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用于 cones 退化的小鼠模型。

Mouse models for cone degeneration.

机构信息

Lab for Retinal Cell Biology, Department of Ophthalmology, University of Zurich, Wagistr 14 Schlieren, 8952, Zurich, Switzerland,

出版信息

Adv Exp Med Biol. 2014;801:567-73. doi: 10.1007/978-1-4614-3209-8_72.

Abstract

Loss of cone vision has devastating effects on everyday life. Even though much effort has been made to understand cone physiology and pathophysiology, no successful therapies are available for patients suffering from cone disorders. As complex retinal interactions cannot be studied in vitro, utilization of different animal models is inevitable. Due to recent advances in transgenesis, mice became the most popular animal model to study human diseases, also in ophthalmology. While there are similarities in retinal anatomy and pathophysiology between mice and humans, there are also differences, most importantly the lack of a cone-rich macula in mice. Instead, cones in mice are rare and distributed over the whole retina, which makes the analysis of cone pathophysiology very difficult in these animals. This hindrance is one of the reasons why our understanding of rod pathophysiological processes is much more advanced. Recently, however, the sparseness of cones was overcome by the generation of the Nrl (- / -) mouse that expresses only cone photoreceptors in the retina. This paper will give a brief overview of some of the known mouse models to study cone degeneration and discuss the current knowledge gained from the analysis of these models.

摘要

锥细胞丧失视力对日常生活有严重影响。尽管人们已经做出了很大努力来理解锥体细胞的生理学和病理生理学,但对于患有锥体细胞疾病的患者,还没有有效的治疗方法。由于复杂的视网膜相互作用无法在体外进行研究,因此不可避免地需要利用不同的动物模型。由于转基因技术的最新进展,老鼠成为研究人类疾病的最受欢迎的动物模型,在眼科领域也是如此。虽然老鼠和人类的视网膜解剖结构和病理生理学有相似之处,但也存在差异,最重要的是老鼠缺乏富含锥体细胞的黄斑。相反,老鼠的锥体细胞很少,分布在整个视网膜,这使得在这些动物中分析锥体细胞的病理生理学非常困难。这一障碍是我们对视杆细胞病理生理过程的理解远远超过对锥体细胞病理生理过程的理解的原因之一。然而,最近通过生成仅在视网膜中表达锥体细胞感光器的 Nrl(-/-)小鼠,克服了锥体细胞稀疏的问题。本文将简要概述一些用于研究锥体细胞变性的已知小鼠模型,并讨论从这些模型分析中获得的当前知识。

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