TDR Targets

Detailed view for Tb927.11.6690

Basic information

TDR Targets ID: 16602
Trypanosoma brucei, NEK family Serine/threonine-protein kinase, putative
Source Database / ID: TriTrypDB GeneDB

pI: 5.2272 | Length (AA): 407 | MW (Da): 45186 | Paralog Number: 0

Signal peptide: N | GPI Anchor: | Predicted trans-membrane segments: 0

Druggability Group : DG4

Targets have been classified into druggability groups (DG) according to their druggability score in network driven prioritizations. DGs range from 1 to 5; the higher the group number, the higher the chance of the target to be druggable

Network

Pfam domains

PF00069 Protein kinase domain

Gene Ontology

Mouse over links to read term descriptions.

GO:0005575 cellular_component
GO:0005524 ATP binding
GO:0004713 protein tyrosine kinase activity
GO:0004674 protein serine/threonine kinase activity
GO:0004672 protein kinase activity
GO:0006468 protein amino acid phosphorylation

Metabolic Pathways

Inositol phosphate metabolism (KEGG)
Benzoate degradation via CoA ligation (KEGG)
Phosphatidylinositol signaling system (KEGG)

Structural information

Modbase 3D models:

There are 4 models calculated for this protein. More info on these models, including the models themselves is available at: Modbase

Target Beg	Target End	Template	Template Beg	Template End	Identity	Evalue	Model Score	MPQS	zDope
11	406	4tnd (A)	96	452	18.00	0	1	1.02707	0.58
190	337	2izr (A)	116	253	26.00	0.53	0.8	0.573836	-0.14
263	406	4lg4 (D)	121	282	22.00	0	0.38	0.607608	-0.53
270	336	4aoj (A)	656	731	40.00	0.45	0.14	0.369819	0.45

Help me make sense of these data.

Target Beg: first modeled residue
Target End: last modeled residue
Template: template structure used for modelling (PDB accession and chain)
Template Beg: first template residue in target-template alignment
Template End: last template residue in target-template alignment
Identity: sequence identity
Evalue: E value for target-template hit
Model Score: GA341 score (>0.7 for reliable model)
MPQS: ModPipe Quality Score (>1.1 for reliable model)
zDope: zDope Score (negative for reliable model)

A more detailed description of these scores is available at the Modbase Model Evaluation Help Pages, and in the papers referenced therein.

PDB Structures:

No structure availble in the PDB for this protein

Expression

Upregulation Percent	Ranking	Stage	Dataset
Upper 60-80% percentile		Procyclic, Bloodstream Form.	Siegel TN

Show/Hide expression data references

Siegel TN

Genome-wide analysis of mRNA abundance in two life-cycle stages of Trypanosoma brucei and identification of splicing and polyadenylation sites.

Orthologs

Ortholog group members (OG5_145884)

Species	Accession	Gene Product
Leishmania braziliensis	LbrM.11.0280	protein kinase, putative
Leishmania donovani	LdBPK_110560.1	protein kinase, putative
Leishmania infantum	LinJ.11.0560	protein kinase, putative
Leishmania major	LmjF.11.0510	protein kinase, putative
Leishmania mexicana	LmxM.11.0510	protein kinase, putative
Trypanosoma brucei gambiense	Tbg972.11.7600	protein kinase, putative
Trypanosoma brucei	Tb927.11.6690	NEK family Serine/threonine-protein kinase, putative
Trypanosoma congolense	TcIL3000_0_06980	protein kinase, putative
Trypanosoma congolense	TcIL3000.11.7250	protein kinase, putative
Trypanosoma cruzi	TcCLB.506773.100	protein kinase, putative
Trypanosoma cruzi	TcCLB.508799.110	protein kinase, putative

Essentiality

Tb927.11.6690 has direct evidence of essentiality

Gene/Ortholog	Organism	Phenotype	Source Study
Tb11.02.4530 this record	Trypanosoma brucei	no significant loss or gain of fitness in bloodstream forms (3 days)	alsford
Tb11.02.4530 this record	Trypanosoma brucei	significant gain of fitness in bloodstream forms (6 days)	alsford
Tb11.02.4530 this record	Trypanosoma brucei	significant loss of fitness in procyclic forms	alsford
Tb11.02.4530 this record	Trypanosoma brucei	significant loss of fitness in differentiation of procyclic to bloodstream forms	alsford

Show/Hide essentiality data references

shigen

Profiling of E. coli Chromosome (PEC)

National Institute of Genetics, Japan

neb

C. elegans RNAi phenotypes

Data obtained from Wormbase WS150, curated by K. Chaudary and T. Carlow, New England Biolabs

plasmo

Functional Profiling of a Plasmodium Genome Reveals an Abundance of Essential Genes.

Bushell, Ellen, et al. "Functional profiling of a Plasmodium genome reveals an abundance of essential genes." Cell 170.2 (2017): 260-272.

blattner

Systematic mutagenesis of the E. coli (MG1655) genome

J Bacteriol 2004, 186:4921-4930

sidik

A Genome-wide CRISPR Screen in Toxoplasma Identifies Essential Apicomplexan Genes.

