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Wikipedia

Cefoxitin

December 15, 2023

Cefoxitin is a second-generation cephamycin antibiotic developed by Merck & Co., Inc. from Cephamycin C in the year following its discovery, 1972. It was synthesized in order to create an antibiotic with a broader spectrum.[3] It is often grouped with the second-generation cephalosporins.[4] Cefoxitin requires a prescription and as of 2010 is sold under the brand name Mefoxin by Bioniche Pharma, LLC. The generic version of cefoxitin is known as cefoxitin sodium.[5][6]

Cefoxitin
Clinical data
Trade namesMefoxin, Renoxitin, others[1]
AHFS/Drugs.comMonograph
MedlinePlusa682737
License data
Pregnancy
category
  • AU: B1
Routes of
administration		Intravenous
ATC code
Legal status
Legal status
Pharmacokinetic data
Metabolismminimal
Elimination half-life41-59 min
Excretion85% urine
Identifiers
  • (6R,7S)-3-(carbamoyloxymethyl)-7-methoxy-
    8-oxo-7-[(2-thiophen-2-ylacetyl)amino]-5-thia-
    1-azabicyclo[4.2.0]oct-2-ene-2-carboxylic acid
CAS Number
  • 35607-66-0 Y
PubChem CID
  • 441199
DrugBank
  • DB01331 N
ChemSpider
  • 389981 Y
UNII
  • 6OEV9DX57Y
KEGG
  • D02345 N
  • as salt: D00913 N
ChEBI
  • CHEBI:209807 N
ChEMBL
  • ChEMBL996 N
CompTox Dashboard (EPA)
  • DTXSID1022764
ECHA InfoCard100.047.841
Chemical and physical data
FormulaC16H17N3O7S2
Molar mass427.45 g·mol−1
3D model (JSmol)
  • Interactive image
Melting point149 to 150 °C (300 to 302 °F) (dec.)
  • O=C2N1/C(=C(\CS[C@@H]1[C@]2(OC)NC(=O)Cc3sccc3)COC(=O)N)C(=O)O
  • InChI=1S/C16H17N3O7S2/c1-25-16(18-10(20)5-9-3-2-4-27-9)13(23)19-11(12(21)22)8(6-26-15(17)24)7-28-14(16)19/h2-4,14H,5-7H2,1H3,(H2,17,24)(H,18,20)(H,21,22)/t14-,16+/m1/s1 Y
  • Key:WZOZEZRFJCJXNZ-ZBFHGGJFSA-N Y
 NY (what is this?)  (verify)

History and discovery edit

Groups of researchers at Merck and Lilly discovered Cephamycin C while looking at penicillin-producing bacteria. This followed their discovery of erythromycin, another antibiotic.[7] Cephamycin C was the first cephem discovered but while it was highly resistant to several beta-lactamases, as is its derivative cefoxitin, it was almost only effective against Gram negative bacteria.[7] The scientists used chemically modified the compound to give cefoxitin, so titled due to its semi-synthetic nature. This new modification broadened its spectrum to include Gram positive bacteria. More than 300 modifications were made to it and tested on the cephalosporin base with methoxy groups at the 7-alpha position. Yet only cefoxitin retained its previous effectiveness against Gram negative bacteria, developed effectiveness against Gram positive bacteria, and resisted breakdown by beta-lactamase.[8]

Cefoxitin, and the cephamycin family as a whole, served as a branching point and impulsed the discovery of more classes of beta-lactams. This is in part due to their primary and early discovery in the broths studied.[7]

Mechanism edit

Cefoxitin is a beta-lactam antibiotic which binds to penicillin binding proteins, or transpeptidases. By binding to PBPs, cefoxitin prevents the PBPs from forming the cross-linkages between the peptidoglycan layers that make up the bacterial cell wall, thereby interfering with cell wall synthesis. It is a strong beta-lactamase inducer, as are certain other antibiotics (such as imipenem). However, cefoxitin is a better substrate than imipenem for beta-lactamases.[9]

Microbiological resistance edit

In the presence of cefoxitin, bacteria that make beta-lactamases will increase their production and secretion to cleave the beta lactam ring. As a cephamycin, cefoxitin is highly resistant to hydrolysis by some beta-lactamases, in part due to the presence of the 7-alpha-methoxy functional group (see skeletal formula above).[10][11][12][13]

Another more efficient form of resistance to cefoxitin is provided by the mecA gene in bacteria. This gene codes for an alternative penicillin binding protein, PBP2a. This PBP has a lower binding affinity for penicillin-based antibiotics such as cefoxitin and will continue to cross-link the peptidoglycan layers of the cell wall even in the presence of the beta-lactam antibiotics. MRSA, or methicillin-resistant Staphylococcus aureus is a strain that has acquired resistance to cefoxitin via this gene.[14] For the purposes of detecting bacterial strains with the mecC gene, which like mecA codes for a different PBP, cefoxitin is more reliable than oxacillin because mecC does not correlate as strongly with oxacillin resistance.[15]

