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Publication : Transforming growth factor-β3 (TGF-β3) knock-in ameliorates inflammation due to TGF-β1 deficiency while promoting glucose tolerance.

First Author  Hall BE Year  2013
Journal  J Biol Chem Volume  288
Issue  44 Pages  32074-92
PubMed ID  24056369 Mgi Jnum  J:204892
Mgi Id  MGI:5543704 Doi  10.1074/jbc.M113.480764
Citation  Hall BE, et al. (2013) Transforming growth factor-beta3 (TGF-beta3) knock-in ameliorates inflammation due to TGF-beta1 deficiency while promoting glucose tolerance. J Biol Chem 288(44):32074-92
abstractText  Three homologues of TGF-beta exist in mammals as follows: TGF-beta1, TGF-beta2, and TGF-beta3. All three proteins share high homology in their amino acid sequence, yet each TGF-beta isoform has unique heterologous motifs that are highly conserved during evolution. Although these TGF-beta proteins share similar properties in vitro, isoform-specific properties have been suggested through in vivo studies and by the unique phenotypes for each TGF-beta knock-out mouse. To test our hypothesis that each of these homologues has nonredundant functions, and to identify such isoform-specific roles, we genetically exchanged the coding sequence of the mature TGF-beta1 ligand with a sequence from TGF-beta3 using targeted recombination to create chimeric TGF-beta1/3 knock-in mice (TGF-beta1(Lbeta3/Lbeta3)). In the TGF-beta1(Lbeta3/Lbeta3) mouse, localization and activation still occur through the TGF-beta1 latent associated peptide, but cell signaling is triggered through the TGF-beta3 ligand that binds to TGF-beta receptors. Unlike TGF-beta1(-/-) mice, the TGF-beta1(Lbeta3/Lbeta3) mice show neither embryonic lethality nor signs of multifocal inflammation, demonstrating that knock-in of the TGF-beta3 ligand can prevent the vasculogenesis defects and autoimmunity associated with TGF-beta1 deficiency. However, the TGF-beta1(Lbeta3/Lbeta3) mice have a shortened life span and display tooth and bone defects, indicating that the TGF-beta homologues are not completely interchangeable. Remarkably, the TGF-beta1(Lbeta3/Lbeta3) mice display an improved metabolic phenotype with reduced body weight gain and enhanced glucose tolerance by induction of beneficial changes to the white adipose tissue compartment. These findings reveal both redundant and unique nonoverlapping functional diversity in TGF-beta isoform signaling that has relevance to the design of therapeutics aimed at targeting the TGF-beta pathway in human disease.
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