Literature DB >> 22414809

Extrahepatic tissues compensate for loss of hepatic taurine synthesis in mice with liver-specific knockout of cysteine dioxygenase.

Iori Ueki1, Heather B Roman, Lawrence L Hirschberger, Carolyn Junior, Martha H Stipanuk.   

Abstract

Because hepatic cysteine dioxygenase (CDO) appears to play the major role in controlling cysteine catabolism in the intact rat, we characterized the effect of a lack of hepatic CDO on the regulation of cysteine and its metabolites at the whole body level. In mice with liver-specific deletion of CDO expression, hepatic and plasma cysteine levels increased. In addition, in mice with liver-specific deletion of CDO expression, the abundance of CDO and the proportion of CDO existing as the mature, more active isoform increased in extrahepatic tissues that express CDO (kidney, brown fat, and gonadal fat). CDO abundance was also increased in the pancreas, where most of the enzyme in both control and liver CDO-knockout mice was in the more active isoform. This upregulation of CDO concentration and active-site cofactor formation were not associated with an increase in CDO mRNA and thus presumably were due to a decrease in CDO degradation and an increase in CDO cofactor formation in association with increased exposure of extrahepatic tissues to cysteine in mice lacking hepatic CDO. Extrahepatic tissues of liver CDO-knockout mice also had higher levels of hypotaurine, consistent with increased metabolism of cysteine by the CDO/cysteinesulfinate decarboxylase pathway. The hepatic CDO-knockout mice were able to maintain normal levels of glutathione, taurine, and sulfate. The maintenance of taurine concentrations in liver as well as in extrahepatic tissues is particularly notable, since mice were fed a taurine-free diet and liver is normally considered the major site of taurine biosynthesis. This redundant capacity for regulation of cysteine concentrations and production of hypotaurine/taurine is additional support for the body's robust mechanisms for control of body cysteine levels and indicates that extrahepatic tissues are able to compensate for a lack of hepatic capacity for cysteine catabolism.

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Year:  2012        PMID: 22414809      PMCID: PMC3361984          DOI: 10.1152/ajpendo.00589.2011

Source DB:  PubMed          Journal:  Am J Physiol Endocrinol Metab        ISSN: 0193-1849            Impact factor:   4.310


  32 in total

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Journal:  Am J Physiol Endocrinol Metab       Date:  2001-05       Impact factor: 4.310

5.  Cre activity in fetal albCre mouse hepatocytes: Utility for developmental studies.

Authors:  Carla M Weisend; Jean A Kundert; Elena S Suvorova; Justin R Prigge; Edward E Schmidt
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Authors:  Jeong-In Lee; Monica Londono; Lawrence L Hirschberger; Martha H Stipanuk
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  14 in total

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Review 2.  H2S and its role in redox signaling.

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Journal:  Biochim Biophys Acta       Date:  2014-01-11

3.  Primary hepatocytes from mice lacking cysteine dioxygenase show increased cysteine concentrations and higher rates of metabolism of cysteine to hydrogen sulfide and thiosulfate.

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Review 4.  Role of taurine, its haloamines and its lncRNA TUG1 in both inflammation and cancer progression. On the road to therapeutics? (Review).

Authors:  Stella Baliou; Anthony M Kyriakopoulos; Demetrios A Spandidos; Vassilios Zoumpourlis
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5.  Bile acids regulate cysteine catabolism and glutathione regeneration to modulate hepatic sensitivity to oxidative injury.

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6.  The cysteine dioxgenase knockout mouse: altered cysteine metabolism in nonhepatic tissues leads to excess H2S/HS(-) production and evidence of pancreatic and lung toxicity.

Authors:  Heather B Roman; Lawrence L Hirschberger; Jakub Krijt; Alessandro Valli; Viktor Kožich; Martha H Stipanuk
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Review 7.  Enzymology of H2S biogenesis, decay and signaling.

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8.  Cysteine dioxygenase is essential for mouse sperm osmoadaptation and male fertility.

Authors:  Atsushi Asano; Heather B Roman; Lawrence L Hirschberger; Ai Ushiyama; Jacquelyn L Nelson; Meleana M Hinchman; Martha H Stipanuk; Alexander J Travis
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9.  Sulfur Metabolism Under Stress.

Authors:  Colin G Miller; Edward E Schmidt
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10.  Propargylglycine inhibits hypotaurine/taurine synthesis and elevates cystathionine and homocysteine concentrations in primary mouse hepatocytes.

Authors:  Halina Jurkowska; Martha H Stipanuk; Lawrence L Hirschberger; Heather B Roman
Journal:  Amino Acids       Date:  2015-03-13       Impact factor: 3.520

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