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Critical Reviews in Food Science and Nutrition Volume 59, 2019 - Issue 7
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Curcumin against advanced glycation end products (AGEs) and AGEs-induced detrimental agents

Mohammad AlizadehAssociate Professor, Department of Nutrition, Tabriz University of Medical Sciences, Tabriz, Iran
&
Sorayya KheirouriAssociate Professor, Department of Nutrition, Tabriz University of Medical Sciences, Tabriz, IranCorrespondence[email protected]
Pages 1169-1177 | Published online: 29 Nov 2017
 
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ABSTRACT

Objectives: This study was aimed to review and collate effects of curcumin on generation of advanced glycation end products (AGEs) and AGEs induced detrimental agents.Methods: Pubmed, Googlescholar, ScienceDirect, and Scopus databases were searched. Searching was not limited to specific publication period. Only English language original articles (in vitro, experimental and human) which had examined the effect of curcumin on AGEs formation and AGEs induced apoptosis, oxidative stress or inflammatory responses were included. To review effect of curcumin on AGEs formation, search terms were as following: ‘‘curcumin” (title) and AGEs or pentosidine or methylglyoxal or carboxymethyllysine or glucosylation (title/abstract). Totally 104 articles were searched which 19 were selected for review. To review effect of curcumin on AGEs induced harmful agents, key words were as following: “curcumin” (title) and AGEs (title/abstract) and apoptosis or oxidative stress or DNA damage or cell injury or inflammatory or cell death or cell proliferation (title/abstract). Totally 126 articles were searched which 18 were found appropriate for review.Results: Regarding curcumin and AGEs formation, ten eligible articles (1 human trial, 5 animal models and 4 in vitro) and with regarding curcumin and AGEs-induced complications, 17 articles (5 on apoptosis, 9 on oxidative stress, and 3 on inflammatory responses) were selected. Except one, all studies indicated that curcumin is able to prevent AGEs formation and AGEs-induced disturbances with different potential mechanisms.Conclusion: Curcumin can inhibit AGEs formation and AGEs-induced disturbances. More RCT researches are suggested to evaluate beneficial effect of curcumin regarding AGEs in different age-related chronic diseases, with specific attention to AGEs memberships.

Conflict of interests

The authors declare that they have no financial or non-financial conflict of interests.

Authors' contributions

Both authors conducted the search, and participated in manuscript writing. Both authors read and approved the final manuscript.

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Related Research Data

Inhibition effect of curcumin on TNF-α and MMP-13 expression induced by advanced glycation end products in chondrocytes.
Source: S. Karger AG
Methylglyoxal-induced neuroinflammatory response in in vitro astrocytic cultures and hippocampus of experimental animals.
Source: Springer Science and Business Media LLC
Curcumin Ameliorates Arterial Dysfunction and Oxidative Stress with Aging
Source: Elsevier BV
Glyoxal and methylglyoxal: autoxidation from dihydroxyacetone and polyphenol cytoprotective antioxidant mechanisms.
Source: Elsevier BV
Advanced Glycation Endproducts Promote Adhesion Molecule (VCAM-1, ICAM-1) Expression and Atheroma Formation in Normal Rabbits
Source: Springer Science and Business Media LLC
Curcumin: A review of anti-cancer properties and therapeutic activity in head and neck squamous cell carcinoma
Source: BMC
Methylglyoxal-derived advanced glycation endproducts in multiple sclerosis
Source: MDPI AG
Curcumin inhibits advanced glycation end product-induced oxidative stress and inflammatory responses in endothelial cell damage via trapping methylglyoxal
Source: Spandidos Publications
Advanced glycation endproduct (AGE) receptor 1 is a negative regulator of the inflammatory response to AGE in mesangial cells
Source: Proceedings of the National Academy of Sciences
Regulation of Human Melanoma Growth and Metastasis by AGE–AGE Receptor Interactions
Source: The Society for Investigative Dermatology, Inc.
Advanced glycation end product cross-linking: pathophysiologic role and therapeutic target in cardiovascular disease.
Source: Wiley
Trapping of Methylglyoxal by Curcumin in Cell-Free Systems and in Human Umbilical Vein Endothelial Cells
Source: American Chemical Society (ACS)
Advanced Glycation End Products: A Molecular Target for Vascular Complications in Diabetes
Source: Springer Science and Business Media LLC
Inhibitory effect of vanillic acid on methylglyoxal-mediated glycation in apoptotic Neuro-2A cells
Source: Elsevier BV
Effect of advanced glycation end-products on cell proliferation and cell death
Source: Elsevier BV
Methylglyoxal augments intracellular oxidative stress in human aortic endothelial cells
Source: Informa UK Limited
Glyoxal and methylglyoxal trigger distinct signals for map family kinases and caspase activation in human endothelial cells.
Source: Elsevier BV
Heme oxygenase-1 induction protects against hypertension associated with diabetes: effect on exaggerated vascular contractility
Source: Springer Science and Business Media LLC
Curcumin Alleviates Diabetic Cardiomyopathy in Experimental Diabetic Rats
Source: Public Library of Science (PLoS)
Inhibitory effects of curcumin derivatives on nonenzymatic glucosylation in vitro
Source: Springer Science and Business Media LLC
Effect of curcumin on the advanced glycation and cross-linking of collagen in diabetic rats.
Source: Elsevier BV
Advanced glycation end products and neurodegenerative diseases: Mechanisms and perspective
Source: Elsevier BV
Polyphenols in Alzheimer's Disease and in the Gut-Brain Axis.
Source: MDPI AG
Curcumin inhibits gene expression of RAGE in HSCs
Source: Wiley
Endogenous formation of Nε(carboxymethyl)lysine is increased in fatty livers and induces inflammatory markers in an in vitro model of hepatic steatosis
Source: Elsevier BV
Carnosine and advanced glycation end products: a systematic review.
Source: Springer Science and Business Media LLC
Curcumin and diabetes: a systematic review
Source: Hindawi Limited
Curcumin eliminates the inhibitory effect of advanced glycation end-products (AGEs) on gene expression of AGE receptor-1 in hepatic stellate cells in vitro.
Source: Springer Science and Business Media LLC

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