Detection and structural characterization of ras oncoprotein-inhibitors complexes by electrospray mass spectrometry

Ashit K. Ganguly,Birendra N. Pramanik,Eric Huang,Stephen D. Liberles,Larry Heimark,Yi-Tsung Liu,Anthony Tsarbopoulos,Ronald J. Doll,Arthur G. Taveras,Stacy W. Remiszewski,M.E. Snow,Yu-Sen Wang,Bancha Vibulbhan,David Cesarz,Joan E. Brown,J. del Rosario,Linda James,Paul Kirschmeier,Viyyoor M. Girijavallabhan

Detection and structural characterization of ras oncoprotein-inhibitors complexes by electrospray mass spectrometry

1997

Ashit K. Ganguly
Birendra N. Pramanik
Eric Huang
Stephen D. Liberles
Larry Heimark
Yi-Tsung Liu
Anthony Tsarbopoulos
Ronald J. Doll
Arthur G. Taveras
Stacy W. Remiszewski
M.E. Snow
Yu-Sen Wang
Bancha Vibulbhan
David Cesarz
Joan E. Brown
J. del Rosario
Linda James
Paul Kirschmeier
Viyyoor M. Girijavallabhan

Abstract MS based methodology employing electrospray ionization (ESI) is described for the detection of ternary complexes in which SCH 54292 or SCH 54341 and GDP are noncovalently bound to oncogenic ras protein. The observed molecular weights of 19,816 and 19,570 Da confirmed the presence of noncovalent complexes of ras-GDP-SCH 54292 and ras-GDP-SCH 54341, respectively. We have also performed selective chemical modification of lysine residues of the ras protein complex followed by enzymatic digestion and on-line LC-ESI MS peptide mapping to determine protein-drug binding topography. There was a good correlation between nucleotide exchange inhibition as determined by the enzyme assay and evidence of complex formation as determined by MS.

Keywords:

Enzyme
Sample preparation in mass spectrometry
Chemical modification
Nucleotide
Biochemistry
Electrospray ionization
Molecular mass
Electrospray
Chemistry
Mass spectrometry
Lysine
Enzyme assay
electrospray mass spectrometry

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