A Review of Dietary Supplement–Induced Renal Dysfunction

A Review of Dietary Supplement–Induced Renal Dysfunction

CJASN ePress. Published on May 30, 2007 as doi: 10.2215/CJN.00500107 Mini-Review A Review of Dietary Supplement–Induced Renal Dysfunction Steven Gabardi,*†‡ Kristin Munz,* and Catherine Ulbricht§ *Department of Pharmacy Services, †Renal Division, Brigham and Women’s Hospital, ‡Harvard Medical School, and §Natural Standard and Department of Pharmacy Services, Massachusetts General Hospital, Boston, Massachusetts Complementary and alternative medicine (CAM) is a multibillion-dollar industry. Almost half of the American popu- lation uses some form of CAM, with many using them in addition to prescription medications. Most patients fail to inform their health care providers of their CAM use, and physicians rarely inquire. Annually, thousands of dietary supplement–induced adverse events are reported to Poison Control Centers nationwide. CAM manufacturers are not responsible for proving safety and efficacy, because the Food and Drug Administration does not regulate them. However, concern exists surrounding the safety of CAM. A literature search using MEDLINE and EMBASE was undertaken to explore the impact of CAM on renal function. English-language studies and case reports were selected for inclusion but were limited to those that consisted of human subjects, both adult and pediatric. This review provides details on dietary supplements that have been associated with renal dysfunction and focuses on 17 dietary supplements that have been associated with direct renal injury, CAM-induced immune-mediated nephrotoxicity, nephrolithiasis, rhabdomyolysis with acute renal injury, and hepatorenal syndrome. It is concluded that it is imperative that use of dietary supplements be monitored closely in all patients. Health care practitioners must take an active role in identifying patients who are using CAM and provide appropriate patient education. Clin J Am Soc Nephrol ●●: ●●●-●●●, ●●●●. doi: 10.2215/CJN.00500107 he use of complementary and alternative medicine CAM-related events were reported to the American Associ- (CAM) is commonplace in the United States (1). In a ation of Poison Control Centers (6). T 2002 survey, 36% of Americans used some form of The Dietary Supplement Health and Education Act (DSHEA) CAM, mostly herbs, nonherbal supplements, and vitamins of 1994 states that dietary supplements are not required to (collectively referred to as dietary supplements) (2–4). In undergo premarket safety and efficacy testing (7). Also, there general, most CAM consumers are not dissatisfied with con- are no requirements for product labeling to warn of known or ventional medicine but instead are aiming to complement potential adverse reactions (8). As a whole, the lack of enforce- mainstream medicine (5). This attitude may be the result of ment of good manufacturing practices in the dietary supple- patients’ attempting to take responsibility for their own well- ment industry is evident in reports of impurities and adulter- being, the perception that “natural” products are harmless, ation (9–11). or simply a testament to the ease of CAM accessibility (2). Drug-induced nephrotoxicity accounts for approximately 7% Only 12% of CAM users have sought care from a physician of all medication-related toxicities; therefore, it is reasonable to or licensed CAM practitioner, which suggests that most peo- expect that some CAM may be nephrotoxic (12,13). However, ple use CAM without consulting a health care provider (2,4). the availability of dietary supplement–induced adverse reac- This is significant because nearly 15 million dietary supple- tion data is limited, because reporting of these events is volun- ment users also use prescription medications (2). This di- tary (14). The majority of available information comes from case lemma may be attributed to the lack of specific questioning reports; therefore, tangible cause-and-effect relationships usu- by practitioners or the patient’s perception that the medical ally cannot be established. The objective of this article is to establishment has a negative attitude toward CAM. Forty-six compile and briefly review the available data on CAM-induced percent of supplements users consider these products to be nephrotoxicity. We provide detail of the renal injury and pos- safe and effective. Unfortunately, most patients likely do not tulated mechanism of toxicity but are often limited by the data comprehend the potential for adverse events or drug–sup- presented by the authors of the case reports. This review fo- plement interactions (2). The prevalence of drug misadven- cuses only on supplements that commonly are available in the tures related to CAM use is high. In 2003, nearly 25,000 US market (Table 1). A variety of foods that are ingested for medicinal purposes have