Trimethoprim/sulfamethoxazole

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Trimethoprim/sulfamethoxazole
Trimethoprim and sulfamethoxazole.svg
Trimethoprim (top) and sulfamethoxazole (bottom)
Combination of
SulfamethoxazoleSulfonamide antibiotic
TrimethoprimDihydrofolate reductase inhibitor
Names
Trade namesBactrim, Cotrim, Septra, others
Other namesCo-trimoxazole (BAN UK)
Clinical data
Drug classAntibiotic
Main usesUrinary tract infections, methicillin-resistant Staphylococcus aureus (MRSA) skin infections, travelers' diarrhea, respiratory tract infections, cholera[1][2]
Side effectsNausea, vomiting, rash, diarrhea[1]
WHO AWaReAccess
Pregnancy
category
  • AU: C[3]
  • US: N (Not classified yet)[3]
Routes of
use
By mouth, intravenous[1]
Defined daily dosenot established[4]
External links
AHFS/Drugs.comMonograph
Legal
License data
Legal status

Trimethoprim/sulfamethoxazole (TMP/SMX), also known as co-trimoxazole among other names, is an antibiotic used to treat a variety of bacterial infections.[1] It is used for urinary tract infections, methicillin-resistant Staphylococcus aureus (MRSA) skin infections, travelers' diarrhea, respiratory tract infections, and cholera, among others.[1][2] It may be used both to treat and prevent pneumocystis pneumonia and toxoplasmosis in people with HIV/AIDS.[1] It can be given by mouth or intravenously.[1]

Common side effects include nausea, vomiting, rash, and diarrhea.[1] Severe allergic reactions and Clostridium difficile diarrhea may occasionally occur.[1] Its use in pregnancy is not recommended.[1][5] It appears to be safe for use during breastfeeding as long as the baby is healthy.[5] TMP/SMX generally results in bacterial death.[1] It works by blocking the making and use of folate by the microorganisms.[1] It consists of one part trimethoprim to five parts sulfamethoxazole.[2]

TMP/SMX was first sold in 1974.[6] It is on the World Health Organization's List of Essential Medicines.[7] It is available as a generic medication and is relatively inexpensive.[2][8] In 2017, it was the 121st most commonly prescribed medication in the United States, with more than six million prescriptions.[9][10]

Medical uses

Before and after actinomycetoma treated with trimethoprim/sulfamethoxazole and amikacin

Co-trimoxazole was claimed to be more effective than either of its components individually in treating bacterial infections, although this was later disputed.[11] Because it has a higher incidence of adverse effects, including allergic responses, its use has been restricted in many countries to very specific circumstances where its improved efficacy has been demonstrated.[12] It may be effective in a variety of upper and lower respiratory tract infections, kidney and urinary tract infections, gastrointestinal tract infections, skin and wound infections, sepsis, and other infections caused by sensitive organisms. Co-trimoxazole decreases the risk of recurrence of retinochoroiditis.[13] The global problem of advancing antimicrobial resistance has led to a renewed interest in the use of co-trimoxazole more recently.[14]

It is in the 'access' group of the WHO AWaRe Classification.[15]

Susceptibility

Organisms against which co-trimoxazole can be effective include:[16][17]

The only notable nonsusceptible organisms are Pseudomonas aeruginosa, the mycoplasmae[17] and Francisella tularensis (the causative organism of tularaemia).[18][19]

Dosage

It can be given by mouth, as a tablet or suspension, or intravenously.[1][20] The defined daily dose is not established.[4]

Adults

The general dose is 1 tab (160mg TMP) PO twice per day for 3 to 14 days.[21]

PCP prevention is 80-160mg TMP PO daily while PCP treatment is 15-20mg/kg/day TMP PO divided q6-8h x 21 days.[21]

Children

An oral solution comes in a solution of 40 mg trimethoprim and 200 mg sulfamethoxazole per 5 mL.[1]

Mild-mod infection[21]

  • 4-5mg/kg TMP PO q12hr

Severe infection[21]

  • 15-20mg/kg/dy TMP PO divided q6-8h

Side effects

Contraindications

Contraindications include the following:[16][22]

  • Known hypersensitivity to trimethoprim, sulphonamides or any other ingredients in the formulations
  • Pregnancy – especially in the period prior to birth
  • Severe hepatic failure, marked liver parenchymal damage or jaundice.
  • Serious haematological disorders and porphyria (due to the sulfonamide component of the preparation).
  • Severe chronic kidney disease (CrCl <15 ml/min) where repeated measurements of the plasma concentration cannot be performed
  • Co-trimoxazole should not be given to neonates during the first 6 weeks, except for the treatment/prophylaxis of pneumocytosis jiroveci (P. carinii) in infants of four weeks of age or greater.

