Life Extension Magazine®

Sugar cube glycation can bind to proteins in body

How Glycation Accelerates Aging

When sugar (glucose) reacts with the body’s proteins, the resulting tissue glycation accelerates aging. There are a number of strategies that reduce toxic glycation reactions and help overcome their consequences.

Scientifically reviewed by: Dr. April Parks, MD, MS, in August 2023. Written by: Stuart Chan.

 

Diabetics suffer accelerated aging and early-onset of degenerative illnesses.

An underlying culprit behind diabetic complications is tissue glycation.1

Glycation occurs when blood glucose links to proteins in the body. The pathologic impact is formation of advanced glycation end products that wreak systemic havoc.2-9

Those with poor sugar control suffer dangerously high glycation levels. These same toxic glucose reactions occur in nondiabetics, but at a slower pace.

For the past 14 years, Life Extension Magazine® has advised readers to avoid or reduce intake of food cooked at high temperatures. The reason is, when you eat these heat-damaged proteins, they inflict glycation damage to your body’s proteins. This is in addition to glycation that occurs as a result of life-long glucose exposure.

In this article, we provide a targeted strategy to defend against glycation-induced tissue damage.

What is Glycation?

Glycation is a process by which sugar molecules react chemically with proteins in the body, causing the proteins to cross-link and lose their functionality.2

Not only does this cross-linking prevent proteins from doing their intended jobs, it creates harmful molecules called advanced glycation end products (or AGEs).3

The acronym AGEs is appropriate considering these toxic protein reactions are a root cause of premature aging.

Ultimately, glycation causes inflammation that damages mitochondria, while mitochondrial dysfunction exacerbates glycation. This result in an age-accelerating cycle as glycated proteins accumulate in tissues throughout the body.4,5

Mitochondria and Aging

Mitochondria
Mitochondria

The human body depends on sugar and oxygen to provide the energy that keeps its heart beating and brain thinking. Intracellular powerhouses called mitochondria work wonders by using glucose, fatty acids, and oxygen. The result is life-giving energy that powers every aspect of the body.

But, like other forms of energy generation, the process produces reactive molecules as byproducts that build up and damage the very cells, tissues, and organs the process is meant to support.

Glycation also damages molecules vital to life, like DNA, enzymes, and structural proteins.

Progressive glycation leads to reduced mitochondrial energy production and increased oxidative stress. Eventually, damaged mitochondria can stop functioning altogether, producing an age-related energy crisis that speeds up and worsens the aging process.6

This is one reason why, as we age, we not only move and think more slowly, but we also repair damage to cells and DNA more slowly, if at all. All of those actions require energy, which is in increasingly short supply.

Impact on the Body

Damaged strand of DNA
Damaged strand of DNA

Together, mitochondrial dysfunction and glycation have a disastrous effect on the body’s systems, and are responsible for many symptoms of aging. Here is a partial list of the types of damage they wreak on the body:

  • The accumulation of advanced glycation end products (AGEs) can contribute to kidney disease and renal failure. When AGEs accumulate in the filtering portions of kidneys, it reduces the ability to excrete waste.7
  • AGEs can lead to neurodegenerative diseases like Alzheimer’s and Parkinson’s because they contribute to the formation of cross-linked proteins. These damaged proteins accumulate in cells, disabling and eventually killing brain cells.8,9
  • When glycation occurs in the skin, it sensitizes the skin to ultraviolet (UV) radiation, triggering oxidative stress that damages DNA and increases the risk of skin cancers.10
  • AGEs damage joint cartilage, resulting in stiffening and loss of ability to handle stresses. AGEs are now recognized as major contributors to osteoarthritis.11
  • When similar AGE-related damage occurs in spinal discs, it can make disc injury and herniation (“slipped disc”) more likely.12
  • Glycation is especially damaging to our eyes. Not only does it lead to clouding of the lens (cataracts), it also causes retinal damage—both of which impair vision and ultimately produce blindness.13,14
  • The protein-rich walls of arteries, and even tiny capillaries, are especially vulnerable to glycation-induced damage.15 The resulting stiffening and inflammatory changes produce atherosclerosis, the cause of heart attacks, strokes, and other vascular disorders of aging.4

In short, glycation, linked to poor mitochondrial function, accelerates every aspect of human aging.

