Voriconazole: Difference between revisions
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== |
==Background== |
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*Azole antifungal |
*Azole antifungal derived from [[fluconazole]] to improve mold coverage |
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*Indications include {{#ask: [[Is treated by::voriconazole]]}} |
*Indications include {{#ask: [[Is treated by::voriconazole]]}} |
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=== |
===Mechanism of Action=== |
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*Like all azoles, inhibits Erg11/Cyp51p lanosterol 14-α-demethylase in the ergosterol synthesis pathway |
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===Pharmacokinetics and Pharmacodynamics=== |
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*Non-linear pharmacokinetics |
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*58% protein-bound |
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*CSF 50% of plasma concentration |
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*Less than 5% excreted unchanged in the urine |
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===Spectrum of Activity=== |
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*Active against [[Aspergillus]] (including [[Aspergillus terreus]]), [[Scedosporium]], [[Fusarium]], and [[Candida]] |
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*Possibly active against [[Cryptococcus]], [[Blastomyces dermatitidis]], [[Coccidioides immitis]], and [[Histoplasma capsulatum]] |
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*Less active against [[Sporothrix schenckii]] |
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===Breakpoints=== |
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{| class="wikitable" |
{| class="wikitable" |
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! rowspan="2" |Species |
! rowspan="2" |Species |
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|[[Cryptococcus neoformans]] |
|[[Cryptococcus neoformans]] |
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|0.25 |
|0.25 |
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| colspan="8" rowspan=" |
| colspan="8" rowspan="2" | |
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|- |
|- |
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|[[Cryptococcus gattii]] |
|[[Cryptococcus gattii]] |
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|[[Aspergillus flavus]] |
|[[Aspergillus flavus]] |
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|2 |
|2 |
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|— |
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| colspan="2" rowspan="5" | |
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|— |
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| colspan="4" rowspan="5" | |
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|- |
|- |
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|[[Aspergillus fumigatus]] |
|[[Aspergillus fumigatus]] |
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|1 |
|1 |
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|≤1 |
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|>1 |
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|- |
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|[[Aspergillus niger]] |
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|1 |
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|≤1 |
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|>1 |
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|- |
|- |
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|[[Aspergillus niger]] |
|[[Aspergillus niger]] |
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|2 |
|2 |
||
|— |
|||
|— |
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|- |
|- |
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|[[Aspergillus terreus]] |
|[[Aspergillus terreus]] |
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|2 |
|2 |
||
|— |
|||
|— |
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|} |
|} |
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==Dosing== |
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==Therapeutic Drug Monitoring== |
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*Voriconazole 6 mg/kg IV q12h x2 followed by 4 mg/kg PO/IV q12h |
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*Voriconazole 200 mg PO q12h if weight >40 kg, or 100 mg PO q12h if weight <40 kg |
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**Give at least 1 hour before or after a meal |
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**Can be preceded by a loading dose of twice the maintenance for 24 hours |
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===Therapeutic Drug Monitoring=== |
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*Measure trough within 7 days of starting, and at regular intervals or following dose adjustment |
*Measure trough within 7 days of starting, and at regular intervals or following dose adjustment |
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|} |
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=== |
=== Monitoring === |
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* Weekly liver enzymes for first month, then monthly thereafter |
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=== Renal Dysfunction === |
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* No dosage adjustment necessary, though for the IV formulation there is a risk of accumulation of sulfobutylether-beta-cyclodextrin (SBECD), which has been associated with renal injury in animal models |
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=== Liver Dysfunction === |
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* For Child-Pugh A and B, consider reducing the maintenance dose to half the usual dose, while keeping the same loading dose |
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==Safety== |
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*Elevated levels predict neurotoxicity, but ''not'' hepatotoxicity |
*Elevated levels predict neurotoxicity, but ''not'' hepatotoxicity |
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==Adverse Drug Reactions== |
===Adverse Drug Reactions=== |
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*Visual, which tend to improve after the first week of therapy and are reversible |
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*Visual |
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**[[Adverse drug reaction::Floaters]] |
**[[Adverse drug reaction::Floaters]] (photopsia) that usually improves with time (30%) |
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**[[Adverse drug reaction::Visual hallucinations]] |
