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S. pneumoniae in Children with Chronic Kidney Disease | CDC EID

EID Journal Home > Volume 17, Number 1–January 2011
Volume 17, Number 1–January 2011
Streptococcus pneumoniae in Urinary Tracts of Children with Chronic Kidney Disease

Irene Burckhardt Comments to Author and Stefan Zimmermann

Author affiliation: University of Heidelberg, Heidelberg, Germany

Suggested citation for this article

Streptococcus pneumoniae is not commonly considered an agent of urinary tract infections. We report 3 children with urinary tract abnormalities who had high numbers of S. pneumoniae in their urine (>104 CFU/mL) and varying clinical symptoms.

The role of Streptococcus pneumoniae as an agent of septicemia, pneumonia, and meningitis is well known (1,2). However, published reports of urinary tract infection (UTI) associated with S. pneumoniae are scarce, and S. pneumoniae generally is not considered an agent of UTI in either adults or children (3,4). We report 3 children with urinary tract abnormalities and high levels of S. pneumoniae in their urine.
Case Reports

In June 2008, a 23-month-old boy (case-patient 1) received care for fever and clinical signs of a UTI at the emergency department of the University of Heidelberg Children's Hospital. He did not show signs of respiratory disease. His medical history was remarkable for bilateral cystic–dysplastic kidneys, a congenital urethral valve (surgery in October 2006), terminal kidney insufficiency and peritoneal dialysis since 2006, renal anemia, hyperparathyroidism, hyperphosphatemia, microcephalus, and failure to thrive. Blood was drawn for culture, and a urine sample was taken. After 9 hours of incubation, the blood culture was positive for S. pneumoniae, and the urine grew 105 CFU/mL of S. pneumoniae. Blood leukocyte levels were elevated (20 cells/nL [normal <13 cells/nL]), as were leukocyte levels in the urine (568 cells/μL [normal <4 cells/μL]). A throat swab was negative for S. pneumoniae. The boy's infection was treated successfully, and he was discharged 4 days after admission. Further analysis showed that both isolates were serotype 15B and were fully susceptible to all antibacterial drugs tested (Table 1).

In September 2009, a 12-year-old boy (case-patient 2) sought care at the nephrology department of the University of Heidelberg Children's Hospital for his yearly control examination 7 years after kidney transplantation. He had no clinical signs of current infection. His medical history was remarkable for kidney insufficiency, congenital obstruction and reflux in the urethral valve, kidney transplantation in 2002, ileocecal pouch, chronic transplant nephropathy, metabolic acidosis, hypertension, and renal anemia. A urine sample showed 105 CFU/mL S. pneumoniae and 103 CFU/mL Enterobacteriaceae. Urine leukocyte levels were slightly elevated (16 cells/μL). Further analysis showed that S. pneumoniae was serotype 34 and fully susceptible to all antibacterial drugs tested (Table 1).

In November 2009, a 7-year-old girl (case-patient 3) was sent to the emergency department of the University of Heidelberg Children's Hospital by her pediatrician because of abnormal results in a control urine sample 4 weeks after percutaneous nephrolithoapraxia and concrement removal. She was known to have cystinuria and had already undergone extracorporeal shock wave treatment with concrement removal in 2004. Her temperature was slightly elevated (37.5°C), but she had no dysuria or pain. Urinalysis showed elevated leukocyte levels (158 cells/μL), and 104 CFU/mL S. pneumoniae could be grown. Because of the mild symptoms, no antimicrobial drug treatment was started. Further analysis showed that the isolate was a 19F serotype (Table 1).

For each patient, urine was routinely cultured as follows: 2 samples of 1 μL each were placed on a 5% sheep-blood agar plate and a MacConkey agar plate. chromID CPS medium (bioMérieux, Nürtingen, Germany) was injected with 10 μL of urine. All plates were incubated for 18–24 h at 36°C ± 1°C in ambient air (5). Susceptibility testing was performed by using the BD Phoenix Automated Microbiology System with SMIC/ID panels (Becton Dickinson, Heidelberg, Germany).
Discussion and Conclusions

The literature on urinary tract infections with S. pneumoniae is scarce. In 1980, Green and Selinger described a patient with a soft tissue abscess and a UTI caused by serotype 3 (6). In 2004, Dufke et al. described a patient with pyelonephritis and urosepsis caused by serotype 6A (7). In 1988, Nguyen and Penn determined the frequency of pneumococci in urine specimens from adults and found 38 (0.18%) of 22,744 samples positive for S. pneumoniae (4). Similarly, Miller et al. determined that the frequency of pneumococci in urine specimens from children was even lower: 43 (0.08%) of 53.499 samples (3). Of 28 patients, for whom clinical data were available, 5 had dysuria, and 2 had pyuria. Three asymptomatic children had medical histories of genitourinary abnormalities; 6 asymptomatic children had medical histories of recurrent UTI with Enterobacteriaceae. The serotypes and antibiotic susceptibilities of the respective isolates were not reported.

