Impairment of calcium ATPases by high glucose and potential pharmacological protection

L. Horáková*, M.K. Strosova, C.M. Spickett, D. Blaskovic

*Corresponding author for this work

Research output: Contribution to journalArticlepeer-review


The review deals with impairment of Ca2+-ATPases by high glucose or its derivatives in vitro, as well as in human diabetes and experimental animal models. Acute increases in glucose level strongly correlate with oxidative stress. Dysfunction of Ca2+-ATPases in diabetic and in some cases even in nondiabetic conditions may result in nitration of and in irreversible modification of cysteine-674. Nonenyzmatic protein glycation might lead to alteration of Ca2+-ATPase structure and function contributing to Ca2+ imbalance and thus may be involved in development of chronic complications of diabetes. The susceptibility to glycation is probably due to the relatively high percentage of lysine and arginine residues at the ATP binding and phosphorylation domains. Reversible glycation may develop into irreversible modifications (advanced glycation end products, AGEs). Sites of SERCA AGEs are depicted in this review. Finally, several mechanisms of prevention of Ca2+-pump glycation, and their advantages and disadvantages are discussed. © 2013 Informa UK, Ltd.

Original languageEnglish
Pages (from-to)81-92
Number of pages12
JournalFree Radical Research
Issue numberS1
Publication statusPublished - Aug 2013


  • cysteine-674
  • diabetes
  • glycation
  • ntrotyrosine
  • pathway
  • polyol


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