Spectrum of bacterial susceptibility edit

Cefoxitin's spectrum of in vitro antimicrobial activity includes a broad range of gram-negative and gram-positive bacteria, including anaerobes. It is inactive against most strains of Pseudomonas aeruginosa and many strains of Enterobacter cloacae. Staphylococci that are resistant to methicillin and oxacillin should also be considered clinically resistant to cefoxitin even if they test susceptible by in vitro methods.[2]

Major bacterial strains susceptible to cefoxitin include:[10]

Major bacteria resistant to cefoxitin include:[10]

Replacement and substitution edit

In a 2005 study, Fernandes et al. determined that cefoxitin serves as an appropriate replacement for methicillin in determining if some bacteria display methicillin resistance.[16] Likewise, Funsun et al. found in a 2009 study that cefoxitin disk assays correctly identified all 60 mecA-positive Staphylococcus aureus, or MRSA isolates, to be resistant to cefoxitin.[17]

Due, in part, to the unavailability of methicillin in the United States, cefoxitin has replaced methicillin for disk diffusion tests, which determine the sensitivity of a bacterial specimen to a given antibiotic.[18] Cefoxitin also yields more accurate results for disk diffusion tests.[18] Interpretive criteria for determining susceptibility to cefoxitin via disk diffusion are greater than or equal to 22mm resulting in a "susceptible" result for Staphylococcus aureus and greater than or equal to 25mm for coagulase-negative staphylococci to be considered susceptible.[18]

The following are susceptibility data for several medically significant microorganisms, measured by minimum inhibitory concentration, which is an alternative, liquid medium test for susceptibility.

  • Escherichia coli: 0.2 μg/ml – 64 μg/ml[citation needed]
  • Haemophilus influenzae: 0.5 μg/ml – 12.5 μg/ml[citation needed]
  • Streptococcus pneumoniae: 0.2 μg/ml – 1 μg/ml[19]

Uses in medicine edit

Cefoxitin is sold in three major IV doses, 1g, 2g, and 10g.[20] It is usually given to adults every six to eight hours in 1g or 2g doses.[21] Cefoxitin may interfere with tests detecting urine glucose and result in a false positive.[22] As with any antibiotic, it should not be given to patients who are allergic to it.[22]

Cefoxitin is used to treat:[23][24][25][26]

  • Skin infections, primarily due to Staphylococcus
  • Urinary tract infections
  • Bronchitis
  • Tonsillitis
  • Ear infections
  • Bacterial pneumonia
  • Sepsis
  • Bone and joint infections
  • Abdominal infections and abscesses
  • Perineum injuries
  • Pelvic inflammatory disease
  • Gonorrhea
  • Infections caused by susceptible bacteria mentioned earlier

Cefoxitin has many other uses; it may be given prior to surgery to prevent the development of surgical wound infections,[27] and when used in third and fourth degree perineal injuries in women after giving vaginal birth, cefoxitin decreases infection rate at two and six weeks.[28] However, the earlier and more times a child is exposed to cefoxitin, as with early and multiple exposure to many antibiotics, the greater the likelihood of developing inflammatory bowel disease later in life. This may be due in part to a decreased variety of microorganisms in the digestive system.[29]

It is also used to treat pelvic inflammatory disease, because it is a broad spectrum antibiotic. For outpatient treatment, oral antibiotics or those with less frequent dosing may be prescribed.[30] As an effective alternative to penicillin and spectinomycin, and replacement for methicillin, cefoxitin is used to treat gonorrhea in both men and women with few side effects.[31]

Side effects edit

Side effects for cefoxitin are regarded as mild.[31] Common side effects include:

  • local tenderness or pain at the site of injection
  • skin color change, mild diarrhea
  • mild nausea
  • headache
  • loss of appetite
  • vaginal discharge and itching
  • swelling of feet or legs.[32][26][21]

While cefoxitin has not been associated with alcohol incompatibility like other members of the second generation cephalosporins class, it has been with a higher risk of coagulopathy, a bleeding disorder.[7]

This is not a comprehensive list and not intended to provide medical advice. If any of the previous side effects are severe, or if an allergic reaction takes place immediately contact your doctor.

Notable drug interactions edit

Contraindications edit

A contraindication means that the drug in question should not be used under particular circumstances. For cefoxitin, this includes patients who are hypersensitive to cephalosporin antibiotics.[33][34]

Patients with colitis, kidney disease, or liver disease are also advised not to take cefoxitin.[35] However, some drug databases will considers the diseases means for caution rather than contraindications.[36]

Major or Severe edit

Aside from the above-mentioned contraindications and diseases which require monitoring by a doctor, the live cholera and live typhoid vaccines are known to have a severe interaction with cefoxitin.[37][38]

Individuals on a low sodium diet, undergoing dialysis, or who have experienced seizures, particularly following antibiotic therapy, should also consult their physician prior to taking cefoxitin.[39]

Moderate edit

Only take additional antibiotics, anticoagulants and blood thinners under doctor supervision.[38] Cefoxitin may decrease the effectiveness of hormonal birth control. This increases the risk for pregnancy and a medical consult will help determine whether backup birth control methods should be used.[40]

Minor edit

Minor drug interactions do not usually require a change in treatment. Your doctor may monitor specific events, such as bleeding, while taking cefoxitin. Two such minor interactions occur between cefoxitin and heparin[41] as well as genistein.[42]

Pharmacodynamic and pharmacokinetic data edit

Pharmocokinetic and pharmacodynamic data for cefoxitin are, as of 2013, considered limited and outdated. A few relatively recent studies have attempted to remedy that.

