Sunday, 4 September 2016 to Wednesday, 7 September 2016
Schedule : Back to Karolina Subrtova
Poster
5

FoF1-ATP synthase subunit α - A tale of two fragments

Authors

K Subrtova1; O Gahura2; M Saldivia3; B Panicucci2; J Mottram3; A Zikova2; A Schnaufer11 Institute of Immunology and Infection Research, University of Edinburgh;  2 Institute of Parasitology, Biology Centre, ASCR, Czech Republic;  3 University of York, Centre for Immunology and Infection

Discussion

The FoF1-ATP synthase is a reversible nanomotor synthesizing ATP in bacteria and eukaryotic mitochondria. The core catalytic F1 moiety of this multisubunit complex is formed by a globular hexamer of alternating subunits α and β sitting on a central stalk consisting of subunit γ and small subunits δ and ε [1]. The composition and structure of the core F1-ATPase is believed to be strictly conserved throughout evolution [1], however this notion is based on the established structures of FoF1-ATP synthase complexes of bacteria and model eukaryotes and may not reflect full eukaryotic diversity. Several reports have indicated that the Euglenozoa F1-ATPase subunit a is split into two fragments, presumably by proteolytic cleavage [2-5]. Both fragments stay associated with the complex. This feature appears to have no parallel in any other group of organisms. In this project, we are investigating whether a cleavage results in novel features of this key enzyme, that are important for the structure/function of FoF1-ATP synthase in trypanosomes. We also aim to identify the protease responsible. 
[1]J.E. Walker, Biochem. Soc. Trans. 41 (2013) 
[2]A. Zikova, et al , PLoS Pathog. 5 (2009) 
[3]D. Speijer, et al , Mol. Biochem. Parasitol. 85 (1997)
[4]R.E. Nelson, et al , Mol. Biochem. Parasitol. 135 (2004) 
[5]E. Perez, et al , Mitochondrion 19 (2014)

Hosted By

British Society for Parasitology (BSP)

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