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Eukaryotic Protein Kinases (ePKs) of the Helminth Parasite Schistosoma mansoni

Author: A Ahier
A Ahier
A Capes-Davis
A Osman
A Rambaut
A Zerlotini
Adhemar Zerlotini
AK Kalis
AL Jackson
AM Gurnett
B Pils
B Stronach
B Zhou
BC Van
BE Swierczewski
C Dissous
C Gally
C Naula
C Notredame
CA Bradham
CA Diaz
CR Caffrey
D Bahia
D Bahia
D Bahia
D Bahia
D Miranda-Saavedra
E Ghedin
EM Zdobnov
F Aguero
F Ludolf
G Manning
G Manning
G Manning
GD Plowman
GI Gallicano
Guilherme Oliveira
H Mellor
H Ramachandran
J Boudeau
J Felsenstein
J Knobloch
J Moffat
J Ren
J Vicogne
Jerônimo C Ruiz
JJ Eckert
JJ Kim
JJ Vowels
JM Fitzpatrick
JP Webster
K Anamika
K Deshmukh
K Kapp
K Kapp
K Katoh
K Kemphues
K Kondoh
K Rutherford
KEGG
KinBase
L Pica-Mattoccia
Laila A Nahum
Larissa L Silva
Luiza F Andrade
Lívia GA Avelar
M Berriman
M Bhagwat
M Knockaert
M Parsons
M Salzet
M Waisberg
M Waisberg
MG Wilkinson
MH Ludtmann
MJ Beall
MJ Doenhoff
MJ Doenhoff
MT Swulius
MV Sundaram
N Khayath
P Ward
PJ Muhlrad
PJ Parker
PR Dohrmann
PT Lin
PT LoVerde
PT LoVerde
R Steinhart
RA Wilson
RD Finn
RG Donald
RM Eglen
S Beckmann
S Caenepeel
S Hunter
S Lehtonen
S Nishimoto
S Noselli
S Verjovski-Almeida
SD Melman
SG Forrester
SJ Davies
SK Hanks
SK Hanks
SK Hanks
SN Boyle
SS Taylor
T Hall
T Tanoue
T Tanoue
V Reinke
W Haas
W Haas
W Hu
W Kunz
Y Yan
ZG Han
Publication venue: BioMed Central
Publication date: 01/01/2011
Field of study

Abstract Background Schistosomiasis remains an important parasitic disease and a major economic problem in many countries. The <it>Schistosoma mansoni </it>genome and predicted proteome sequences were recently published providing the opportunity to identify new drug candidates. Eukaryotic protein kinases (ePKs) play a central role in mediating signal transduction through complex networks and are considered druggable targets from the medical and chemical viewpoints. Our work aimed at analyzing the <it>S. mansoni </it>predicted proteome in order to identify and classify all ePKs of this parasite through combined computational approaches. Functional annotation was performed mainly to yield insights into the parasite signaling processes relevant to its complex lifestyle and to select some ePKs as potential drug targets. Results We have identified 252 ePKs, which corresponds to 1.9% of the <it>S. mansoni </it>predicted proteome, through sequence similarity searches using HMMs (Hidden Markov Models). Amino acid sequences corresponding to the conserved catalytic domain of ePKs were aligned by MAFFT and further used in distance-based phylogenetic analysis as implemented in PHYLIP. Our analysis also included the ePK homologs from six other eukaryotes. The results show that <it>S. mansoni </it>has proteins in all ePK groups. Most of them are clearly clustered with known ePKs in other eukaryotes according to the phylogenetic analysis. None of the ePKs are exclusively found in <it>S. mansoni </it>or belong to an expanded family in this parasite. Only 16 <it>S. mansoni </it>ePKs were experimentally studied, 12 proteins are predicted to be catalytically inactive and approximately 2% of the parasite ePKs remain unclassified. Some proteins were mentioned as good target for drug development since they have a predicted essential function for the parasite. Conclusions Our approach has improved the functional annotation of 40% of <it>S. mansoni </it>ePKs through combined similarity and phylogenetic-based approaches. As we continue this work, we will highlight the biochemical and physiological adaptations of <it>S. mansoni </it>in response to diverse environments during the parasite development, vector interaction, and host infection.</p

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