Literature DB >> 11331749

Changes in global gene expression patterns during development and maturation of the rat kidney.

R O Stuart1, K T Bush, S K Nigam.   

Abstract

We set out to define patterns of gene expression during kidney organogenesis by using high-density DNA array technology. Expression analysis of 8,740 rat genes revealed five discrete patterns or groups of gene expression during nephrogenesis. Group 1 consisted of genes with very high expression in the early embryonic kidney, many with roles in protein translation and DNA replication. Group 2 consisted of genes that peaked in midembryogenesis and contained many transcripts specifying proteins of the extracellular matrix. Many additional transcripts allied with groups 1 and 2 had known or proposed roles in kidney development and included LIM1, POD1, GFRA1, WT1, BCL2, Homeobox protein A11, timeless, pleiotrophin, HGF, HNF3, BMP4, TGF-alpha, TGF-beta2, IGF-II, met, FGF7, BMP4, and ganglioside-GD3. Group 3 consisted of transcripts that peaked in the neonatal period and contained a number of retrotransposon RNAs. Group 4 contained genes that steadily increased in relative expression levels throughout development, including many genes involved in energy metabolism and transport. Group 5 consisted of genes with relatively low levels of expression throughout embryogenesis but with markedly higher levels in the adult kidney; this group included a heterogeneous mix of transporters, detoxification enzymes, and oxidative stress genes. The data suggest that the embryonic kidney is committed to cellular proliferation and morphogenesis early on, followed sequentially by extracellular matrix deposition and acquisition of markers of terminal differentiation. The neonatal burst of retrotransposon mRNA was unexpected and may play a role in a stress response associated with birth. Custom analytical tools were developed including "The Equalizer" and "eBlot," which contain improved methods for data normalization, significance testing, and data mining.

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Year:  2001        PMID: 11331749      PMCID: PMC33267          DOI: 10.1073/pnas.091110798

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  23 in total

1.  Signaling and circuitry of multiple MAPK pathways revealed by a matrix of global gene expression profiles.

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2.  Gene ontology: tool for the unification of biology. The Gene Ontology Consortium.

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Review 3.  Branching morphogenesis during kidney development.

Authors:  M Pohl; R O Stuart; H Sakurai; S K Nigam
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4.  Physiological stresses increase mouse short interspersed element (SINE) RNA expression in vivo.

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Review 9.  Interspersed repeats and other mementos of transposable elements in mammalian genomes.

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  48 in total

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Review 2.  Building an atlas of gene expression driving kidney development: pushing the limits of resolution.

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5.  Organogenesis forum lecture: In vitro kidney development, tissue engineering and systems biology.

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Review 6.  Concise review: can the intrinsic power of branching morphogenesis be used for engineering epithelial tissues and organs?

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9.  Dynamic changes of gene expression profiles during postnatal development of the heart in mice.

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10.  Hs2st mediated kidney mesenchyme induction regulates early ureteric bud branching.

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