daf-16 is a forkhead-type transcription factor, functioning downstream of insulin-like signals, and is known to be critical to the regulation of life span in Caenorhabditis elegans. Mammalian DAF-16 homologues include AFX, FKHR and FKHRL1, which contain a conserved forkhead domain and three putative phosphorylation sites for the Ser/Thr kinase Akt/protein kinase B (PKB), as well as for DAF-16. To assess the function of the homologues, we examined tissue distribution patterns of mRNAs for DAF-16 homologues in mice. In the embryos, expressions of AFX, FKHR and FKHRL1 mRNAs were complementary to each other and were highest in muscle, adipose tissue and embryonic liver. The characteristic expression pattern remained in the adult, except that signals of FKHRL1 became evident in more tissues, including the brain. In order to clarify whether each DAF-16 homologue had different target genes, we determined the consensus sequences for the binding of DAF-16 and the mouse homologues. The binding sequences for all four proteins shared a core sequence, TTGTTTAC, daf-16 family protein-binding element (DBE) binding protein. However, electrophoretic mobility shift assay showed that the binding affinity of DAF-16 homologues to the core sequence was stronger than that to the insulin-responsive element in the insulin-like growth factor binding protein-1 promoter region, which has been identified as a binding sequence for them. We identified one copy of the DBE upstream of the first exon of sod-3 by searching the genomic database of C. elegans. Taken together, DAF-16 homologues can fundamentally regulate the common target genes in insulin-responsive tissues and the specificity to target genes of each protein is partially determined by the differences in their expression patterns.
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Research Article|
July 10 2000
Identification of the differential distribution patterns of mRNAs and consensus binding sequences for mouse DAF-16 homologues
Tatsuo FURUYAMA;
Tatsuo FURUYAMA
1
*Laboratory of Genetics of Aging, Department of Molecular Genetic Research, National Institute for Longevity Sciences (NILS), 36-3 Gengo, Morioka, Oobu, Aichi 474-8522, Japan
1To whom correspondence should be addressed (e-mail tfuruyam@;nils.go.jp).
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Toru NAKAZAWA;
Toru NAKAZAWA
*Laboratory of Genetics of Aging, Department of Molecular Genetic Research, National Institute for Longevity Sciences (NILS), 36-3 Gengo, Morioka, Oobu, Aichi 474-8522, Japan
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Itsuko NAKANO;
Itsuko NAKANO
†CREST, Science and Technology Corporation of Japan (JST), 36-3 Gengo, Morioka, Oobu, Aichi 474-8522, Japan
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Nozomu MORI
Nozomu MORI
*Laboratory of Genetics of Aging, Department of Molecular Genetic Research, National Institute for Longevity Sciences (NILS), 36-3 Gengo, Morioka, Oobu, Aichi 474-8522, Japan
†CREST, Science and Technology Corporation of Japan (JST), 36-3 Gengo, Morioka, Oobu, Aichi 474-8522, Japan
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Publisher: Portland Press Ltd
Received:
October 25 1999
Revision Received:
April 07 2000
Accepted:
May 09 2000
Online ISSN: 1470-8728
Print ISSN: 0264-6021
The Biochemical Society, London © 2000
2000
Biochem J (2000) 349 (2): 629–634.
Article history
Received:
October 25 1999
Revision Received:
April 07 2000
Accepted:
May 09 2000
Citation
Tatsuo FURUYAMA, Toru NAKAZAWA, Itsuko NAKANO, Nozomu MORI; Identification of the differential distribution patterns of mRNAs and consensus binding sequences for mouse DAF-16 homologues. Biochem J 15 July 2000; 349 (2): 629–634. doi: https://doi.org/10.1042/bj3490629
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