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MICROSPORIDIOSIS IN TRAVEL-ASSOCIATED CHRONIC DIARRHEA IN IMMUNE-COMPETENT PATIENTS

ABSTRACT

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We analyzed retrospectively 21 immune-competent travelers with chronic traveler’s diarrhea (3–6 weeks) after returning from recreational travel to the tropics with stool samples positive for microsporidia. Nine patients had been treated with albendazole and 12 patients had been treated symptomatically. Diarrhea resolved in 8 of 9 and 12 of 12 patients, respectively. In the albendazole group, Encephalitozoon intestinalis was cleared in 4 of 4 patients and Enterocytozoon bieneusi persisted in 7of 7 patients (2 patients were lost to follow-up). In the symptomatic treated group microsporidia persisted in stool samples of all patients. We conclude that there is only a transient correlation between detection of microsporidia in stool and gastrointestinal symptoms, and suggest that microsporidia infection may cause clinical symptoms during the early stages of infection that resolve even though the microsporidia may persist.

INTRODUCTION

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Microsporidia, the intracellular spore-forming protozoa, have been recognized in various hosts¹ and in humans.^2–4 Among the more than 1,000 species of microsporidia, Enterocytozoon bieneusi and Encephalitozoon intestinalis have been associated with diarrhea in immune-incompetent patients, in particular in the context of human immunodeficiency virus/acquired immunodeficiency syndrome (HIV/AIDS) and organ transplantation.⁵ Albendazole is the recommended treatment for intestinal microsporidiosis in immune-suppressed patients, especially for E. intestinalis.^6–8 However, only little data are available on their role in causing diarrhea in travelers⁹ and the efficacy of albendazole in microsporidia-associated diarrhea in immune-competent persons.^10,11

We performed a retrospective chart review of 21 patients with chronic diarrhea after returning from recreational travel to the tropics with positive stool samples for microsporidia. Therapy was left to the discretion of the treating physician; 12 patients were treated only symptomatically, and 9 received albendazole in addition to symptomatic treatment. The Ethics Committee of our institution waived the need for informed consent.

SUBJECTS AND METHODS

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We investigated 21 immune-competent travelers between 18 and 49 years of age (median = 26 years, 9 men and 12 women) who attended our infectious diseases outpatient clinic for chronic diarrhea lasting for more than 3 weeks (3–6 weeks, median = 4 weeks) after return from traveling to the tropics from January 2003 to January 2004 in whom stool samples were positive for microsporidia (E. bieneusi and/or E. intestinalis). Stool samples were obtained after return from travel and not prior to travel. A calcofluor white immunofluorescence stain was done as described and read at 360 nm.^12,13 Speciation was done by size: E. bieneusi spores measure approximately 0.9 x 1.5 mm and E. intestinalis measure approximately 1.5 x 3.0 mm. After the exclusion of other causes for diarrhea, all patients with chronic diarrhea attending our clinic during this time had stool samples tested for microsporidia. Their medical history and results of physical examinations were otherwise unremarkable in all cases, the patients did not have any underlying diseases (had no risk factors) and none was taking medication. The patients returned from recreational travel to India (n = 4), Thailand (n = 11), Indonesia (n = 2), Zaire (n = 2), and Nigeria (n = 2). There was no occupational exposure. The duration of travel was between 2 and 16 weeks (median = 4 weeks). Two of the patients had a history of previous travel (both visited Thailand for the second time). All patients had a history of prior evaluation by a primary care physician, which resulted in no diagnosis with respect to diarrhea and lead to the transfer of the patients to our clinic. Routine blood samples showed no electrolyte disturbance, a normal blood count and differential count, and normal liver and renal function test results in all patients. All patients were HIV negative. Four patients had a history of Entamoeba histolytica– (n = 1) or Giardia lamblia– (n = 3) associated diarrhea, which was treated effectively with standard courses of metronidazole prior to enrollment in this series. The control stool samples, which were obtained 3 and 4 weeks after the metronidazole standard treatment course, were negative for Entamoeba histolytica or Giardia lamblia, but diarrhea persisted for an additional 4–5 weeks in all cases. Thereafter, stool samples (chronic diarrhea 4 weeks) were tested for microsporidia. Two of these patients were treated with albendazole and two with symptomatic therapy.

RESULTS

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The symptoms of the patients included watery, bloody surface, or unspecific diarrhea, abdominal discomfort, cramps, flatulence, fatigue, weight loss, loss of appetite, and subfebrile temperatures (Table 1). There was no difference in the duration of symptoms between the groups (Table 1). Twelve patients were treated symptomatically, and 9 of 21 received albendazole (400 mg twice a day for 4 weeks). Control stool samples were tested for microsporidia after four weeks. The laboratory was not biased by prior diagnosis, since no information regarding diagnosis or treatment was provided. Two of the albendazole-treated patients received a second treatment course with albendazole (for three and four weeks, respectively) for persisting symptoms and/or persisting positive stool samples; the remaining denied a second cycle. None of the treatments were interrupted due to adverse drug reactions.

DISCUSSION

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Albendazole is the currently recommended treatment for microsporidiosis, especially for E. intestinalis, in immune-suppressed patients.^6–8 In E. bieneusi infections, however, albendazole was reported to improve only the clinical status, while it failed to eliminate the organism from the stool.^6–8 Our data are consistent with this finding^6–8,11 since microbiologic efficacy of albendazole was seen only in E. intestinalis infection but not in E. bieneusi infection. However, since the microsporidia are so small, and size discrimination between Encephalitozoon and Enterocytozoon is inaccurate and often not possible (Table 2), a polymerase chain reaction (PCR) should be conducted to more reliably identify these species, and ultimately the efficacy of albendazole. Unfortunately, this was not possible in this study since stool samples were not available for PCR testing.

In immunocompetent individuals, microsporidia infections may persist even after clinical symptoms resolve, as this has been observed in other mammals. Thus, only a transient pathogenic role of microsporida in immunocompetent patients with traveler’s diarrhea is likely: Microsporidia infection may cause clinical symptoms during the early stages of infection (e.g., diarrhea) that resolve even though the microsporidia may persist. Since other microorganisms that might contribute to diarrhea were not identified, since albendazole is ineffective against E. bieneusi, and since immunocompetent laboratory animals remain persistently infected with microsporidia after resolution of clinical symptoms, our study supports the likelihood that microsporidiosis does contribute to chronic travelers’ diarrhea.^9,11,14–17

Received September 27, 2004. Accepted for publication February 26, 2005.

Acknowledgment: We thank the nursing staff of our department for continuous support.

^* Address correspondence to Christoph Wenisch, Medizinische Abteilung mit Infektions und Tropenmedizin, SMZ-Süd KFJ-Spital, Kundratstrasse 3, A-1100 Wien. E-mail: christoph.wenisch{at}wienkav.at

Authors’ addresses: Erika Wichro, David Hoelzl, Robert Krause, and Georg Bertha, Department of Internal Medicine, University Hospital Graz, Auenbruggerplatz 15, A-8036 Graz, Austria, Telephone: 43-316-385-81808, Fax: 43-316-385-4622. Franz Reinthaler, Institute of Hygiene, Medical University, Graz, Austria. Christoph Wenisch, Medizinische Abteilung mit Infektions und Tropenmedizin, SMZ-Süd-Kaiser Franz Josef Spital, Kundratstraße 3, A-1100 Wien, Telephone: 43-1-60191-2401, Fax: 43-1-60191-2419, E-mail: christoph.wenisch{at}wienkav.at.

REFERENCES

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