Literature DB >> 24309209

Zebrafish nephrogenesis is regulated by interactions between retinoic acid, mecom, and Notch signaling.

Yue Li1, Christina N Cheng1, Valerie A Verdun1, Rebecca A Wingert2.   

Abstract

The zebrafish pronephros provides a conserved model to study kidney development, in particular to delineate the poorly understood processes of how nephron segment pattern and cell type choice are established. Zebrafish nephrons are divided into distinct epithelial regions that include a series of proximal and distal tubule segments, which are comprised of intercalated transporting epithelial cells and multiciliated cells (MCC). Previous studies have shown that retinoic acid (RA) regionalizes the renal progenitor field into proximal and distal domains and that Notch signaling later represses MCC differentiation, but further understanding of these pathways has remained unknown. The transcription factor mecom (mds1/evi1 complex) is broadly expressed in renal progenitors, and then subsequently marks the distal tubule. Here, we show that mecom is necessary to form the distal tubule and to restrict both proximal tubule formation and MCC fate choice. We found that mecom and RA have opposing roles in patterning discrete proximal and distal segments. Further, we discovered that RA is required for MCC formation, and that one mechanism by which RA promotes MCC fate choice is to inhibit mecom. Next, we determined the epistatic relationship between mecom and Notch signaling, which limits MCC fate choice by lateral inhibition. Abrogation of Notch signaling with the γ-secretase inhibitor DAPT revealed that Notch and mecom did not have additive effects in blocking MCC formation, suggesting that they function in the same pathway. Ectopic expression of the Notch signaling effector, Notch intracellular domain (NICD), rescued the expansion of MCCs in mecom morphants, indicating that mecom acts upstream to induce Notch signaling. These findings suggest a model in which mecom and RA arbitrate proximodistal segment domains, while MCC fate is modulated by a complex interplay in which RA inhibition of mecom, and mecom promotion of Notch, titrates MCC number. Taken together, our studies have revealed several essential and novel mechanisms that control pronephros development in the zebrafish.
© 2013 The Authors. Published by Elsevier Inc. All rights reserved.

Entities:  

Keywords:  4-diethylamino-benzaldehyde; CS; DE; DEAB; DL; G; IM; MCC; MET; N; NICD; Nephrogenesis; Notch; Notch intracellular domain; PCT; PD; PM; PST; Pronephros; RA; RARE; Retinoic acid; Segmentation; corpuscle of Stannius; days post-fertilization; distal early; distal late; dpf; glomerulus; hours post-fertilization; hpf; intermediate mesoderm; mds1/evi1 complex; mecom; mesenchymal to epithelial transition; multiciliated cell; neck; paraxial mesoderm; pronephric duct; proximal convoluted tubule; proximal straight tubule; retinoic acid; retinoic acid response element

Mesh:

Substances:

Year:  2013        PMID: 24309209      PMCID: PMC3920184          DOI: 10.1016/j.ydbio.2013.11.021

Source DB:  PubMed          Journal:  Dev Biol        ISSN: 0012-1606            Impact factor:   3.582


  29 in total

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4.  Evi-1 expression in Xenopus.

Authors:  Paul E Mead; Evan Parganas; Shiro Ohtsuka; Kazuhiro Morishita; Laura Gamer; Emin Kuliyev; Christopher V E Wright; James N Ihle
Journal:  Gene Expr Patterns       Date:  2005-06       Impact factor: 1.224

5.  Evi1 is specifically expressed in the distal tubule and duct of the Xenopus pronephros and plays a role in its formation.

Authors:  Claude Van Campenhout; Massimo Nichane; Aline Antoniou; Hélène Pendeville; Odile J Bronchain; Jean-Christophe Marine; Andre Mazabraud; Marianne L Voz; Eric J Bellefroid
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  46 in total

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Review 6.  Pronephric tubule formation in zebrafish: morphogenesis and migration.

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Journal:  Pediatr Nephrol       Date:  2016-03-04       Impact factor: 3.714

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9.  Nephrotoxin Microinjection in Zebrafish to Model Acute Kidney Injury.

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