To the Editor: The CTX-M–type β-lactamases are non-TEM and non-SHV plasmid-mediated, class A, extended-spectrum β-lactamases (ESBLs). The CTX-M–type β-lactamases have recently emerged as the most common type of ESBLs, with a global distribution (1). In contrast, the CTX-M–type ESBLs are rarely reported in the United States and have not been identified in pathogens isolated from infected patients with gastroenteritis.

We screened 637 Salmonella and 126 Shigella isolates, collected in the state of Washington during 2003–2004, for CTX-M–type β-lactamases. Of these, 60 Salmonella isolates that exhibited an ESBL phenotype were further characterized by PCR for TEV, SHV, CTM-X, and CMY. All were positive for the CMY-2 or TEM-1 β-lactam genes. One Shigella sonnei isolate (WA7593), cultured from a fecal specimen in August 2004, tested positive with an ESBL confirmatory disk diffusion panel (ceftazidime 24 mm, ceftazidime/clavulanate 32 mm, cefotaxime 14 mm, and cefotaxime/clavulanate 34 mm; [2]). The patient had recently traveled to Pakistan and likely became ill there and returned to the United States while still sick. The transfer of extended-spectrum cephalosporin resistance was tested by conjugation to Escherichia coli J53 azi^R (3). The MIC for S. sonnei WA7593 and its transconjugant, WA7593TC1, were tested by using the E-test (AB Biodisk, Solna, Sweden). Both strains were resistant to cefotaxime and susceptible to ceftazidime and showed almost the same antimicrobial susceptibility patterns as β-lactam antimicrobial drugs (Table).

The type of ESBL produced by these strains was determined by using PCR specific for TEM and CTX-M (4,5). Both strains were PCR positive for TEM and CTX-M. The TEM type PCR products were then sequenced and identified as TEM-1; no variation was found on the promoter region of bla_TEM-1. The entire sequence of bla _CTX-M from WA7593 was then sequenced (1), and the product showed 100% homology with bla_CTX-M-15 (GenBank accession no. AY960984). The mobile element associated with the transfer of bla_CTX-M-15 was investigated by sequencing the flanking regions. PCRs were performed with primers from the internal regions of bla _CTX-M gene and primers for insertion sequences ISEcp1 and IS903 (4,5). Positive PCR products were obtained with primers ISEcp1F and CTX2 (943 bp); no amplified product was produced with primers CTX1 and IS903R. Sequencing of a 943-bp amplicon showed that bla_CTX-M15 was flanked upstream by an ISEcp1-like element.

The presence of an integron in S. sonnei WA7593 and WA7593TC1 was investigated by using integron-specific primers hep35 and hep36 (2). Only S. sonnei WA7593 produced a PCR product. This finding suggests that the transmission of bla_CTX-M15 is not by integron-mediated transfer. A further 162 Shigella spp. and 260 Salmonella spp. isolated from 2003 through 2005 were also screened for ESBL production; no further isolates were identified.

The presence of a CTX-M–type, ESBL-producing isolate is rarely reported in the United States. The only other reference was from a multistate study in 2001–2002 that identified CTX-M type from E. coli isolates from urine, sputum, and blood (6). No further reports about CTX-M–producing organisms have been disseminated. Our investigation suggests that CTX-M–type ESBLs may spread throughout the United States through infected travelers. This finding is notable because S. sonnei is a common enteric pathogen. Our results further emphasize that travelers from others parts of the world can introduce highly mobile and clinically important resistance mechanisms into the community. The spread of CTX-M ESBLs may be faster and more widespread than previously thought; therefore, CTX-M type should be taken seriously as a surveillance target in the United States, especially in patients with a history of travel outside North America.