AUTHOR=Wang Yu-Bing , Song Ning-Ning , Zhang Lei , Ma Pengcheng , Chen Jia-Yin , Huang Ying , Hu Ling , Mao Bingyu , Ding Yu-Qiang 

TITLE=Rnf220 is Implicated in the Dorsoventral Patterning of the Hindbrain Neural Tube in Mice

JOURNAL=Frontiers in Cell and Developmental Biology

VOLUME=10

YEAR=2022

URL=https://www.frontiersin.org/journals/cell-and-developmental-biology/articles/10.3389/fcell.2022.831365

DOI=10.3389/fcell.2022.831365

ISSN=2296-634X

ABSTRACT=<p>Rnf220 is reported to regulate the patterning of the ventral spinal neural tube in mice. The brainstem has divergent connections with peripheral and central targets and contains unique internal neuronal groups, but the role of Rnf220 in the early development of the hindbrain has not been explored. In this study, <italic>Nestin</italic>-Cre-mediated conditional knockout (<italic>Rnf220</italic><sup>Nestin</sup> CKO) mice were used to examine if <italic>Rnf220</italic> is involved in the early morphogenesis of the hindbrain. <italic>Rnf220</italic> showed restricted expression in the ventral half of ventricular zone (VZ) of the hindbrain at embryonic day (E) 10.5, and as development progressed, <italic>Rnf220</italic>-expressing cells were also present in the mantle zone outside the VZ at E12.5. In <italic>Rnf220</italic><sup>Nestin</sup> CKO embryos, alterations of progenitor domains in the ventral VZ were observed at E10.5. There were significant reductions of the p1 and p2 domains shown by expression of <italic>Dbx1</italic>, Olig2, and Nkx6.1, accompanied by a ventral expansion of the Dbx1<sup>+</sup> p0 domain and a dorsal expansion of the Nkx2.2<sup>+</sup> p3 domain. Different from the case in the spinal cord, the Olig2<sup>+</sup> pMN (progenitors of somatic motor neuron) domain shifted and expanded dorsally. Notably, the total range of the ventral VZ and the extent of the dorsal tube were unchanged. In addition, the post-mitotic cells derived from their corresponding progenitor domain, including oligodendrocyte precursor cells (OPCs) and serotonergic neurons (5-HTNs), were also changed in the same trend as the progenitor domains do in the CKO embryos at E12.5. In summary, our data suggest similar functions of Rnf220 in the hindbrain dorsoventral (DV) patterning as in the spinal cord with different effects on the pMN domain. Our work also reveals novel roles of Rnf220 in the development of 5-HTNs and OPCs.</p>