Riboflavin

October 3, 2020

Overview

Riboflavin is a B vitamin. It is involved in many processes in the body and is necessary for normal cell growth and function. It can be found in certain foods such as milk, meat, eggs, nuts, enriched flour, and green vegetables. Riboflavin is frequently used in combination with other B vitamins in vitamin B complex products.

Some people take riboflavin by mouth to prevent low levels of riboflavin (riboflavin deficiency) in the body, for various types of cancer, and for migraine headaches. It is also taken by mouth for acne, muscle cramps, burning feet syndrome, carpal tunnel syndrome, and blood disorders such as congenital methemoglobinemia and red blood cell aplasia. Some people use riboflavin for eye conditions including eye fatigue, cataracts, and glaucoma.

Some people also take riboflavin by mouth to maintain healthy hair, skin, and nails, to slow aging, for canker sores, multiple sclerosis, memory loss including Alzheimer's disease, high blood pressure, burns, liver disease, and sickle cell anemia.

Classification

Is a Form of:

B vitamin

Primary Functions:

Prevent low levels of riboflavin

Also Known As:

B Complex Vitamin, Complexe de Vitamines B, Flavin

How Does It Work?

Riboflavin is required for the proper development of many things in the body including the skin, lining of the digestive tract, blood cells, and brain function.

Uses

Preventing and treating low riboflavin levels (riboflavin deficiency).In adults and children who have too little riboflavin in their body, taking riboflavin by mouth can increase levels of riboflavin in the body.

Cataracts.People who eat more riboflavin as part of their diet seem to have a lower risk of developing cataracts. Also, taking supplements containing riboflavin plus niacin seems to help prevent cataracts.
High amounts of homocysteine in the blood (hyperhomocysteinemia). Taking riboflavin by mouth for 12 weeks decreases levels of homocysteine by up to 40% in some people. Also, taking riboflavin along with folic acid and pyridoxine seems to lower homocysteine levels by 26% in people with high homocysteine levels caused by drugs that are used to prevent seizures.
Migraine headaches. Taking high-dose riboflavin by mouth seems to reduce the number of migraine headache attacks, by about 2 attacks per month. Taking riboflavin in combination with other vitamin sand minerals seems to also reduce the amount of pain experienced during a migraine.

Recommended Dosing

The following doses have been studied in scientific research:

ADULTS

BY MOUTH:

General: The recommended dietary allowance (RDA) of riboflavin for adults is 1.3 mg per day for males, 1.1 mg per day for women, 1.4 mg per day for pregnant females, and 1.6 mg per day for lactating women. There is no daily Upper Intake Levels (UL) for riboflavin, which is the highest level of intake that is likely to pose no risk of adverse effects.
For preventing and treating low levels of riboflavin (riboflavin deficiency): Riboflavin 5-30 mg daily has been used.
For cataracts: A combination of riboflavin 3 mg plus niacin 40 mg daily for 5-6 years has been used.
For high levels of homocysteine in the blood): Riboflavin 1.6 mg daily for 12 weeks has been used. A combination containing 75 mg of riboflavin, 0.4 mg of folic acid, and 120 mg of pyridoxine daily for 30 days has also been used.
For migraine headaches: The most common dose is riboflavin 400 mg daily for at least three months. A specific product (Dolovent; Linpharma Inc., Oldsmar, FL ) dosed at two capsules in morning and two capsules in the evening for 3 months has also been used. This dose provides a total of riboflavin 400 mg, magnesium 600 mg, and coenzyme Q10 150 mg per day.