Pregnancy and breast feeding

Its use during pregnancy is contraindicated, although it has been placed in Australian pregnancy category C and American pregnancy category D.[16] Its use during the first trimester (during organogenesis) and 12 weeks prior to pregnancy has been associated with an increased risk of congenital malformations, especially malformations associated with maternal folic acid deficiency (which is most likely related to the mechanism of action of co-trimoxazole) such as neural tube defects such as spina bifida, cardiovascular malformations (e.g. Ebstein's anomaly), urinary tract defects, oral clefts, and club foot in epidemiological studies.[16] Its use later on during pregnancy also increases the risk of preterm labour (odds ratio: 1.51) and low birth weight (odds ratio: 1.67).[23][24] Animal studies have yielded similarly discouraging results.[25]

It appears to be safe for use during breastfeeding as long as the baby is healthy.[5]

Babies

Its use in those less than 1 to 2 months of age is not recommended due to the risk of adverse side effects.[26][27]

Interactions

Its use is advised against in patients being concomitantly treated with:[16][25][22][28][29][30]

  • ACE inhibitors like captopril, enalapril, lisinopril, perindopril, and ramipril due to the potential for additive hyperkalaemic effects[22]
  • Prilocaine — additive risk of methaemoglobinaemia
  • Antiarrhythmics like amiodarone (increased risk of ventricular arrhythmias) and dofetilide (increased risk of QT interval prolongation)
  • Antibacterials like dapsone (increases plasma levels of both drugs), methenamine (increased risk of crystalluria) and rifampicin (as it may lead to an increased plasma level of rifampicin and lower plasma levels of trimethoprim)
  • Anticoagulants like warfarin and acenocoumarol — anticoagulant effects of either drug is potentiated by this combination
  • Sulfonylureas — effects enhanced
  • Phenytoin, half-life of phenytoin is increased
  • Antifolates like pyrimethamine, proguanil and methotrexate increase the risk of associated side effects like bone marrow toxicity, folic acid supplementation should be considered. A significant risk of megaloblastic anaemia exists with doses of pyrimethamine in excess of 25 mg/wk.
  • Antivirals, more specifically, lamivudine (increased plasma concentrations of lamivudine), zalcitabine (increased plasma concentrations of zalcitabine) and zidovudine (increased risk of haematological reactions)
  • Procainamide and/or amantadine may have their plasma concentrations increased bilaterally or unilaterally.
  • Clozapine and other antipsychotics — increased risk of haematological side effects
  • Nucleoside analogue antineoplastics like azathioprine and mercaptopurine — increased risk of haematological toxicity
  • Digoxin — increase in digoxin levels in a proportion of elderly patients
  • Diuretics — elderly patients receiving thiazide diuretics are at a heightened risk for developing thrombocytopaenia while on co-trimoxazole
  • Ciclosporin — patients who have received a kidney transplant and are receiving co-trimoxazole and ciclosporin concomitantly are at an increased risk of having a reversible deterioration in their kidney function.
  • Spironolactone — concurrent use can increase the likelihood of hyperkalemia, especially in the elderly. The trimethoprim portion acts to prevent potassium excretion in the distal tubule of the nephron.[31]
  • Potassium aminobenzoate — effects of sulfonamides (like sulfamethoxazole) inhibited.
  • Laboratory tests; trimethoprim and sulfonamides have been reported to interfere with diagnostic tests, including serum-methotrexate and elevated serum creatinine levels,[32] also urea, urinary glucose and urobilinogen tests.

Overdose

Likely signs of toxicity include:[25]

  • Nausea
  • Vomiting
  • Dizziness
  • Headache
  • Mental depression
  • Confusion
  • Thrombocytopenia
  • Uremia
  • Bone marrow depression
  • Loss of appetite
  • Colic
  • Drowsiness
  • Unconsciousness

The recommended treatment for overdose includes:[25]

  • Administration of activated charcoal
  • Stomach pumping
  • General supportive measures
  • Haemodialysis, which is moderately effective in clearing co-trimoxazole from the plasma.
  • Calcium folinate treatment in cases of blood dyscrasias
  • Forcing oral fluids

Alkalinisation of the urine may reduce the toxicity of sulfamethoxazole, but it may increase the toxic effects of trimethoprim.[25]

Pharmacology

Tetrahydrofolate synthesis pathway

The synergy between trimethoprim and sulfamethoxazole was first described in the late 1960s.[33][34][35] Trimethoprim and sulfamethoxazole have a greater effect when given together than when given separately, because they inhibit successive steps in the folate synthesis pathway. They are given in a one-to-five ratio in their tablet formulations so that when they enter the body their concentration in the blood and tissues is roughly one-to-twenty — the exact ratio required for a peak synergistic effect between the two.[17]

Sulfamethoxazole, a sulfonamide, induces its therapeutic effects by interfering with the de novo (that is, from within the cell) synthesis of folate inside microbial organisms such as protozoa, fungi and bacteria. It does this by competing with p-aminobenzoic acid (PABA) in the biosynthesis of dihydrofolate.[17]

Trimethoprim serves as a competitive inhibitor of dihydrofolate reductase (DHFR), hence inhibiting the de novo synthesis of tetrahydrofolate, the biologically active form of folate.[17]

Tetrahydrofolate is crucial in the synthesis of purines, thymidine, and methionine which are needed for the production of DNA and proteins[36] during bacterial replication. Thus the net effect of each of these drugs is a bacteriostatic halt in replication. When combined, TMP and SMX are bactericidal.