While we are exposed to glycation on a daily basis, we are not helpless in the face of its destructive effects. A huge volume of published data support the use of specific nutrients that work hand-in-hand to reduce glycation and its effects, while also supporting healthy, energy-producing mitochondria.

What You Need to Know
Glycation and Aging

Glycation and Aging

  • Humans’ dependence on energy derived from using sugar molecules and oxygen comes at a cost: toxic and reactive molecules interact with essential proteins and fats, damaging cells’ ability to function and accelerating their aging.
  • Glycation, the binding of sugar molecules to cellular structures, triggers massive inflammation and releases chemically stressful small molecules, which in turn damage mitochondria.
  • Mitochondria lose their efficiency and eventually fade away under this chemical onslaught.
  • The combination of glycation and mitochondrial dysfunction and loss rapidly accelerates aging, leading to chronic disorders that shorten life and reduce its quality.
  • Natural compounds have been identified that are capable of reversing this accelerated aging.
  • Benfotiamine, luteolin, pyridoxal-5-phosphate, and carnosine block glycation and prevent its destructive consequences.
  • PQQ, R-lipoic acid, and taurine enhance mitochondrial resistance to glycation-induced oxidative stress. Both, PQQ and R-lipoic acid, promote formation of youthful new mitochondria.
  • This combination of nutrients can be expected to rejuvenate cellular energy levels while reducing chemically-induced damage to cells, thereby reversing the age-accelerating trend.

Antiglycation Nutrients

Four compounds have been identified to reduce the rate of glycation and control the consequences when it occurs.

The first is a fat-soluble form of vitamin B1 (thiamine) called benfotiamine.16,17 Lab studies have shown that benfotiamine can prevent glycation, and human studies have shown that it can help prevent the damage caused by glycation.16,18

In a study of type II diabetics, benfotiamine helped prevent blood-vessel damage caused by glycation. For the study, subjects ate a meal high in AGEs (caused by high-heat cooking), then took benfotiamine for three days, and then ate the same high-AGE meal again.18

Initially, the AGE-rich meal reduced blood flow throughout the subjects’ bodies as a result of the impact of AGEs on blood vessels. But after supplementing with benfotiamine for just three days, blood flow measurements completely normalized, demonstrating just how quickly benfotiamine exerts its powerful impact.

A later study of diabetic animals further demonstrated the ability of benfotiamine to improve heart and blood vessel function, while also reducing death and scarring of vital heart cells.19

Lab studies have given us insight into how benfotiamine works to prevent glycation itself, as well as the damage it can cause. Through at least three biochemical pathways, benfotiamine has now been shown to improve function of tiny capillaries in the retina, increase mitochondrial energy production in muscle cells, protect against kidney and other tissue damage in dialysis, and prevent DNA damage.17,20-24

Pyridoxal 5’-phosphate

Pyridoxal 5’-phosphate is an active form of vitamin B625 that is receiving growing attention as a natural complement to benfotiamine. Like benfotiamine, this active form of vitamin B6 has the dual benefit of helping prevent glycation as well as its harmful effects (such as the buildup of gunked-up proteins and AGEs).26,27

Pyridoxal 5’-phosphate is one of the most effective compounds known to inhibit glycation of fats (lipids) and proteins.28 This is an important protective function, since lipid glycation is a major threat to the function of cell membranes, which is an underlying factor in numerous age-related conditions.29,30

This metabolically active form of vitamin B6 (pyridoxal 5’-phosphate) works by essentially trapping glucose breakdown products before they can participate in dangerous glycation reactions.25

Avoid Foods Cooked at High Temperatures
Avoid Foods Cooked at High Temperatures

The way you cook your food can affect your chances of becoming diabetic.

A randomized, controlled trial looked at two groups of obese subjects.68 The first group ingested a diet typically high in advanced glycation end-products (AGEs), which are proteins and lipids in foods that are often damaged by high temperature cooking.

The second group was required to eat food cooked at low temperatures (stewed, steamed or poached) and avoid food that was fried, baked or grilled.

