Recognition of Chronic Alcoholism Key to Successful Treatment of Pellagra: A Case Report
Pellagra is a disease characterized by a lack of cellular niacin, generally caused by a dietary insufficiency of nicotinic acid (niacin) or its essential amino acid precursor tryptophan.1 Historically, systemic complications caused by niacin-deficient diets were of epidemic proportions, though the malady was nearly eradicated once government dietary supplementation programs began fortifying flour with B-vitamins during World War II.2 Nonetheless, pellagra still remains a threat in various niche patient populations across the developed world. Contemporarily, it is found only in patients with excessive leucine intake, patients who take medicines that inhibit or disrupt vitamin absorption, anorexics, and most often, patients who have malabsorptive gastrointestinal complications caused by a certain illness.1-5 We herein report a case of early-stage pellagra induced by chronic alcohol abuse and resolved with niacinamide treatment.
CASE REPORT
A 51-year-old man with a history of chronic alcohol abuse and an alcohol-related cognitive disorder visited our free clinic complaining of an intense pruritic skin rash that had been progressively worsening over the past two months. Upon examination, the primary care physician (PCP) observed “red, coalescing papulovesicular lesions above distribution with crusting” on the patient’s distal extremities. Of note, the patient explained that he had been previously treated with a ceramide-rich hydrating lotion and triamcinolone 0.1% emollience at an outside hospital, but exhibited no improvement or relief. Before referring the patient to the clinic’s staff dermatologist, the patient’s PCP initiated treatment with hydroxyzine 25mg PO TID for itching, suspecting a quetiapine-induced drug flare.
At the one-week follow up with the dermatologist, the patient stated that the hydroxyzine treatment led to only slight improvement of the severe pruritus and had no effect on the progressive eruption. The dermatologist reassessed the patient, noting instead the presence of moderate-to-severe eczematous dermatitis with numerous excoriated papules, some of which were perifollicular (none with evident purpura) on the dorsum of hands and distal extremities, ears, and slightly on the neck. The dermatitis spared protected areas except for waistline where there was involvement. Marginal glossitis was noted as well.
Due to the insidious nature of the skin eruptions and their inception having preceded the initiation of quetiapine treatment, the Seroquel drug-flare hypothesis was considered less likely to account for the cutaneous eruption. The patient’s continued long history of alcohol abuse, malnutrition, memory loss, depression, glossitis, and severe dermatitis were consistent with the causes and symptoms of vitamin B3 deficiency, satisfying the diagnostic criteria for pellagra. Consequently, the dermatologist prescribed niacinamide 500mg QD and OTC multivitamins QD, and discussed dietary management as well as proper sun protection techniques.
At the one-month follow up, the patient displayed a marked decrease of eczematous dermatitis and improved skin turgor with less desiccation. The healing excoriations indicated the resolution of pruritus, as well. The patient detailed rapid improvement of the pruritus and skin involvement upon starting niacinamide 500mg and MVI QD, indicating the successful diagnosis and appropriate treatment of vitamin B3 deficiency caused by alcohol-induced pellagra.
After one additional month of daily niacinamide 500mg and MVI, treatment was discontinued, as the clinical manifestations of pellagra were resolved. The patient decided not to attend the subsequent dermatology follow up, indicative of his improved affect post treatment.
DISCUSSION
Pellagra can be identified by a number of neurological, gastrointestinal, and integumentary clinical symptoms; however, the classic “Three Ds” of the disease (dementia, dermatitis, and diarrhea) are manifested differently in nearly every patient.3,6 Its present-day rarity, compounded with its idiosyncratic nature, makes it a very dangerous case for any physician despite the ease of treatment. In modern-day pellagra, the delay in recognition and treatment is the most dangerous risk factor for sequelae. In this case, an appreciation for the wide range of predisposing factors of the disease allowed an early diagnosis and prompt treatment of an otherwise fatal condition.
