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-   -   [NMR paper] A mini-protein designed by removing a module from barnase: molecular modeling and NMR (http://www.bionmr.com/forum/journal-club-9/mini-protein-designed-removing-module-barnase-molecular-modeling-nmr-9258/)

nmrlearner 11-18-2010 08:31 PM

A mini-protein designed by removing a module from barnase: molecular modeling and NMR
 
A mini-protein designed by removing a module from barnase: molecular modeling and NMR measurements of the conformation.

Related Articles A mini-protein designed by removing a module from barnase: molecular modeling and NMR measurements of the conformation.

Protein Eng. 1999 Aug;12(8):673-80

Authors: Takahashi K, Noguti T, Hojo H, Yamauchi K, Kinoshita M, Aimoto S, Ohkubo T, G? M

A globular domain can be decomposed into compact modules consisting of contiguous 10-30 amino acid residues. The correlation between modules and exons observed in different proteins suggests that each module was encoded by an ancestral exon and that modules were combined into globular domains by exon fusion. Barnase is a single domain RNase consisting of 110 amino acid residues and was decomposed into six modules. We designed a mini-protein by removing the second module, M2, from barnase in order to gain an insight into the structural and functional roles of the module. In the molecular modeling of the mini-protein, we evaluated thermodynamic stability and aqueous solubility together with mechanical stability of the model. We chemically synthesized a mini-barnase with (15)N-labeling at 10 residues, whose corresponding residues in barnase are all found in the region around the hydrophobic core. Circular dichroism and NMR measurements revealed that mini-barnase takes a non-random specific conformation that has a similar hydrophobic core structure to that of barnase. This result, that a module could be deleted without altering the structure of core region of barnase, supports the view that modules act as the building blocks of protein design.

PMID: 10469828 [PubMed - indexed for MEDLINE]



Source: PubMed


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