[Emerging Infectious Diseases * Volume 3 * Number 4 * October - December 1997]

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Letters

Non-O157 Shiga Toxin˜Producing Escherichia coli Infections in Europe

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To the Editor: Shiga toxin—producing Escherichia coli (STEC) infections are
an important cause of severe human disease. Although most infections are
caused by strains of serogroup O157, STEC pathogenic to humans may belong
to other serogroups usually referred to as non-O157 STEC.

Recently, Tarr et al. (1) and Acheson et al. (2) described infections
attributable to STEC O103 and expressed concern that non-O157 STEC may pose
an underestimated threat to public health in the United States. In fact,
non-O157 STEC is often overlooked in clinical microbiology laboratories
because the toxigenic phenotype is not exploited to identify such
pathogens. Rather, most laboratories use sorbitol MacConkey agar and
serotyping (which cannot detect most non-O157 STEC) to identify E. coli
O157:H7.

Since the end of the 1980s, non-O157 STEC infections have caused as many as
10% to 30% of sporadic cases of hemolytic uremic syndrome (HUS) in Germany
(3), Italy (4), and the United Kingdom (5). Moreover, HUS outbreaks have
been associated with STEC O111:H- in Italy (6) and France (7).

During 1996, we observed a sudden increase in infections attributable to
STEC O103 and O26 in Germany and Italy. In our laboratory in Germany, E.
coli O103:H2 was not identified among 345 non-O157 STEC isolated between
1985 and 1995 but represented 12 (18.2%) of 66 of the non-O157 STEC
isolated during 1996. HUS developed in two infected patients.

Among cases reported to Italy's nationwide HUS surveillance system from
1988 to 1995, evidence of infection with STEC O103 or O26 was found in two
(1.5%) and nine (6.6%) of 135 cases, respectively. Since 1996, infection
with STEC O103 and O26 has been diagnosed in three (11%) and nine (33%) of
27 HUS cases, respectively.

These observations indicate that identification of non-O157 STEC should be
considered by clinical laboratories. Immunoenzymatic tests (based on either
toxin antibodies or receptors) that detect Shiga toxins produced by fecal
bacterial isolates or present in stool specimens are now available (8,9).
Use of these tests should be considered in analyzing the stools of patients
with HUS, bloody diarrhea, or painful nonbloody diarrhea, if classic
microbiologic analysis fails to yield E. coli O157:H7 or another standard
enteric pathogen, such as Campylobacter, Salmonella, or Shigella.

The sudden appearance or increase of rare non-O157 STEC in our populations
is worrisome. Most non-O157 STEC, as well as the sorbitol fermenting
O157:H- strains (10) associated with HUS in several European countries,
would be missed by laboratories using standard microbiologic detection
methods, such as sorbitol MacConkey agar screening. Because of the
considerable clinical and epidemiologic urgency, clinical microbiologists
and physicians should seek out these such pathogens in appropriate clinical
situations.

Alfredo Caprioli,* Alberto E. Tozzi,* Gianfranco Rizzoni,† and Helge Karch‡

*Istituto Superiore di Sanità, Rome, Italy; †Ospedale Pediatrico Bambino
Gesù, Rome, Italy; ‡Universitat Wuerzburg, Germany

References

  1. Tarr PI, Fouser LS, Stapleton AE, Wilson RA, Kim HH, Vary JC, Clausen
     CR. Hemolytic-uremic syndrome in a six-year-old girl after a urinary
     tract infection with Shiga-toxin-producing Escherichia coli O103:H2. N
     Engl J Med 1996;335:635-8.
  2. Acheson DWK, Wolf LE, Park CH. Escherichia coli and the
     hemolytic-uremic syndrome. N Engl J Med 1997;336:515.
  3. Bitzan M, Moebius E, Ludwig K, Muller-Wiefel DE, Heesemann J, Karch H.
     High incidence of serum antibodies to Escherichia coli O157
     lipopolysaccharide in children with the hemolytic uremic syndrome. J
     Pediatr 1991;119:380-5.
  4. Caprioli A, Luzzi I, Rosmini F, Pasquini P, Cirrincione R, Gianviti A,
     et al. Hemolytic-uremic syndrome and vero-cytotoxin-producing
     Escherichia coli infection in Italy. J Infect Dis 1992;166:154-8.
  5. Kleanthous H, Smith HR, Scotland SM, Gross RJ, Rowe B, Taylor CM,
     Milford DV. Haemolytic-uraemic syndromes in the British Isles, 1985-8:
     association with verocytotoxin producing Escherichia coli. Part 2:
     microbiological aspects. Arch Dis Child 1990;65:722-7.
  6. Caprioli A, Luzzi I, Rosmini F, Resti C, Edefonti A, Perfumo F, et al.
     Communitywide outbreak of hemolytic-uremic syndrome associated with
     non-O157 verocytotoxin-producing Escherichia coli. J Infect Dis
     1994;169:208-11.
  7. Boudaillez B, Berquin P, Mariani-Kurkdjian P, Bef D, Cuvelier B, Capek
     J, et al. Possible person-to-person transmission of Escherichia coli
     O111-associated hemolytic uremic syndrome. Pediatr Nephrol
     1997;11:36-9.
  8. Kehl KS, Havens P, Behnke CE, Acheson DWK. Evaluation of the premier
     EHEC assay for detection of Shiga-toxin-producing Escherichia coli. J
     Clin Microbiol 1997;35:2051-4.
  9. Basta M, Karmali M, Lingwood C. Sensitive receptor-specified
     enzyme-linked immunosorbent assay for Escherichia coli verocytotoxin.
     J Clin Microbiol 1989;27:1617-22.
 10. Gunzer F, Bohm H, Russmann H, Bitzan M, Aleksic S, Karch H. Molecular
     detection of sorbitol-fermenting Escherichia coli O157 in patients
     with hemolytic-uremic syndrome. J Clin Microbiol 1992;30:1807-10.

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