Specific ablation of Hippo signalling component Yap1 in retinal progenitors and Müller cells results in late onset retinal degeneration

Specific ablation of Hippo signalling component Yap1 in retinal progenitors and Müller cells results in late onset retinal degeneration

Yes‐associated protein (YAP) is a major component of the Hippo pathway involved in development, growth, repair and homeostasis. Nonsense YAP1 mutations in humans result in autosomal dominant coloboma. Here, we generated a conditional knockout mouse model in which Yap1 was specifically deleted in emb...

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Bibliographic Details
Published in:Journal of cellular physiology Vol. 237; no. 6; pp. 2673 - 2689
Main Authors: Yang, Yeming, Jiang, Xiaoyan, Li, Xiao, Sun, Kuanxiang, Zhu, Xianjun, Zhou, Bo
Format: Journal Article
Language:English
Published: Hoboken Wiley Subscription Services, Inc 01-06-2022
Subjects:
Ablation
Amacrine cells
Apoptosis
Bipolar cells
Cell number
Cell proliferation
Degeneration
Embryogenesis
Ganglion cells
Gliosis
Hippo signalling
Homeostasis
Horizontal cells
Immunofluorescence
knockout model
Mueller cells
Mutation
Neural stem cells
Photoreceptors
Progenitor cells
Retina
Retinal cells
Retinal degeneration
Signal transduction
Stem cells
Yap1
Yes-associated protein
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Summary:Yes‐associated protein (YAP) is a major component of the Hippo pathway involved in development, growth, repair and homeostasis. Nonsense YAP1 mutations in humans result in autosomal dominant coloboma. Here, we generated a conditional knockout mouse model in which Yap1 was specifically deleted in embryonic retinal progenitor cells (RPCs) and in mature Müller cells using a Chx10‐Cre driver. Our data demonstrated that the conditional ablation of Yap1 in embryonic RPCs does not prevent normal retinal development and caused no gross changes in retinal structure during embryonic and early postnatal life. Nevertheless, Yap1 deficient in retinal Müller cells in adult mice leads to impaired visual responses and extensive late‐onset retinal degeneration, characterized by reduced cell number in all retinal layers. Immunofluorescence data further revealed the degeneration and death of rod and cone photoreceptors, bipolar cells, horizontal cells, amacrine cells and ganglion cells to varying degrees in aged knockout mice. Moreover, alteration of glial homeostasis and reactive gliosis were also observed. Finally, cell proliferation and TUNEL assay revealed that the broad retinal degeneration is mainly caused by enhanced apoptosis in late period. Together, this work uncovers that YAP is essential for the normal vision and retinal maintenance, highlighting the crucial role of YAP in retinal function and homeostasis. Yes‐associated protein (YAP) is a major component of the Hippo pathway involved in development, growth, repair and homeostasis. Yap1 deficient in retinal Müller cells in adult mice leads to impaired visual responses and extensive late‐onset retinal degeneration, characterized by reduced cell number in all retinal layers. Immunofluorescence data further revealed the degeneration and death of rod and cone photoreceptors, bipolar cells, horizontal cells, amacrine cells and ganglion cells to varying degrees in aged knockout mice. This work uncovers that YAP is essential for the normal vision and retinal maintenance, highlighting the crucial role of YAP in retinal function and homeostasis.
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ISSN:0021-9541
1097-4652
DOI:10.1002/jcp.30757