186`	`5`	`Nuclear localization signal (By similarity).`
`ACT_SITE`	`1013 1013`		`For cysteine protease nsP2 activity (By similarity).`
`ACT_SITE`	`1083 1083`		`For cysteine protease nsP2 activity (By similarity).`
`SITE`	`535 536`	`2`	`Cleavage; by nsP2 (By similarity).`
`SITE`	`1333 1334`	`2`	`Cleavage; by nsP2 (By similarity).`
`SITE`	`1863 1864`	`2`	`Cleavage; by nsP2 (By similarity).`
`LIPID`	`417 417`		`S-palmitoyl cysteine; by host (By similarity).`
`LIPID`	`419 419`		`S-palmitoyl cysteine; by host (By similarity).`

Sequence information

Length: 2474 AA [This is the length of the unprocessed precursor]

Molecular weight: 275652 Da [This is the MW of the unprocessed precursor]

CRC64: 97D250B9EB5A3BB0 [This is a checksum on the sequence]

        10         20         30         40         50         60 
MDPVYVDIDA DSAFLKALQR AYPMFEVEPR QVTPNDHANA RAFSHLAIKL IEQEIDPDST 

        70         80         90        100        110        120 
ILDIGSAPAR RMMSDRKYHC VCPMRSAEDP ERLANYARKL ASAAGKVLDR NISGKIGDLQ 

       130        140        150        160        170        180 
AVMAVPDTET PTFCLHTDVS CRQRADVAIY QDVYAVHAPT SLYHQAIKGV RLAYWVGFDT 

       190        200        210        220        230        240 
TPFMYNAMAG AYPSYSTNWA DEQVLKAKNI GLCSTDLTEG RRGKLSIMRG KKLEPCDRVL 

       250        260        270        280        290        300 
FSVGSTLYPE SRKLLKSWHL PSVFHLKGKL SFTCRCDTVV SCEGYVVKRI TMSPGLYGKT 

       310        320        330        340        350        360 
TGYAVTHHAD GFLMCKTTDT VDGERVSFSV CTYVPATICD QMTGILATEV TPEDAQKLLV 

       370        380        390        400        410        420 
GLNQRIVVNG RTQRNTNTMK NYMIPVVAQA FSKWAKECRK DMEDEKLLGV RERTLTCCCL 

       430        440        450        460        470        480 
WAFKKQKTHT VYKRPDTQSI QKVQAEFDSF VVPSLWSSGL SIPLRTRIKW LLSKVPKTDL 

       490        500        510        520        530        540 
TPYSGDAQEA RDAEKEAEEE REAELTLEAL PPLQAAQEDV QVEIDVEQLE DRAGAGIIET 

       550        560        570        580        590        600 
PRGAIKVTAQ PTDHVVGEYL VLSPQTVLRS QKLSLIHALA EQVKTCTHSG RAGRYAVEAY 

       610        620        630        640        650        660 
DGRVLVPSGY AISPEDFQSL SESATMVYNE REFVNRKLHH IAMHGPALNT DEESYELVRA 

       670        680        690        700        710        720 
ERTEHEYVYD VDQRRCCKKE EAAGLVLVGD LTNPPYHEFA YEGLKIRPAC PYKIAVIGVF 

       730        740        750        760        770        780 
GVPGSGKSAI IKNLVTRQDL VTSGKKENCQ EITTDVMRQR GLEISARTVD SLLLNGCNRP 

       790        800        810        820        830        840 
VDVLYVDEAF ACHSGTLLAL IALVRPRQKV VLCGDPKQCG FFNMMQMKVN YNHNICTQVY 

       850        860        870        880        890        900 
HKSISRRCTL PVTAIVSSLH YEGKMRTTNE YNKPIVVDTT GSTKPDPGDL VLTCFRGWVK 

       910        920        930        940        950        960 
QLQIDYRGHE VMTAAASQGL TRKGVYAVRQ KVNENPLYAS TSEHVNVLLT RTEGKLVWKT 

       970        980        990       1000       1010       1020 
LSGDPWIKTL QNPPKGNFKA TIKEWEVEHA SIMAGICSHQ MTFDTFQNKA NVCWAKSLVP 

      1030       1040       1050       1060       1070       1080 
ILETAGIKLN DRQWSQIIQA FKEDKAYSPE VALNEICTRM YGVDLDSGLF SKPLVSVYYA 

      1090       1100       1110       1120       1130       1140 
DNHWDNRPGG KMFGFNPEAA SILERKYPFT KGKWNINKQI CVTTRRIEDF NPTTNIIPAN 

      1150       1160       1170       1180       1190       1200 
RRLPHSLVAE HRPVKGERME WLVNKINGHH VLLVSGCSLA LPTKRVTWVA PLGVRGADYT 

