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3.A.24.1.1
The RD1 (ESX-1) protein secretion complex (Type VII protein secretion system, T7SS).  EccA1 may be a secreted protein while ECCB1 - E1 may comprise the system (Houben et al. 2012).  This system (ESX-1) is present in the avirulent species, Mycobacterium smegmatis, where it is involved in conjugation (Coros et al. 2008).  ESX-1 uses the ESX-1-specific chaparone protein, EspG to interact with the secreted PE/PPE complex, while a homologous EspG specific for ESX-5 functions with the PE/PPE complex secreted by ESX-5.  Thus, EspG proteins may be system-specific chaparones for T7SSs (Daleke et al. 2012).  The main secreted virulence protein complex is a heterodimer: EsxA(ESAT-6)/EsxB(CFP-10) (Rosenberger et al. 2012). EccB, a periplasmic homoheximer with the ATP-binding active site shared by two adjacent subunits, may act as the energy provider in the transport of T7SS virulence factors and may be involved in the formation of a channel across the mycomembrane (Zhang et al. 2015). ESX-1 functions in resistance to and evasion of host responses.  It induces phagosomal rupture which releases bacteria into the cytosol of the host phagocytes (Gröschel et al. 2016). ESX-1 secrete EsxA and EsxB, which form a heterodimer, seem to have differing functions as EsxA can disrupt lipid bilayers (RBC and artificial membranes.  Thus EsxA may form pores as a prelude to membrane disruption (Gröschel et al. 2016).

Accession Number:O69736
Protein Name:Rv3871
Length:591
Molecular Weight:64561.00
Species:Mycobacterium tuberculosis [1773]
Number of TMSs:1
Location1 / Topology2 / Orientation3: Cytoplasm1
Substrate

Cross database links:

RefSeq: NP_218388.1    NP_338539.1   
Entrez Gene ID: 886202    926284   
Pfam: PF01580   
KEGG: mtc:MT3985    mtu:Rv3871   

Gene Ontology

GO:0016021 C:integral to membrane
GO:0005524 F:ATP binding
GO:0003677 F:DNA binding
GO:0017111 F:nucleoside-triphosphatase activity
GO:0007049 P:cell cycle
GO:0051301 P:cell division
GO:0007059 P:chromosome segregation

References (8)

[1] “Deciphering the biology of Mycobacterium tuberculosis from the complete genome sequence.”  Cole S.T.et.al.   9634230
[2] “Whole-genome comparison of Mycobacterium tuberculosis clinical and laboratory strains.”  Fleischmann R.D.et.al.   12218036
[3] “Acute infection and macrophage subversion by Mycobacterium tuberculosis require a specialized secretion system.”  Stanley S.A.et.al.   14557536
[4] “Dissection of ESAT-6 system 1 of Mycobacterium tuberculosis and impact on immunogenicity and virulence.”  Brodin P.et.al.   16368961
[5] “C-terminal signal sequence promotes virulence factor secretion in Mycobacterium tuberculosis.”  Champion P.A.et.al.   16973880
[6] “A mycobacterium ESX-1-secreted virulence factor with unique requirements for export.”  McLaughlin B.et.al.   17676952
[7] “targetTB: a target identification pipeline for Mycobacterium tuberculosis through an interactome, reactome and genome-scale structural analysis.”  Raman K.et.al.   19099550
[8] “Systematic genetic nomenclature for type VII secretion systems.”  Bitter W.et.al.   19876390

External Searches:

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Predict TMSs (Predict number of transmembrane segments)
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FASTA formatted sequence
1:	MTAEPEVRTL REVVLDQLGT AESRAYKMWL PPLTNPVPLN ELIARDRRQP LRFALGIMDE 
61:	PRRHLQDVWG VDVSGAGGNI GIGGAPQTGK STLLQTMVMS AAATHSPRNV QFYCIDLGGG 
121:	GLIYLENLPH VGGVANRSEP DKVNRVVAEM QAVMRQRETT FKEHRVGSIG MYRQLRDDPS 
181:	QPVASDPYGD VFLIIDGWPG FVGEFPDLEG QVQDLAAQGL AFGVHVIIST PRWTELKSRV 
241:	RDYLGTKIEF RLGDVNETQI DRITREIPAN RPGRAVSMEK HHLMIGVPRF DGVHSADNLV 
301:	EAITAGVTQI ASQHTEQAPP VRVLPERIHL HELDPNPPGP ESDYRTRWEI PIGLRETDLT 
361:	PAHCHMHTNP HLLIFGAAKS GKTTIAHAIA RAICARNSPQ QVRFMLADYR SGLLDAVPDT 
421:	HLLGAGAINR NSASLDEAVQ ALAVNLKKRL PPTDLTTAQL RSRSWWSGFD VVLLVDDWHM 
481:	IVGAAGGMPP MAPLAPLLPA AADIGLHIIV TCQMSQAYKA TMDKFVGAAF GSGAPTMFLS 
541:	GEKQEFPSSE FKVKRRPPGQ AFLVSPDGKE VIQAPYIEPP EEVFAAPPSA G