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• W2171124019 abstract "Aldo-keto reductase 1 member B1 (AKR1B1) is pathogenically involved in diabetic complications by driving glucose flux through polyol pathway; a variety of AKR1B1 inhibitors has been developed for the treatment of diabetic complications and a body of invaluable preclinical and clinical data have been collected through decades efforts. Recent studies have shown that some AKR1B1 inhibitors demonstrate strong inhibitory activity to aldo-keto reductase family 1 member B10 (AKR1B10), a protein identical to AKR1B1, in vitro and in cancer cells. AKR1B1 and AKR1B10 are overexpressed in human tumors, such as liver, breast, and lung cancer, and may play a critical role in the development and progression of cancer through carbonyl detoxification, retinoic acid homeostatic regulation, and lipid metabolic control, as well as the activation of tobacco smoke carcinogens. Therefore, AKR1B1 inhibitors may represent a novel class of antitumor agents; and the clinical data assembled in diabetic clinics would greatly assist the transition of these inhibitors to cancer clinics. This article summaries the current understanding of the expression and function of AKR1B1 and AKR1B10 in human cancers and reviews the patents and papers of AKR1B1 inhibitors. Authors opinions concerning the current and future development of AKR1B1 and/or AKR1B10-specific inhibitors are discussed. Keywords: Aldose reductase, aldose reductase-like-1, Aldo-keto reductase family 1 B1, Aldo-keto reductase family 1 B10, AR, ARL-1, AKR1B1, AKR1B10, aldose reductase inhibitor, ARI" @default.
• W2171124019 created "2016-06-24" @default.
• W2171124019 creator A5043385269 @default.
• W2171124019 creator A5063441337 @default.
• W2171124019 creator A5066877119 @default.
• W2171124019 date "2009-11-01" @default.
• W2171124019 modified "2023-10-01" @default.
• W2171124019 title "Aldo-Keto Reductase Family 1 Member B1 Inhibitors: Old Drugs with New Perspectives" @default.
• W2171124019 cites W1595134965 @default.
• W2171124019 cites W1652262185 @default.
• W2171124019 cites W1676132058 @default.
• W2171124019 cites W182700988 @default.
• W2171124019 cites W1964932306 @default.
• W2171124019 cites W1966233962 @default.
• W2171124019 cites W1975727569 @default.
• W2171124019 cites W1986604347 @default.
• W2171124019 cites W1988244470 @default.
• W2171124019 cites W1993075341 @default.
• W2171124019 cites W1996337164 @default.
• W2171124019 cites W1997595033 @default.
• W2171124019 cites W1998118806 @default.
• W2171124019 cites W1999827072 @default.
• W2171124019 cites W2000218602 @default.
• W2171124019 cites W2001244799 @default.
• W2171124019 cites W2006510296 @default.
• W2171124019 cites W2009940306 @default.
• W2171124019 cites W2012886938 @default.
• W2171124019 cites W2016250363 @default.
• W2171124019 cites W2016927144 @default.
• W2171124019 cites W2018146693 @default.
• W2171124019 cites W2018323250 @default.
• W2171124019 cites W2019014760 @default.
• W2171124019 cites W2020073319 @default.
• W2171124019 cites W2021640840 @default.
• W2171124019 cites W2022033436 @default.
• W2171124019 cites W2024586219 @default.
• W2171124019 cites W2025701628 @default.
• W2171124019 cites W2028644941 @default.
• W2171124019 cites W2033979611 @default.
• W2171124019 cites W2036045723 @default.
• W2171124019 cites W2037093159 @default.
• W2171124019 cites W2039115551 @default.
• W2171124019 cites W2041524061 @default.
• W2171124019 cites W2043940598 @default.
• W2171124019 cites W2045604514 @default.
• W2171124019 cites W2048548143 @default.
• W2171124019 cites W2054657968 @default.
• W2171124019 cites W2054763317 @default.
• W2171124019 cites W2057093372 @default.
• W2171124019 cites W2060033906 @default.
• W2171124019 cites W2061505784 @default.
• W2171124019 cites W2066518128 @default.
• W2171124019 cites W2070889802 @default.
• W2171124019 cites W2070927097 @default.
• W2171124019 cites W2080608495 @default.
• W2171124019 cites W2083825751 @default.
• W2171124019 cites W2086989377 @default.
• W2171124019 cites W2087644601 @default.
• W2171124019 cites W2089021918 @default.
• W2171124019 cites W2093265805 @default.
• W2171124019 cites W2093367519 @default.
• W2171124019 cites W2094587681 @default.
• W2171124019 cites W2099660560 @default.
• W2171124019 cites W2101324933 @default.
• W2171124019 cites W2107066255 @default.
• W2171124019 cites W2109029434 @default.
• W2171124019 cites W2113244663 @default.
• W2171124019 cites W2122617375 @default.
• W2171124019 cites W2122815214 @default.
• W2171124019 cites W2124676948 @default.
• W2171124019 cites W2126243275 @default.
• W2171124019 cites W2126847998 @default.
• W2171124019 cites W2128514914 @default.
• W2171124019 cites W2129475394 @default.
• W2171124019 cites W2133543344 @default.
• W2171124019 cites W2134983606 @default.
• W2171124019 cites W2136043142 @default.
• W2171124019 cites W2136779207 @default.
• W2171124019 cites W2138393164 @default.
• W2171124019 cites W2139320397 @default.
• W2171124019 cites W2144312770 @default.
• W2171124019 cites W2152218732 @default.
• W2171124019 cites W2154789716 @default.
• W2171124019 cites W2154893083 @default.
• W2171124019 cites W2157877381 @default.
• W2171124019 cites W2158046708 @default.
• W2171124019 cites W2160217760 @default.
• W2171124019 cites W2160667076 @default.
• W2171124019 cites W2164531086 @default.
• W2171124019 cites W2166832580 @default.
• W2171124019 cites W2283130574 @default.
• W2171124019 cites W2329990470 @default.
• W2171124019 cites W2416162336 @default.
• W2171124019 cites W2465420215 @default.
• W2171124019 doi "https://doi.org/10.2174/157489209789206931" @default.
• W2171124019 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/19522700" @default.
• W2171124019 hasPublicationYear "2009" @default.
• W2171124019 type Work @default.

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