The effects of trimethoprim causes a backlog of dihydrofolate (DHF) and this backlog can work against the inhibitory effect the drug has on tetrahydrofolate biosynthesis; this is where the sulfamethoxazole comes in, its role is in depleting the excess DHF by preventing it from being synthesised in the first place.[17]

Pharmacokinetics of co-trimoxazole[16][25]
Component Tmax (h) Vd (L) Protein binding t1/2 (h) Excretion
Sulfamethoxazole 1-4 20 66% 8-10 Renal
Trimethoprim 1-4 130 42-45% 10 Renal

Society and culture

Trade names

Trimethoprim/sulfamethoxazole may be abbreviated as SXT, TMP-SMX, TMP-SMZ, or TMP-sulfa.

Co-trimoxazole (BAN) is manufactured and sold by many different companies. The following list of brand names is incomplete:

  • Bactrim, Bactrimel (manufactured by Roche and distributed in Europe)
  • Bactrom (Venezuela)
  • Bibactin (manufactured by PPM and distributed in Cambodia and some African countries)
  • Biseptol
  • Co-trimoxazole (Sandoz)
  • Cotrim
  • Deprim (AFT Pharmaceuticals)
  • Diseptyl (Israel)
  • Graprima Forte Kaplet (manufactured by PT Graha Farma and distributed in Indonesia)
  • Infectrin, Bactrim (Brazil)
  • Novo-Trimel[37]
  • Primotren (Lek in Slovenia and other countries)
  • Polytrim
  • Resprim
  • Sanprima (manufactured by PT Sanbe Farma and distributed in Indonesia)
  • Septra (Aspen Pharmacare and formerly GlaxoSmithKline)
  • Septram (Panama)
  • Septran (GlaxoSmithKline)[38]
  • Septrin (Spain)[39]
  • Sulfatrim
  • Trisul
  • Vactrim (manufactured and distributed in Laos)

Cost

Trimethoprim/sulfamethoxazole is relatively inexpensive as of 2019.[8] In the United States, it is about US$0.40 per dose.[1]

Approval

Indications for co-trimoxazole
Indication United States
FDA-labelled indication?
Australia
TGA-labelled indication?
United Kingdom
MHRA-labelled indication?
Literature support
Acute infective exacerbation of COPD Yes No No Clinical trials are lacking.
Prophylaxis in HIV-infected individuals No No No Effective in one Ugandan study on morbidity, mortality, CD4-cell count, and viral load in HIV infection.[40]
Otitis media Paediatric population only No Yes Clinical trials have confirmed its efficacy in chronic active otitis media[41] and acute otitis media.[42]
Travellers' diarrhoea, treatment & prophylaxis Yes No No Clinical trials have confirmed its efficacy as a treatment for travellers' diarrhoea.[43][44][45]
Urinary tract infection Yes No Yes Clinical trials have confirmed its efficacy in this indication.[17]
Bacterial infections
Acne vulgaris No No No At least one clinical trial supports its use in this indication.[46]
Listeria No Yes No Well-designed clinical trials are lacking.
Melioidosis No Yes No Clinical trials have confirmed its efficacy, with or without adjunctive doxycycline; although, co-trimoxazole alone seems preferable.[47][48][49]
Pertussis (whooping cough) No No No One cochrane review supports its efficacy in preventing the spread of pertussis.[50]
Shigellosis Yes Yes No Generally accepted treatment for shigellosis.[51] A recent Cochrane review found that while it is an effective treatment for shigellosis it also produces more significant adverse effects than other antibiotic drugs.[52]
Staphylococcus aureus infections No No No In vitro and in vivo activity against both non-resistant and methicillin-resistant Staphylococcus aureus (MRSA) infections.[53][54][55][56][57][58][59]
Tuberculosis No No No In vitro and in vivo activity against both nonresistant and MDR strains of TB.[60][61][62]
Whipple's disease No No No Co-trimoxazole is the recommended standard treatment for whipple's disease in some treatment protocols.[63][64][65]
Fungal and protozoal infections
Isosporiasis No No No Clinical trials have confirmed its use in this indication.[66]
Malaria No No No Clinical trials have confirmed its efficacy in both the treatment and prevention of malaria.[67]
Pneumocystis jirovecii pneumonia Yes Yes Yes Its use as a prophylactic treatment is supported by one clinical trial involving children with acute lymphoblastic leukaemia.[68] Other than this and one other clinical trial into its efficacy as a treatment for pneumocystis pneumonia,[69] data on its use in both the treatment and prevention of pneumocystis pneumonia is significantly lacking.
Toxoplasmosis Yes Prevention only Yes Clinical trials have confirmed its prophylactic and therapeutic utility in cases of toxoplasmosis.[70][71][72][73][74][75]

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