CHILDREN

BY MOUTH:

General: The recommended dietary allowance (RDA) of riboflavin is 0.3 mg per day for infants up to 6 months old, 0.4 mg per day for infants 6-12 months old, 0.5 mg per day for children 1-3 years old, 0.6 mg per day for children 4-8 years old, 0.9 mg per day for children 9-13 years old, 1.3 mg per day for males 14-18 years old, and 1.0 mg per day for females 14-18. There is no daily Upper Intake Levels (UL) for riboflavin, which is the highest level of intake that is likely to pose no risk of adverse effects.
For preventing and treating low levels of riboflavin (riboflavin deficiency): Riboflavin 2 mg once, then 0.5-1.5 mg daily for 14 days has been used. Riboflavin 2-5 mg daily for up to two months has been used. Riboflavin 5 mg five days per week for up to one year has also been used.

Riboflavin Supplements Frequently Asked Questions

Is too much riboflavin bad for you?

The primary risk of excess B-2 is damage to the liver. However, excess riboflavin, or riboflavin toxicity, is rare. You could get too much vitamin B-2 through supplements in oral or injection form, but this is also rare because your body doesn't store the vitamin.

What is b2 riboflavin needed for?

Vitamin B2 helps break down proteins, fats, and carbohydrates. It plays a vital role in maintaining the body's energy supply. Riboflavin helps convert carbohydrates into adenosine triphosphate (ATP). The human body produces ATP from food, and ATP produces energy as the body requires it.

When should I take riboflavin?

Riboflavin is best absorbed when taken between meals. People who do not eat a balanced diet every day may benefit from taking a multivitamin and mineral complex.

Is riboflavin and b2 the same thing?

Riboflavin (also known as vitamin B2) is one of the B vitamins, which are all water soluble. Riboflavin is naturally present in some foods, added to some food products, and available as a dietary supplement.

What are the side effects of riboflavin?

Riboflavin is LIKELY SAFE for most people when taken by mouth. In some people, riboflavin can cause the urine to turn a yellow-orange color. When taken in high doses, riboflavin might cause diarrhea, an increase in urine, and other side effects.

What are the benefits of taking riboflavin?

Benefits. Riboflavin is a vitamin that is needed for growth and overall good health. It helps the body break down carbohydrates, proteins and fats to produce energy, and it allows oxygen to be used by the body.

How long does vitamin b2 take to work?

For treating low levels of riboflavin (riboflavin deficiency) in adults: 5-30 mg of riboflavin (Vitamin B2) daily in divided doses. For preventing migraine headaches: 400 mg of riboflavin (Vitamin B2) per day. It may take up to three months to get best results.

What are the signs of a riboflavin deficiency?

The signs and symptoms of riboflavin deficiency (also known as ariboflavinosis) include skin disorders, hyperemia (excess blood) and edema of the mouth and throat, angular stomatitis (lesions at the corners of the mouth), cheilosis (swollen, cracked lips), hair loss, reproductive problems, sore throat, itchy and red

What is the main function of riboflavin?

Can Vegans eat riboflavin?

Why It's Important: Riboflavin is involved in healthy growth of your skin, hair, eyes and liver. Many good sources of riboflavin are animal products like dairy, eggs, fish and meat. Therefore, vegans should make sure they are consuming at least a couple of good plant-based sources of riboflavin each day.

Is 20 mg of riboflavin too much?

There is no daily Upper Intake Levels (UL) for riboflavin, which is the highest level of intake that is likely to pose no risk of adverse effects. For preventing and treating low levels of riboflavin (riboflavin deficiency): Riboflavin 5-30 mg daily has been used.

Can you take riboflavin and magnesium together?

You have to take magnesium for three months to get a benefit, says DeRossett. "People sometimes give up on it too soon." Taking the correct dosage is important as well: 500 mg magnesium, 400 mg riboflavin (vitamin B-2), and 150 mg coenzyme Q10. The herb butterbur can also help prevent migraine attacks, she adds.

Can riboflavin upset your stomach?

While any supplement taken into the stomach can cause nausea, riboflavin is well known for this. Thus, medical care providers often recommend a lower dose at first, which is increased over time. However, riboflavin is water-soluble and excessive amounts are excreted by the kidneys, so toxicity is unlikely.

Does riboflavin make you tired?

