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Functional photoreceptor loss revealed with adaptive optics: An alternate cause of color blindness

机译:自适应光学元件揭示了功能性感光体的损失:色盲的另一种原因

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摘要

There is enormous variation in the X-linked L/M (long/middle wavelength sensitive) gene array underlying “normal” color vision in humans. This variability has been shown to underlie individual variation in color matching behavior. Recently, red–green color blindness has also been shown to be associated with distinctly different genotypes. This has opened the possibility that there may be important phenotypic differences within classically defined groups of color blind individuals. Here, adaptive optics retinal imaging has revealed a mechanism for producing dichromatic color vision in which the expression of a mutant cone photopigment gene leads to the loss of the entire corresponding class of cone photoreceptor cells. Previously, the theory that common forms of inherited color blindness could be caused by the loss of photoreceptor cells had been discounted. We confirm that remarkably, this loss of one-third of the cones does not impair any aspect of vision other than color.
机译:X连锁的L / M(长/中波长敏感)基因阵列在人类“正常”色彩视觉中有着巨大的差异。已经表明这种可变性是颜色匹配行为的个体变化的基础。最近,红绿色盲症也被证明与明显不同的基因型有关。这开辟了可能性,即在经典定义的色盲人群中可能存在重要的表型差异。在这里,自适应光学视网膜成像揭示了一种产生双色彩色视觉的机制,其中突变体视锥色素基因的表达导致整个相应类别的视锥细胞受体细胞的丢失。以前,关于遗传性色盲的常见形式可能由感光细胞丧失引起的理论已经被轻视。我们确认,非常明显的是,视锥细胞的三分之一的损失不会损害颜色以外的视力。

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