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NRAGE:分支形态发生过程中的一个潜在变阻器。

NRAGE: a potential rheostat during branching morphogenesis.

作者信息

Nikopoulos George N, Martins Joao Ferreira, Adams Tamara L, Karaczyn Aldona, Adams Derek, Vary Calvin, Oxburgh Leif, Verdi Joseph M

机构信息

Maine Medical Center Research Institute, Center for Molecular Medicine, Scarborough, ME 04074, USA.

出版信息

Mech Dev. 2009 May-Jun;126(5-6):337-49. doi: 10.1016/j.mod.2009.02.005. Epub 2009 Mar 4.

Abstract

Branching morphogenesis is a developmental process characteristic of many organ systems. Specifically, during renal branching morphogenesis, its been postulated that the final number of nephrons formed is one key clinical factor in the development of hypertension in adulthood. As it has been established that BMPs regulate, in part, renal activity of p38 MAP kinase (p38(MAPK)) and it has demonstrated that the cytoplasmic protein Neurotrophin Receptor MAGE homologue (NRAGE) augments p38(MAPK) activation, it was hypothesized that a decrease in the expression of NRAGE during renal branching would result in decreased branching of the UB that correlated with changes in p38(MAPK) activation. To verify this, the expression of NRAGE was reduced in ex vivo kidney explants cultures using antisense morpholino. Morpholino treated ex vivo kidney explants expression were severely stunted in branching, a trait that was rescued with the addition of exogenous GDNF. Renal explants also demonstrated a precipitous drop in p38(MAPK) activation that too was reversed in the presence of recombinant GDNF. RNA profiling of NRAGE diminished ex vivo kidney explants resulted in altered expression of GDNF, Ret, BMP7 and BMPRIb mRNAs. Our results suggested that in early kidney development NRAGE might have multiple roles during renal branching morphogenesis through association with both the BMP and GDNF signaling pathways.

摘要

分支形态发生是许多器官系统特有的发育过程。具体而言,在肾脏分支形态发生过程中,据推测,成年期高血压发展的一个关键临床因素是形成的肾单位最终数量。由于已经确定骨形态发生蛋白(BMP)部分调节p38丝裂原活化蛋白激酶(p38(MAPK))的肾脏活性,并且已经证明细胞质蛋白神经营养因子受体MAGE同源物(NRAGE)增强p38(MAPK)的活化,因此推测在肾脏分支过程中NRAGE表达的降低将导致输尿管芽分支减少,这与p38(MAPK)活化的变化相关。为了验证这一点,使用反义吗啉代在离体肾外植体培养物中降低NRAGE的表达。用吗啉代处理的离体肾外植体的表达在分支方面严重受阻,添加外源性胶质细胞源性神经营养因子(GDNF)可挽救该性状。肾外植体还显示p38(MAPK)活化急剧下降,在重组GDNF存在下也可逆转。对NRAGE减少的离体肾外植体进行RNA谱分析,结果显示GDNF、Ret、BMP7和BMPRIb mRNA的表达发生改变。我们的结果表明,在肾脏早期发育中,NRAGE可能通过与BMP和GDNF信号通路相关联,在肾脏分支形态发生过程中发挥多种作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1bb7/2702142/89e646c939fb/nihms120627f1.jpg

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