been associated with nephrotoxicity. Published online ahead of print. Publication date available at www.cjasn.org. A discussion of these medicinal foodstuffs (e.g., star fruit, Je- hring-fruit, Djenkol beans, Cape aloes) and their risk for neph- Address correspondence to: Dr. Steven Gabardi, Renal Division/Department of Pharmacy Services, Brigham and Women’s Hospital, 75 Francis Street, Boston, MA rotoxicity is beyond the scope of this article. It should be noted 02115-6110. Phone: 617-732-7658; Fax: 617-732-7507; E-mail: [email protected] that many widely used dietary supplements are not generally Copyright © ●●●● by the American Society of Nephrology ISSN: 1555-9041/●●●●–0001 2 Clinical Journal of the American Society of Nephrology Clin J Am Soc Nephrol ●●: ●●●-●●●, ●●●● Table 1. Review of nephrotoxic dietary supplementsa Common Name Familiar Indications Nephrotoxic Manifestations Cat’s claw Anti-inflammatory Acute allergic interstitial nephritis (43) GI disorder Chaparral Antibiotic Renal cystic disease and low-grade cystic Anti-inflammatory renal cell carcinoma (34) Antioxidant Chromium Glucose control ATN (15,17) Lipid lowering Interstitial nephritis (16) Weight loss Cranberry Antibiotic Nephrolithiasis secondary to oxaluria (58) Urinary acidifier and deodorizer Creatine Enhancement of muscle performance Acute focal interstitial nephritis and focal during brief, high-intensity exercise tubular injury (18) Nonspecific renal dysfunction (19) AKI secondary to rhabdomyolysis (61–63) Ephedra Allergic rhinitis Nephrolithiasis secondary to ephedrine, Asthma norephedrine, and pseudoephedrine stone Hypotension formation (55,56) Sexual arousal Weight loss Germanium Anti-inflammatory Tubular degeneration with minor glomerular Immunostimulant abnormalities (23–32) Hydrazine Anorexia and cachexia Autolysis of the kidneys in the setting of Chemotherapeutic hepatorenal syndrome (40) Licorice Antibiotic Renal tubular injury secondary to prolonged Anti-inflammatory hypokalemia (64–66) GI disorders AKI secondary to hypokalemic rhabdomyolysis in the setting of pseudoaldosteronism (65) l-Lysine Antiviral Fanconi syndrome and tubulointerstitial Wound healing nephritis (33) Pennyroyal Abortifacient Edematous hemorrhagic kidneys with ATN Menstrual stimulant and proximal tubular degeneration in the setting of hepatorenal syndrome (69,71) Thunder god vine Immunosuppressant Unknown supplement effects in conjunction with prolonged shock (42) Vitamin C Enhance iron absorption Nephrolithiasis secondary to oxaluria (45–53) Prevention of cancer and heart disease Wound healing Willow bark Analgesic Necrotic papillae consistent with analgesic Anti-inflammatory nephropathy (41) Wormwood oil Anemia AKI secondary to rhabdomyolysis in the Antipyretic setting of supplement-induced tonic-clonic Appetite stimulant seizures (60) Asthma GI disorders Yellow oleander Anti-inflammatory Renal tubular necrosis with vacuolated areas in the glomerular spaces in the setting of hepatorenal syndrome (73) Yohimbe Erectile dysfunction SLE with resultant renal dysfunction (37) Sexual arousal aAKI, acute kidney injury; ATN, acute tubular necrosis; GI, gastrointestinal; SLE, systemic lupus erythematosus. taken in pure form but are mixtures of a variety of entities, anemia, hemolysis, thrombocytopenia, hepatic dysfunction, which may have multiple interactions with each other. This and acute kidney injury (AKI) (15). Chromium levels were makes it more difficult to identify the offending nephrotoxin in three times normal. An abdominal ultrasound revealed en- patients who consume CAM. larged kidneys, with muddy brown casts and urine microscopy consistent with acute tubular necrosis (ATN). No biopsy was Direct Nephrotoxicity/Immune-Mediated performed. The patient’s renal function improved after several Nephrotoxicity days of hemodialysis (HD) (15). A second case of ATN was seen Chromium Picolinate in a 24-yr-old man who presented with AKI after a 2-wk history There are three case reports of renal dysfunction secondary to of consuming a supplement that contained CP (17). A com- chromium picolinate (CP) (15–17). The first patient had a 5-mo puted tomography scan and an abdominal ultrasound showed history of ingesting 1200 to 2400 ␮g/d CP and presented with inflammation in the right, sole kidney. A renal biopsy revealed Clin J Am Soc Nephrol ●●: ●●●-●●●, ●●●● Nephrotoxic CAM 3 necrotic tubular epithelium with intraluminal debris consistent search excluded major causes of cystic renal disease. The au- with ATN. The patient was treated with HD, plasmapheresis, thors concluded that nordihydroguaiaretic acid, in the form of and corticosteroids and ultimately regained normal renal func- chaparral, was the most likely cause of the carcinoma. Nordi- tion (17). Another patient ingested 600 ␮g/d CP for 6 wk

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