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光感受器多样性的转录因子。

Transcription factors underlying photoreceptor diversity.

机构信息

Unit of Retinal Neurophysiology, National Eye Institute, National Institutes of Health, Bethesda, United States.

Section on Sensory Cell Development and Function, National Institute on Deafness and Other Communication Disorders, National Institutes of Health, Bethesda, United States.

出版信息

Elife. 2023 Feb 6;12:e81579. doi: 10.7554/eLife.81579.

Abstract

During development, retinal progenitors navigate a complex landscape of fate decisions to generate the major cell classes necessary for proper vision. Transcriptional regulation is critical to generate diversity within these major cell classes. Here, we aim to provide the resources and techniques required to identify transcription factors necessary to generate and maintain diversity in photoreceptor subtypes, which are critical for vision. First, we generate a key resource: a high-quality and deep transcriptomic profile of each photoreceptor subtype in adult zebrafish. We make this resource openly accessible, easy to explore, and have integrated it with other currently available photoreceptor transcriptomic datasets. Second, using our transcriptomic profiles, we derive an in-depth map of expression of transcription factors in photoreceptors. Third, we use efficient CRISPR-Cas9 based mutagenesis to screen for null phenotypes in F0 larvae (F0 screening) as a fast, efficient, and versatile technique to assess the involvement of candidate transcription factors in the generation of photoreceptor subtypes. We first show that known phenotypes can be easily replicated using this method: loss of S cones in mutants and loss of rods in mutants. We then identify novel functions for the transcription factor Tbx2, demonstrating that it plays distinct roles in controlling the generation of all photoreceptor subtypes within the retina. Our study provides a roadmap to discover additional factors involved in this process. Additionally, we explore four transcription factors of unknown function (Skor1a, Sall1a, Lrrfip1a, and Xbp1), and find no evidence for their involvement in the generation of photoreceptor subtypes. This dataset and screening method will be a valuable way to explore the genes involved in many other essential aspects of photoreceptor biology.

摘要

在发育过程中,视网膜祖细胞在复杂的命运决策景观中导航,以产生适当视觉所必需的主要细胞类型。转录调控对于在这些主要细胞类型中产生多样性至关重要。在这里,我们旨在提供识别产生和维持光感受器亚型多样性所需的转录因子所需的资源和技术,这些转录因子对于视觉至关重要。首先,我们生成了一个关键资源:成年斑马鱼中每种光感受器亚型的高质量和深度转录组图谱。我们使这个资源开放、易于探索,并将其与其他当前可用的光感受器转录组数据集集成在一起。其次,我们使用我们的转录组图谱,得出了光感受器中转录因子表达的深入图谱。第三,我们使用高效的 CRISPR-Cas9 基诱变来筛选 F0 幼虫中的无效表型(F0 筛选),作为一种快速、高效和通用的技术,以评估候选转录因子在光感受器亚型生成中的参与情况。我们首先表明,使用这种方法可以轻松复制已知表型: 突变体中 S 锥细胞的缺失和 突变体中杆状细胞的缺失。然后,我们确定了转录因子 Tbx2 的新功能,证明它在控制视网膜中所有光感受器亚型的产生中发挥着不同的作用。我们的研究为发现该过程中涉及的其他因素提供了路线图。此外,我们还探索了四个功能未知的转录因子(Skor1a、Sall1a、Lrrfip1a 和 Xbp1),没有证据表明它们参与光感受器亚型的产生。这个数据集和筛选方法将是探索光感受器生物学许多其他重要方面涉及的基因的宝贵途径。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d69d/9901936/797fffb62b80/elife-81579-fig1.jpg

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