Analysis of waveform and amplitude of mouse rod and cone flash responses.

The Journal of Physiology Pub Date : 2021-07-01 Epub Date: 2021-06-08 DOI:10.1113/JP281225
Annia Abtout, Gordon Fain, Jürgen Reingruber
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引用次数: 5

Abstract

Key points: Most vertebrate eyes have rod and cone photoreceptors, which use a signal transduction pathway consisting of many biological processes to transform light into an electrical response. We dissect and quantify the contribution of each of these processes to the photoreceptor light response by using a novel method of analysis that provides an analytical solution for the entire time course of the dim-flash light response. We find that the shape of the light response is exclusively controlled by deactivation parameters. Activation parameters scale this shape and alter the response amplitude. We show that the rising phase of the response depends on Ca2+ feedback, and we identify the deactivation parameters that control the recovery phase of the response. We devise new methods to extract values for deactivation and activation parameters from a separate analysis of response shape and response amplitude.

Abstract: Vertebrate eyes have rod and cone photoreceptors, which use a complex transduction pathway comprising many biological processes to transform the absorption of light into an electrical response. A fundamental question in sensory transduction is how these processes contribute to the response. To study this question, we use a well-accepted phototransduction model, which we analyse with a novel method based on the log transform of the current. We derive an analytical solution that describes the entire time course of the photoreceptor response to dim flashes of light. We use this solution to dissect and quantify the contribution of each process to the response. We find that the entire dim-flash response is proportional to the flash intensity. By normalizing responses to unit amplitude, we define a waveform that is independent of the light intensity and characterizes the invariant shape of dim-flash responses. We show that this waveform is exclusively determined by deactivation rates; activation rates only scale the waveform and affect the amplitude. This analysis corrects a previous assumption that the rising phase is determined entirely by activation rates. We further show that the rising phase depends on Ca2+ feedback to the cyclase, contrary to current belief. We identify the deactivation rates that control the recovery phase of the response, and we devise new methods to extract activation and deactivation rates from an analysis of response shape and response amplitude. In summary, we provide a comprehensive understanding of how the various transduction processes produce the cellular response.

Abstract Image

Abstract Image

小鼠杆状和锥状闪光响应的波形和振幅分析。
重点:大多数脊椎动物的眼睛都有杆状和锥状光感受器,它们利用由许多生物过程组成的信号转导途径将光转化为电反应。我们通过使用一种新的分析方法来剖析和量化每个过程对光感受器光响应的贡献,该分析方法为暗闪光响应的整个时间过程提供了分析解决方案。我们发现光响应的形状完全由失活参数控制。激活参数调整这种形状并改变响应幅度。我们表明,响应的上升阶段取决于Ca2+反馈,我们确定了控制响应恢复阶段的失活参数。我们设计了新的方法,从响应形状和响应幅度的单独分析中提取失活和激活参数的值。脊椎动物的眼睛具有杆状和锥状光感受器,它们通过复杂的转导途径将光的吸收转化为电响应,其中包括许多生物过程。感觉转导的一个基本问题是这些过程是如何促成反应的。为了研究这个问题,我们使用了一个公认的光导模型,我们用一种基于电流对数变换的新方法对其进行了分析。我们推导了一个解析解,它描述了光感受器对微弱闪光的反应的整个时间过程。我们使用这个解决方案来剖析和量化每个过程对响应的贡献。我们发现整个暗闪光响应与闪光强度成正比。通过对单位振幅的响应进行归一化,我们定义了一个与光强度无关的波形,并表征了暗闪光响应的不变形状。我们表明,该波形完全由失活率决定;激活率只影响波形和振幅。这一分析纠正了先前的假设,即上升阶段完全由激活率决定。我们进一步表明,上升阶段取决于Ca2+反馈到环化酶,与目前的看法相反。我们确定了控制响应恢复阶段的失活率,并设计了从响应形状和响应振幅分析中提取激活和失活率的新方法。总之,我们提供了各种转导过程如何产生细胞反应的全面理解。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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