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Published April 15, 2003 | Published + Supplemental Material
Journal Article Open

Induced nucleotide specificity in a GTPase

Abstract

In signal-recognition particle (SRP)-dependent protein targeting to the bacterial plasma membrane, two GTPases, Ffh (a subunit of the bacterial SRP) and FtsY (the bacterial SRP receptor), act as GTPase activating proteins for one another. The molecular mechanism of this reciprocal GTPase activation is poorly understood. In this work, we show that, unlike other GTPases, free FtsY exhibits only low preference for GTP over other nucleotides. On formation of the SRP⋅FtsY complex, however, the nucleotide specificity of FtsY is enhanced 10^3-fold. Thus, interactions with SRP must induce conformational changes that directly affect the FtsY GTP-binding site: in response to SRP binding, FtsY switches from a nonspecific "open" state to a "closed" state that provides discrimination between cognate and noncognate nucleotides. We propose that this conformational change leads to more accurate positioning of the nucleotide and thus could contribute to activation of FtsY's GTPase activity by a novel mechanism.

Additional Information

© 2003 The National Academy of Sciences. Edited by Jennifer A. Doudna, University of California, Berkeley, CA, and approved February 5, 2003 (received for review December 17, 2002). We thank A. E. Johnson for advice on fluorescence experiments and T. Powers, R. Gilmore, H. Bourne, R. Stroud, and members of the Walter and Stroud laboratories for comments on the manuscript. This work was supported by National Institutes of Health Grant GM 32384 (to P.W.). P.W. is an Investigator of the Howard Hughes Medical Institute, and S.S. is a Cancer Research Fund Fellow of the Damon Runyon–Walter Winchell Foundation. This paper was submitted directly (Track II) to the PNAS office.

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Supplemental Material - 7693Fig7.jpg

Supplemental Material - 7693SuppText.pdf

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