Among gram-negative bacteria, the emergence of resistance to extended-spectrum cephalosporins has been a major concern. It appeared initially in a limited number of bacterial species (
E. cloacae,
C. freundii,
S. marcescens, and
P. aeruginosa) that could mutate to hyperproduce their chromosomal class C β-lactamase. A few years later, resistance appeared in bacterial species not naturally producing AmpC enzymes (
K. pneumoniae,
Salmonella spp.,
P. mirabilis) due to the production of TEM- or SHV-type ESBLs (extended spectrum beta lactamases). Characteristically, such resistance has included oxyimino- (for example
ceftizoxime,
cefotaxime,
ceftriaxone, and
ceftazidime, as well as the oxyimino-monobactam
aztreonam), but not 7-alpha-methoxy-cephalosporins (
cephamycins; in other words,
cefoxitin and
cefotetan); has been blocked by inhibitors such as
clavulanate,
sulbactam or
tazobactam and did not involve
carbapenems and
temocillin. Chromosomal-mediated AmpC β-lactamases represent a new threat, since they confer resistance to 7-alpha-methoxy-cephalosporins (
cephamycins) such as
cefoxitin or
cefotetan but are not affected by commercially available β-lactamase inhibitors, and can, in strains with loss of outer membrane porins, provide resistance to carbapenems.
Extended-spectrum beta-lactamase (ESBL) Members of this family commonly express β-lactamases (e.g., TEM-3, TEM-4, and SHV-2 ) which confer resistance to expanded-spectrum (extended-spectrum) cephalosporins. In the mid-1980s, this new group of enzymes, the extended-spectrum β-lactamases (ESBLs), was detected (first detected in 1979). The prevalence of ESBL-producing bacteria have been gradually increasing in acute care hospitals. The prevalence in the general population varies between countries, e.g. approximately 6% in Germany and France, 13% in Saudi Arabia, and 63% in Egypt. ESBLs are beta-lactamases that hydrolyze extended-spectrum cephalosporins with an oxyimino side chain. These cephalosporins include
cefotaxime,
ceftriaxone, and
ceftazidime, as well as the oxyimino-monobactam
aztreonam. Thus, ESBLs confer
multi-resistance to these antibiotics and related oxyimino-beta lactams. In typical circumstances, they derive from genes for TEM-1, TEM-2, or SHV-1 by mutations that alter the amino acid configuration around the active site of these β-lactamases. A broader set of β-lactam antibiotics are susceptible to hydrolysis by these enzymes. An increasing number of ESBLs not of TEM or SHV lineage have recently been described. The ESBLs are frequently plasmid encoded. Plasmids responsible for ESBL production frequently carry genes encoding resistance to other drug classes (for example, aminoglycosides). Therefore, antibiotic options in the treatment of ESBL-producing organisms are extremely limited.
Carbapenems are the treatment of choice for serious infections due to ESBL-producing organisms, yet carbapenem-resistant (primarily
ertapenem-resistant) isolates have recently been reported. ESBL-producing organisms may appear susceptible to some extended-spectrum
cephalosporins. However, treatment with such antibiotics has been associated with high failure rates.
Types TEM beta-lactamases (class A) TEM-1 is the most commonly encountered beta-lactamase in
gram-negative bacteria. Up to 90% of ampicillin resistance in
E. coli is due to the production of TEM-1. Also responsible for the ampicillin and penicillin resistance that is seen in
Haemophilus influenzae and
Neisseria gonorrhoeae in increasing numbers. Although TEM-type beta-lactamases are most often found in
Escherichia coli and
Klebsiella pneumoniae, they are also found in other species of gram-negative bacteria with increasing frequency. The amino acid substitutions responsible for the
extended-spectrum beta lactamase (ESBL) phenotype cluster around the active site of the enzyme and change its configuration, allowing access to oxyimino-beta-lactam substrates. Opening the active site to beta-lactam substrates also typically enhances the susceptibility of the enzyme to β-lactamase inhibitors, such as clavulanic acid. Single amino acid substitutions at positions 104, 164, 238, and 240 produce the ESBL phenotype, but ESBLs with the broadest spectrum usually have more than a single amino acid substitution. Based upon different combinations of changes, currently 140 TEM-type enzymes have been described. TEM-10, TEM-12, and TEM-26 are among the most common in the United States. The term TEM comes from the name of the Athenian patient (Temoniera) from which the isolate was recovered in 1963.
SHV beta-lactamases (class A) SHV-1 shares 68 percent of its amino acids with TEM-1 and has a similar overall structure. The SHV-1 beta-lactamase is most commonly found in
K. pneumoniae and is responsible for up to 20% of the plasmid-mediated ampicillin resistance in this species. ESBLs in this family also have amino acid changes around the active site, most commonly at positions 238 or 238 and 240. More than 60 SHV varieties are known. SHV-5 and SHV-12 are among the most common.
