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Folding funnels, binding funnels, and protein function

Published online by Cambridge University Press:  01 June 1999

CHUNG-JUNG TSAI
Affiliation:
Laboratory of Experimental and Computational Biology, NCI-FCRDC, Bldg. 469, Room 151, Frederick, Maryland 21702
SANDEEP KUMAR
Affiliation:
Intramural Research Support Program—SAIC, Laboratory of Experimental and Computational Biology, NCI-FCRDC, Bldg. 469, Room 151, Frederick, Maryland 21702
BUYONG MA
Affiliation:
Laboratory of Experimental and Computational Biology, NCI-FCRDC, Bldg. 469, Room 151, Frederick, Maryland 21702
RUTH NUSSINOV
Affiliation:
Intramural Research Support Program—SAIC, Laboratory of Experimental and Computational Biology, NCI-FCRDC, Bldg. 469, Room 151, Frederick, Maryland 21702 Sackler Institute of Molecular Medicine, Sackler Faculty of Medicine, Tel Aviv University, Tel Aviv 69978, Israel
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Abstract

Folding funnels have been the focus of considerable attention during the last few years. These have mostly been discussed in the general context of the theory of protein folding. Here we extend the utility of the concept of folding funnels, relating them to biological mechanisms and function. In particular, here we describe the shape of the funnels in light of protein synthesis and folding; flexibility, conformational diversity, and binding mechanisms; and the associated binding funnels, illustrating the multiple routes and the range of complexed conformers. Specifically, the walls of the folding funnels, their crevices, and bumps are related to the complexity of protein folding, and hence to sequential vs. nonsequential folding. Whereas the former is more frequently observed in eukaryotic proteins, where the rate of protein synthesis is slower, the latter is more frequent in prokaryotes, with faster translation rates. The bottoms of the funnels reflect the extent of the flexibility of the proteins. Rugged floors imply a range of conformational isomers, which may be close on the energy landscape. Rather than undergoing an induced fit binding mechanism, the conformational ensembles around the rugged bottoms argue that the conformers, which are most complementary to the ligand, will bind to it with the equilibrium shifting in their favor. Furthermore, depending on the extent of the ruggedness, or of the smoothness with only a few minima, we may infer nonspecific, broad range vs. specific binding. In particular, folding and binding are similar processes, with similar underlying principles. Hence, the shape of the folding funnel of the monomer enables making reasonable guesses regarding the shape of the corresponding binding funnel. Proteins having a broad range of binding, such as proteolytic enzymes or relatively nonspecific endonucleases, may be expected to have not only rugged floors in their folding funnels, but their binding funnels will also behave similarly, with a range of complexed conformations. Hence, knowledge of the shape of the folding funnels is biologically very useful. The converse also holds: If kinetic and thermodynamic data are available, hints regarding the role of the protein and its binding selectivity may be obtained. Thus, the utility of the concept of the funnel carries over to the origin of the protein and to its function.

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REVIEWS
Copyright
© 1999 The Protein Society

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