A UTI is defined as bacteriuria (>105 CFU/mL in adults, >104 CFU/mL in children) of 1 uropathogen and typical clinical signs, i.e., dysuria and urgency. Depending on the age of the patient, clinical signs might be less typical, especially in children <2 years of age. Generally pyuria is present (8,9). By contrast, asymptomatic bacteriuria is defined as a uropathogen (>105 CFU/mL in adults, >104 CFU/mL in children) without pyuria (<10 leukocytes/μL) (9).

Applying these criteria to the 3 cases in this report yields the following results. Assuming that S. pneumoniae is a uropathogen, case 1 is a UTI accompanied by septicemia. No other focus of infection with S. pneumoniae was apparent or could be identified. We believe this is an ascending UTI in a boy with known oliguria from bilateral cystic–dysplastic kidneys. Because case-patient 3 showed only mild symptoms, diagnosis of UTI is not obligatory. Nevertheless, it is not a mere pneumococcosuria because of the high numbers of leukocytes in the urine (158 cells/μL).

Case 2 is more difficult to classify. The episode described might be pneumococcosuria because the leukocyte level is not high; nevertheless, it is above normal. Reassessment of all microbiological data of case-patient 2 indicated that since 2005 we have received 29 different urine samples. In March 2007, we had already identified S. pneumoniae (104 CFU/mL) and pyuria (92 CFU/μL). Additionally, 104 CFU/mL Proteus mirabilis had been present and considered the cause of the pyuria; 11 of 27 samples had contained α-hemolytic streptococci >103 CFU/mL (Table 2). Unfortunately, no test to differentiate between pneumococci and the other α-hemolytic streptococci was originally performed on these bacteria. Therefore, we can only speculate whether at least some of these samples contained S. pneumoniae. Taking these facts into account, we believe that this might be a case of bacterial persistence according to the criteria described by Chang and Shortliffe (cultures ± same organism) (8).

Reassessment of all available laboratory data on case-patient 1 showed that we received 3 urine samples before the described episode and 8 afterward. In none of the samples did we find S. pneumoniae or α-hemolytic streptococci. From case-patient 3 we did not receive any other material than described.

Further analysis of the S. pneumoniae isolates indicated that all 3 children were affected by different serotypes. Therefore, we do not have an indication that a single serotype has a predilection for the urinary tract. In theory, 2 cases could have been avoided by vaccination, i.e., case 3 (serotype 19F) and case 1 (serotype 15B). However, case-patient 3 was 4 years of age when the routine vaccination program aimed at children <2 years of age started in Germany in 2006. Because no catch-up program existed, this child was never vaccinated against pneumococci. Case-patient 1 was regularly vaccinated with heptavalent pneumococcal conjugate vaccine in 2006–2007 but was just 23 months old at disease onset disease, i.e., 1 month too young to be eligible for the 23-valent pneumococcal polysaccharide vaccine. Case-patient 2 is not yet vaccinated against pneumococci. Thus, we suggest that S. pneumoniae be added to the potential UTI-causing pathogens in children with urinary tract abnormalities.

Serotypes and bile solubility were determined at the National Reference Center for Streptococci, Aachen, Germany.

Dr Burckhardt is a consultant for microbiology, virology, and epidemiology of infectious diseases who works at the Department for Infectious Diseases, Microbiology and Hygiene at the University of Heidelberg, Germany. Her main interest is the clinical manifestation and epidemiology of pneumococcal diseases and identification of risk factors for pneumococcal diseases.

Dr Zimmermann is a consultant for microbiology, virology, and epidemiology of infectious diseases. He is the senior physician at the Department for Infectious Diseases, Microbiology and Hygiene at the University of Heidelberg, Germany. His primary research interests include leptospirosis and leishmaniasis.


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Table 1. Characteristics of Streptococcus pneumoniae isolates in 3 children with chronic kidney disease, Germany, 2005–2010
Table 2. Results of urine samples of 12-year-old boy with chronic kidney disease, Germany, 2005–2010

Suggested Citation for this Article

Burckhardt I, Zimmermann S. Streptococcus pneumoniae in urinary tracts of children with chronic kidney disease. Emerg Infect Dis [serial on the Internet]. 2011 Jan [date cited]. http://www.cdc.gov/EID/content/17/1/120.htm

DOI: 10.3201/eid1701.100895

Comments to the Authors

Please use the form below to submit correspondence to the authors or contact them at the following address:

Irene Burckhardt, Department for Infectious Diseases, Microbiology and Hygiene Im Neuenheimer Feld 324, D-69115 Heidelberg, Germany;
email: irene.burckhardt@med.uni-heidelberg.de

S. pneumoniae in Children with Chronic Kidney Disease | CDC EID

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