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Journal of Clinical Microbiology, December 2003, p. 5830-5832, Vol. 41, No. 12
0095-1137/03/$08.00+0 DOI: 10.1128/JCM.41.12.5830-5832.2003
Copyright © 2003, American Society for Microbiology. All Rights Reserved.
Ram Manohar Lohia Hospital,1 All India Institute of Medical Sciences, New Delhi, India2
Received 23 May 2003/ Returned for modification 22 July 2003/ Accepted 27 August 2003
| ABSTRACT |
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| CASE REPORT |
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The routine microscopic examination of feces did not reveal the presence of any protozoan or helminth. While fecal cultures grew a non-lactose-fermenting motile organism, the routine biochemical tests (indole, triple-sugar iron agar, citrate, urea, mannitol, and motility) for this isolate were obfuscating. The isolate was subjected to antimicrobial susceptibility testing by the Kirby-Bauer disk diffusion method and was found sensitive to furazolidone (Furoxane), ciprofloxacin, ofloxacin, ceftriaxone, and piperacillin-tazobactam. However, it revealed resistance to chloramphenicol, tetracycline, nalidixic acid, and gentamicin. Extended biotyping eventually identified the isolate as Salmonella enterica subsp. arizonae. This was further confirmed by the rapid API identification kit (Bio-Mureiux). The isolate was also subsequently identified as a Salmonella species by a flagellin gene PCR-restriction fragment length polymorphism analysis using genus-specific primer pairs (R. Chaudhry and D. S. Chandel, Abstr. Infect. Dis. Soc. Am. 39th Int. Meet., abstr. 291, 2001).
Following confirmed isolation of this organism in the fecal specimen, the patient's history was further elicited to trace the possibility of any contact with reptiles. Strikingly, our site investigations revealed that the child's father was a snake charmer, having a professional interaction with reptiles at home. Despite all efforts, the child's condition gradually worsened. Finally, the patient succumbed to this rare infection.
Discussion. Our report highlights a severe case of S. enterica subsp. arizonae gastroenteritis in an infant born to a family of snake charmers. To the best of our knowledge this is only the second case of isolation of S. enterica subsp. arizonae as a human pathogen in India and is probably the first reported case in the world of fatal S. enterica subsp. arizonae infection in an infant with microcephaly.
Reptiles, particularly snakes, are the natural reservoirs of S. enterica subsp. arizonae (20). This organism has also been responsible for severe outbreaks in turkeys and sheep (6). Though the organism is rare, several studies suggest that snakes and reptiles harbor it and transmit it to humans, resulting in gastroenteritis and systemic infections (12, 23). Such cases often occur in immunocompromised adults and young children (23). Most cases are in children less than 5 years of age. However, infants are at a particular risk (25). Reptiles are symptomless carriers of this pathogen and are probably infected through contaminated water, feed, or soil (25). Earlier findings indicate that these bacteria probably exist as commensal flora in the animal gut. Widespread contamination of the home environment and a significant number of cases occur due to pet reptiles (22). Often these infections are invasive and lead to complications such as meningitis, septicemia, and osteomyelitis (G. Makin, M. Abu Harb, A. Finn, and S. Partridge, Letter, Lancet 348:200, 1996).
S. enterica subsp. arizonae was first described by Caldwell and Ryerson in 1939 (5) and was named Salmonella dar-es-salaam (after the African city where it was first isolated). It was subsequently placed in genus Arizona, with a single species, A. hinshawii, within the tribe Salmonella based on biochemical properties (12). The placement and nomenclature of this species have constantly remained a matter of scientific debate. However, DNA homology studies helped to reclassify it as Salmonella enterica subsp. arizonae (1983). Since its first description in 1939, it was subsequently reported in snakes (14), lizards, and turtles. It appears to be more prevalent in snakes, with as many as 78.8% harboring the organism (13). Later it was also isolated from fowl, turkeys, ducks, and mammals, such as dogs, cats, monkeys, and goats (11).