One such study was by the Hôpitaux de Paris in collaboration with the French Ministry of Health.[43] However, while the clinical trials were completed in 2015, no study data have been published.[44] The expected results from using cefoxitin over carbapenems, another type of antibiotic with a wider bacterial spectrum, included effective treatment of E. coli produce extended spectrum beta-lactamase, less selective pressure on the GI tract which better maintains balanced flora, and a lower treatment cost.[43]

This followed a 2012 French study on the same E. coli strain with CTX-M-15 extended release beta-lactamase.[45] Lepeule et al. determined that in mice, the ideal pharmacodynamic target of fT>MIC=33%, where MIC is the minimum inhibitory concentration, was obtained with 200 mg/kg every four hours.[45] The fT>MIC (%) was increased by 11% when the administration frequency was increased from every four hours to every three hours.[45] This implied that increasing the frequency might yield similar results in humans. The study also found no significant difference between the effectiveness of carbapenems and cefoxitin and suggested that cefoxitin can be used as an alternative treatment for CTX-M producing E. coli to carbapenems such as imipenem and ertapenem.[45]

References edit

  1. ^ "Cefoxitin International". Drugs.com. 2 November 2020. Retrieved 8 November 2020.
  2. ^ a b "Cefoxitin- cefoxitin sodium powder, for solution". DailyMed. 10 June 2020. Retrieved 8 November 2020.
  3. ^ Gootz TD (January 1990). "Discovery and development of new antimicrobial agents". Clinical Microbiology Reviews. 3 (1): 13–31. doi:10.1128/cmr.3.1.13. PMC 358138. PMID 2404566.
  4. ^ Levy SB (2013-11-11). The Antibiotic Paradox: How Miracle Drugs Are Destroying the Miracle. Springer. ISBN 9781489960429.
  5. ^ "Orange Book: Approved Drug Products with Therapeutic Equivalence Evaluations". www.accessdata.fda.gov. Retrieved 2017-05-04.
  6. ^ "Supplement Approval" (PDF). Food and Drug Administration. Department of Health and Human Services.
  7. ^ a b c d Dougherty TJ, Pucci MJ (2011-12-21). Antibiotic Discovery and Development. Springer Science & Business Media. ISBN 9781461413998.
  8. ^ Sneader W (2005-06-23). Drug Discovery: A History. John Wiley & Sons. ISBN 9780471899792.
  9. ^ Phillips I, Shannon K (1993). "Importance of beta-lactamase induction". European Journal of Clinical Microbiology & Infectious Diseases. 12 (Suppl 1): S19-26. doi:10.1007/bf02389873. PMID 8477758. S2CID 22945967.
  10. ^ a b c Moellering RC, Dray M, Kunz LJ (September 1974). "Susceptibility of clinical isolates of bacteria to cefoxitin and cephalothin". Antimicrobial Agents and Chemotherapy. 6 (3): 320–3. doi:10.1128/aac.6.3.320. PMC 444644. PMID 15830480.
  11. ^ Shaikh S, Fatima J, Shakil S, Rizvi SM, Kamal MA (January 2015). "Antibiotic resistance and extended spectrum beta-lactamases: Types, epidemiology and treatment". Saudi Journal of Biological Sciences. Special issue: Biological Aspects of Global Health Issues. 22 (1): 90–101. doi:10.1016/j.sjbs.2014.08.002. PMC 4281622. PMID 25561890.
  12. ^ Onishi HR, Daoust DR, Zimmerman SB, Hendlin D, Stapley EO (January 1974). "Cefoxitin, a semisynthetic cephamycin antibiotic: resistance to beta-lactamase inactivation". Antimicrobial Agents and Chemotherapy. 5 (1): 38–48. doi:10.1128/aac.5.1.38. PMC 428916. PMID 4599124.
  13. ^ Fonzé E, Vanhove M, Dive G, Sauvage E, Frère JM, Charlier P (February 2002). "Crystal structures of the Bacillus licheniformis BS3 class A beta-lactamase and of the acyl-enzyme adduct formed with cefoxitin" (PDF). Biochemistry. 41 (6): 1877–85. doi:10.1021/bi015789k. PMID 11827533.
  14. ^ Paterson GK, Harrison EM, Holmes MA (January 2014). "The emergence of mecC methicillin-resistant Staphylococcus aureus". Trends in Microbiology. 22 (1): 42–7. doi:10.1016/j.tim.2013.11.003. PMC 3989053. PMID 24331435.
  15. ^ Skov R, Larsen AR, Kearns A, Holmes M, Teale C, Edwards G, Hill R (January 2014). "Phenotypic detection of mecC-MRSA: cefoxitin is more reliable than oxacillin". The Journal of Antimicrobial Chemotherapy. 69 (1): 133–5. doi:10.1093/jac/dkt341. PMID 24038776.
  16. ^ Fernandes CJ, Fernandes LA, Collignon P (April 2005). "Cefoxitin resistance as a surrogate marker for the detection of methicillin-resistant Staphylococcus aureus". The Journal of Antimicrobial Chemotherapy. 55 (4): 506–10. doi:10.1093/jac/dki052. PMID 15743899.
