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A new Cre driver mouse line, Tcf21/Pod1-Cre, targets metanephric mesenchyme.

Abstract

Conditional gene targeting in mice has provided great insight into the role of gene function in kidney development and disease. Although a number of Cre-driver mouse strains already exist for the kidney, development of additional strains with unique expression patterns is needed. Here we report the generation and validation of a Tcf21/Pod1-Cre driver strain that expresses Cre recombinase throughout the condensing and stromal mesenchyme of developing kidneys and in their derivatives including epithelial components of the nephron and interstitial cells. To test the efficiency of this line, we crossed it to mice transgenic for either loss or gain of function β-catenin conditional alleles. Mice with deletion of β-catenin from Tcf21-expressing cells are born with hypoplastic kidneys, hydroureters and hydronephrosis. By contrast, Tcf21-Cre driven gain of function for β-catenin in mice results in fused midline kidneys and hypoplastic kidneys. Finally, we report the first renal mesenchymal deletion of Patched1 (Ptch1), the receptor for sonic hedgehog (Shh), which results in renal cysts demonstrating a functional role of Shh signaling pathway in renal cystogensis. In summary, we report the generation and validation of a new Cre driver strain that provides robust excision in metanephric mesenchyme.

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  • Authors

    Maezawa Y, Binnie M, Li C, Thorner P, Hui CC, Alman B, Taketo MM, Quaggin SE

    Institution

    The Samuel Lunenfeld Research Institute, Mount Sinai Hospital, Toronto, Ontario, Canada.

    Source

    PloS one 7:7 2012 pg e40547

    MeSH

    Animals
    Basic Helix-Loop-Helix Transcription Factors
    Breeding
    Female
    Gene Deletion
    Gene Expression Regulation, Developmental
    Gene Order
    Gene Targeting
    Genetic Vectors
    Integrases
    Kidney
    Male
    Mesoderm
    Mice
    Mice, Transgenic
    Polycystic Kidney Diseases
    Promoter Regions, Genetic
    Receptors, Cell Surface
    beta Catenin

    Pub Type(s)

    Journal Article
    Research Support, Non-U.S. Gov't

    Language

    eng

    PubMed ID

    22792366