1). In this
study, we demonstrate that a simple elastic network model, GNM/ANM,
can predict the most probable reconfigurations of Hb, i.e. the
transition between the T and R2 forms. Numerous liganded and
unliganded Hb revealed a number of structures that fall in between T
and R2. Our studies tie the global motion of Hb directly to this
functional conformational transition.
2). Numerous mutational and
spectroscopic studies have shown that the hydrogen bond and salt
bridge formation at the
a1b2
interface are key to the allosteric
activity of Hb. Without knowledge of any chemical and biological data
on Hb function, using structural (purely geometric) information alone,
we show that the hinge center for the most coordinated motion of Hb
corresponds to the switch region at the
a1b2
interface.
3). We
identify a number of other interactions at the
a1-b1
interface, which can
play a role in establishing the communication of the dimers.
