Abstract
Retinal rods function as accurate photon counters to provide for vision under very dim light. To do so, rods must generate highly amplified, reproducible responses to single photons, yet outer segment architecture and randomness in the location of rhodopsin photoisomerization on the surface of an internal disk introduce variability to the rising phase of the photon response. Soon after a photoisomerization at a disk rim, depletion of cGMP near the plasma membrane closes ion channels and hyperpolarizes the rod. But with a photoisomerization in the center of a disk, local depletion of cGMP is distant from the channels in the plasma membrane. Thus, channel closure is delayed by the time required for the reduction of cGMP concentration to reach the plasma membrane. Moreover, the local fall in cGMP dissipates over a larger volume before affecting the channels, so response amplitude is reduced. This source of variability increases with disk radius. Using a fully space-resolved biophysical model of rod phototransduction, we quantified the variability attributable to randomness in the location of photoisomerization as a function of disk structure. In mouse rods that have small disks bearing a single incisure, this variability was negligible in the absence of the incisure. Variability was increased slightly by the incisure, but randomness in the shutoff of rhodopsin emerged as the main source of single photon response variability at all but the earliest times. Variability arising from randomness in the transverse location of photoisomerization increased in magnitude and persisted over a longer period in the photon response of large salamander rods. A symmetric arrangement of multiple incisures in the disks of salamander rods greatly reduced this variability during the rising phase, but the incisures had the opposite effect on variability arising from randomness in rhodopsin shutoff at later times.
Highlights
In the vertebrate retina, rod photoreceptors provide visual input under very dim light
Photoisomerization of rhodopsin initiates a G protein cascade restricted to one face of a disk, that culminates in the hydrolysis of cGMP by activated phosphodiesterase (PDE )
The ensuing fall in cGMP concentration in the cytosolic volume between disks that propagates to their rims closes cyclic nucleotide gated (CNG) channels in the plasma membrane
Summary
Rod photoreceptors provide visual input under very dim light. Greater access of PDE to cGMP in the outer shell with incisures caused SPRs due to R s at all locations on the disk to more closely resemble the response to an R at the rim in size, and in exhibiting the damped oscillation in the recovery phase.
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