In the group avoiding food cooked at a dry heat or high temperatures (low-AGE diet), insulin resistance significantly improved, and body weight was mildly reduced.

The high-AGE group’s markers of insulin resistance, on the other hand, were at higher levels compared to baseline.

Head researcher Helen Vlassara, MD, remarked:

“While food AGEs are prevalent, particularly in Western diets, our study showed that avoiding foods high in AGEs could actually reverse the damage that had been done. This can provide us with new clinical approaches to prediabetes, potentially helping protect certain at-risk individuals from developing full diabetes and its devastating consequences.”

Life Extension first warned about the dangers of eating foods cooked at high temperature in the May 2003 issue of this magazine.

Luteolin

Luteolin is a flavonoid found abundantly in many plants. Since one of the main consequences of glycation is inflammation, luteolin’s anti-inflammatory properties make it an ideal natural complement to benfotiamine and pyridoxal 5’-phosphate. Inflammation is widely recognized for its association with cancer, atherosclerosis, and virtually all other chronic diseases.31

Luteolin works by suppressing the activation of the master inflammatory complex called NF-kB, which triggers the production of a wide variety of pro-inflammatory signaling molecules (cytokines).

The anti-inflammatory actions of luteolin have been demonstrated in tissues throughout the body, including the brain, blood vessel lining, skin, intestines, lungs, gums, and bone.32-39

A study published in the American Journal of Respiratory and Critical Care Medicine gives us insight into how monumental luteolin’s anti-inflammatory impact truly is. When mice were exposed to a bacterial toxin, only 4.1% of them survived. But when mice that were given luteolin were exposed to the same toxin, it promoted survival in 48% of the mice.40

Carnosine

Carnosine is a potent free-radical scavenger and anti-glycating agent that inhibits AGE formation and its cross-linked proteins, helping to keep them functioning properly.41-44

Carnosine has powerful lipid glycation-preventing properties and profound impacts on fundamental AGE-signaling pathways, making it a highly promising anti-aging drug candidate.45

Studies show that carnosine prevents protein cross-linking and the accumulation of the tangled protein clumps associated with Alzheimer’s disease.46,47

Carnosine has also been shown to lower blood-lipid levels, reduce the metabolic stress induced by high-fat diets, and, very importantly, to help stabilize atherosclerotic plaques, reducing their risk of rupturing and triggering a heart attack or stroke.15,48

Finally, carnosine works in numerous ways to help protect mitochondria from the destructive effects of cellular oxidative stresses.43

Nutrients that Enhance Mitochondrial Function

As we discussed earlier, preventing glycation is one piece of the puzzle. It is equally important to preserve mitochondrial function in the face of glycation-induced damage. Three unique compounds have been identified in the scientific literature that can lend new life to aging mitochondria.

Pyrroloquinoline quinone (PQQ)

Pyrroloquinoline quinone (PQQ) is a vitamin-like molecule that promotes the production of new mitochondria in cells, helping to restore cellular energy.6,49 The result of insufficient cellular PQQ is reduced numbers of mitochondria.49

In a clever experiment, researchers treated animals with a toxic chemical that induces Parkinson’s disease-like symptoms. They then fed the rats a probiotic made of bacteria that had been engineered to produce PQQ.6

Initially, the chemically-treated rats lost mitochondria and showed obvious evidence of oxidant damage in their organs. But after receiving the PQQ-supplying probiotic, those changes were reversed, new mitochondria formed, and the animals recovered from severe metabolic damage.

R-Lipoic Acid

R-lipoic acid is essential to enzyme systems involved in extracting energy from food.50,51 This makes it vital for efficient mitochondrial function.

Studies show that giving older animals R-lipoic acid leads to improved metabolic function, healthier mitochondria, and reduced production of oxidative stress-inducing byproducts.

In addition, animals supplemented with R-lipoic acid age more slowly than they otherwise would. This is because R-lipoic acid also protects liver, heart, and brain cells from mitochondria-induced oxidative stress.52-58

Due to these abilities, R-lipoic acid is emerging as a popular anti-aging supplement.

