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Alteration of hydrogen bonding in the vicinity of histidine 48 disrupts millisecond motions in RNase A.

Biochemistry. 2011; 
DoucetNicolas,KhirichGennady,KovriginEvgenii L,LoriaJ Pat
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摘要

The motion of amino acid residues on the millisecond (ms) time scale is involved in the tight regulation of catalytic function in numerous enzyme systems. Using a combination of mutational, enzymological, and relaxation-compensated N Carr-Purcell-Meiboom-Gill (CPMG) methods, we have previously established the conformational significance of the distant His48 residue and the neighboring loop 1 in RNase A function. These studies suggested that RNase A relies on an intricate network of hydrogen bonding interactions involved in propagating functionally relevant, long-range ms motions to the catalytic site of the enzyme. To further investigate the dynamic importance of this H-bonding network, this study fo... More

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