Carbapenem: Difference between revisions

Core structure of the carbapenem molecules

Carbapenems are antibiotics used for the treatment of infections known or suspected to be caused by multi-drug resistant bacteria. Their use is primarily in people who are hospitalized.

Like the penicillins and cephalosporins, they are members of the beta lactam class of antibiotics, which kill bacteria by binding to penicillin-binding proteins and inhibiting cell wall synthesis. They exhibit a broader spectrum of activity compared to cephalosporins and penicillins. Their effectiveness is less affected by many common mechanisms of antibiotic resistance than other beta lactams.

Carbapenem antibiotics were originally developed at Merck and Co. from the carbapenem thienamycin, a naturally derived product of Streptomyces cattleya.^[1][2] Concern has arisen in recent years over increasing rates of resistance to carbapenems, as there are few therapeutic options for treating infections caused by carbapenem-resistant bacteria.^[3][4][5]

Medical uses

Abdominal infections

The carbapenem ertapenem is one of several first-line agents recommended by the Infectious Disease Society of America for the empiric treatment of community-acquired intra-abdominal infections of mild-to-moderate severity. Agents with anti-pseudomonal activity, including doripenem, imipenem, and meropenem are not recommended in this population. Doripenem, imipenem, and meropenem are recommended for high-risk community-acquired abdominal infections and for abdominal infections that are hospital-acquired.^[6]

Complicated urinary tract infections

A 2015 systematic review found little evidence that would support the identification of a best antimicrobial regimen for complicated urinary tract infections, but identified three high-quality trials supporting high cure rates with doripenem, including in patients with levofloxacin-resistant E. coli infections.^[7]

Pneumonia

The carbapenems imipenem and meropenem are recommended by the American Thoracic Society and the Infectious Disease Society of America as one of several first-line therapy options for people with late-onset hospital-acquired or ventilator-associated pneumonia, especially when Pseudomonas, Acinetobacter, or extended spectrum beta-lactamase producing Enterobactericeace are suspected pathogens. Combination therapy, typically with an aminoglycoside, is recommended for Psuedomonas infections to avoid resistance development during treatment.^[8]

Carbapenems are less commonly used in the treatment of community-acquired pneumonia, as community-acquired strains of the most common responsible pathogens (Streptocuccus pneumoniae, Haemophilus influenazae, atypical bacteria, and Enterobactericeace) are typically susceptible to narrower spectrum and/or orally administered agents such as fluoroquinolones, amoxicillin, or azithromycin. Imipenem and meropenem are useful in cases in which P. aeruginosa is a suspected pathogen.^[9]

Bloodstream Infections

A 2015 meta analysis concluded that the anti-pseudomonal penicillin-beta lactamase inhibitor combination piperacillin-tazobactam gives results equivalent to treatment with a carbapenem in patients with sepsis.^[10] In 2015, the National Institute for Health and Care Excellence recommended piperacillin-tazobactam as first line therapy for the treatment of bloodstream infections in neutropenic cancer patients.^[11]

For bloodstream infections known to be due to extended spectrum beta-lactamase producing Enterobacteriaceace, carbapenems are superior to alternative treatments.^[12]

Spectrum of activity

Carbapenems exhibit broad spectrum activity against Gram-(-) bacteria and somewhat narrower activity against Gram-(+) bacteria. For empiric therapy (treatment of infections prior to identification of the responsible pathogen) they are often combined with a second drug having broader spectrum Gram-(+) activity.

Gram-(-) pathogens

The spectrum of activity of the carbapenems imipenem, doripenem, and meropenem includes most Enterobactericeace species, including Escherichia coli, Klebsiella pneumoniae, Enterobacter cloacae, Citrobacter freundii, Proteus mirabilis, and Serratia marcescens. Activity is maintained against most strains of E. coli and K. pneumoniae that are resistant to cephalosporins due to the production of extended spectrum beta-lactamases. Imipenem, doripenem, and meropenem also exhibit good activity against most strains of Pseudomonas aeruginosa and Acinetobacter species. The observed activity against these pathogens is especially valued as they are intrinsically resistant to many other antibiotic classes.^[3]

Gram-(+) pathogens

The spectrum of activity of the carbapenems against Gram-(+) bacteria is fairly broad, but not as exceptionally so as in the case of Gram-(-) bacteria. Good activity is seen against methicillin-sensitive strains of Staphylococcus species, but many other antibiotics provide coverage for such infections. Good activity is also observed for most Streptococcus species, including penicillin-resistant strains. Carbapenems are not highly active against methicillin-resistant Staphyloccus aureus or most enterococcal infections because carbapenems do not bind to the penicillin-binding protein used by these pathogens.^[3]

Other

Carbapenems generally exhibit good activity against anaerobes such as Bacteriodes fragilis. Like other beta lactam antibiotics, they lack activity against atypical bacteria, which do not have a cell wall and are thus not affected by cell wall synthesis inhibitors.^[3]

Contraindications

Carbapenems are contraindicated in patients with prior allergic reactions to beta lactam antibiotics. In addition, as the intramuscular formulations of ertrapenem and imipenem are formulated with lidocaine, the intramuscular formulation of these two drugs are contraindicated in patients with prior adverse reactions to lidocaine.^[13][14]

Adverse effects

Serious and occasionally fatal allergic reactions can occur in people treated with carbapenems.^[15] Seizures are a dose-limiting toxicity for both imipenem and meropenem.^[16] Clostridium difficile-related diarrhea may occur in people treated with carbapenems or other broad spectrum antibiotics.^[17]

Examples

Approved for clinical use

Imipenenem, the first clinically used carbapenem ,was developed at Merck and Co. It was approved for use in the United States in 1985.^[18] Imipenem is hydrolyzed in the mammalian kidney by a dehydropeptidase enzyme to a nephrotoxic intermediate, and thus is co-formulated with the dehydropeptidase inhibitor cilistatin.^[4] Imipenem is available in both intravenous^[19] and intramuscular^[20] formulations.

