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virulence, detoxification, adaptation

information pathways

cell wall and cell processes

stable RNAs

insertion seqs and phages

PE/PPE

intermediary metabolism and respiration

unknown

regulatory proteins

conserved hypotheticals

lipid metabolism

pseudogenes

Gene summary information

Gene name	Rv0519c
Gene length	903 bp
Identifier	Rv0519c
Location	611172 bp

Protein summary information

Molecular mass	31349.7 Da
Isoelectric point	8.4778
Protein length	300 amino acids

Structural information

PFAM	O33364

Orthologs

M. bovis AF2122-97	Mb0532c
M. leprae TN	ML2417
M. marinum M	MMAR_0858
M. tuberculosis 18b	MT18B_0647
M. tuberculosis MTBC0	mtbc0_000547

Cross-references

UniProt	O33364
SWISS-MODEL	O33364
TB database	Rv0519c

Interacting Drugs/Compounds

TDR Targets	Link

Precomputed results

BLAST	Report

General annotation

Type	CDS
Function	Unknown; could have possibly a lipolytic activity.
Product	Possible conserved membrane protein
Comments	Rv0519c, (MTCY20G10.09c), len: 300 aa. Possible conserved membrane protein, with hydrophobic region near N-terminus. Could be a lipase. Similar to Rv0774c\|MTCY369.19c\|A70708 from Mycobacterium tuberculosis (312 aa), FASTA scores: opt: 1092, E(): 0, (57.9% identity in 299 aa overlap). Contains PS00120 Lipases, serine active site.
Functional category	Cell wall and cell processes
Proteomics	Identified by mass spectrometry in the culture filtrate of M. tuberculosis H37Rv but not the membrane protein fraction or whole cell lysates (See de Souza et al., 2011).
Transcriptomics	DNA microarrays show lower level of expression in M. tuberculosis H37Rv than in phoP\|Rv0757 mutant (See Walters et al., 2006).
Mutant	Non-essential gene for in vitro growth of H37Rv in a MtbYM rich medium, by Himar1 transposon mutagenesis (see Minato et al. 2019). Disruption of this gene provides a growth advantage for in vitro growth of H37Rv, by analysis of saturated Himar1 transposon libraries (see DeJesus et al. 2017). Non essential gene by Himar1 transposon mutagenesis in H37Rv and CDC1551 strains (see Sassetti et al., 2003 and Lamichhane et al., 2003). Non-essential gene for in vitro growth of H37Rv, by Himar1 transposon mutagenesis (See Griffin et al., 2011). Check for mutants available at TARGET website

Coordinates

Type	Start	End	Orientation
CDS	611172	612074	-

Genomic sequence

Feature type Upstream flanking region (bp) Downstream flanking region (bp) Update

Protein sequence

>Mycobacterium tuberculosis H37Rv|Rv0519c|Rv0519c
VLRRGCAGNTDRRGIMTPMADLTRRALLRWGAGAGAGAAGVWAFGALVDPLEPQAAPAPFEPPTAGSSLPTRISGSFISAARGGIKTNWVISMPPGQSGQLRPVIALHGKDGNAGMMLDLGVEQGLARLVKEGKPAFAVVGVDGGNTYWHRRSSGGDSGAMVLDELLPMLTSMGMDTSRVGFLGWSMGGYGALLLGARLGPARTAGICAISPALFTSFTGSTPGAFDSYDDYVQHSVLGLPALNSIPLRVDCGTSDRFYFATRQFVNQLHQPPAGSFSPGGHDASYWREQLPGELAWMAS

Bibliography

Lamichhane G et al. [2003]. A postgenomic method for predicting essential genes at subsaturation levels of mutagenesis: application to Mycobacterium tuberculosis. Mutant
Sassetti CM et al. [2003]. Genes required for mycobacterial growth defined by high density mutagenesis. Mutant
Walters SB et al. [2006]. The Mycobacterium tuberculosis PhoPR two-component system regulates genes essential for virulence and complex lipid biosynthesis. Transcriptome
Griffin JE et al. [2011]. High-resolution phenotypic profiling defines genes essential for mycobacterial growth and cholesterol catabolism. Mutant
de Souza GA et al. [2011]. Bacterial proteins with cleaved or uncleaved signal peptides of the general secretory pathway. Proteomics
DeJesus MA et al. [2017]. Comprehensive Essentiality Analysis of the Mycobacterium tuberculosis Genome via Saturating Transposon Mutagenesis. Mutant
Minato Y et al. [2019]. Genomewide Assessment of Mycobacterium tuberculosis Conditionally Essential Metabolic Pathways. Mutant