  17. ^ Akcam FZ, Tinaz GB, Kaya O, Tigli A, Ture E, Hosoglu S (2009-01-01). "Evaluation of methicillin resistance by cefoxitin disk diffusion and PBP2a latex agglutination test in mecA-positive Staphylococcus aureus, and comparison of mecA with femA, femB, femX positivities". Microbiological Research. 164 (4): 400–3. doi:10.1016/j.micres.2007.02.012. PMID 17481872.
  18. ^ a b c "Laboratory Testing for MRSA". CDC.gov. CDC. Retrieved 9 May 2017.
  19. ^ "Cefoxitin Susceptibility and Minimum Concentration (MIC) Data" (PDF). Toku-e.
  20. ^ "Mefoxin Drug Information, Indications & Other Medicaments". www.catalog.md. Retrieved 2017-04-28.
  21. ^ a b Cunha J. "Common Side Effects of Mefoxin (Cefoxitin) Drug Center - RxList". RxList. Retrieved 2017-05-02.
  22. ^ a b "Mefoxin tablet :: Generic, Side effects, Interchangeable drugs, etc." edudrugs.com. Retrieved 2017-04-28.
  23. ^ "Mefoxin Indication, Action of Mefoxin, Interactions." edudrugs.com. Retrieved 2017-04-28.
  24. ^ "Cefoxitin Mefoxitin 1g". Marzan Pharma Corporation. Retrieved 2017-04-28.[permanent dead link]
  25. ^ "Méfoxin generic. Price of méfoxin. Uses, Indications and Description". ndrugs. Retrieved 2017-04-28.
  26. ^ a b "Cefoxitin (By injection) - National Library of Medicine". PubMed Health. U.S. National Library of Medicine. 1 April 2017. Retrieved 2017-04-28.
  27. ^ Bratzler DW, Houck PM (April 2005). "Antimicrobial prophylaxis for surgery: an advisory statement from the National Surgical Infection Prevention Project". American Journal of Surgery. 189 (4): 395–404. doi:10.1016/j.amjsurg.2005.01.015. PMID 15820449. S2CID 6496587.
  28. ^ Buppasiri P, Lumbiganon P, Thinkhamrop J, Thinkhamrop B (October 2014). "Antibiotic prophylaxis for third- and fourth-degree perineal tear during vaginal birth". The Cochrane Database of Systematic Reviews (10): CD005125. doi:10.1002/14651858.CD005125.pub4. PMC 10542915. PMID 25289960.
  29. ^ Kronman MP, Zaoutis TE, Haynes K, Feng R, Coffin SE (October 2012). "Antibiotic exposure and IBD development among children: a population-based cohort study". Pediatrics. 130 (4): e794-803. doi:10.1542/peds.2011-3886. PMC 4074626. PMID 23008454.
  30. ^ Sexually transmitted diseases :treatment guidelines. Atlanta, GA: U.S. Department of Health and Human Services. hdl:2027/uiug.30112023431809.
  31. ^ a b Survey of research on sexually transmitted diseases /. Atlanta, Ga. 1985-01-01. hdl:2027/umn.31951000325661b.
  32. ^ "Méfoxin Side effects, Contraindications". ndrugs. Retrieved 2017-05-02.
  33. ^ "Mefoxin (Cefoxitin) Drug Information: Overdosage and Contraindications - Prescribing Information at RxList". RxList. Retrieved 2017-05-29.
  34. ^ "Mefoxin (Cefoxitin) - Drug Interactions, Contraindications, Other Rx Info". www.druglib.com. Retrieved 2017-05-29.
  35. ^ "Contraindications for Cefoxitin Vial". WebMD. Retrieved 2017-05-29.
  36. ^ "cefoxitin Contraindications and Cautions - Epocrates Online". online.epocrates.com. Retrieved 2017-05-29.
  37. ^ "Cefoxitin Drug Interactions". Drugs.com. Retrieved 2017-05-29.
  38. ^ a b "Cefoxitin Vial Interactions with Other Medication". WebMD. Retrieved 2017-05-29.
  39. ^ "Cefoxitin Drug Interactions". Drugs.com. Retrieved 2017-05-29.
  40. ^ "Camrese and cefoxitin Drug Interactions". Drugs.com. Retrieved 2017-05-29.
  41. ^ "Cefoxitin and heparin Drug Interactions". Drugs.com. Retrieved 2017-05-29.
  42. ^ "Cefoxitin and cholecalciferol / genistein / zinc chelazome Drug Interactions". Drugs.com. Retrieved 2017-05-29.
  43. ^ a b "Efficacy and Pharmacokinetic/Pharmacodynamic Parameters of Cefoxitin in Women With Acute Pyelonephritis Without Severity Symptoms Due to Extended-spectrum β-lactamase Producing Escherichia Coli". ICH GCP - Clinical Trials Registry. Retrieved 2017-05-29.
  44. ^ Clinical trial number NCT01820793 for "Efficacy and Pharmacokinetic/Pharmacodynamic Parameters of Cefoxitin in Women With Acute Pyelonephritis Without Severity Symptoms Due to Extended-spectrum β-lactamase Producing Escherichia Coli" at ClinicalTrials.gov
  45. ^ a b c d Lepeule R, Ruppé E, Le P, Massias L, Chau F, Nucci A, et al. (March 2012). "Cefoxitin as an alternative to carbapenems in a murine model of urinary tract infection due to Escherichia coli harboring CTX-M-15-type extended-spectrum β-lactamase". Antimicrobial Agents and Chemotherapy. 56 (3): 1376–81. doi:10.1128/AAC.06233-11. PMC 3294923. PMID 22214774.

