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斑马鱼的Lmx1b.1和Lmx1b.2是中脑-后脑组织者维持所必需的。

Zebrafish Lmx1b.1 and Lmx1b.2 are required for maintenance of the isthmic organizer.

作者信息

O'Hara F Patrick, Beck Ernestine, Barr Lauren K, Wong Lily L, Kessler Daniel S, Riddle Robert D

机构信息

Department of Cell and Developmental Biology, University of Pennsylvania School of Medicine, Philadelphia, PA 19104, USA.

出版信息

Development. 2005 Jul;132(14):3163-73. doi: 10.1242/dev.01898. Epub 2005 Jun 8.

Abstract

The mesencephalic and metencephalic region (MMR) of the vertebrate central nervous system develops in response to signals produced by the isthmic organizer (IsO). We have previously reported that the LIM homeobox transcription factor Lmx1b is expressed within the chick IsO, where it is sufficient to maintain expression of the secreted factor wnt1. In this paper, we show that zebrafish express two Lmx1b orthologs, lmx1b.1 and lmx1b.2, in the rostral IsO, and demonstrate that these genes are necessary for key aspects of MMR development. Simultaneous knockdown of Lmx1b.1 and Lmx1b.2 using morpholino antisense oligos results in a loss of wnt1, wnt3a, wnt10b, pax8 and fgf8 expression at the IsO, leading ultimately to programmed cell death and the loss of the isthmic constriction and cerebellum. Single morpholino knockdown of either Lmx1b.1 or Lmx1b.2 has no discernible effect on MMR development. Maintenance of lmx1b.1 and lmx1b.2 expression at the isthmus requires the function of no isthmus/pax2.1, as well as Fgf signaling. Transient misexpression of Lmx1b.1 or Lmx1b.2 during early MMR development induces ectopic wnt1 and fgf8 expression in the MMR, as well as throughout much of the embryo. We propose that Lmx1b.1- and Lmx1b.2-mediated regulation of wnt1, wnt3a, wnt10b, pax8 and fgf8 maintains cell survival in the isthmocerebellar region.

摘要

脊椎动物中枢神经系统的中脑和后脑区域(MMR)是响应峡部组织者(IsO)产生的信号而发育的。我们之前报道过,LIM同源框转录因子Lmx1b在鸡的IsO中表达,在那里它足以维持分泌因子wnt1的表达。在本文中,我们表明斑马鱼在吻侧IsO中表达两个Lmx1b直系同源基因,lmx1b.1和lmx1b.2,并证明这些基因是MMR发育关键方面所必需的。使用吗啉代反义寡核苷酸同时敲低Lmx1b.1和Lmx1b.2会导致IsO处wnt1、wnt3a、wnt10b、pax8和fgf8表达缺失,最终导致程序性细胞死亡以及峡部缩窄和小脑缺失。单独敲低Lmx1b.1或Lmx1b.2中的任何一个对MMR发育没有明显影响。峡部lmx1b.1和lmx1b.2的表达维持需要no isthmus/pax2.1的功能以及Fgf信号传导。在MMR早期发育期间短暂错误表达Lmx1b.1或Lmx1b.2会在MMR以及整个胚胎的大部分区域诱导异位wnt1和fgf8表达。我们提出,Lmx1b.1和Lmx1b.2介导的对wnt1、wnt3a、wnt10b、pax8和fgf8的调节维持了峡小脑区域的细胞存活。

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