Monograph
L01BA01 - Methotrexate |
Propably not porphyrinogenic |
PNP |
Rationale
Methotrexate is primarily excreted unchanged through the kidneys, and there is no evidence of CYP-metabolism. It does not inhibit nor induce CYP3A4. No reports of drug interactions indicating induction or inhibition of CYP2C9. However, side effects such as nausea, anorexia and vomiting may be potentially porphyrinogenic through reduction in caloric intake.
Chemical description
Methotrexate is a mixture containing at least 85% 4-amino-10-methylfolic acid, calculated on the anhydrous basis, and small amounts of related compounds. Structurally, the primary constituent of methotrexate differs from folic acid in the substitution of an amino group for a hydroxyl group in the pteridine nucleus and in the addition of a methyl group on the amino nitrogen between the pteroyl and benzoyl groups.
Therapeutic characteristics
Methotrexate, a folic acid antagonist, is an antineoplastic agent and immunosuppressant used in the management of acute lymphoblastic leukaemia, for Burkitts and other non-Hodgkins lymphomas, as well as in the treatment of choriocarcinoma and other gestational trophoblastic tumours, and for the adjuvant therapy of osteosarcoma and breast cancer. It may also be used in malignant neoplasms of the bladder and head and neck, and some other neoplasms. It is also used in the treatment of active rheumatoid arthritis and psoriasis.
Methotrexate has two different ATC-codes, L01BA01 describes parenteral use, while methotrexate in oral formulations is classified in L04AX03.
Common adverse reactions of methotrexate that can be confused with an acute porphyric attack are abdominal distress, vomiting and diarrhoea. Side effects such as nausea, anorexia and vomiting may be potentially porphyrinogenic through reduction in caloric intake.
Metabolism and pharmacokinetics
Methotrexate is excreted primarily unchanged by the kidneys via glomerular filtration and active transport. 58-92% of a single dose is excreted within 24 hours following IV administration. Methotrexate does not appear to undergo significant metabolism at low doses; after high-dose therapy the 7-hydroxy metabolite has been detected. When high-dose methotrexate is administered as a short intravenous infusion (4–6 h), most of the drug is cleared by the kidneys, but with longer infusions (24 h), about 40% of the drug is metabolised in the liver (Relling, 2000). Methotrexate did not activate PXR or increase CYP3A4 or CYP2B6 activity (Luo, 2002; Faucette, 2004; Sinz, 2006). Methotrexate did not affect the metabolism of vinblastine (Zhou-Pan, 1993). Methotrexate was not found to inhibit CYP3A4 activity (Baumhakel, 2001). No reports of drug interactions indicating induction or inhibition of CYP2C9.
Personal communication
Used uneventfully by 55 year old AIP woman (S. Thunell, Sweden). Uneventful use reported in one patient with AIP (C. Andersson, Sweden).
Published experience
Uneventful use reported in three patients with PV (Samuels, 1984).
IPNet drug reports
Uneventful use reported in 4 patients with acute porphyria, also uneventful use of methotrexate under the ATC-code L04AX03 is reported by 1 patient.
Similar drugs
References
| # | Citation details | PMID |
|---|---|---|
| * | Scientific articles | |
| 1. | Baumhäkel M, Kasel D, Screening for inhibitory effects of antineoplastic agents on CYP3A4 in human liver microsomes.
Int J Clin Pharmacol Ther. 2001;39(12):517-28. |
11770832 |
| 2. | Sinz, M, Kim, S, et al. Evaluation of 170 xenobiotics as transactivators of hPXR and correaltion to CYP 3A4 drug interactions. Curr Drug metabol 2006; 7:375-388.
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| 3. | Regulation of CYP2B6 in primary human hepatocytes by prototypical inducers.
Faucette SR, Wang H, et al. Drug Metab Dispos. 2004;32(3):348-58. |
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| 4. | CYP3A4 induction by drugs: correlation between a pregnane X receptor reporter gene assay and CYP3A4 expression in human hepatocytes.
Luo G, Cunningham M, et al. Drug Metab Dispos. 2002;30(7):795-804. |
12065438 |
| 5. | Adverse effect of anticonvulsants on efficacy of chemotherapy for acute lymphoblastic leukaemia.
Relling MV, Pui CH, et al. Lancet. 2000;356(9226):285-90. |
11071183 |
| 6. | Chemotherapy in porphyria.
Samuels B, Bezwoda WR, et al. S Afr Med J. 1984;65(23):924-6. |
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| 7. | Involvement of human liver cytochrome P450 3A in vinblastine metabolism: drug interactions.