The history of epidemic pellagra and the history of vitamin deficient maize-based diets are one in the same. Gaspar Casal recorded the first case in 1735, correlating the disease outbreak with the influx of New World maize consumed by poor populations that could not afford high protein meals.7 Similarly, pellagra proliferated through the American South at the turn of the twentieth century when poverty stricken families were forced to abandon the costly proteinous parts of their diets with nutrient-poor milled corn.8-10 There were more than three million cases and 100,000 pellagra-related deaths in the United States between 1900 and 1940.11 Unknown at the time, the shortage of niacin and tryptophan in the maize-based food supply was the culprit. After extensive dietary detective work by Dr. Joseph Goldberger and the expansion of dietary supplementation programs during WWII, pellagra was seemingly overcome.2 Although outbreaks of the disease are still found during major humanitarian crises in developing countries, diagnoses of pellagra are very scarce. One 2011 study of emergency room patients in Spain estimated that the current annual incidence is approximately only 0.5 pellagra cases per 100,000 patients.12
Paradoxically, this past scientific success has now become a burden for our generation of physicians. The contemporary rarity of pellagra has limited the scope of clinical exposure to the illness, resulting in failure to recognize, diagnose, and treat in its early stages. Consequently, it is often mistaken for a vast array of different diseases1,12 or as in our case, an atypical, adverse drug reaction. This is due to the inconsistency of the clinical manifestations of dementia, dermatitis, and diarrhea in niacin deficient patients. For example, one hospital did a retrospective analysis of the seven pellagra patients it encountered over an 11-year span, and although all seven displayed a form of skin involvement, only three were diagnosed correctly with pellagra initially. Meanwhile, only four displayed a neurological defect and only three experienced diarrhea.12 In another 42-patient pellagra study in which dermatitis was a prerequisite for diagnosis, only 10 exhibited any form of dementia.13 In a similar study of 18 patients, just four had the complete triad.14 Our patient manifested just the symptoms of dermatitis and dementia.
Several reports have commented on the fatal consequence of delaying the diagnosis of pellagra,15-17 highlighting the need for physicians to appreciate when the predisposing factors for niacin deficiency correlate with the varying presence of dementia, dermatitis, and diarrhea in any patient. The common predisposing factors for pellagra are alcohol dependency, anorexia nervosa, excess leucine diets, peculiar food fads diets, and a history of disease or drugs that cause niacin or tryptophan-specific malabsorptive states.1,5 If any of these are present simultaneously with a clinical observation of any of the “Three Ds,” pellagra should remain an option within the differential diagnosis. In our case, the malnourishment induced by chronic alcohol abuse was first marker for the patient’s niacin deficiency.
Fortunately, the one definitive way to diagnose and treat pellagra is to provide the patient with physiological doses of niacin or equivalent doses of its reciprocal amide, niacinamide.1,6 Treatment with these medications is simple, cheap, swift, and relatively harmless. Skin lesions and other clinical manifestations begin to resolve quickly if the diagnosis of pellagra is correct.1,6 Furthermore, if there is no sign of improvement, there is little to no risk in providing the patient with the physiological doses of either available form of Vitamin B3.18 Of note, some physicians recommend taking 24-hour urine studies or blood samples for detecting abnormally low levels of niacin metabolites to confirm the diagnosis,5,6 but our free clinic does not have these capabilities.
Niacinamide, also known as nicotinamide, is very safe at physiological doses19 and has been frequently used to treat several other inflammatory skin conditions, most commonly necrobiosis lipoidica, bollus pemphigoid, acne vulgaris, rosacea and granuloma annulare.20 Furthermore, its widespread OTC use as a vitamin or supplement makes it a valuable treatment for uninsured patients who are diagnosed with pellagra, such as our own. The limiting side effects are flushing and plethora, which are less pronounced than with its precursor niacin secondary to the terminal amide substitution. The FDA approved, relatively non-toxic drug is ubiquitously used in cosmetic products with over 30 commercially-consumed cosmetic formulations.18,19
Conclusion
Pellagra is difficult to diagnose, easy to treat, and extremely important to recognize early to prevent systematic sequelae. In all patients in whom there is reason to suspect illness due to correlation of any of the “Three Ds” and its predisposing factors, a physiological dose of niacin or niacinamide is most likely warranted. Delaying the diagnosis may have much more serious consequences, and the absence of a response to Vitamin B3 replacement therapy will only further the diagnosis process. Patients with a history of chronic alcoholism and dermatitis should be considered at-risk for pellagra.
