2010
DOI: 10.2337/db10-0308
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Tauroursodeoxycholic Acid May Improve Liver and Muscle but Not Adipose Tissue Insulin Sensitivity in Obese Men and Women

Abstract: OBJECTIVEInsulin resistance is commonly associated with obesity. Studies conducted in obese mouse models found that endoplasmic reticulum (ER) stress contributes to insulin resistance, and treatment with tauroursodeoxycholic acid (TUDCA), a bile acid derivative that acts as a chemical chaperone to enhance protein folding and ameliorate ER stress, increases insulin sensitivity. The purpose of this study was to determine the effect of TUDCA therapy on multiorgan insulin action and metabolic factors associated wi… Show more

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Cited by 348 publications
(259 citation statements)
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“…The expansion of ISCs in Xbp1 /(IEC) mice, and the desire to delineate the specific tumor-promoting role of Xbp1 deficiency specifically in IECs, prompted us to Epithelial Xbp1 suppresses tumor formation in Apc min/+ mice Inflammatory signaling is an important contributor to CAC but also to sporadic and familial CRC (Rakoff-Nahoum and Medzhitov, 2007; Lee et al, 2010), with overlapping and distinct inflammatory pathways being involved (Salcedo et al, 2010). ER stress in various organs, including the liver, skeletal muscle, adipose tissue (Ozcan et al, 2004;Gregor et al, 2009;Kars et al, 2010), and intestinal crypts (Hodin et al, 2011), is associated with obesity, which is epidemiologically closely associated with increased cancer incidence, most notably CRC (Calle et al, 2003). CRC and CAC exhibit distinguishing features with regard to their molecular genetic underpinning; ;Apc min mice allowed crypt-specific stratification of Olfm4 + cell enumeration in lysozyme + and lysozyme  crypts (n = 4/4; two-sided Student's t test).…”
Section: Isc Expansion Is Dependent On Overactivation Of Ire1mentioning
confidence: 99%
“…The expansion of ISCs in Xbp1 /(IEC) mice, and the desire to delineate the specific tumor-promoting role of Xbp1 deficiency specifically in IECs, prompted us to Epithelial Xbp1 suppresses tumor formation in Apc min/+ mice Inflammatory signaling is an important contributor to CAC but also to sporadic and familial CRC (Rakoff-Nahoum and Medzhitov, 2007; Lee et al, 2010), with overlapping and distinct inflammatory pathways being involved (Salcedo et al, 2010). ER stress in various organs, including the liver, skeletal muscle, adipose tissue (Ozcan et al, 2004;Gregor et al, 2009;Kars et al, 2010), and intestinal crypts (Hodin et al, 2011), is associated with obesity, which is epidemiologically closely associated with increased cancer incidence, most notably CRC (Calle et al, 2003). CRC and CAC exhibit distinguishing features with regard to their molecular genetic underpinning; ;Apc min mice allowed crypt-specific stratification of Olfm4 + cell enumeration in lysozyme + and lysozyme  crypts (n = 4/4; two-sided Student's t test).…”
Section: Isc Expansion Is Dependent On Overactivation Of Ire1mentioning
confidence: 99%
“…Ancak, her iki grupta da kas ve adipoz dokudaki ER stres markerlerinde bir değişiklik görülmemiştir. 110 …”
Section: İnsan çAlişmalariunclassified
“…However, it is not yet understood whether chemical chaperones could directly improve kidney function or whether these results are simply confounded by the improvement in glycaemic control observed with this class of agents. Despite a recent clinical investigation determining that oral TUDCA administration can increase both hepatic and muscular insulin sensitivities in obese non-diabetic patients (Kars et al 2010), markers of ER stress were not improved and therefore it is evident that there is still relatively little known about the long-term efficacy and target specificity of these ER stress modulators in humans. Enhanced mTORC1 activity in the PTCs not only contributes to proapoptotic pathways, but through the selective activation of the IRE1-JNK pathway could also lead to decreased responsiveness to insulin in the PTCs.…”
Section: Therapeutic Implications Of Er Stress Modulatorsmentioning
confidence: 99%