Zhou-Pan XR, Sérée E, et al. Cancer Res. 1993;53(21):5121-6. |
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| * | Drug reference publications | |
| 8. | McEvoy GK, editor. Methotrexate. The AHFS Drug Information 2008. Bethesda, MD: American Society of Health-System Pharmacists; 2009. Electronic version (05.07.10).
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| 9. | Sweetman SC, editor. Martindale: The complete drug reference. Methotrexate. Pharmaceutical Press 2009.
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Tradenames
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In some cases, a more comprehensive list of available drug packages is included.
Consequently, very similar terms may therefore appear multiple times.
Bold names are the searchable terms, while the gray names that follow are all mapped to the bolded term.
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Jylamvo 2mg/ml, drank · Methotrexaat Accord 100 mg/ml, concentraat voor oplossing voor intraveneuze infusie · Methotrexaat Accord 25 mg/ml, oplossing voor injectie · Methotrexaat Sandoz 10 mg, tabletten · Methotrexaat Sandoz 2,5 mg, tabletten · Methotrexaat Teva 10 mg, tabletten · Methotrexaat Teva 2,5 mg, tabletten 
Emthexate · Emthexate 1 000 mg/40 ml sol. inj. i.th?c./i.art?r./i.ventricul./i.v./i.m. flac. · Emthexate 5 000 mg/50 ml sol. inj. i.th?c./i.art?r./i.ventricul./i.v./i.m. flac. · Emthexate 5 mg/2 ml sol. inj. i.th?c./i.art?r./i.ventricul./i.v. flac. · Emthexate 50 mg/2 ml sol. inj. i.th?c./i.art?r./i.ventricul./i.v./i.m. flac. · Emthexate 500 mg/20 ml sol. inj. i.th?c./i.art?r./i.ventricul./i.v./i.m. flac. · Methotrexate · Methotrexate Accord Healthcare 100 mg/ml sol. perf. (? diluer) i.v. flac. · Methotrexate Accord Healthcare 25 mg/ml sol. inj. i.th?c./i.art?r./i.v./i.m. flac. · Metoject · Metoject 50 mg/ml sol. inj. s.c. ser. pr?remplie · Nordimet · Nordimet 10 mg sol. inj. s.c. ser. pr?remplie · Nordimet 10 mg sol. inj. s.c. stylo pr?rempli · Nordimet 12.5 mg sol. inj. s.c. ser. pr?remplie · Nordimet 12.5 mg sol. inj. s.c. stylo pr?rempli · Nordimet 15 mg sol. inj. s.c. ser. pr?remplie · Nordimet 15 mg sol. inj. s.c. stylo pr?rempli · Nordimet 17.5 mg sol. inj. s.c. ser. pr?remplie · Nordimet 17.5 mg sol. inj. s.c. stylo pr?rempli · Nordimet 20 mg sol. inj. s.c. ser. pr?remplie · Nordimet 20 mg sol. inj. s.c. stylo pr?rempli · Nordimet 22.5 mg sol. inj. s.c. ser. pr?remplie · Nordimet 22.5 mg sol. inj. s.c. stylo pr?rempli · Nordimet 25 mg sol. inj. s.c. ser. pr?remplie · Nordimet 25 mg sol. inj. s.c. stylo pr?rempli · Nordimet 7.5 mg sol. inj. s.c. ser. pr?remplie · Nordimet 7.5 mg sol. inj. s.c. stylo pr?rempli 
Metotrexato · Metotrexato Accord 100 mg/ml Concentrado Para Solucion Para Perfusion · Metotrexato Accord 25 mg/ml Solucion Inyectable efg · Metotrexato Pfizer 25 mg/ml Solucion Inyectable efg · Metotrexato Semanal Accord 2.5 mg Comprimidos efg · METOTREXATO WYETH 2,5 mg COMPRIMIDOS · METOTREXATO WYETH 5 g SOLUCION INYECTABLE 
Methotrexate 
JYLAMVO 2 mg/ml · METHOTREXAT \"EBEWE\" 5000 mg/50 ml · METOTREXAT SANDOZ 2,5 mg (vezi L04AX03) · METOTREXAT VITEMA 2,5 mg 
Methotrexate · Nordimet · Zlatal 
Methotrexat Accord · Methotrexat Ebewe · Methotrexate Pfizer 
Ebetrex · Methotrexat Accord · Methotrexat-GRY farma mondo · Metotressato teva 
Metex PEN · Methofill SD · Methotrexat-Ebewe · Metotreksat Accord · Trexan Neo 
Jylamvo · Methotrexat Ebewe · Metoject 
Methotrexat Accord · Methotrexat Ebewe 
Jylamvo · Methotrexat-Ebewe · Methotrexate "Ebewe" · Methotrexate Accord 
Methotrexat Ebewe® · Methotrexate Pfizer · Metotreksat Remedica
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