Neither of the authors report any conflicts of interest.
1. Hegyi J, Schwartz RA, Hegyi V: Pellagra: dermatitis, dementia, and diarrhea. Int J Dermatol 2004; 43:1–5
2. Sydenstricker VP: The history of pellagra, its recognition as a disorder of nutrition and its conquest. Am J Clin Nutr 1958; 6:409-414
3. Hendricks WM. Pellagra and pellagralike dermatoses: etiology, differential diagnosis, dermatopathology, and treatment. Semin Dermatol. 1991;10:282-92.
4. Bender DA. Nutritional biochemistry of the vitamins. New York: Cambridge University Press; 1992.
5. Valerie B. Lyon, Janet A. Fairley, Anticonvulsant-induced pellagra. Journal of the American Academy of Dermatology, 2002;46;4:597-599
6. Brown TM. Pellagra: an old enemy of timeless importance. Psychosomatics 2010;51: 93-7
7. Major RH: Don Gasper Casal, Francois Thiery and pellagra. Bull Hist Med 1944; 16:351-361
8. Goldberger, Joseph, Wheeler G. A., and Sydenstricker Edgar. “Pellagra Incidence in Relation to Sex, Age, Season, Occupation, and “Disabling Sickness” in Seven Cotton-Mill Villages of South Carolina during 1916.” Public Health Reports (1896-1970) 35, no. 28 (1920): 1650-664.
9. Goldberger J, Wheeler GA, Sydenstricker E: A study of the relation of diet to pellagra incidence in seven textile-mill communities of South Carolina in 1916. Public Health Rep 1920; 35:648-713
10. Rajakumar K. Pellagra in the United States: a historical perspective. South Med J. 2000;93(3):272–277.
11. Bollet AJ: Politics and pellagra: the epidemic of pellagra in the US in the early twentieth century. Yale J Biol Med 1992; 65:211-221
12. Piqué-Duran E, Pérez-Cejudo JA, Cameselle D, et al. Pellagra: a clinical, histopathological, and epidemiological study of 7 cases. Actas Dermosifiliogr 2012;103:51–8
13. Turner RH: The pathologic physiology of pellagra, I: Tabulated clinical and physiologic data. J Clin Invest 1931; 10:111–120
14. Spivak JL, Jackson DL: Pellagra: an analysis of 18 patients and a review of the literature. Johns Hopkins Med J 1977; 140:295– 309
15. Kertesz SG. Pellagra in 2 homeless men. Mayo Clin Proc. 2001;76:315–318.
16. Ishii N, Nishihara Y. Pellagra encephalopathy among tuberculous patients: its relation to isoniazid therapy. J Neurol Neurosurg Psychiatry. 1985;48:628-634.
17. Ishii N, Nishihara Y. Pellagra among chronic alcoholics: clinical and pathological study of 20 necropsy cases. J Neurol Neurosurg Psychiatry. 1981;44:209-215.
18. Food and Drug Administration. Database of select committee on GRAS substances (SCOGS) reviews: niacinamide (nicotinamide). Report No. 108. http://www.accessdata.fda.gov/scripts/fcn/fcnDetailNavigation.cfm?rpt=scogsListing&id=221. Accessed 14 July 2016.
19. Cosmetic Ingredient Review Expert Panel. Final report of safety assessment of niacinamide and niacin. Int J Toxicol. 2005;24(Suppl 5):1–31.
20. Tosti A, Hexsel D. Update in Cosmetic Dermatology; Springer, 2013. pp. 91–92.
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