Severe, long-term riboflavin deficiency causes a shortage of red blood cells (anemia), which makes you feel weak and tired. It also causes clouding of the lens in your eyes (cataracts), which affects your vision.

Does riboflavin make your pee yellow?

What's happening is that urine will turn a bright, sometimes neon, yellow in response to excess riboflavin. Riboflavin, also known as vitamin B2, is a common ingredient in almost all multi-vitamins.

Is Vitamin b2 good for skin?

Vitamin B2

Riboflavin is an important vitamin for those prone to acne as it helps to maintain the mucus secretion of the skin to prevent acne breakouts and dry skin. Vitamin B2 can even help to clear up pesky spots and revitalize the skin by promoting healthy cell turnover.

How do you prevent riboflavin deficiency?

The RDA for riboflavin (1.3 mg/day for men and 1.1 mg/day for women), which should prevent deficiency in most individuals, is easily met by eating a varied diet. Consuming a varied diet should supply 1.5 mg to 2 mg of riboflavin a day.

How much riboflavin will cause a false positive?

The authors found that the accuracy of discrimination increased with riboflavin dose, and reached 100% with measurement 2 to 8 hours after a 50 mg dose, although there was an average 21.2% false positive rate.

How much riboflavin should I take for migraines?

A combination containing 75 mg of riboflavin, 0.4 mg of folic acid, and 120 mg of pyridoxine daily for 30 days has also been used. For migraine headaches: The most common dose is riboflavin 400 mg daily for at least three months.

Can riboflavin cause dizziness?

A very serious allergic reaction to this vitamin is rare. However, get medical help right away if you notice any symptoms of a serious allergic reaction, including: rash, itching/swelling (especially of the face/tongue/throat), severe dizziness, trouble breathing.