It was initially considered to be a reptile pathogen; the first report of human infection came in 1944 (J. M. Croop, B. Shapiro, G. Alpert, J. M. Campos, and W. Zavod, Letter, Pediatr. Infect. Dis. 3:188, 1984). Turtle-associated salmonellosis was also reported in 1963 (7). Now it is established as a well-known pathogen in young children and in patients with impaired immunity.
S. enterica subsp. arizonae is a gram-negative bacillus and a member of the Enterobacteriaceae. The distinguishing biochemical features include the ability to ferment lactose, utilize malonate, and liquefy gelatin and the inability to grow in the presence of KCN. As many S. enterica subsp. arizonae strains ferment lactose within 48 h, they may be routinely discarded as nonpathogens if grown from feces (28). The presence of H2S is an important diagnostic clue for routine screening (8). In the present case the isolate did not ferment lactose after 24 h of incubation (a routine test in our laboratory) but had distinguishing biochemical features.
Salmonellas are well adapted to diverse niches, capably surviving 89 days in tap water, 115 days in pond water, and over 30 months in bovine manure (21). S. enterica subsp. arizonae is no exception. Reptiles get infected by this group of organisms through soil, water, or feed. The organism can also penetrate turtle eggs (9), and transovarian passage in turtles has also been reported (17).
Human infection commonly occurs in individuals with underlying disease or immunodeficiency or in infants infected by intimate contacts with reptile pets. The most common infection is gastroenteritis (20), with 73% of illnesses occurring in the first 3 months of exposure (27). The gastroenteritis associated with S. enterica subsp. arizonae is similar to other salmonellosis. It requires an incubation of 2 to 48 h and is characterized by fever, headache, abdominal pain, vomiting, and diarrhea. Stools are expulsive, copious, and frequently mixed with blood and mucus (Croop et al., letter). There is a substantial risk of dehydration due to the severity of diarrheal illness. This was observed in this case, where the child could not sustain severe dehydration, developed shock, and eventually died of cardiorespiratory arrest.
A literature survey (Table 1) yielded 17 case reports of S. enterica subsp. arizonae infection, of which 11 were children, including 4 infants. Eleven of those 17 had an underlying disease such as AIDS, systemic lupus erythematosus (SLE), cancer, or leukemia. Clinical presentations varied: four cases each with gastroenteritis, bacteremia, and osteomyelitis; two with pleural effusion; and one each with otitis media, peritonitis, meningitis, and wound infection. Most of these strains of S. enterica subsp. arizonae were sensitive to all common antibiotics.
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A carrier state is not uncommon, and a recurrence of S. enterica subsp. arizonae sepsis in immunocompromised patients after 1 year has been reported (Croop et al., letter). In addition to gastroenteritis, complications such as bacteremia, sepsis, osteomyelitis, and meningitis have also been reported (4).
We suggest that the identification of this organism with routine biochemical tests and serological reagents may be problematic. Such cases, when presented with a suggestive history, should be handled with extra care. Molecular techniques, such as a Salmonella-specific PCR, may prove a valuable tool for confirming the etiology, allowing timely institution of appropriate therapy to prevent morbidity and mortality due to this rare human pathogen.
S. enterica subsp. arizonae, though an uncommon human pathogen, is a common organism in reptiles, particularly snakes. The prevalence of human infections is probably underestimated since the gastrointestinal problems they generate were considered usually benign. However, this pathogen should be considered in the differential diagnoses of patients with sepsis and severe gastroenteritis who have a history of contact with reptiles or ingestion of snake meat preparations, e.g., as powdered capsules. Young children are at a particular risk of acquiring such infections. Therefore, proper history should be obtained in such cases. Ownership of reptiles should be discouraged, especially in households with children less then 5 years of age.
| ACKNOWLEDGMENTS |
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