Meropenem is stable to mammalian dehydropeptidases and does not require co-administration of cilastin. It was approved for use in the United States in 1996. In most indications it is somewhat more convenient to administer than imipenem, 3 times a day rather than 4. Doses of less than one gram may be administered as an IV bolus, whereas imipenem is usually administered as a 20 minute to one hour infusion. Meropenem is somewhat less potent than imipenem against Gram-(+) pathogens, and somewhat more potent against Gram-(-) infections. Unlike imipenem, which produced an unacceptable rate of seizures in a phase 2 trial, meropenem is effective for the treatment of bacterial meningitis.^[21] A systematic review performed by an employee of the company that markets meropenem concluded that it provides a higher bacterial response and lower adverse event rates than imipenem in people with severe infections, but no difference in mortality rate.^[22]

Ertapenem is administered once daily as an intravenous infusion or intramuscular injection. It lacks useful activity against the P. aeruginosa and Acetinobacter species, both of which are important causes of hospital-acquired infections.^[23]

Doripenem has a spectrum of activity very similar to that of meropenem. Its greater stability in solution allows the use of prolonged infusions and it is somewhat less likely to produce seizures than other carbapenems.^[24]

Panipenem/betamipron (Japanese approval 1993)

Biapenem (Japanese approval 2001) exhibits similar efficacy and adverse event rates as other carbapenems.^[25]

Unapproved/experimental

• Razupenem (PZ-601)
  • PZ-601 is a carbapenem antibiotic currently being tested as having a broad spectrum of activity including strains resistant to other carbapenems. Despite early Phase II promise, Novartis (who acquired PZ-601 in a merger deal with Protez Pharmaceuticals) recently dropped PZ-601, citing a high rate of adverse events in testing.^[26]
• Tebipenem
  • Tebipenem is the first carbapenem whose prodrug form, the pivalyl ester, is orally available.^[27]
• Lenapenem
• Tomopenem
• Thienamycin (thienpenem) the first discovered carbapenem

Spectrum of use

These agents have the broadest antibacterial spectrum compared to other β-lactam classes such as penicillins and cephalosporins. In addition, they are generally resistant to the typical bacterial enzyme, β-lactamase, which is one of the principal β-lactam resistance mechanisms of bacteria. Carbapenems circumvent β-lactamase by binding it with high affinity and acylating the enzyme, rendering it inactive.^[28] Carbapenems are active against both Gram-positive and Gram-negative bacteria, and anaerobes, with the exception of intracellular bacteria (atypicals), such as the Chlamydiae. Carbapenems also are thus far the only β-lactams capable of inhibiting l,d-transpeptidases ^[29]

Emergence of bacterial resistance

In the United States and United Kingdom, strains of carbapenem-resistant enteric bacteria have been isolated from patients having received recent medical care in Pakistan, Bangladesh, and India.^[30] These strains carry a gene called New Delhi metallo-β-lactamase (shortened NDM-1) that is responsible for the production of a metallo-β-lactamase enzyme that hydrolyses carbapenem.^[31][32] A clinical isolate of E. coli from the sputum sample of a patient admitted to a Beijing hospital was found to show unusual resistance to carbapenem that does not rely on the presence of carbapenemase. The isolate was determined to have four separate mutations to acquire the resistance to carbapenems. Two mutations removed the outer membrane proteins OmpF and OmpC to prevent the antibiotics from reaching the PBPs (penicillin binding proteins) in the inner membrane.^[28] A regulator gene marR was mutated and a normally non-translated membrane protein yedS was expressed; both were demonstrated to have effects on the ability of this strain of E.coli to resist carbapenems. The bacteria also increased the expression of a multidrug efflux pump.^[33][34]

In 2014, researchers in Canada found carbapenem-resistant bacteria in a sample of frozen squid sold at a Chinese grocery store in Saskatoon, Canada. The squid reportedly originated in South Korea and was purchased in January 2014. University of Saskatchewan researcher Joseph Rubin called the find "extremely disturbing".^[35]

Structure

In terms of structure, the carbapenems are very similar to the penicillins (penams), but the sulfur atom in position 1 of the structure has been replaced with a carbon atom, and an unsaturation has been introduced—hence the name of the group, the carbapenems.

Biosynthesis

The carbapenems are thought to share their early biosynthetic steps in which the core ring system is formed. Malonyl-CoA is condensed with glutamate-5-semialdehyde with concurrent formation of the five-membered ring. Next, a β-lactam synthetase uses ATP to form the β-lactam and the saturated carbapenam core. Further oxidation and ring inversion provides the basic carbapenem.

Administration

Due to their expanded spectra, the desire to avoid generation of resistance and the fact that, in general, they have poor oral bioavailability, they are administered intravenously in hospital settings for more serious infections. However, research is underway to develop an effective oral carbapenem.^[36]

See also

• Faropenem is closely related, but it is a penem, not a carbapenem.^[37]
• Drug resistance

References

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External links

• Structure Activity Relationships "Antibacterial Agents; Structure Activity Relationships," André Bryskier MD; beginning at pp131
• Page 2: Ertapenem vs. Meropenem: Equivalency of Clinical and Microbiological Outcomes. 2010