CTX-M beta-lactamases (class A) These enzymes were named for their greater activity against
cefotaxime than other oxyimino-beta-lactam substrates (e.g.,
ceftazidime,
ceftriaxone, or
cefepime). Rather than arising by mutation, they represent examples of plasmid acquisition of beta-lactamase genes normally found on the chromosome of
Kluyvera species, a group of rarely pathogenic commensal organisms. These enzymes are not very closely related to TEM or SHV beta-lactamases in that they show only approximately 40% identity with these two commonly isolated beta-lactamases. More than 172 CTX-M enzymes are currently known. Despite their name, a few are more active on
ceftazidime than
cefotaxime. They are widely described among species of
Enterobacteriaceae, mainly
E. coli and
K. pneumoniae. Detected in the 1980s they have since the early 2000s spread and are the now the predominant ESBL type in the world. They are generally clustred into five groups based on sequencing homologies; CTX-M-1, CTX-M-2, CTX-M-8, CTX-M-9 and CTX-M-25. CTX-M-15 (belonging to the CTX-M-1 cluster) is the most prevalent CTX-M-gene. An example of beta-lactamase CTX-M-15, along with IS
Ecp1, has been found to have transposed onto the chromosome of
Klebsiella pneumoniae ATCC BAA-2146. The initials stand for "Cefotaxime-Munich".
OXA beta-lactamases (class D) OXA beta-lactamases were long recognized as a less common but also plasmid-mediated beta-lactamase variety that could hydrolyze
oxacillin and related anti-staphylococcal penicillins. These beta-lactamases differ from the TEM and SHV enzymes in that they belong to molecular class D and functional group 2d. The OXA-type beta-lactamases confer resistance to
ampicillin and
cephalothin and are characterized by their high hydrolytic activity against
oxacillin and
cloxacillin and the fact that they are poorly inhibited by
clavulanic acid. Amino acid substitutions in OXA enzymes can also give the ESBL phenotype. While most ESBLs have been found in
E. coli,
K. pneumoniae, and other
Enterobacteriaceae, the OXA-type ESBLs have been found mainly in
P. aeruginosa. OXA-type ESBLs have been found mainly in
Pseudomonas aeruginosa isolates from Turkey and France. The OXA beta-lactamase family was originally created as a phenotypic rather than a genotypic group for a few beta-lactamases that had a specific hydrolysis profile. Therefore, there is as little as 20% sequence homology among some of the members of this family. However, recent additions to this family show some degree of homology to one or more of the existing members of the OXA beta-lactamase family. Some confer resistance predominantly to ceftazidime, but OXA-17 confers greater resistance to cefotaxime and cefepime than it does resistance to ceftazidime.
Others Other plasmid-mediated ESBLs, such as PER, VEB, GES, and IBC beta-lactamases, have been described but are uncommon and have been found mainly in
P. aeruginosa and at a limited number of geographic sites. PER-1 in isolates in Turkey, France, and Italy; VEB-1 and VEB-2 in strains from Southeast Asia; and GES-1, GES-2, and IBC-2 in isolates from South Africa, France, and Greece. PER-1 is also common in multiresistant acinetobacter species in Korea and Turkey. Some of these enzymes are found in Enterobacteriaceae as well, whereas other uncommon ESBLs (such as BES-1, IBC-1, SFO-1, and TLA-1) have been found only in Enterobacteriaceae.
Treatment While ESBL-producing organisms were previously associated with hospitals and institutional care, these organisms are now increasingly found in the community. CTX-M-15-positive
E. coli are a cause of community-acquired
urinary infections in the UK, and tend to be resistant to all oral β-lactam antibiotics, as well as
quinolones and
sulfonamides. Treatment options may include
nitrofurantoin,
fosfomycin,
mecillinam and
chloramphenicol. In desperation, once-daily
ertapenem or
gentamicin injections may also be used.
Inhibitor-resistant β-lactamases Although the inhibitor-resistant β-lactamases are not ESBLs, they are often discussed with ESBLs because they are also derivatives of the classical TEM- or SHV-type enzymes. These enzymes were at first given the designation IRT for inhibitor-resistant TEM β-lactamase; however, all have subsequently been renamed with numerical TEM designations. There are at least 19 distinct inhibitor-resistant TEM β-lactamases. Inhibitor-resistant TEM β-lactamases have been found mainly in clinical isolates of
E. coli, but also some strains of
K. pneumoniae,
Klebsiella oxytoca,
P. mirabilis, and
Citrobacter freundii. Although the inhibitor-resistant TEM variants are resistant to inhibition by
clavulanic acid and
sulbactam, thereby showing clinical resistance to the beta-lactam—lactamase inhibitor combinations of
amoxicillin-
clavulanate (
co-amoxiclav),
ticarcillin-
clavulanate (
co-ticarclav), and
ampicillin/sulbactam, they normally remain susceptible to inhibition by
tazobactam and subsequently the combination of
piperacillin/tazobactam, although resistance has been described. This is no longer a primarily European epidemiology, it is found in northern parts of America often and should be tested for with complex UTI's. AmpC-type β-lactamase organisms are often clinically grouped through the acronym, "SPACE":
Serratia, Pseudomonas or
Proteus, Acinetobacter, Citrobacter, and
Enterobacter. ==Carbapenemases==