Taurine

Taurine is an amino acid that has been found in extremely high concentrations inside mitochondria, where it regulates the enzymes responsible for harvesting energy from food molecules.59

Because of this important function, taurine is found most abundantly in heart and skeletal muscle, brain tissues, and the retina—all of which have extremely high metabolic rates that burn out mitochondria.60-63

Insufficient taurine in these tissues produces an energy crisis that results in accelerated aging.64,65 The good news is that adding taurine back to such cells in crisis can reduce oxidative stress and maintain – and often restore – mitochondrial function in aging cells.62,63,66

Indeed, taurine is one of the few nutrients capable of spurring brain cells to put out new shoots, called neurites, enhancing brain cell connections that preserve cognition and memory.67

Summary

Glycation  

Glycation of our body’s tissues is a normal consequence of aging. Those with poor blood sugar control suffer more glycation reactions and prematurely age.

Ultimately, glycation and mitochondrial dysfunction together produce ever-faster aging.

Fortunately, scientists have uncovered several nutrients that function to support healthy mitochondrial function while reducing glycation and its damaging effects.

These nutrients work together to rejuvenate cell energy levels while reducing tissue damage.

If you have any questions on the scientific content of this article, please call a Life Extension® Wellness Specialist at 1-866-864-3027.

References

  1. Semba RD, Nicklett EJ, Ferrucci L. Does accumulation of advanced glycation end products contribute to the aging phenotype? J Gerontol A Biol Sci Med Sci. 2010;65(9):963-75.
  2. Yim MB, Yim HS, Lee C, et al. Protein glycation: creation of catalytic sites for free radical generation. Ann N Y Acad Sci. 2001;928:48-53.
  3. Krone CA, Ely JT. Ascorbic acid, glycation, glycohemoglobin and aging. Med Hypotheses. 2004;62(2):275-9.
  4. Ward MS, Fortheringham AK, Cooper ME, et al. Targeting advanced glycation endproducts and mitochondrial dysfunction in cardiovascular disease. Curr Opin Pharmacol. 2013;13(4):654-61.
  5. Hipkiss AR. Mitochondrial dysfunction, proteotoxicity, and aging: causes or effects, and the possible impact of NAD+-controlled protein glycation. Adv Clin Chem. 2010;50:123-50.
  6. Singh AK, Pandey SK, Saha G, et al. Pyrroloquinoline quinone (PQQ) producing Escherichia coli Nissle 1917 (EcN) alleviates age associated oxidative stress and hyperlipidemia, and improves mitochondrial function in ageing rats. Exp Gerontol. 2015;66:1-9.
  7. Fukami K, Yamagishi S, Ueda S, et al. Role of AGEs in diabetic nephropathy. Curr Pharm Des. 2008;14(10):946-52.
  8. Kikuchi S, Shinpo K, Takeuchi M, et al. Glycation--a sweet tempter for neuronal death. Brain Res Brain Res Rev. 2003;41(2-3):306-23.
  9. Hipkiss AR. Aging risk factors and Parkinson’s disease: contrasting roles of common dietary constituents. Neurobiol Aging. 2014;35(6):1469-72.
  10. Wondrak GT, Roberts MJ, Jacobson MK, et al. Photosensitized growth inhibition of cultured human skin cells: mechanism and suppression of oxidative stress from solar irradiation of glycated proteins. J Invest Dermatol. 2002;119(2):489-98.
  11. Verzijl N, DeGroot J, Ben ZC, et al. Crosslinking by advanced glycation end products increases the stiffness of the collagen network in human articular cartilage: a possible mechanism through which age is a risk factor for osteoarthritis. Arthritis Rheum. 2002;46(1):114-23.
  12. Tsuru M, Nagata K, Jimi A, et al. Effect of AGEs on human disc herniation: intervertebral disc hernia is also effected by AGEs. Kurume Med J. 2002;49(1-2):7-13.
