Journal of Structural Biology, Vol.155, No.2, 263-272, 2006
Mechanical properties of cardiac titin's N2B-region by single-molecule atomic force spectroscopy
Titin is a giant protein responsible for passive-tension generation in muscle sarcomeres. Here, we used single-molecule AFM force spectroscopy to investigate the mechanical characteristics of a recombinant construct from the human cardiac-specific N2B-region, which harbors a 572-residue unique sequence flanked by two immunoglobulin (Ig) domains on either side. Force-extension curves of the N2B-construct revealed mean unfolding forces for the Ig-domains similar to those of a recombinant fragment from the distal Ig-region in titin (191-98). The mean contour length of the N2B-unique sequence was 120 rim, but there was a bimodal distribution centered at similar to 95 nm (major peak) and 180 nm (minor peak). These values are lower than expected if the N2B-unique sequence were a permanently unfolded entropic spring, but are consistent with the similar to 100 nm maximum extension of that segment measured in isolated stretched cardiomyofibrils. A contour-length below 200 nm would be reasonable, however, if the N2B-unique sequence were stabilized by a disulphide bridge, as suggested by several disulphide connectivity prediction algorithms. Since the N2B-unique sequence can be phosphorylated by protein kinase A (PKA), which lowers titin-based stiffness, we studied whether addition of PKA (+ATP) affects the mechanical properties of the N2B-construct, but found no changes. The softening effect of PKA on N2B-titin may require specific conditions/factors present inside the cardiomyocytes. (c) 2006 Elsevier Inc. All rights reserved.
Keywords:connectin;titin;single-molecule;muscle mechanics;elasticity;AFM spectroscopy;protein unfolding;immunoglobulin domain;protein kinase A