Clinical Studies

^ a b Nebbioso M1, et al. Treatment of glaucomatous patients by means of food supplement to reduce the ocular discomfort: a double blind randomized trial. Eur Rev Med Pharmacol Sci. (2013)
^ a b Northrop-Clewes CA, Thurnham DI. The discovery and characterization of riboflavin. Ann Nutr Metab. (2012)
^ a b Sheraz MA, et al. Photo, thermal and chemical degradation of riboflavin. Beilstein J Org Chem. (2014)
^ Astanov S, et al. Spectroscopic study of photo and thermal destruction of riboflavin. J Mol Struct. (2014)
^ Sue-Chu M, Kristensen S, Tønnesen HH. Influence of lag-time between light exposure and color evaluation of riboflavin in the solid state. Pharmazie. (2008)
^ a b Sue-Chu M, Kristensen S, Tønnesen HH. Photoinduced color changes in two different qualities of riboflavin in the solid state and in various tablet formulations photoreactivity of biologically active compounds. XX. Pharmazie. (2009)
^ a b Habib MJ, Asker AF. Photostabilization of riboflavin by incorporation into liposomes. J Parenter Sci Technol. (1991)
^ Loukas YL. A Plackett-Burnam screening design directs the efficient formulation of multicomponent DRV liposomes. J Pharm Biomed Anal. (2001)
^ a b Lienhart WD, Gudipati V, Macheroux P. The human flavoproteome. Arch Biochem Biophys. (2013)
^ a b McCormick DB. Two interconnected B vitamins: riboflavin and pyridoxine. Physiol Rev. (1989)
^ Tu BP, Weissman JS. Oxidative protein folding in eukaryotes: mechanisms and consequences. J Cell Biol. (2004)
^ a b c d e Dietary Reference Intakes for Thiamin, Riboflavin, Niacin, Vitamin B6, Folate, Vitamin B12, Pantothenic Acid, Biotin, and Choline.
^ Kodentsova VM, Vrzhesinskaya OA. Evaluation of the vitamin status in nursing women by vitamin content in breast milk. Bull Exp Biol Med. (2006)
^ Allen LH. B vitamins in breast milk: relative importance of maternal status and intake, and effects on infant status and function. Adv Nutr. (2012)
^ a b Blumberg JB, et al. Contribution of Dietary Supplements to Nutritional Adequacy by Socioeconomic Subgroups in Adults of the United States. Nutrients. (2017)
^ Hoey L, McNulty H, Strain JJ. Studies of biomarker responses to intervention with riboflavin: a systematic review. Am J Clin Nutr. (2009)
^ Prentice AM, et al. The influence of G-6-PD activity on the response of erythrocyte glutathione reductase to riboflavin deficiency. Int J Vitam Nutr Res. (1981)
^ Madigan SM, et al. Riboflavin and vitamin B-6 intakes and status and biochemical response to riboflavin supplementation in free-living elderly people. Am J Clin Nutr. (1998)
^ a b c d Powers HJ, et al. Correcting a marginal riboflavin deficiency improves hematologic status in young women in the United Kingdom (RIBOFEM). Am J Clin Nutr. (2011)
^ a b c McKinley MC, et al. Effect of riboflavin supplementation on plasma homocysteine in elderly people with low riboflavin status. Eur J Clin Nutr. (2002)
^ Bailey AL, et al. Relationships between micronutrient intake and biochemical indicators of nutrient adequacy in a "free-living' elderly UK population. Br J Nutr. (1997)
^ a b c Gariballa S, Forster S, Powers H. Riboflavin status in acutely ill patients and response to dietary supplements. JPEN J Parenter Enteral Nutr. (2009)
^ a b Dietary Reference Intakes for Thiamin, Riboflavin, Niacin, Vitamin B6, Folate, Vitamin B12, Pantothenic Acid, Biotin, and Choline.
^ Merrill AH Jr, et al. Formation and mode of action of flavoproteins. Annu Rev Nutr. (1981)
^ Akiyama T, Selhub J, Rosenberg IH. FMN phosphatase and FAD pyrophosphatase in rat intestinal brush borders: role in intestinal absorption of dietary riboflavin. J Nutr. (1982)
^ Daniel H, Binninger E, Rehner G. Hydrolysis of FMN and FAD by alkaline phosphatase of the intestinal brush-border membrane. Int J Vitam Nutr Res. (1983)