External links edit

  • "Cefoxitin". Drug Information Portal. U.S. National Library of Medicine.
  • "Cefoxitin sodium". Drug Information Portal. U.S. National Library of Medicine.

December 15, 2023
cefoxitin, second, generation, cephamycin, antibiotic, developed, merck, from, cephamycin, year, following, discovery, 1972, synthesized, order, create, antibiotic, with, broader, spectrum, often, grouped, with, second, generation, cephalosporins, requires, pr. Cefoxitin is a second generation cephamycin antibiotic developed by Merck amp Co Inc from Cephamycin C in the year following its discovery 1972 It was synthesized in order to create an antibiotic with a broader spectrum 3 It is often grouped with the second generation cephalosporins 4 Cefoxitin requires a prescription and as of 2010 is sold under the brand name Mefoxin by Bioniche Pharma LLC The generic version of cefoxitin is known as cefoxitin sodium 5 6 CefoxitinClinical dataTrade namesMefoxin Renoxitin others 1 AHFS Drugs comMonographMedlinePlusa682737License dataUS DailyMed CefoxitinPregnancycategoryAU B1Routes ofadministrationIntravenousATC codeJ01DC01 WHO Legal statusLegal statusAU S4 Prescription only UK POM Prescription only US only 2 Pharmacokinetic dataMetabolismminimalElimination half life41 59 minExcretion85 urineIdentifiersIUPAC name 6R 7S 3 carbamoyloxymethyl 7 methoxy 8 oxo 7 2 thiophen 2 ylacetyl amino 5 thia 1 azabicyclo 4 2 0 oct 2 ene 2 carboxylic acidCAS Number35607 66 0 YPubChem CID441199DrugBankDB01331 NChemSpider389981 YUNII6OEV9DX57YKEGGD02345 Nas salt D00913 NChEBICHEBI 209807 NChEMBLChEMBL996 NCompTox Dashboard EPA DTXSID1022764ECHA InfoCard100 047 841Chemical and physical dataFormulaC 16H 17N 3O 7S 2Molar mass427 45 g mol 13D model JSmol Interactive imageMelting point149 to 150 C 300 to 302 F dec SMILES O C2N1 C C CS C H 1 C 2 OC NC O Cc3sccc3 COC O N C O OInChI InChI 1S C16H17N3O7S2 c1 25 16 18 10 20 5 9 3 2 4 27 9 13 23 19 11 12 21 22 8 6 26 15 17 24 7 28 14 16 19 h2 4 14H 5 7H2 1H3 H2 17 24 H 18 20 H 21 22 t14 16 m1 s1 YKey WZOZEZRFJCJXNZ ZBFHGGJFSA N Y N Y what is this verify Contents 1 History and discovery 2 Mechanism 3 Microbiological resistance 4 Spectrum of bacterial susceptibility 5 Replacement and substitution 6 Uses in medicine 7 Side effects 8 Notable drug interactions 8 1 Contraindications 8 2 Major or Severe 8 3 Moderate 8 4 Minor 9 Pharmacodynamic and pharmacokinetic data 10 References 11 External linksHistory and discovery editGroups of researchers at Merck and Lilly discovered Cephamycin C while looking at penicillin producing bacteria This followed their discovery of erythromycin another antibiotic 7 Cephamycin C was the first cephem discovered but while it was highly resistant to several beta lactamases as is its derivative cefoxitin it was almost only effective against Gram negative bacteria 7 The scientists used chemically modified the compound to give cefoxitin so titled due to its semi synthetic nature This new modification broadened its spectrum to include Gram positive bacteria More than 300 modifications were made to it and tested on the cephalosporin base with methoxy groups at the 7 alpha position Yet only cefoxitin retained its previous effectiveness against Gram negative bacteria developed effectiveness against Gram positive bacteria and resisted breakdown by beta lactamase 8 Cefoxitin and the cephamycin family as a whole served as a branching point and impulsed the discovery of more classes of beta lactams This is in part due to their primary and early discovery in the broths studied 7 Mechanism editCefoxitin is a beta lactam antibiotic which binds to penicillin binding proteins or transpeptidases By binding to PBPs cefoxitin prevents the PBPs from forming the cross linkages between the peptidoglycan layers that make up the bacterial cell wall thereby interfering with cell wall synthesis It is a strong beta lactamase inducer as are certain other antibiotics such as imipenem However cefoxitin is a better substrate than imipenem for beta lactamases 9 Microbiological resistance editIn the presence of cefoxitin bacteria that make beta lactamases will increase their production and secretion to cleave the beta lactam ring As a cephamycin cefoxitin is highly resistant to hydrolysis by some beta lactamases in part due to the presence of the 7 alpha methoxy functional group see skeletal formula above 10 11 12 13 Another more efficient form of resistance to cefoxitin is provided by the mecA gene in bacteria This gene codes for an alternative penicillin binding protein PBP2a This PBP has a lower binding affinity for penicillin based antibiotics such as cefoxitin and will continue to cross link the peptidoglycan layers of the cell wall even in the presence of the beta lactam antibiotics MRSA or methicillin resistant Staphylococcus aureus is a strain that has acquired resistance to cefoxitin via this