Literature DB >> 23832868

Development of high-content assays for kidney progenitor cell expansion in transgenic zebrafish.

Subramaniam Sanker1, Maria Cecilia Cirio, Laura L Vollmer, Natasha D Goldberg, Lee A McDermott, Neil A Hukriede, Andreas Vogt.   

Abstract

Reactivation of genes normally expressed during organogenesis is a characteristic of kidney regeneration. Enhancing this reactivation could potentially be a therapeutic target to augment kidney regeneration. The inductive events that drive kidney organogenesis in zebrafish are similar to the initial steps in mammalian kidney organogenesis. Therefore, quantifying embryonic signals that drive zebrafish kidney development is an attractive strategy for the discovery of potential novel therapeutic modalities that accelerate kidney regeneration. The Lim1 homeobox protein, Lhx1, is a marker of kidney development that is also expressed in the regenerating kidneys after injury. Using a fluorescent Lhx1a-EGFP transgene whose phenotype faithfully recapitulates that of the endogenous protein, we developed a high-content assay for Lhx1a-EGFP expression in transgenic zebrafish embryos employing an artificial intelligence-based image analysis method termed cognition network technology (CNT). Implementation of the CNT assay on high-content readers enabled automated real-time in vivo time-course, dose-response, and variability studies in the developing embryo. The Lhx1a assay was complemented with a kidney-specific secondary CNT assay that enables direct measurements of the embryonic renal tubule cell population. The integration of fluorescent transgenic zebrafish embryos with automated imaging and artificial intelligence-based image analysis provides an in vivo analysis system for structure-activity relationship studies and de novo discovery of novel agents that augment innate regenerative processes.

Entities:  

Keywords:  Zebrafish; high-content screening; image analysis; in vivo screening; phenotypic drug discovery

Mesh:

Substances:

Year:  2013        PMID: 23832868      PMCID: PMC3830658          DOI: 10.1177/1087057113495296

Source DB:  PubMed          Journal:  J Biomol Screen        ISSN: 1087-0571


  22 in total

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9.  Lhx1 is required for specification of the renal progenitor cell field.

Authors:  M Cecilia Cirio; Zhao Hui; Caroline E Haldin; Chiara Cianciolo Cosentino; Carsten Stuckenholz; Xiongfong Chen; Sung-Kook Hong; Igor B Dawid; Neil A Hukriede
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  13 in total

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Review 5.  Flow Cytometry: Impact on Early Drug Discovery.

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Review 6.  Sepsis-Associated Acute Kidney Injury: A Problem Deserving of New Solutions.

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10.  Delayed treatment with PTBA analogs reduces postinjury renal fibrosis after kidney injury.

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Journal:  Am J Physiol Renal Physiol       Date:  2015-12-09
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