^ a b Yonezawa A1, Inui K. Novel riboflavin transporter family RFVT/SLC52: identification, nomenclature, functional characterization and genetic diseases of RFVT/SLC52. Mol Aspects Med. (2013)
^ Sabui S1, Ghosal A1, Said HM2. Identification and characterization of 5'-flanking region of the human riboflavin transporter 1 gene (SLC52A1). Gene. (2014)
^ Yao Y1, et al. Involvement of riboflavin transporter RFVT2/Slc52a2 in hepatic homeostasis of riboflavin in mice. Eur J Pharmacol. (2013)
^ Ghosal A1, Sabui S1, Said HM2. Identification and characterization of the minimal 5'-regulatory region of the human riboflavin transporter -3 (SLC52A3) in intestinal epithelial cells. Am J Physiol Cell Physiol. (2014)
^ a b Yoshimatsu H1, et al. Functional involvement of RFVT3/SLC52A3 in intestinal riboflavin absorption. Am J Physiol Gastrointest Liver Physiol. (2014)
^ a b c Jusko WJ, Levy G. Absorption, metabolism, and excretion of riboflavin-5'-phosphate in man. J Pharm Sci. (1967)
^ Dainty JR1, et al. Quantification of the bioavailability of riboflavin from foods by use of stable-isotope labels and kinetic modeling. Am J Clin Nutr. (2007)
^ Zempleni J1, Galloway JR, McCormick DB. Pharmacokinetics of orally and intravenously administered riboflavin in healthy humans. Am J Clin Nutr. (1996)
^ Zielińska-Dawidziak M1, et al. Transport of high concentration of thiamin, riboflavin and pyridoxine across intestinal epithelial cells Caco-2. J Nutr Sci Vitaminol (Tokyo). (2008)
^ a b Yuasa H1, et al. Carrier-mediated transport of riboflavin in the rat colon. Biopharm Drug Dispos. (2000)
^ Tomei S1, et al. Transport functions of riboflavin carriers in the rat small intestine and colon: site difference and effects of tricyclic-type drugs. Drug Deliv. (2001)
^ IINUMA S. Synthesis of riboflavin by intestinal bacteria. J Vitaminol (Kyoto). (1955)
^ Hill MJ. Intestinal flora and endogenous vitamin synthesis. Eur J Cancer Prev. (1997)
^ LeBlanc JG1, et al. Bacteria as vitamin suppliers to their host: a gut microbiota perspective. Curr Opin Biotechnol. (2013)
^ a b c Subramanian VS1, et al. Chronic alcohol feeding inhibits physiological and molecular parameters of intestinal and renal riboflavin transport. Am J Physiol Cell Physiol. (2013)
^ a b c Colombo B1, Saraceno L, Comi G. Riboflavin and migraine: the bridge over troubled mitochondria. Neurol Sci. (2014)
^ Barbiroli B1, et al. Complicated migraine studied by phosphorus magnetic resonance spectroscopy. Cephalalgia. (1990)
^ Sacquegna T1, et al. Brain energy metabolism studied by 31P-MR spectroscopy in a case of migraine with prolonged aura. Acta Neurol Scand. (1992)
^ Welch KM1, et al. Preliminary observations on brain energy metabolism in migraine studied by in vivo phosphorus 31 NMR spectroscopy. Neurology. (1989)
^ Barbiroli B1, et al. Abnormal brain and muscle energy metabolism shown by 31P magnetic resonance spectroscopy in patients affected by migraine with aura. Neurology. (1992)
^ Montagna P1, et al. 31P-magnetic resonance spectroscopy in migraine without aura. Neurology. (1994)
^ a b Penn AM1, et al. MELAS syndrome with mitochondrial tRNA(Leu)(UUR) mutation: correlation of clinical state, nerve conduction, and muscle 31P magnetic resonance spectroscopy during treatment with nicotinamide and riboflavin. Neurology. (1992)
^ a b Boehnke C1, et al. High-dose riboflavin treatment is efficacious in migraine prophylaxis: an open study in a tertiary care centre. Eur J Neurol. (2004)
^ Schoenen J1, Jacquy J, Lenaerts M. Effectiveness of high-dose riboflavin in migraine prophylaxis. A randomized controlled trial. Neurology. (1998)
^ a b Condò M1, et al. Riboflavin prophylaxis in pediatric and adolescent migraine. J Headache Pain. (2009)
^ a b Di Lorenzo C1, et al. Mitochondrial DNA haplogroups influence the therapeutic response to riboflavin in migraineurs. Neurology. (2009)
^ a b Maizels M1, Blumenfeld A, Burchette R. A combination of riboflavin, magnesium, and feverfew for migraine prophylaxis: a randomized trial. Headache. (2004)
^ MacLennan SC1, et al. High-dose riboflavin for migraine prophylaxis in children: a double-blind, randomized, placebo-controlled trial. J Child Neurol. (2008)
^ Bruijn J1, et al. Medium-dose riboflavin as a prophylactic agent in children with migraine: a preliminary placebo-controlled, randomised, double-blind, cross-over trial. Cephalalgia. (2010)
^ Buzina R, et al. Nutritional status and physical working capacity. Hum Nutr Clin Nutr. (1982)
^ a b Ajayi OA1, Okike OC, Yusuf Y. Haematological response to supplements of riboflavin and ascorbic acid in Nigerian young adults. Eur J Haematol. (1990)
^ Powers HJ, et al. The relative effectiveness of iron and iron with riboflavin in correcting a microcytic anaemia in men and children in rural Gambia. Hum Nutr Clin Nutr. (1983)
^ Powers HJ, Bates CJ, Lamb WH. Haematological response to supplements of iron and riboflavin to pregnant and lactating women in rural Gambia. Hum Nutr Clin Nutr. (1985)
^ a b Fairweather-Tait SJ1, et al. Riboflavin deficiency and iron absorption in adult Gambian men. Ann Nutr Metab. (1992)
^ a b Tavares NR1, Moreira PA, Amaral TF. Riboflavin supplementation and biomarkers of cardiovascular disease in the elderly. J Nutr Health Aging. (2009)
^ Humphrey LL1, et al. Homocysteine level and coronary heart disease incidence: a systematic review and meta-analysis. Mayo Clin Proc. (2008)
^ Wierzbicki AS. Homocysteine and cardiovascular disease: a review of the evidence. Diab Vasc Dis Res. (2007)
^ Finkelstein JD. Methionine metabolism in mammals. J Nutr Biochem. (1990)
^ a b Frosst P, et al. A candidate genetic risk factor for vascular disease: a common mutation in methylenetetrahydrofolate reductase. Nat Genet. (1995)
^ Jacques PF1, et al. Relation between folate status, a common mutation in methylenetetrahydrofolate reductase, and plasma homocysteine concentrations. Circulation. (1996)
^ Yamada K1, et al. Effects of common polymorphisms on the properties of recombinant human methylenetetrahydrofolate reductase. Proc Natl Acad Sci U S A. (2001)
^ Varga EA1, et al. Cardiology patient pages. Homocysteine and MTHFR mutations: relation to thrombosis and coronary artery disease. Circulation. (2005)
^ a b Klerk M1, et al. MTHFR 677C-->T polymorphism and risk of coronary heart disease: a meta-analysis. JAMA. (2002)
^ Wilcken B, et al. Geographical and ethnic variation of the 677C>T allele of 5,10 methylenetetrahydrofolate reductase (MTHFR): findings from over 7000 newborns from 16 areas world wide. J Med Genet. (2003)
^ a b McNulty H1, et al. Riboflavin lowers homocysteine in individuals homozygous for the MTHFR 677C->T polymorphism. Circulation. (2006)
^ a b García-Minguillán CJ1, et al. Riboflavin status modifies the effects of methylenetetrahydrofolate reductase (MTHFR) and methionine synthase reductase (MTRR) polymorphisms on homocysteine. Genes Nutr. (2014)
^ Quinlivan EP, et al. Importance of both folic acid and vitamin B12 in reduction of risk of vascular disease. Lancet. (2002)
^ McKinley MC1, et al. Low-dose vitamin B-6 effectively lowers fasting plasma homocysteine in healthy elderly persons who are folate and riboflavin replete. Am J Clin Nutr. (2001)
^ Jhee KH1, Kruger WD. The role of cystathionine beta-synthase in homocysteine metabolism. Antioxid Redox Signal. (2005)
^ Wilson CP1, et al. Blood pressure in treated hypertensive individuals with the MTHFR 677TT genotype is responsive to intervention with riboflavin: findings of a targeted randomized trial. Hypertension. (2013)
^ Horigan G1, et al. Riboflavin lowers blood pressure in cardiovascular disease patients homozygous for the 677C-->T polymorphism in MTHFR. J Hypertens. (2010)
^ Wilson CP1, et al. Riboflavin offers a targeted strategy for managing hypertension in patients with the MTHFR 677TT genotype: a 4-y follow-up. Am J Clin Nutr. (2012)
^ Damian DL1, Matthews YJ, Halliday GM. Topical riboflavin attenuates ultraviolet B- and ultraviolet A-induced immunosuppression in humans. Photodermatol Photoimmunol Photomed. (2010)
^ Halliday GM1. Inflammation, gene mutation and photoimmunosuppression in response to UVR-induced oxidative damage contributes to photocarcinogenesis. Mutat Res. (2005)
^ Said HM. Recent advances in transport of water-soluble vitamins in organs of the digestive system: a focus on the colon and the pancreas. Am J Physiol Gastrointest Liver Physiol. (2013)
^ Ghosal A1, Said HM. Mechanism and regulation of vitamin B2 (riboflavin) uptake by mouse and human pancreatic β-cells/islets: physiological and molecular aspects. Am J Physiol Gastrointest Liver Physiol. (2012)
^ Cobianchi L1, et al. Riboflavin inhibits IL-6 expression and p38 activation in islet cells. Cell Transplant. (2008)
^ Batey DW1, Eckhert CD. Identification of FAD, FMN, and riboflavin in the retina by microextraction and high-performance liquid chromatography. Anal Biochem. (1990)
^ Miyamoto Y1, Sancar A. Vitamin B2-based blue-light photoreceptors in the retinohypothalamic tract as the photoactive pigments for setting the circadian clock in mammals. Proc Natl Acad Sci U S A. (1998)
^ a b Takami Y1, Gong H, Amemiya T. Riboflavin deficiency induces ocular surface damage. Ophthalmic Res. (2004)
^ Cumming RG1, Mitchell P, Smith W. Diet and cataract: the Blue Mountains Eye Study. Ophthalmology. (2000)
^ Batey DW1, Daneshgar KK, Eckhert CD. Flavin levels in the rat retina. Exp Eye Res. (1992)
^ Batey DW1, Eckhert CD. Analysis of flavins in ocular tissues of the rabbit. Invest Ophthalmol Vis Sci. (1991)
^ Said HM1, Wang S, Ma TY. Mechanism of riboflavin uptake by cultured human retinal pigment epithelial ARPE-19 cells: possible regulation by an intracellular Ca2+-calmodulin-mediated pathway. J Physiol. (2005)
^ Zschäbitz S1, et al. B vitamin intakes and incidence of colorectal cancer: results from the Women's Health Initiative Observational Study cohort. Am J Clin Nutr. (2013)
^ a b Naghashpour M1, et al. Riboflavin Supplementation to Patients with Multiple Sclerosis does not Improve Disability Status nor is Riboflavin Supplementation Correlated to Homocysteine. Int J Vitam Nutr Res. (2013)
^ Campuzano V1, et al. Friedreich's ataxia: autosomal recessive disease caused by an intronic GAA triplet repeat expansion. Science. (1996)
^ Cossée M1, et al. Friedreich's ataxia: point mutations and clinical presentation of compound heterozygotes. Ann Neurol. (1999)
^ Gonzalez-Cabo P1, Ros S, Palau F. Flavin adenine dinucleotide rescues the phenotype of frataxin deficiency. PLoS One. (2010)
^ Boddaert N1, et al. Selective iron chelation in Friedreich ataxia: biologic and clinical implications. Blood. (2007)
^ Pandolfo M1, Hausmann L. Deferiprone for the treatment of Friedreich's ataxia. J Neurochem. (2013)
^ Arpa J1, et al. Triple therapy with deferiprone, idebenone and riboflavin in Friedreich's ataxia - open-label trial. Acta Neurol Scand. (2014)
^ Sturm B1, et al. Recombinant human erythropoietin: effects on frataxin expression in vitro. Eur J Clin Invest. (2005)
^ Arpa J1, et al. Triple therapy with darbepoetin alfa, idebenone, and riboflavin in Friedreich's ataxia: an open-label trial. Cerebellum. (2013)
^ Neville JN, et al. Nutritional status of alcoholics. Am J Clin Nutr. (1968)
^ Leevy CM, Baker H. Vitamins and alcoholism. Introduction. Am J Clin Nutr. (1968)
^ Majumdar SK, Shaw GK, Thomson AD. Vitamin utilization status in chronic alcoholics. Int J Vitam Nutr Res. (1981)
^ FENNELLY J, et al. PERIPHERAL NEUROPATHY OF THE ALCOHOLIC: I, AETIOLOGICAL ROLE OF ANEURIN AND OTHER B-COMPLEX VITAMINS. Br Med J. (1964)