gene 14 For the purposes of detecting bacterial strains with the mecC gene which like mecA codes for a different PBP cefoxitin is more reliable than oxacillin because mecC does not correlate as strongly with oxacillin resistance 15 Spectrum of bacterial susceptibility editCefoxitin s spectrum of in vitro antimicrobial activity includes a broad range of gram negative and gram positive bacteria including anaerobes It is inactive against most strains of Pseudomonas aeruginosa and many strains of Enterobacter cloacae Staphylococci that are resistant to methicillin and oxacillin should also be considered clinically resistant to cefoxitin even if they test susceptible by in vitro methods 2 Major bacterial strains susceptible to cefoxitin include 10 methicillin susceptible Staphylococcus aureus Streptococcus sp E coli Salmonella sp Proteus vulgaris Flavobacterium sp Klebsiella sp Major bacteria resistant to cefoxitin include 10 methicillin resistant Staphylococcus aureus Enterococci Listeria monocytogenes Enterobacter sp Bacteroides sp Replacement and substitution editIn a 2005 study Fernandes et al determined that cefoxitin serves as an appropriate replacement for methicillin in determining if some bacteria display methicillin resistance 16 Likewise Funsun et al found in a 2009 study that cefoxitin disk assays correctly identified all 60 mecA positive Staphylococcus aureus or MRSA isolates to be resistant to cefoxitin 17 Due in part to the unavailability of methicillin in the United States cefoxitin has replaced methicillin for disk diffusion tests which determine the sensitivity of a bacterial specimen to a given antibiotic 18 Cefoxitin also yields more accurate results for disk diffusion tests 18 Interpretive criteria for determining susceptibility to cefoxitin via disk diffusion are greater than or equal to 22mm resulting in a susceptible result for Staphylococcus aureus and greater than or equal to 25mm for coagulase negative staphylococci to be considered susceptible 18 The following are susceptibility data for several medically significant microorganisms measured by minimum inhibitory concentration which is an alternative liquid medium test for susceptibility Escherichia coli 0 2 mg ml 64 mg ml citation needed Haemophilus influenzae 0 5 mg ml 12 5 mg ml citation needed Streptococcus pneumoniae 0 2 mg ml 1 mg ml 19 Uses in medicine editCefoxitin is sold in three major IV doses 1g 2g and 10g 20 It is usually given to adults every six to eight hours in 1g or 2g doses 21 Cefoxitin may interfere with tests detecting urine glucose and result in a false positive 22 As with any antibiotic it should not be given to patients who are allergic to it 22 Cefoxitin is used to treat 23 24 25 26 Skin infections primarily due to Staphylococcus Urinary tract infections Bronchitis Tonsillitis Ear infections Bacterial pneumonia Sepsis Bone and joint infections Abdominal infections and abscesses Perineum injuries Pelvic inflammatory disease Gonorrhea Infections caused by susceptible bacteria mentioned earlierCefoxitin has many other uses it may be given prior to surgery to prevent the development of surgical wound infections 27 and when used in third and fourth degree perineal injuries in women after giving vaginal birth cefoxitin decreases infection rate at two and six weeks 28 However the earlier and more times a child is exposed to cefoxitin as with early and multiple exposure to many antibiotics the greater the likelihood of developing inflammatory bowel disease later in life This may be due in part to a decreased variety of microorganisms in the digestive system 29 It is also used to treat pelvic inflammatory disease because it is a broad spectrum antibiotic For outpatient treatment oral antibiotics or those with less frequent dosing may be prescribed 30 As an effective alternative to penicillin and spectinomycin and replacement for methicillin cefoxitin is used to treat gonorrhea in both men and women with few side effects 31 Side effects editSide effects for cefoxitin are regarded as mild 31 Common side effects include local tenderness or pain at the site of injection skin color change mild diarrhea mild nausea headache loss of appetite vaginal discharge and itching swelling of feet or legs 32 26 21 While cefoxitin has not been associated with alcohol incompatibility like other members of the second generation cephalosporins class it has been with a higher risk of coagulopathy a bleeding disorder 7 This is not a comprehensive list and not intended to provide medical advice If any of the previous side effects are severe or if an allergic reaction takes place immediately contact your doctor Notable drug interactions editContraindications edit A contraindication means that the drug in question should not be used under particular circumstances For cefoxitin this includes patients who are hypersensitive to cephalosporin