  13. Burd J, Lum S, Cahn F, et al. Simultaneous noninvasive clinical measurement of lens autofluorescence and rayleigh scattering using a fluorescence biomicroscope. J Diabetes Sci Technol. 2012;6(6):1251-9.
  14. Kessel L, Hougaard JL, Sander B, et al. Lens ageing as an indicator of tissue damage associated with smoking and non-enzymatic glycation--a twin study. Diabetologia. 2002;45(10):1457-62.
  15. Brown BE, Kim CH, Torpy FR, et al. Supplementation with carnosine decreases plasma triglycerides and modulates atherosclerotic plaque composition in diabetic apo E(-/-) mice. Atherosclerosis. 2014;232(2):403-9.
  16. Pomero F, Molinar Min A, La Selva M, et al. Benfotiamine is similar to thiamine in correcting endothelial cell defects induced by high glucose. Acta Diabetol. 2001;38(3):135-8.
  17. Schmid U, Stopper H, Heidland A, et al. Benfotiamine exhibits direct antioxidative capacity and prevents induction of DNA damage in vitro. Diabetes Metab Res Rev. 2008;24(5):371-7.
  18. Stirban A, Negrean M, Stratmann B, et al. Benfotiamine prevents macro-and microvascular endothelial dysfunction and oxidative stress following a meal rich in advanced glycation end products in individuals with type 2 diabetes. Diabetes Care. 2006;29(9):2064-71.
  19. Katare RG, Caporali A, Oikawa A, et al. Vitamin B1 analog benfotiamine prevents diabetes-induced diastolic dysfunction and heart failure through Akt/Pim-1-mediated survival pathway. Circ Heart Fail. 2010;3(2):294-305.
  20. Fraser DA, Hessvik NP, Nikolic N, et al. Benfotiamine increases glucose oxidation and downregulates NADPH oxidase 4 expression in cultured human myotubes exposed to both normal and high glucose concentrations. Genes Nutr. 2012;7(3):459-69.
  21. Tarallo S, Beltramo E, Berrone E, et al. Human pericyte-endothelial cell interactions in co-culture models mimicking the diabetic retinal microvascular environment. Acta Diabetol. 2012;49 Suppl 1:S141-51.
  22. Kihm LP, Muller-Krebs S, Klein J, et al. Benfotiamine protects against peritoneal and kidney damage in peritoneal dialysis. J Am Soc Nephrol. 2011;22(5):914-26.
  23. Balakumar P, Rohilla A, Krishan P, et al. The multifaceted therapeutic potential of benfotiamine. Pharmacol Res. 2010;61(6):482-8.
  24. Hammes HP, Du X, Edelstein D, et al. Benfotiamine blocks three major pathways of hyperglycemic damage and prevents experimental diabetic retinopathy. Nat Med. 2003;9(3):294-9.
  25. Nakamura S, Niwa T. Pyridoxal phosphate and hepatocyte growth factor prevent dialysate-induced peritoneal damage. J Am Soc Nephrol. 2005;16(1):144-50.
  26. Lehman TD, Ortwerth BJ. Inhibitors of advanced glycation end product-associated protein cross-linking. Biochim Biophys Acta. 2001;1535(2):110-9.
  27. Khatami M, Suldan Z, David I, et al. Inhibitory effects of pyridoxal phosphate, ascorbate and aminoguanidine on nonenzymatic glycosylation. Life Sci. 1988;43(21):1725-31.
  28. Miyazawa T, Nakagawa K, Shimasaki S, et al. Lipid glycation and protein glycation in diabetes and atherosclerosis. Amino Acids. 2012;42(4):1163-70.
  29. Nakagawa K, Ibusuki D, Yamashita S, et al. Glycation of plasma lipoprotein lipid membrane and screening for lipid glycation inhibitor. Ann N Y Acad Sci. 2008;1126:288-90.
  30. Suzuki K, Nakagawa K, Miyazawa T. Augmentation of blood lipid glycation and lipid oxidation in diabetic patients. Clin Chem Lab Med. 2014;52(1):47-52.
  31. Harris GK, Qian Y, Leonard SS, et al. Luteolin and chrysin differentially inhibit cyclooxygenase-2 expression and scavenge reactive oxygen species but similarly inhibit prostaglandin-E2 formation in RAW 264.7 cells. J Nutr. 2006;136(6):1517-21.
