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Aldo-Keto Reductases and Toxicant Metabolism (ACS Symposium)
 
 
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Aldo-Keto Reductases and Toxicant Metabolism (ACS Symposium) [Hardcover]

Trevor M. Penning (Editor), J. Mark Petrash (Editor)

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Book Description

0841238464 978-0841238466 November 20, 2003
Aldo-Keto Reductases and Toxicant Metabolism provides an overview of the rapidly growing Aldo-Keto Reductase (AKR) superfamily and its role in the metabolism of endogenous and exogenous toxicants. This book discusses the ability of AKRs to metabolize endogenous toxicants including: sugar aldehydes, advanced glycosylation end products, and lipid aldehydes (products of lipid peroxidation decomposition).

The relevance to diabetic complications is also stressed. The role of AKRs to metabolize exogenous toxicants including tobacco carcinogens (tobacco specific nitrosamine ketones and trans-dihydrodiols derived from polycyclic aromatic hydrocarbons), mycotoxins (aflatoxin dialdehydes), and unnatural aldehydes is covered in detail. In the case of PAH trans-dihydrodiols, a clear example is given that AKRs may not always be chemoprotective; in this instance, reactive and redox-active quinones are formed. What emerges is that AKRs play a central role in toxicant metabolism.

Aldo-Keto Reductases and Toxicant Metabolism shows how evolutionary AKRs are conserved in prokaryotes through eukaroytes and can thus be considered primordial genes. They are also regulated by primordial stress signals (osmotic stress, reactive oxygen species, and electrophiles) to respond to toxic insult. The role of AKRs to respond to stress in vivo is given in a model of myocardial ischemia and re-perfusion injury. The power of functional yeast genomics is described to generate AKR null yeast strains and a resultant phenotype.

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Editorial Reviews

About the Author

Trevor M. Penning is at University of Pennsylvania School of Medicine. J. Mark Petrash is at Washington University School of Medicine.

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Inside This Book (learn more)
First Sentence:
Aldo-Keto Reductases (AKRs) are a rapidly growing gene superfamily involved in the formation of hyperosmotic sugars, which can contribute to diabetic complications. Read the first page
Key Phrases - Statistically Improbable Phrases (SIPs): (learn more)
aflatoxin aldehyde reductase, depurinating adducts, exogenous toxicants, secondary diabetic complications, human aldose reductase, using gradient system, null strain, dihydrodiol dehydrogenase, carbonyl reduction, mitogenic role, diabetic tissues, endogenous toxicants, carbonyl reductase, aldehyde functional group, derived aldehydes, toxic aldehydes, polyol pathway, reactive aldehydes, sorbitol accumulation, succinic semialdehyde, stable adducts, aldehyde reductases, reactive carbonyls, dehydrogenase type, inhibitor sensitivity
Key Phrases - Capitalized Phrases (CAPs): (learn more)
Cancer Res, Vander Jagt, American Chemical Society, Free Radic, Eye Res, School of Medicine, University of Pennsylvania, Cancer Lett, New York, University of Louisville, University of Texas Medical Branch, Academic Press, Cancer Epidemiol, Chem Biol Interact, Department of Medicine, Drug Metab, Research Centre, San Jose, Tetrahedron Lett, Thermo Finnigan, University of Chicago
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