antibiotics 33 34 Patients with colitis kidney disease or liver disease are also advised not to take cefoxitin 35 However some drug databases will considers the diseases means for caution rather than contraindications 36 Major or Severe edit Aside from the above mentioned contraindications and diseases which require monitoring by a doctor the live cholera and live typhoid vaccines are known to have a severe interaction with cefoxitin 37 38 Individuals on a low sodium diet undergoing dialysis or who have experienced seizures particularly following antibiotic therapy should also consult their physician prior to taking cefoxitin 39 Moderate edit Only take additional antibiotics anticoagulants and blood thinners under doctor supervision 38 Cefoxitin may decrease the effectiveness of hormonal birth control This increases the risk for pregnancy and a medical consult will help determine whether backup birth control methods should be used 40 Minor edit Minor drug interactions do not usually require a change in treatment Your doctor may monitor specific events such as bleeding while taking cefoxitin Two such minor interactions occur between cefoxitin and heparin 41 as well as genistein 42 Pharmacodynamic and pharmacokinetic data editPharmocokinetic and pharmacodynamic data for cefoxitin are as of 2013 considered limited and outdated A few relatively recent studies have attempted to remedy that One such study was by the Hopitaux de Paris in collaboration with the French Ministry of Health 43 However while the clinical trials were completed in 2015 no study data have been published 44 The expected results from using cefoxitin over carbapenems another type of antibiotic with a wider bacterial spectrum included effective treatment of E coli produce extended spectrum beta lactamase less selective pressure on the GI tract which better maintains balanced flora and a lower treatment cost 43 This followed a 2012 French study on the same E coli strain with CTX M 15 extended release beta lactamase 45 Lepeule et al determined that in mice the ideal pharmacodynamic target of fT gt MIC 33 where MIC is the minimum inhibitory concentration was obtained with 200 mg kg every four hours 45 The fT gt MIC was increased by 11 when the administration frequency was increased from every four hours to every three hours 45 This implied that increasing the frequency might yield similar results in humans The study also found no significant difference between the effectiveness of carbapenems and cefoxitin and suggested that cefoxitin can be used as an alternative treatment for CTX M producing E coli to carbapenems such as imipenem and ertapenem 45 References edit Cefoxitin International Drugs com 2 November 2020 Retrieved 8 November 2020 a b Cefoxitin cefoxitin sodium powder for solution DailyMed 10 June 2020 Retrieved 8 November 2020 Gootz TD January 1990 Discovery and development of new antimicrobial agents Clinical Microbiology Reviews 3 1 13 31 doi 10 1128 cmr 3 1 13 PMC 358138 PMID 2404566 Levy SB 2013 11 11 The Antibiotic Paradox How Miracle Drugs Are Destroying the Miracle Springer ISBN 9781489960429 Orange Book Approved Drug Products with Therapeutic Equivalence Evaluations www accessdata fda gov Retrieved 2017 05 04 Supplement Approval PDF Food and Drug Administration Department of Health and Human Services a b c d Dougherty TJ Pucci MJ 2011 12 21 Antibiotic Discovery and Development Springer Science amp Business Media ISBN 9781461413998 Sneader W 2005 06 23 Drug Discovery A History John Wiley amp Sons ISBN 9780471899792 Phillips I Shannon K 1993 Importance of beta lactamase induction European Journal of Clinical Microbiology amp Infectious Diseases 12 Suppl 1 S19 26 doi 10 1007 bf02389873 PMID 8477758 S2CID 22945967 a b c Moellering RC Dray M Kunz LJ September 1974 Susceptibility of clinical isolates of bacteria to cefoxitin and cephalothin Antimicrobial Agents and Chemotherapy 6 3 320 3 doi 10 1128 aac 6 3 320 PMC 444644 PMID 15830480 Shaikh S Fatima J Shakil S Rizvi SM Kamal MA January 2015 Antibiotic resistance and extended spectrum beta lactamases Types epidemiology and treatment Saudi Journal of Biological Sciences Special issue Biological Aspects of Global Health Issues 22 1 90 101 doi 10 1016 j sjbs 2014 08 002 PMC 4281622 PMID 25561890 Onishi HR Daoust DR Zimmerman SB Hendlin D Stapley EO January 1974 Cefoxitin a semisynthetic cephamycin antibiotic resistance to beta lactamase inactivation Antimicrobial Agents and Chemotherapy 5 1 38 48 doi 10 1128 aac 5 1 38 PMC 428916 PMID 4599124 Fonze E Vanhove M Dive G Sauvage E Frere JM Charlier P February 2002 Crystal structures of the Bacillus licheniformis BS3 class A beta lactamase and of the acyl enzyme adduct formed with cefoxitin PDF Biochemistry 41 6 1877 85 doi 10 1021 bi015789k PMID 11827533 Paterson GK Harrison EM Holmes MA January 2014 The emergence of mecC methicillin