Kh. Jung et al., Transducer-binding and transducer-mutations modulate photoactive-site-deprotonation in sensory rhodopsin I, BIOCHEM, 38(40), 1999, pp. 13270-13274
Sensory rhodopsin I (SRI) is a seven-transmembrane helix retinylidene prote
in that mediates color-sensitive phototaxis responses through its bound tra
nsducer HtrI in the archaeon Halobacterium salinarum. Deprotonation of the
Schiff base attachment site of the chromophore accompanies formation of the
SRI signaling state, S-373. We measured the rate of laser flash-induced S3
73 formation in the presence and absence of HtrI, and the effects of mutati
ons in SRI or HtrI on the kinetics of this process. In the absence of HtrI,
deprotonation occurs rapidly (halftime 10 mu s) if the proton acceptor Asp
76 is ionized (pK(a) = similar to 7), and only very slowly (halftime > 10 m
s) when Asp76 is protonated. Transducer-binding, although it increases the
pK(a) of Asp76 so that it is protonated throughout the range of pH studied,
results in a first order, pH-independent rate of S373 formation of similar
to 300 mu s. Therefore, the complexation of HtrI facilitates the proton-tr
ansfer reaction, increasing the rate similar to 50-fold at pH6. Arrhenius a
nalysis shows that Htr-binding accelerates the reaction primarily by an ent
ropic effect, suggesting HtrI constrains the SRI molecule in the complex. F
unction-perturbing mutations in SRI and HM also alter the rate of S373 form
ation and the lambda(max) of the parent state as assessed by laser flash-in
duced kinetic difference spectroscopy, and shifts to longer wavelength are
correlated with slower deprotonation. The data indicate that HtrI affects e
lectrostatic interactions of the protonated Schiff base and not only receiv
es the signal from SRI but also optimizes the photochemical reaction proces
s for SRI signaling.