  32. Deqiu Z, Kang L, Jiali Y, et al. Luteolin inhibits inflammatory response and improves insulin sensitivity in the endothelium. Biochimie. 2011;93(3):506-12.
  33. Kim JE, Son JE, Jang YJ, et al. Luteolin, a novel natural inhibitor of tumor progression locus 2 serine/threonine kinase, inhibits tumor necrosis factor-alpha-induced cyclooxygenase-2 expression in JB6 mouse epidermis cells. J Pharmacol Exp Ther. 2011;338(3):1013-22.
  34. Rezai-Zadeh K, Ehrhart J, Bai Y, et al. Apigenin and luteolin modulate microglial activation via inhibition of STAT1-induced CD40 expression. J Neuroinflammation. 2008;5:41.
  35. Chen CY, Peng WH, Tsai KD, et al. Luteolin suppresses inflammation-associated gene expression by blocking NF-kappaB and AP-1 activation pathway in mouse alveolar macrophages. Life Sci. 2007;81(23-24):1602-14.
  36. Zhu LH, Bi W, Qi RB, et al. Luteolin inhibits microglial inflammation and improves neuron survival against inflammation. Int J Neurosci. 2011;121(6):329-36.
  37. Gutierrez-Venegas G, Kawasaki-Cardenas P, Arroyo-Cruz SR, et al. Luteolin inhibits lipopolysaccharide actions on human gingival fibroblasts. Eur J Pharmacol. 2006;541(1-2):95-105.
  38. Chen HQ, Jin ZY, Wang XJ, et al. Luteolin protects dopaminergic neurons from inflammation-induced injury through inhibition of microglial activation. Neurosci Lett. 2008;448(2):175-9.
  39. Kim JS, Jobin C. The flavonoid luteolin prevents lipopolysaccharide-induced NF-kappaB signalling and gene expression by blocking IkappaB kinase activity in intestinal epithelial cells and bone-marrow derived dendritic cells. Immunology. 2005;115(3):375-87.
  40. Kotanidou A, Xagorari A, Bagli E, et al. Luteolin reduces lipopolysaccharide-induced lethal toxicity and expression of proinflammatory molecules in mice. Am J Respir Crit Care Med. 2002;165(6): 818-23.
  41. Reddy VP, Garrett MR, Perry G, et al. Carnosine: a versatile antioxidant and antiglycating agent. Sci Aging Knowledge Environ. 2005;2005(18):pe12.
  42. Hipkiss AR. Would carnosine or a carnivorous diet help suppress aging and associated pathologies? Ann N Y Acad Sci. 2006;1067:369-74.
  43. Cheng J, Wang F, Yu DF, et al. The cytotoxic mechanism of malondialdehyde and protective effect of carnosine via protein cross-linking/mitochondrial dysfunction/reactive oxygen species/MAPK pathway in neurons. Eur J Pharmacol. 2011;650(1):184-94.
  44. Baye E, Ukropcova B, Ukropec J, et al. Physiological and therapeutic effects of carnosine on cardiometabolic risk and disease. Amino Acids. 2016;48(5):1131-49.
  45. Hipkiss AR, Baye E, de Courten B. Carnosine and the processes of ageing. Maturitas. 2016;93:28-33.
  46. Hipkiss AR. Could carnosine or related structures suppress Alzheimer’s disease? J Alzheimers Dis. 2007;11(2):229-40.
  47. Babizhayev MA, Deyev AI, Yegorov YE. Olfactory dysfunction and cognitive impairment in age-related neurodegeneration: prevalence related to patient selection, diagnostic criteria and therapeutic treatment of aged clients receiving clinical neurology and community-based care. Curr Clin Pharmacol. 2011;6(4):236-59.
  48. Stegen S, Stegen B, Aldini G, et al. Plasma carnosine, but not muscle carnosine, attenuates high-fat diet-induced metabolic stress. Appl Physiol Nutr Metab. 2015;40(9):868-76.
  49. Chowanadisai W, Bauerly KA, Tchaparian E, et al. Pyrroloquinoline quinone stimulates mitochondrial biogenesis through cAMP response element-binding protein phosphorylation and increased PGC-1alpha expression. J Biol Chem. 2010;285(1):142-52.
