The exceptional versatility of calmodulin (CaM) three-dimensional arrangement is reflected in the growing number of structural models of CaM/protein complexes currently available in the Protein Data Bank (PDB) database, revealing a great diversity of conformations, domain organization, and structural responses to Ca2 +. Understanding CaM binding is complicated by the diversity of target proteins sequences. Data mining of the structures shows that one face of each of the eight CaM helices can contribute to binding, with little overall difference between the Ca2 + loaded N- and C-lobes and a clear prevalence of the C-lobe low Ca2 + conditions. The structures reveal a remarkable variety of configurations where CaM binds its targets in a preferred orientation that can be reversed and where CaM rotates upon Ca2 + binding, suggesting a highly dynamic metastable relation between CaM and its targets. Recent advances in structure-function studies and the discovery of CaM mutations being responsible for human diseases, besides expanding the role of CaM in human pathophysiology, are opening new exciting avenues for the understanding of the how CaM decodes Ca2 +-dependent and Ca2 +-independent signals. © 2014 Elsevier Ltd.
The ever changing moods of calmodulin: How structural plasticity entails transductional adaptability / Villarroel, A.; Taglialatela, M.; Bernardo-Seisdedos, G.; Alaimo, A.; Agirre, J.; Alberdi, A.; Gomis-Perez, C.; Soldovieri, M. V.; Ambrosino, P.; Malo, C.; Areso, P.. - In: JOURNAL OF MOLECULAR BIOLOGY. - ISSN 0022-2836. - 426:15(2014), pp. 2717-2735. [10.1016/j.jmb.2014.05.016]
The ever changing moods of calmodulin: How structural plasticity entails transductional adaptability
Alaimo A.;
2014-01-01
Abstract
The exceptional versatility of calmodulin (CaM) three-dimensional arrangement is reflected in the growing number of structural models of CaM/protein complexes currently available in the Protein Data Bank (PDB) database, revealing a great diversity of conformations, domain organization, and structural responses to Ca2 +. Understanding CaM binding is complicated by the diversity of target proteins sequences. Data mining of the structures shows that one face of each of the eight CaM helices can contribute to binding, with little overall difference between the Ca2 + loaded N- and C-lobes and a clear prevalence of the C-lobe low Ca2 + conditions. The structures reveal a remarkable variety of configurations where CaM binds its targets in a preferred orientation that can be reversed and where CaM rotates upon Ca2 + binding, suggesting a highly dynamic metastable relation between CaM and its targets. Recent advances in structure-function studies and the discovery of CaM mutations being responsible for human diseases, besides expanding the role of CaM in human pathophysiology, are opening new exciting avenues for the understanding of the how CaM decodes Ca2 +-dependent and Ca2 +-independent signals. © 2014 Elsevier Ltd.I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione