Hyperuricemia
Hyperuricemia | |
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Specialty | Endocrinology |
Hyperuricemia is an abnormally high level of uric acid in the blood. In the pH conditions of body fluid, uric acid exists largely as urate, the ion form.[1][2] The amount of urate in the body depends on the balance between the amount of purines eaten in food, the amount of urate synthesised within the body (e.g., through cell turnover), and the amount of urate that is excreted in urine or through the gastrointestinal tract.[2] In humans, the upper end of the normal range is 360 µmol/L (6 mg/dL) for women and 400 µmol/L (6.8 mg/dL) for men.[3]
Causes
Many factors contribute to hyperuricemia, including genetics, insulin resistance, hypertension, hypothyroidism, renal insufficiency, obesity, diet, use of diuretics, and consumption of alcoholic beverages.[4] Of these, alcohol consumption is the most important.[5]
Causes of hyperuricemia can be classified into three functional types:[6] increased production of uric acid, decreased excretion of uric acid, and mixed type. Causes of increased production include high levels of purine in the diet and increased purine metabolism. Causes of decreased excretion include kidney disease, certain drugs, and competition for excretion between uric acid and other molecules. Mixed causes include high levels of alcohol and/or fructose in the diet, and starvation.
Increased production of uric acid
A purine-rich diet is a common but minor cause of hyperuricemia. Diet alone generally is not sufficient to cause hyperuricemia. Purine content of foods varies (see Gout). Foods high in the purines adenine and hypoxanthine may be more potent in exacerbating hyperuricemia.[7]
Hyperuricemia of this type is a common complication of solid organ transplant.[8] Apart from normal variation (with a genetic component), tumor lysis syndrome produces extreme levels of uric acid, mainly leading to renal failure. The Lesch-Nyhan syndrome is also associated with extremely high levels of uric acid.
Decreased excretion of uric acid
The principal drugs that contribute to hyperuricemia by decreased excretion are the primary antiuricosurics. Other drugs and agents include diuretics, salicylates, pyrazinamide, ethambutol, nicotinic acid, ciclosporin, 2-ethylamino-1,3,4-thiadiazole, and cytotoxic agents.[9]
The gene SLC2A9 encodes a protein that helps to transport uric acid in the kidney. Several single nucleotide polymorphisms of this gene are known to have a significant correlation with blood uric acid.[10] Hyperuricemia cosegregating with osteogenesis imperfecta has been shown to be associated with a mutation in GPATCH8 using exome sequencing[11]
A ketogenic diet impairs the ability of the kidney to excrete uric acid, due to competition for transport between uric acid and ketones.[12]
Elevated blood lead is significantly correlated with both impaired kidney function and hyperuricemia (although the causal relationship among these correlations is not known). In a study of over 2500 people resident in Taiwan, a blood lead level exceeding 7.5 microg/dL (a small elevation) had odds ratios of 1.92 (95% CI: 1.18-3.10) for renal dysfunction and 2.72 (95% CI: 1.64-4.52) for hyperuricemia.[13][14]
Mixed type
Causes of hyperuricemia that are of mixed type have a dual action, both increasing production and decreasing excretion of uric acid.
High intake of alcohol (ethanol), a significant cause of hyperuricemia, has a dual action that is compounded by multiple mechanisms. Ethanol increases production of uric acid by increasing production of lactic acid, hence lactic acidosis. Ethanol also increases the plasma concentrations of hypoxanthine and xanthine via the acceleration of adenine nucleotide degradation, and is a possible weak inhibitor of xanthine dehydrogenase. As a byproduct of its fermentation process, beer additionally contributes purines. Ethanol decreases excretion of uric acid by promoting dehydration and (rarely) clinical ketoacidosis.[5]
High dietary intake of fructose contributes significantly to hyperuricemia.[15][16][17] In a large study in the United States, consumption of four or more sugar-sweetened soft drinks per day gave an odds ratio of 1.82 for hyperuricemia.[18] Increased production of uric acid is the result of interference, by a product of fructose metabolism, in purine metabolism. This interference has a dual action, both increasing the conversion of ATP to inosine and hence uric acid and increasing the synthesis of purine.[19] Fructose also inhibits the excretion of uric acid, apparently by competing with uric acid for access to the transport protein SLC2A9.[20] The effect of fructose in reducing excretion of uric acid is increased in people with a hereditary (genetic) predisposition toward hyperuricemia and/or gout.[19]
Starvation causes the body to metabolize its own (purine-rich) tissues for energy. Thus, like a high purine diet, starvation increases the amount of purine converted to uric acid. A very low calorie diet without carbohydrate can induce extreme hyperuricemia; including some carbohydrate (and reducing the protein) reduces the level of hyperuricemia.[21] Starvation also impairs the ability of the kidney to excrete uric acid, due to competition for transport between uric acid and ketones.[22]
Treatment
Precipitation of uric acid crystals, and conversely their dissolution, is known to be dependent on the concentration of uric acid in solution, pH, sodium concentration, and temperature. Established treatments address these parameters.
Concentration
Following Le Chatelier's principle, lowering the blood concentration of uric acid may permit any existing crystals of uric acid to be gradually dissolved into the blood, from whence the dissolved uric acid can be excreted. Maintaining a lower blood concentration of uric acid similarly should reduce the formation of new crystals. If the person has chronic gout or known tophi, then large quantities of uric acid crystals may have accumulated in joints and other tissues, and aggressive and/or long duration use of medications may be needed.
Medications most often used to treat hyperuricemia are of two kinds: xanthine oxidase inhibitors and uricosurics. Xanthine oxidase inhibitors decrease the production of uric acid, by interfering with xanthine oxidase. Uricosurics increase the excretion of uric acid, by reducing the reabsorption of uric acid once the kidneys have filtered it out of the blood. Some of these medications are used as indicated, others are used off-label. Several other kinds of medications have potential for use in treating hyperuricemia. In people receiving hemodialysis, sevelamer can significantly reduce serum uric acid,[23][24] apparently by adsorbing urate in the gut.[24] In women, use of combined oral contraceptive pills is significantly associated with lower serum uric acid.[25]
Non-medication treatments for hyperuricemia include a low purine diet (see Gout) and a variety of dietary supplements. Treatment with lithium salts has been used as lithium improves uric acid solubility.
pH
Serum pH is neither safely or easily altered. Therapies that alter pH principally alter the pH of urine, to discourage a possible complication of uricosuric therapy: formation of uric acid kidney stones due to increased uric acid in the urine (see Nephrolithiasis). Dietary supplements that can be used to make the urine more alkaline include sodium bicarbonate, potassium citrate, magnesium citrate, and Shohl's Solution (now replaced by Bicitra[26]). Medications that have a similar effect include acetazolamide.
Temperature
Low temperature is a commonly reported trigger of acute gout: an example would be a day spent standing in cold water, followed by an attack of gout the next morning. This is believed to be due to temperature-dependent precipitation of uric acid crystals in tissues at below normal temperature. Thus, one aim of prevention is to keep the hands and feet warm, and soaking in hot water may be therapeutic.
Prognosis
Increased levels predispose for gout and, if very high, kidney failure. The metabolic syndrome often presents with hyperuricemia.
People with gout, and by inference hyperuricemia, are significantly less likely to develop Parkinson's disease, unless they also require diuretics.[27]
Dalmatian dogs
In Dalmatian dogs, a lack of uricase (a genetic trait fixed in this breed) contributes to hyperuricemia and corresponding hyperuricosuria.
See also
References
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- ^ Chizyński K, Rózycka M (2005). "Hyperuricemia". Pol. Merkur. Lekarski (in Polish). 19 (113): 693–6. PMID 16498814.
- ^ Sam Z Sun; Brent D Flickinger; Patricia S Williamson-Hughes; Mark W Empie (March 2010). "Lack of association between dietary fructose and hyperuricemia risk in adults". Nutrition & Metabolism. 7 (16): 16. doi:10.1186/1743-7075-7-16.
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- ^ Yamamoto T (April 2008). "[Definition and classification of hyperuricemia]". Nippon Rinsho (in Japanese). 66 (4): 636–40. PMID 18409507.
- ^ Brulé D, Sarwar G, Savoie L (1992). "Changes in serum and urinary uric acid levels in normal human subjects fed purine-rich foods containing different amounts of adenine and hypoxanthine". J Am Coll Nutr. 11 (3): 353–8. doi:10.1080/07315724.1992.10718238. PMID 1619189.
- ^ Stamp L, Searle M, O'Donnell J, Chapman P (2005). "Gout in solid organ transplantation: a challenging clinical problem". Drugs. 65 (18): 2593–611. doi:10.2165/00003495-200565180-00004. PMID 16392875.
- ^ Scott JT (April 1991). "Drug-induced gout". Baillieres Clin Rheumatol. 5 (1): 39–60. doi:10.1016/S0950-3579(05)80295-X. PMID 2070427.
- ^ Brandstätter A, Kiechl S, Kollerits B, Hunt SC, Heid IM, Coassin S, Willeit J, Adams TD, Illig T, Hopkins PN, Kronenberg F (August 2008). "Sex-specific association of the putative fructose transporter SLC2A9 variants with uric acid levels is modified by BMI". Diabetes Care. 31 (8): 1662–7. doi:10.2337/dc08-0349. PMC 2494626. PMID 18487473.
- ^ Kaneko, Hiroshi; Kitoh Hiroshi; Matsuura Tohru; Masuda Akio; Ito Mikako; Mottes Monica; Rauch Frank; Ishiguro Naoki; Ohno Kinji (Nov 2011). "Hyperuricemia cosegregating with osteogenesis imperfecta is associated with a mutation in GPATCH8". Hum. Genet. 130 (5). Germany: 671–83. doi:10.1007/s00439-011-1006-9. PMID 21594610.
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- ^ Lai LH, Chou SY, Wu FY, Chen JJ, Kuo HW (August 2008). "Renal dysfunction and hyperuricemia with low blood lead levels and ethnicity in community-based study". Sci. Total Environ. 401 (1–3): 39–43. doi:10.1016/j.scitotenv.2008.04.004. PMID 18514766.
- ^ Shadick NA, Kim R, Weiss S, Liang MH, Sparrow D, Hu H. (2000 ), Effect of low level lead exposure on hyperuricemia and gout among middle aged and elderly men: the normative aging study ; J Rheumatol. 2000 Jul; 27(7):1708-12 (abstract).
- ^ Nakagawa T; Hu H; Zharikov S; et al. (2006). "A causal role for uric acid in fructose-induced metabolic syndrome". Am. J. Physiol. Renal Physiol. 290 (3): F625–31. doi:10.1152/ajprenal.00140.2005. PMID 16234313.
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- ^ Miller A, Adeli K (March 2008). "Dietary fructose and the metabolic syndrome". Curr. Opin. Gastroenterol. 24 (2): 204–9. doi:10.1097/MOG.0b013e3282f3f4c4. PMID 18301272.
- ^ Choi JW, Ford ES, Gao X, Choi HK (January 2008). "Sugar-sweetened soft drinks, diet soft drinks, and serum uric acid level: the Third National Health and Nutrition Examination Survey". Arthritis Rheum. 59 (1): 109–16. doi:10.1002/art.23245. PMID 18163396.
- ^ a b Mayes PA (November 1993). "Intermediary metabolism of fructose". Am. J. Clin. Nutr. 58 (5 Suppl): 754S–765S. PMID 8213607.
- ^ Vitart V, Rudan I, Hayward C, Gray NK, Floyd J, Palmer CN, Knott SA, Kolcic I, Polasek O, Graessler J, Wilson JF, Marinaki A, Riches PL, Shu X, Janicijevic B, Smolej-Narancic N, Gorgoni B, Morgan J, Campbell S, Biloglav Z, Barac-Lauc L, Pericic M, Klaric IM, Zgaga L, Skaric-Juric T, Wild SH, Richardson WA, Hohenstein P, Kimber CH, Tenesa A, Donnelly LA, Fairbanks LD, Aringer M, McKeigue PM, Ralston SH, Morris AD, Rudan P, Hastie ND, Campbell H, Wright AF (April 2008). "SLC2A9 is a newly identified urate transporter influencing serum urate concentration, urate excretion and gout". Nat. Genet. 40 (4): 437–42. doi:10.1038/ng.106. PMID 18327257.
- ^ Howard AN (1981). "The historical development, efficacy and safety of very-low-calorie diets". Int J Obes. 5 (3): 195–208. PMID 7024153.
- ^ Kirch W, von Gicycki C (April 1980). "[Renal function in therapeutic starvation (author's transl)]". Wien. Klin. Wochenschr. (in German). 92 (8): 263–6. PMID 7405247.
- ^ Garg JP; Chasan-Taber S; Blair A; et al. (January 2005). "Effects of sevelamer and calcium-based phosphate binders on uric acid concentrations in patients undergoing hemodialysis: a randomized clinical trial". Arthritis and rheumatism. 52 (1): 290–5. doi:10.1002/art.20781. PMID 15641045.
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- ^ Gresser U, Gathof B, Zöllner N (December 1990). "Uric acid levels in southern Germany in 1989. A comparison with studies from 1962, 1971, and 1984". Klin. Wochenschr. 68 (24): 1222–8. doi:10.1007/BF01796514. PMID 2290309.
- ^ Ross, Mary. Rx Update December 1993. University of Iowa. 2009-02-16. URL:http://www.healthcare.uiowa.edu/pharmacy/RxUpdate/1993/12.December.html. Accessed: 2009-02-16. (Archived by WebCite at http://www.webcitation.org/5ecekFVcC)
- ^ De Vera M, Rahman MM, Rankin J, Kopec J, Gao X, Choi H (November 2008). "Gout and the risk of Parkinson's disease: a cohort study". Arthritis Rheum. 59 (11): 1549–54. doi:10.1002/art.24193. PMID 18975349.
Further reading
- Nuki G, Simkin PA (2006). "A concise history of gout and hyperuricemia and their treatment". Arthritis Research & Therapy. 8 Suppl 1 (Suppl 1): S1. doi:10.1186/ar1906. PMC 3226106. PMID 16820040.
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External links
- GeneReviews/NCBI/NIH/UW entry on UMOD-Related Kidney Disease Includes: Familial Juvenile Hyperuricemic Nephropathy, Medullary Cystic Kidney Disease 2
- OMIM entries on UMOD-Related Kidney Disease Includes: Familial Juvenile Hyperuricemic Nephropathy, Medullary Cystic Kidney Disease 2
- GeneReviews/NCBI/NIH/UW entry on Familial Juvenile Hyperuricemic Nephropathy Type 2
- OMIM entries on Familial Juvenile Hyperuricemic Nephropathy Type 2