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Rho GTPase Rnd3 的基因缺失会引发内囊和苍白球形成的发育缺陷。

Genetic ablation of the Rho GTPase Rnd3 triggers developmental defects in internal capsule and the globus pallidus formation.

机构信息

IRBLLEIDA/Universitat de Lleida, Lleida, Spain.

Departamento de Medicina y Cirugía Animal, Facultad de Veterinaria, Universidad CEU Cardenal Herrera, Valencia, Spain.

出版信息

J Neurochem. 2021 Jul;158(2):197-216. doi: 10.1111/jnc.15322. Epub 2021 Feb 24.

DOI:10.1111/jnc.15322
PMID:33576044
Abstract

The forebrain includes the cerebral cortex, the thalamus, and the striatum and globus pallidus (GP) in the subpallium. The formation of these structures and their interconnections by specific axonal tracts take place in a precise and orchestrated time and spatial-dependent manner during development. However, the knowledge of the molecular and cellular mechanisms that are involved is rather limited. Moreover, while many extracellular cues and specific receptors have been shown to play a role in different aspects of nervous system development, including neuron migration and axon guidance, examples of intracellular signaling effectors involved in these processes are sparse. In the present work, we have shown that the atypical RhoGTPase, Rnd3, is expressed very early during brain development and keeps a dynamic expression in several brain regions including the cortex, the thalamus, and the subpallium. By using a gene-trap allele (Rnd3 ) and immunological techniques, we have shown that Rnd3 embryos display severe defects in striatal and thalamocortical axonal projections (SAs and TCAs, respectively) and defects in GP formation already at early stages. Surprisingly, the corridor, an important intermediate target for TCAs is still present in these mutants. Mechanistically, a conditional genetic deletion approach revealed that Rnd3 is primarily required for the normal development of Medial Ganglionic Eminence-derived structures, such as the GP, and therefore acts non-cell autonomously in SAs and TCAs. In conclusion, we have demonstrated the important role of Rnd3 as an early regulator of subpallium development in vivo and revealed new insights about SAs and TCAs development.

摘要

前脑包括大脑皮层、丘脑和亚皮层的纹状体和苍白球(GP)。这些结构的形成及其特定轴突束的连接在发育过程中以精确和协调的时间和空间依赖性方式发生。然而,涉及的分子和细胞机制的知识相当有限。此外,虽然许多细胞外线索和特定受体已被证明在神经系统发育的不同方面发挥作用,包括神经元迁移和轴突导向,但涉及这些过程的细胞内信号效应物的例子很少。在本工作中,我们表明,非典型 RhoGTPase Rnd3 在大脑发育的早期表达,并在包括皮层、丘脑和亚皮层在内的几个脑区保持动态表达。通过使用基因陷阱等位基因(Rnd3 )和免疫技术,我们表明 Rnd3 胚胎在纹状体和丘脑皮质轴突投射(分别为 SAs 和 TCAs)以及 GP 形成方面表现出严重缺陷,甚至在早期阶段也是如此。令人惊讶的是,在这些突变体中, corridor,TCAs 的一个重要中间靶标仍然存在。从机制上讲,条件性基因缺失方法表明 Rnd3 主要是正常发育的必需条件中脑隆起源性结构,如 GP,因此在 SAs 和 TCAs 中发挥非细胞自主作用。总之,我们证明了 Rnd3 在体内作为亚皮层发育的早期调节剂的重要作用,并揭示了 SAs 和 TCAs 发育的新见解。

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