      1210       1220       1230       1240       1250       1260 
YNLELGLPAT LGRYDLVVIN IHTPFRIHHY QQCVDHAMKL QMLGGDSLRL LKPGGSLLIR 

      1270       1280       1290       1300       1310       1320 
AYGYADRTSE RVICVLGRKF RSSRALKPPC VTSNTEMFFL FSNFDNGRRN FTTHVMNNQL 

      1330       1340       1350       1360       1370       1380 
NAAFVGQATR AGCAPSYRVK RMDIAKNDEE CVVNAANPRG LPGDGVCKAV YKKWPESFKN 

      1390       1400       1410       1420       1430       1440 
SATPVGTAKT VMCGTYPVIH AVGPNFSNYS ESEGDRELAA AYREVAKEVT RLGVNSVAIP 

      1450       1460       1470       1480       1490       1500 
LLSTGVYSGG KDRLTQSLNH LFTAMDSTDA DVVIYCRDKE WEKKISEAIQ MRTQVELLDE 

      1510       1520       1530       1540       1550       1560 
HISIDCDVVR VHPDSSLAGR KGYSTTEGAL YSYLEGTRFH QTAVDMAEIY TMWPKQTEAN 

      1570       1580       1590       1600       1610       1620 
EQVCLYALGE SIESIRQKCP VDDADASSPP KTVPCLCRYA MTPERVTRLR MNHVTSIIVC 

      1630       1640       1650       1660       1670       1680 
SSFPLPKYKI EGVQKVKCSK VMLFDHNVPS RVSPREYRPS QESVQEASTT TSLTHSQFDL 

      1690       1700       1710       1720       1730       1740 
SVDGKILPVP SDLDADAPAL EPALDDGAIH TLPSATGNLA AVSDWVMSTV PVAPPRRRRG 

      1750       1760       1770       1780       1790       1800 
RNLTVTCDER EGNITPMASV RFFRAELCPV VQETAETRDT AMSLQAPPST ATELSHPPIS 

      1810       1820       1830       1840       1850       1860 
FGAPSETFPI TFGDFNEGEI ESLSSELLTF GDFLPGEVDD LTDSDWSTCS DTDDELRLDR 

      1870       1880       1890       1900       1910       1920 
AGGYIFSSDT GPGHLQQKSV RQSVLPVNTL EEVHEEKCYP PKLDEAKEQL LLKKLQESAS 

      1930       1940       1950       1960       1970       1980 
MANRSRYQSR KVENMKATII QRLKRGCRLY LMSETPKVPT YRTTYPAPVY SPPINVRLSN 

      1990       2000       2010       2020       2030       2040 
PESAVAACNE FLARNYPTVS SYQITDEYDA YLDMVDGSES CLDRATFNPS KLRSYPKQHA 

      2050       2060       2070       2080       2090       2100 
YHAPSIRSAV PSPFQNTLQN VLAAATKRNC NVTQMRELPT LDSAVFNVEC FKKFACNQEY 

      2110       2120       2130       2140       2150       2160 
WEEFAASPIR ITTENLTTYV TKLKGPKAAA LFAKTHNLLP LQEVPMDRFT VDMKRDVKVT 

      2170       2180       2190       2200       2210       2220 
PGTKHTEERP KVQVIQAAEP LATAYLCGIH RELVRRLNAV LLPNVHTLFD MSAEDFDAII 

      2230       2240       2250       2260       2270       2280 
AAHFKPGDTV LETDIASFDK SQDDSLALTA LMLLEDLGVD HSLLDLIEAA FGEISSCHLP 

      2290       2300       2310       2320       2330       2340 
TGTRFKFGAM MKSGMFLTLF VNTLLNITIA SRVLEDRLTK SACAAFIGDD NIIHGVVSDE 

      2350       2360       2370       2380       2390       2400 
LMAARCATWM NMEVKIIDAV VSQKAPYFCG GFILHDIVTG TACRVADPLK RLFKLGKPLA 

      2410       2420       2430       2440       2450       2460 
AGDEQDEDRR RALADEVVRW QRTGLIDELE KAVYSRYEVQ GISVVVMSMA TFASSRSNFE 

      2470 
KLRGPVVTLY GGPK

Q8JUX6 in FASTA format

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View entry in raw text format (no links)
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	BLAST submission on ExPASy/SIB or at NCBI (USA)		Sequence analysis tools: ProtParam, ProtScale, Compute pI/Mw, PeptideMass, PeptideCutter, Dotlet (Java)
	ScanProsite, MotifScan		Submit a homology modeling request to SWISS-MODEL
	NPSA Sequence analysis tools