Sidik, Saima M., et al. "A genome-wide CRISPR screen in toxoplasma identifies essential apicomplexan genes." Cell 166.6 (2016): 1423-1435.

yeastgenome

Systematic deletion of yeast genes

Saccharomyces Genome Database

goodall

The Essential Genome of Escherichia coli K-12 (Transposon directed high-throughput mutagenesis)

Goodall, Emily CA, et al. "The essential genome of Escherichia coli K-12." mBio 9.1 (2018): e02096-17.

alsford

High-throughput phenotyping using parallel sequencing of RNA interference targets in the African trypanosome

Genome Res 2011, 21:915-924

wormbase

C. elegans RNAi experiments

WormBase web site, http://www.wormbase.org, release WS170

gerdes

Experimental determination and system-level analysis of essential genes in E. coli MG1655

Gerdes et al., J Bacteriol. 2003 185:5673-84

keio

Systematic single-gene knock-out mutants of E. coli K12

The Keio Collection

nmpdr

Genome-scale essentiality datasets from published studies (M. tuberculosis)

National Microbial Pathogen Data Resource

Phenotypes and Validation (curated)

Annotated phenotypes:

Affected Entity	Phenotypic quality	Occurs in	Occurs at	Evidence	Observed in	Drugs/Inhibitors
cell proliferation (GO:0008283)	normal (PATO:0000461)		bloodstream stage trypomastigotes (PLO:0027)	inferred from RNAi experiment (ECO:0000019)		No drug identifiers listed for this gene.
Annotator:	fernan@iib.unsam.edu.ar.	Comment:	normal cell proliferation (no significant loss or gain of fitness) in bloodstream forms (stage 3 days).		References:	21363968
cell proliferation (GO:0008283)	increased (PATO:0000470)		bloodstream stage trypomastigotes (PLO:0027)	inferred from RNAi experiment (ECO:0000019)		No drug identifiers listed for this gene.
Annotator:	fernan@iib.unsam.edu.ar.	Comment:	increased cell proliferation (significant gain of fitness) in bloodstream forms (stage 6 days).		References:	21363968
cell proliferation (GO:0008283)	decreased (PATO:0000468)		procyclic (PLO:0034)	inferred from RNAi experiment (ECO:0000019)		No drug identifiers listed for this gene.
Annotator:	fernan@iib.unsam.edu.ar.	Comment:	decreased cell proliferation (significant loss of fitness) in differentiation of procyclic to bloodstream forms .		References:	21363968

In TDR Targets, information about phenotypes that are caused by drugs, or by genetic manipulation of cells (e.g. gene knockouts or knockdowns) is manually curated from the literature. These descriptions help to describe the potential of the target for drug development. If no information is available for this gene or if the information is incomplete, this may mean that i) the papers containing this information either appeared after the curation effort for this organism was carried out or they were inadvertently missed by curators; or that ii) the curation effort for this organism has not yet started.

In any case, if you have information about papers containing relevant validation data for this target, please contact us.

Annotated validation

No validation data for this target

Associated compounds / Druggability

Druggability index (range: 0 to 1): 0.5

Known modulators for this target

No chemical compounds associated to this gene

Predicted associations

By orthology with druggable targets

Non orthologous druggable targets

By sequence similarity to non orthologous druggable targets

Species	Target	Length	Identity	Alignment span	Linked Drugs	Reference
Plasmodium falciparum (isolate 3D7)	Cell division control protein 2 homolog	288 aa	20.6%	326 aa	Compounds	References
Xenopus laevis	Aurora kinase B-B	368 aa	24.0%	300 aa	Compounds	References
Xenopus laevis	Aurora kinase B-A	361 aa	23.3%	300 aa	Compounds	References
Patiria pectinifera	Cdc2	300 aa	23.5%	243 aa	Compounds	References
Rattus norvegicus	MAP kinase p38 alpha	360 aa	23.9%	318 aa	Compounds	References

Ranking Plot

Putative Drugs List

Raw	Global	Species
0.0012	0.5	0.5
0.0098	0.3242	0.2614
0.0056	1	0.5
0.0088	0.4477	0.5
0.0063	1	0.5
0.0016	0.5	0.5
0.0023	0.5	0.5
0.0011	1	0.5
0.0029	0.5	0.5
0.0093	0.8828	0
0.0037	1	0.5
0.0018	0.5	0.5
0.0062	0.6935	0
0.0016	0.5	0.5
0.0059	1	1
0.0032	0.5	0.5
0.0007	0.5	0.5
0.0033	0.5	0.5
0.0012	0.5	0.5
0.0007	0.5	0.5
0.0064	0.3377	0
0.0059	1	1
0.0026	0.5	0.5
0.0091	1	0.5
0.0032	0.5	0.5
0.0012	0.5	0.5
0.0027	1	0.5
0.0069	0.3067	1
0.0063	0.7244	0.2543
0.0039	0.5	0.5
0.0061	0.6883	0.5304
0.0003	0.5	0.5
0.0007	0.5	0.5
0.0092	1	0.5
0.0033	1	0.5
0.0039	0.9485	0.5
0.0004	0.5	0.5
0.0059	1	1
0.0081	0.5	0.5
0.0039	0.5	0.5
0.0042	0.5	0.5
0.0067	0.5	0.5
0.0081	1	0.5
0.0066	0.3101	0
0.0008	0.5	0.5
0.0022	0.5	0.5
0.0036	0.5	0.5

Assayability

Assay information

No assay information for this target.

Reagent availability

No reagent availability information for this target.

Bibliographic References

27 literature references were collected for this gene.

If you have references for this gene, please enter them in a user comment (below) or Contact us.

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Gene identifier	Tb927.11.6690 (Trypanosoma brucei), NEK family Serine/threonine-protein kinase, putative

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