In rabbit muscle G-actin, Cys-257 was the most reactive thiol group to DACM, while upon polymerization to F-actin, practically all thiol groups became inaccessible.
The study demonstrates that Cys-257 is the most surface-exposed thiol in G-actin, and that polymerization to F-actin induces a drastic conformational change rendering all thiols inaccessible to DACM.
The accessibility of the cysteine residues of actin from rabbit muscles to the thiol-targeted reagent 7-dimethylamino-4-methyl-(N-maleimidyl)coumarin (DACM) was investigated. Under conditions where the actin is in the unpolymerized form (G-actin), the most reactive thiol group was Cys-257, suggesting that it was located on the surface of the actin molecule. The selective modification of Cys-374 for this reagent as reported by Sutoh (1982) Biochemistry 21, 3654-3661 was not observed. Cys-10, Cys-217 and Cys-374 were much less reactive and only gradually became extensively modified when the concentration of DACM approached 5 molar equivalents of actin. Presumably these thiol groups were located further inward away from the surface or situated in a different environment that rendered them less reactive. On the other hand, Cys-285 was completely inaccessible and presumably was buried. The lack of preferential labelling of Cys-374 by DACM is incompatible with the finding with iodoacetic acid as the reagent as reported by Elzinga & Collins (1975) J. Biol. Chem. 250, 5897-5905. This discrepancy, however, might well be due to the different reagents employed. The DACM-G-actin largely retained its competence for polymerization. Upon polymerization of G-actin, practically all the thiol groups became inaccessible to DACM, suggesting that a drastic change occurred in the conformation of actin units in the transition of monomers to filamentous actin.
Liu et al. (Thu,) reported a other. 7-dimethylamino-4-methyl-(N-maleimidyl)coumarin (DACM) was evaluated on Accessibility of cysteine residues to DACM. In rabbit muscle G-actin, Cys-257 was the most reactive thiol group to DACM, while upon polymerization to F-actin, practically all thiol groups became inaccessible.
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