  50. Goraca A, Huk-Kolega H, Piechota A, et al. Lipoic acid - biological activity and therapeutic potential. Pharmacol Rep. 2011;63(4): 849-58.
  51. Morikawa T, Yasuno R, Wada H. Do mammalian cells synthesize lipoic acid? Identification of a mouse cDNA encoding a lipoic acid synthase located in mitochondria. FEBS Lett. 2001;498(1):16-21.
  52. Jiang T, Yin F, Yao J, et al. Lipoic acid restores age-associated impairment of brain energy metabolism through the modulation of Akt/JNK signaling and PGC1alpha transcriptional pathway. Aging Cell. 2013;12(6):1021-31.
  53. Suh JH, Moreau R, Heath SH, et al. Dietary supplementation with (R)-alpha-lipoic acid reverses the age-related accumulation of iron and depletion of antioxidants in the rat cerebral cortex. Redox Rep. 2005;10(1):52-60.
  54. Suh JH, Wang H, Liu RM, et al. (R)-alpha-lipoic acid reverses the age-related loss in GSH redox status in post-mitotic tissues: evidence for increased cysteine requirement for GSH synthesis. Arch Biochem Biophys. 2004;423(1):126-35.
  55. Suh JH, Shigeno ET, Morrow JD, et al. Oxidative stress in the aging rat heart is reversed by dietary supplementation with (R)-(alpha)-lipoic acid. FASEB J. 2001;15(3):700-6.
  56. Hagen TM, Vinarsky V, Wehr CM, et al. (R)-alpha-lipoic acid reverses the age-associated increase in susceptibility of hepatocytes to tert-butylhydroperoxide both in vitro and in vivo. Antioxid Redox Signal. 2000;2(3):473-83.
  57. Hagen TM, Ingersoll RT, Lykkesfeldt J, et al. (R)-alpha-lipoic acid-supplemented old rats have improved mitochondrial function, decreased oxidative damage, and increased metabolic rate. FASEB J. 1999;13(2):411-8.
  58. Liu J, Head E, Gharib AM, et al. Memory loss in old rats is associated with brain mitochondrial decay and RNA/DNA oxidation: partial reversal by feeding acetyl-L-carnitine and/or R-alpha -lipoic acid. Proc Natl Acad Sci U S A. 2002;99(4):2356-61.
  59. Hansen SH, Birkedal H, Wibrand F, et al. Taurine and regulation of mitochondrial metabolism. Adv Exp Med Biol. 2015;803:397-405.
  60. Ripps H, Shen W. Review: taurine: a “very essential” amino acid. Mol Vis. 2012;18:2673-86.
  61. Froger N, Moutsimilli L, Cadetti L, et al. Taurine: the comeback of a neutraceutical in the prevention of retinal degenerations. Prog Retin Eye Res. 2014;41:44-63.
  62. De Luca A, Pierno S, Camerino DC. Taurine: the appeal of a safe amino acid for skeletal muscle disorders. J Transl Med. 2015;13:243.
  63. Ramila KC, Jong CJ, Pastukh V, et al. Role of protein phosphorylation in excitation-contraction coupling in taurine deficient hearts. Am J Physiol Heart Circ Physiol. 2015;308(3):H232-9.
  64. Gebara E, Udry F, Sultan S, et al. Taurine increases hippocampal neurogenesis in aging mice. Stem Cell Res. 2015;14(3):369-79.
  65. Militante J, Lombardini JB. Age-related retinal degeneration in animal models of aging: possible involvement of taurine deficiency and oxidative stress. Neurochem Res. 2004;29(1):151-60.
  66. Xu S, He M, Zhong M, et al. The neuroprotective effects of taurine against nickel by reducing oxidative stress and maintaining mitochondrial function in cortical neurons. Neurosci Lett. 2015;590: 52-7.
  67. Chou CT, Lin HT, Hwang PA, et al. Taurine resumed neuronal differentiation in arsenite-treated N2a cells through reducing oxidative stress, endoplasmic reticulum stress, and mitochondrial dysfunction. Amino Acids. 2015;47(4):735-44.
  68. Vlassara H, Cai W, Tripp E, et al. Oral AGE restriction ameliorates insulin resistance in obese individuals with the metabolic syndrome: a randomised controlled trial. Diabetologia. 2016;59(10):2181-92.