**[[Adverse drug reaction::Visual hallucinations]] (5%) |
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**[[Adverse drug reaction::Colour vision loss]] |
**[[Adverse drug reaction::Colour vision loss]], [[Adverse drug reaction::blurred vision]], [[Adverse drug reaction::photophobia]] |
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*Dermatologic |
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*[[Adverse drug reaction::Photosensitivity]] |
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**Rashes, usually mild |
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*[[Adverse drug reaction::Hepatotoxicity]] |
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**[[Stevens-Johnson syndrome]] and [[toxic epidermal necrolysis]] (rare) |
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**[[Adverse drug reaction::Photosensitivity]] |
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*[[Adverse drug reaction::Hepatotoxicity]][[CiteRef::mihăilă2015vo]] |
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**Risk factors include higher trough (though can occur at any level), other hepatotoxic medications (and specifically [[tigecycline]] and [[TMP-SMX]]), and septic shock[[CiteRef::wang2022vo]] |
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**In critically ill patients, mostly occurs within 7 days of starting |
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**Primarily cholestasis, but can be hepatocellular damage or mixed |
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**Resolves with discontinuation, but can take 1 to 3 months |
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**See also [https://www.ncbi.nlm.nih.gov/books/NBK547891/ LiverTox] |
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*[[Adverse drug reaction::QTc prolongation]] |
*[[Adverse drug reaction::QTc prolongation]] |
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*Headache, nausea and vomiting, diarrhea, abdominal pain |
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===Drug-Drug Interactions=== |
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*Voriconazole is metabolised by [[Metabolized by::CYP450]] enzymes |
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*Voriconazole also inhibits [[Inhibits::CYP3A4]] and [[Inhibits::CYP2C9]] |
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{| class="wikitable" |
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!Drug |
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!Recommendation |
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|- |
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! colspan="2" |Decreases voriconazole levels |
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|- |
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|[[carbamazepine]] |
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|contraindicated |
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|- |
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|long-acting [[Barbiturate|barbiturates]] |
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|contraindicated |
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|- |
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|[[rifampin]] |
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|contraindicated |
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|- |
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! colspan="2" |Levels increased by voriconazole |
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|- |
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|[[astemizole]] |
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|contraindicated |
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|- |
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|[[cisapride]] |
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|contraindicated |
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|- |
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|[[cyclosporine]] |
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|reduce cyclosporine dosage 50% and monitor levels |
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|- |
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|ergot alkaloids |
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|contraindicated |
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|- |
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|[[omeprazole]] |
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|reduce omeprazole by 50% |
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|- |
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|[[quinidine]] |
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|contraindicated |
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|- |
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|[[sirolimus]] |
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|contraindicated |
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|- |
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|[[tacrolimus]] |
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|reduce tacrolimus levels to 33% and monitor levels |
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|- |
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|[[terfenadine]] |
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|contraindicated |
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|- |
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|[[warfarin]] |
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|monitor INR |
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|- |
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! colspan="2" |Decreases voriconazole levels, and levels increased by voriconazole |
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|- |
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|[[rifabutin]] |
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|contraindicated |
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|- |
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|[[phenytoin]] |
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|double voriconazole, and monitor phenytoin levels |
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|- |
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! colspan="2" |Levels likely increased by voriconazole |
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|- |
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|sulfonylureas |
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| rowspan="5" |monitor for side effects of drug and consider decreasing dosage |
