4.7 Article

Characterization of 14-3-3 Isoforms Expressed in the Echinococcus granulosus Pathogenic Larval Stage

Journal

JOURNAL OF PROTEOME RESEARCH
Volume 14, Issue 4, Pages 1700-1715

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/pr5010136

Keywords

14-3-3 proteins; Echinococcus granulosus; protein-protein interactions; host-parasite interactions

Funding

  1. CAPES [AUX-PE-PARASITOLOGIA-1278/2011]
  2. CNPq in Brazil [490923/2008-9]
  3. CONICYT
  4. FONDECYT in Chile [1130113, 1130717]
  5. CAPES
  6. PRODOC/CAPES
  7. FAPERGS

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The 14-3-3 protein family of eukaryotic regulators was studied in Echinococcus granulosus, the causative agent of cystic hydatid disease. These proteins mediate important cellular processes in eukaryotes and are expected to play important roles in parasite biology. Six isoforms of E. granulosus 14-3-3 genes and proteins (Eg14-3-3.1-6) were analyzed, and their phylogenetic relationships were established with bona fide 14-3-3 orthologous proteins from eukaryotic species. Eg14-3-3 isoforms with previous evidence of expression (Eg14-3-3.1-4) in E. granulosus pathogenic larval stage (metacestode) were cloned, and recombinant proteins were used for functional studies. These protein isoforms were detected in different components of E. granulosus metacestode, including interface components with the host. The roles that are played by Eg14-3-3 proteins in parasite biology were inferred from the repertoires of interacting proteins with each isoform, as assessed by gel overlay, cross-linking, and affinity chromatography assays. A total of 95 Eg14-3-3 protein ligands were identified by mass spectrometry. Eg14-3-3 isoforms have shared partners (44 proteins), indicating some overlapping functions; however, they also bind exclusive partners (51 proteins), suggesting Eg14-3-3 functional specialization. These ligand repertoires indicate the involvement of Eg14-3-3 proteins in multiple biochemical pathways in the E. granulosus metacestode and note some degree of isoform specialization.

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