bmp7b 和 bmpr1ba 脆皮斑马鱼的全脑畸形和单眼畸形

Valentyn Kyrychenko, Philipp Rensinghoff, Johannes Bulk, Constanze Frey, Stephan Heermann
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摘要

视觉系统高度专业化,其功能在很大程度上取决于眼睛的正常发育。眼睛的早期发育始于单眼视野的形成,它位于前神经板(ANP)内。单眼球连续分裂,两侧出现两个视泡。这些小泡随后转化为视杯,未来的视网膜就是从视杯中分化出来的。全脑畸形(HPE)是一种常见的前脑发育障碍,其中 ANP 域的分裂受到阻碍。HPE 大多与遗传有关,我们最近发现,BMP 拮抗作用对眼球和端脑的分裂非常重要。在本研究中,我们以斑马鱼为模型,通过对F0代的急性CRISPR/ Cas9分析,证明了bmp7b和bmpr1ba对前脑正常发育的必要性。在这两个基因的 Crispants 中,我们发现了 HPE 表型,例如回旋畸形。对 bmp7b Crispants 的进一步分析表明,受影响的主要是眼区,而不是端脑前体域。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Holoprosencephaly and Cyclopia in bmp7b and bmpr1ba Crispant zebrafish
The visual system is highly specialized and its function is substantially depending on the proper development of the eyes. Early eye development starts with the definition of a single eye field, which is localized within the anterior neural plate (ANP). This single eye field is split consecutively and two optic vesicles emerge at the sides. These vesicles are then transformed into optic cups, out of which the future retinae are differentiating. Holoprosencephaly (HPE) is a frequent developmental forebrain disorder, in which the splitting of ANP domains is hampered. HPE is mostly genetically linked and we recently showed that BMP antagonism is important for the eye field and the telencephalic anlage to split. Excessive BMP induction led to retinal progenitors stuck inside a dysmorphic forebrain. In this study, using the zebrafish as a model, we show with acute CRISPR/ Cas9 analysis in the F0 generation, the necessity of bmp7b and bmpr1ba for proper forebrain development. In Crispants for both genes we found HPE phenotypes, e.g. cyclopia. Further analysis of bmp7b Crispants indicated that predominantly the eye field is affected, rather than the telencephalic precursor domain.
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