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|- |
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|statins |
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|- |
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|vinca alkaloids |
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|- |
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|calcium channel blockers |
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|- |
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|benzodiazepines |
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|} |
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==Further Reading== |
==Further Reading== |
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*Voriconazole Dose Modification Guideline to Optimize Therapeutic Levels in Patients With Hematologic Malignancies. ''Open Forum Infect Dis''. 2015;2(S1):810. doi: [https://doi.org/10.1093/ofid/ofv133.527 10.1093/ofid/ofv133.527] |
*Voriconazole Dose Modification Guideline to Optimize Therapeutic Levels in Patients With Hematologic Malignancies. ''Open Forum Infect Dis''. 2015;2(S1):810. doi: [https://doi.org/10.1093/ofid/ofv133.527 10.1093/ofid/ofv133.527] |
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[[Category: |
[[Category:Triazoles]] |
Latest revision as of 13:10, 22 October 2024
Background
- Azole antifungal derived from fluconazole to improve mold coverage
- Indications include Alternaria, Blastomyces dermatitidis, Coccidioides immitis, Exophiala, Exserohilum, Fungal endocarditis, Histoplasma capsulatum, Rasamsonia
Mechanism of Action
- Like all azoles, inhibits Erg11/Cyp51p lanosterol 14-α-demethylase in the ergosterol synthesis pathway
Pharmacokinetics and Pharmacodynamics
- Non-linear pharmacokinetics
- 58% protein-bound
- CSF 50% of plasma concentration
- Less than 5% excreted unchanged in the urine
Spectrum of Activity
- Active against Aspergillus (including Aspergillus terreus), Scedosporium, Fusarium, and Candida
- Possibly active against Cryptococcus, Blastomyces dermatitidis, Coccidioides immitis, and Histoplasma capsulatum
- Less active against Sporothrix schenckii
Breakpoints
Species | ECV (μg/mL) | Breakpoints (μg/mL) | Breakpoints (mm) | ||||||
---|---|---|---|---|---|---|---|---|---|
S | I | SDD | R | S | I | SDD | R | ||
Candida albicans | 0.3 | ≤0.12 | 0.25-0.5 | — | ≥1 | ≥17 | 15-16 | — | ≤14 |
Candida glabrata | 0.25 | — | — | — | — | — | — | — | — |
Candida krusei | 0.5 | ≤0.5 | 1 | — | ≥2 | ≥15 | 13-14 | — | ≤12 |
Candida parapsilosis | 0.03 | ≤0.12 | 0.25-0.5 | — | ≥1 | ≥17 | 15-16 | — | ≤14 |
Candida tropicalis | 0.12 | ≤0.12 | 0.25-0.5 | — | ≥1 | ≥17 | 15-16 | — | ≤14 |
Cryptococcus neoformans | 0.25 | ||||||||
Cryptococcus gattii | 0.5 | ||||||||
Aspergillus flavus | 2 | — | — | ||||||
Aspergillus fumigatus | 1 | ≤1 | >1 | ||||||
Aspergillus niger | 1 | ≤1 | >1 | ||||||
Aspergillus niger | 2 | — | — | ||||||
Aspergillus terreus | 2 | — | — |
Dosing
- Voriconazole 6 mg/kg IV q12h x2 followed by 4 mg/kg PO/IV q12h
- Voriconazole 200 mg PO q12h if weight >40 kg, or 100 mg PO q12h if weight <40 kg
- Give at least 1 hour before or after a meal
- Can be preceded by a loading dose of twice the maintenance for 24 hours
Therapeutic Drug Monitoring
- Measure trough within 7 days of starting, and at regular intervals or following dose adjustment
- Target trough > 1 mg/L for prophylaxis and treatment
Trough (mcg/mL) | Recommendation |
---|---|
0.0 to 0.6 | Increase dose by 100 mg and recheck trough on day 5 of new regimen |
0.7 to 0.9 | Increase dose by 50 mg and recheck trough on day 5 of new regimen |
1.0 to 4.0 | At target, no dose adjustment needed |
4.1 to 5.5 | Decrease dose by 50 mg and recheck trough on day 5 of new regimen |
5.6 to 7.9 | Hold dose. Follow daily trough levels, then restart when trough is ≤2.5 at a dose decreased by 100 mg. Recheck trough on day 5 of new regimen. |
≥8.0 | Hold dose. Follow daily trough levels, then restart when trough is ≤2.5 at a dose decreased by 50%. Recheck trough level on day 5 of new regimen. |
Monitoring
- Weekly liver enzymes for first month, then monthly thereafter
Renal Dysfunction
- No dosage adjustment necessary, though for the IV formulation there is a risk of accumulation of sulfobutylether-beta-cyclodextrin (SBECD), which has been associated with renal injury in animal models
Liver Dysfunction
- For Child-Pugh A and B, consider reducing the maintenance dose to half the usual dose, while keeping the same loading dose
Safety
- Elevated levels predict neurotoxicity, but not hepatotoxicity
Adverse Drug Reactions
- Visual, which tend to improve after the first week of therapy and are reversible
- Floaters (photopsia) that usually improves with time (30%)
- Visual hallucinations (5%)
- Colour vision loss, blurred vision, photophobia
- Dermatologic
- Rashes, usually mild
- Stevens-Johnson syndrome and toxic epidermal necrolysis (rare)
- Photosensitivity
- Hepatotoxicity1
- Risk factors include higher trough (though can occur at any level), other hepatotoxic medications (and specifically tigecycline and TMP-SMX), and septic shock2
- In critically ill patients, mostly occurs within 7 days of starting
- Primarily cholestasis, but can be hepatocellular damage or mixed
- Resolves with discontinuation, but can take 1 to 3 months
- See also LiverTox
- QTc prolongation
- Headache, nausea and vomiting, diarrhea, abdominal pain
Drug-Drug Interactions
Drug | Recommendation |
---|---|
Decreases voriconazole levels | |
carbamazepine | contraindicated |
long-acting barbiturates | contraindicated |
rifampin | contraindicated |
Levels increased by voriconazole | |
astemizole | contraindicated |
cisapride | contraindicated |
cyclosporine | reduce cyclosporine dosage 50% and monitor levels |
ergot alkaloids | contraindicated |
omeprazole | reduce omeprazole by 50% |
quinidine | contraindicated |
sirolimus | contraindicated |
tacrolimus | reduce tacrolimus levels to 33% and monitor levels |
terfenadine | contraindicated |
warfarin | monitor INR |
Decreases voriconazole levels, and levels increased by voriconazole | |
rifabutin | contraindicated |
phenytoin | double voriconazole, and monitor phenytoin levels |
Levels likely increased by voriconazole | |
sulfonylureas | monitor for side effects of drug and consider decreasing dosage |
statins | |
vinca alkaloids | |
calcium channel blockers | |
benzodiazepines |
Further Reading
- Voriconazole Dose Modification Guideline to Optimize Therapeutic Levels in Patients With Hematologic Malignancies. Open Forum Infect Dis. 2015;2(S1):810. doi: 10.1093/ofid/ofv133.527
References
- ^ Romeo-Gabriel Mihăilă. Voriconazole and the liver. World Journal of Hepatology. 2015;7(13):1828. doi:10.4254/wjh.v7.i14.1828.