resistant Staphylococcus aureus Trends in Microbiology 22 1 42 7 doi 10 1016 j tim 2013 11 003 PMC 3989053 PMID 24331435 Skov R Larsen AR Kearns A Holmes M Teale C Edwards G Hill R January 2014 Phenotypic detection of mecC MRSA cefoxitin is more reliable than oxacillin The Journal of Antimicrobial Chemotherapy 69 1 133 5 doi 10 1093 jac dkt341 PMID 24038776 Fernandes CJ Fernandes LA Collignon P April 2005 Cefoxitin resistance as a surrogate marker for the detection of methicillin resistant Staphylococcus aureus The Journal of Antimicrobial Chemotherapy 55 4 506 10 doi 10 1093 jac dki052 PMID 15743899 Akcam FZ Tinaz GB Kaya O Tigli A Ture E Hosoglu S 2009 01 01 Evaluation of methicillin resistance by cefoxitin disk diffusion and PBP2a latex agglutination test in mecA positive Staphylococcus aureus and comparison of mecA with femA femB femX positivities Microbiological Research 164 4 400 3 doi 10 1016 j micres 2007 02 012 PMID 17481872 a b c Laboratory Testing for MRSA CDC gov CDC Retrieved 9 May 2017 Cefoxitin Susceptibility and Minimum Concentration MIC Data PDF Toku e Mefoxin Drug Information Indications amp Other Medicaments www catalog md Retrieved 2017 04 28 a b Cunha J Common Side Effects of Mefoxin Cefoxitin Drug Center RxList RxList Retrieved 2017 05 02 a b Mefoxin tablet Generic Side effects Interchangeable drugs etc edudrugs com Retrieved 2017 04 28 Mefoxin Indication Action of Mefoxin Interactions edudrugs com Retrieved 2017 04 28 Cefoxitin Mefoxitin 1g Marzan Pharma Corporation Retrieved 2017 04 28 permanent dead link Mefoxin generic Price of mefoxin Uses Indications and Description ndrugs Retrieved 2017 04 28 a b Cefoxitin By injection National Library of Medicine PubMed Health U S National Library of Medicine 1 April 2017 Retrieved 2017 04 28 Bratzler DW Houck PM April 2005 Antimicrobial prophylaxis for surgery an advisory statement from the National Surgical Infection Prevention Project American Journal of Surgery 189 4 395 404 doi 10 1016 j amjsurg 2005 01 015 PMID 15820449 S2CID 6496587 Buppasiri P Lumbiganon P Thinkhamrop J Thinkhamrop B October 2014 Antibiotic prophylaxis for third and fourth degree perineal tear during vaginal birth The Cochrane Database of Systematic Reviews 10 CD005125 doi 10 1002 14651858 CD005125 pub4 PMC 10542915 PMID 25289960 Kronman MP Zaoutis TE Haynes K Feng R Coffin SE October 2012 Antibiotic exposure and IBD development among children a population based cohort study Pediatrics 130 4 e794 803 doi 10 1542 peds 2011 3886 PMC 4074626 PMID 23008454 Sexually transmitted diseases treatment guidelines Atlanta GA U S Department of Health and Human Services hdl 2027 uiug 30112023431809 a b Survey of research on sexually transmitted diseases Atlanta Ga 1985 01 01 hdl 2027 umn 31951000325661b Mefoxin Side effects Contraindications ndrugs Retrieved 2017 05 02 Mefoxin Cefoxitin Drug Information Overdosage and Contraindications Prescribing Information at RxList RxList Retrieved 2017 05 29 Mefoxin Cefoxitin Drug Interactions Contraindications Other Rx Info www druglib com Retrieved 2017 05 29 Contraindications for Cefoxitin Vial WebMD Retrieved 2017 05 29 cefoxitin Contraindications and Cautions Epocrates Online online epocrates com Retrieved 2017 05 29 Cefoxitin Drug Interactions Drugs com Retrieved 2017 05 29 a b Cefoxitin Vial Interactions with Other Medication WebMD Retrieved 2017 05 29 Cefoxitin Drug Interactions Drugs com Retrieved 2017 05 29 Camrese and cefoxitin Drug Interactions Drugs com Retrieved 2017 05 29 Cefoxitin and heparin Drug Interactions Drugs com Retrieved 2017 05 29 Cefoxitin and cholecalciferol genistein zinc chelazome Drug Interactions Drugs com Retrieved 2017 05 29 a b Efficacy and Pharmacokinetic Pharmacodynamic Parameters of Cefoxitin in Women With Acute Pyelonephritis Without Severity Symptoms Due to Extended spectrum b lactamase Producing Escherichia Coli ICH GCP Clinical Trials Registry Retrieved 2017 05 29 Clinical trial number NCT01820793 for Efficacy and Pharmacokinetic Pharmacodynamic Parameters of Cefoxitin in Women With Acute Pyelonephritis Without Severity Symptoms Due to Extended spectrum b lactamase Producing Escherichia Coli at ClinicalTrials gov a b c d Lepeule R Ruppe E Le P Massias L Chau F Nucci A et al March 2012 Cefoxitin as an alternative to carbapenems in a murine model of urinary tract infection due to Escherichia coli harboring CTX M 15 type extended spectrum b lactamase Antimicrobial Agents and Chemotherapy 56 3 1376 81 doi 10 1128 AAC 06233 11 PMC 3294923 PMID 22214774 External links edit Cefoxitin Drug Information Portal U S National Library of Medicine Cefoxitin sodium Drug Information Portal U S National Library of Medicine Portal nbsp Medicine Retrieved from https en wikipedia org w index php title Cefoxitin amp oldid 1186207340, wikipedia, wiki, book, books, library,

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