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Structural insights into kinetoplastid coronin oligomerization domain and F-actin interaction

Authors :
Pankaj Singh Parihar
Aastha Singh
Sharanbasappa Shrimant Karade
Amogh Anant Sahasrabuddhe
J. Venkatesh Pratap
Source :
Current Research in Structural Biology, Vol 3, Iss , Pp 268-276 (2021)
Publication Year :
2021
Publisher :
Elsevier, 2021.

Abstract

The two-domain actin associated protein coronin interacts with filamentous (F-) actin, facilitating diverse biological processes including cell proliferation, motility, phagocytosis, host-parasite interaction and cargo binding. The conserved N-terminal β-propeller domain is involved in protein: protein interactions, while the C-terminal coiled-coil domain mediates oligomerization, transducing conformational changes. The L. donovani coronin coiled-coil (LdCoroCC) domain exhibited a novel topology and oligomer association with an inherent asymmetry, caused primarily by three a residues of successive heptads. In the T.brucei homolog (TbrCoro), two of these ‘a’ residues are different (Val 493 & 507 replacing LdCoroCC Ile 486 and Met 500 respectively). The elucidated structure possesses a similar topology and assembly while comparative structural analysis shows that the T.brucei coronin coiled-coil domain (TbrCoroCC) too possesses the asymmetry though its magnitude is smaller. Analysis identifies that the asymmetric state is stabilized via cyclic salt bridges formed by Arg 497 and Glu 504. Co-localization studies (LdCoro, TbrCoro and corresponding mutant coiled coil constructs) with actin show that there are subtle differences in their binding patterns, with the double mutant V493I–V507M showing maximal effect. None of the constructs have an effect on F-actin length. Taken together with LdCoroCC, we therefore conclude that the inherent asymmetric structures are essential for kinetoplastids, and are of interest in understanding and exploiting actin dynamics.

Details

Language :
English
ISSN :
2665928X
Volume :
3
Issue :
268-276
Database :
Directory of Open Access Journals
Journal :
Current Research in Structural Biology
Publication Type :
Academic Journal
Accession number :
edsdoj.7219acf9e9984228b7c66f53117c554c
Document Type :
article
Full Text :
https://doi.org/10.1016/j.crstbi.2021.10.002