Monograph
J01AA02 - Doxycycline |
Propably not porphyrinogenic |
PNP |
Rationale
Doxycycline is not listed as an inducer or as a mechanism–based inhibitor of any CYP enzymes. It is mainly excreted unchanged in urine and faeces. CYP enzymes are most probably only involved in the metabolism to a minor extent.
Side effects such as nausea, vomiting and diarrhoea may be potentially porphyrinogenic through reduction in carbohydrate intake.
Chemical description
Doxycycline is a tetracycline broadspectrum antibiotic with alkylamino group. It is 3-5 times more lipophilic than tetracycline (Agwuh 2006, Whelton 1974).
Therapeutic characteristics
It is used in the treatment of infections caused by tetracycline sensitive aerobe and anaerobe Gram-positive and Gram-negative microorganisms. Nausea, vomiting and diarrhoea are reported as very common side effects.
Hepatic exposure
Significant.
Metabolism and pharmacokinetics
In vitro studies suggests that doxycycline might be a substrate or an inhibitor of CYP3A4 (Eisen 2010, Zhao 1997, 1999) but no data indicates mechanism-based inhibition. It is highly protein bound (90%) and diffuses from blood into the intestinal lumen, where cationic chelation occurs. This prevents reabsorption (Whelton 1974) and it is then excreted in faeces. The remainder (30-60%) of administered doxycycline is normally excreted unchanged in urine (Agwuh 2006, Houin 1983, SPC). Half-life elimination: single dose 16-18 hours, following multiple doses: 22 hours.
In vivo studies have shown that the half-life of doxycycline shortens when administered with phenobarbital, an inducer of CYP enzymes (Nuevonen 1974). Rifampicin, an inducer of CYP enzymes as well (Kolars 1992) has also been shown to lower the levels of doxycycline in plasma when co-administered (Colmenero 1994). These data indicates that doxycycline might be a substrate of CYP enzymes and that CYP enzymes may be involved in its metabolism to some extent. There are no reports of doxycycline as a perpetrator in drug-drug-interactions concerning CYP enzymes.
Personal communication
S. Thunell: 2 reports of safe use.
Published experience
One report of uneventful use of doxycycline in female AIP patient (7 days). Urinary porphyrin concentrations was measured before and after treatment, and doxycycline was considered entirely safe (Smith JR 1989).
IPNet drug reports
Uneventful use reported in 9 patients with acute porphyria.
Similar drugs
References
| # | Citation details | PMID |
|---|---|---|
| * | Scientific articles | |
| 1. | Colmenero JD, Fernández-Gallardo LC Possible Implications of Doxycycline-Rifampin interaction for Treatment of Brucellosis.
Antimicrobial Agents Chemotherapy. 1994 Dec;38(12):2798-802. |
7695265 |
| 2. | N. and MacGowan A. Pharmacokinetics and pharmacodynamics of the tetracyclines including glycylcyclines.
Agwuh K. Journal of Antimicrobial Chemotherapy. 2006;58:256â-265. |
16816396 |
| 3. | Doxycycline. Kucers’ the Use of Antibiotics 6th Edition, by Grayson L. M, Kucers A.
Eisen DP. et al. 2010. 851-871. |
|
| 4. | The effects of chronic renal insufficiency on the pharmacokinetics of doxycycline in man. Br. J. clin.
Houin G, Brunner F. Pharmac. 1983;16:245-252. |
|
| 5. | Identification of rifampin-inducible P450IIIA4 (CYP3A4) in human small bowel enterocytes.
Kolars JC, Schmiedlin-Ren P, Schuetz JD, Fang C, Watkins PB. J Clin Invest. 1992 Nov;90(5):1871-8. |
1430211 |
| 6. | Interaction between Doxycycline and Barbiturates.
Neuvonen PJ and Penttilä O. British Medical Journal. 1974;1:535-536. |
4817187 |
| 7. | Chlamydial infection: which antibiotic for patients with acute intermittent porphyria?
Smith JR and Forster SM. Genitourin Med. 1989 Jun;65(3):199-200. |
2759614 |
| 8. | Doxycycline pharmacokinetics in the absence of renal function.
Whelton A. Kidney international. 1974;5:365-371. |
4427416 |
| 9. | A further interaction study of quinine with clinically important drugs by human liver microsomes: determinations of inhibition constant (Ki) and type of inhibition.
Zhao XJ and Ishizaki T. Eur J Drug Metab Pharmacokinet. 1999 Jul-Sep; 24(3):272-8. |
10716067 |
| 10. | Metabolic interactions of selected antimalarial and non-antimalarial drugs with the major pathway (3-hydroxylation) of quinine in human liver microsomes.
Zhao XJ and Ishizaki T. Br J Clin Pharmacol. 1997 Nov; 44(5):505-11. |
9384469 |
| * | Drug reference publications | |
| 11. | Up to date. Doxycycline.
|
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| * | Summary of Product Characteristics | |
| 12. | Norwegian medicines agency. Summary of Product Characteristics (SPC). Doksysyklin.
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Doxycycline · Efracea 
Doxycycline · Doxylets · Doxynord · Efracea 
Dosil · Doxiciclina · Doxiclat · Doxipil · Doxitén bio · Oracea · Proderma · Rexilen · Vibracina · Vibravenosa 
Bassado · Farmodoxi · Miraclin 
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Demix · Doxycyclin · Doxycycline · Doxyhexal SF · Doxylar · Efracea · Periostat · Vibramycin · Vibramycin 50 · Vibramycin Acne Pack · Vibramycin-D · Vibrox 
Doxycyclin · Doxycyklin · Doxyprim · Oracea · Vibradox 
Doksycyklin · Doxycyclin · Doxyferm · Doxylin · Oracea · Vibracina · Vibramycin 
Doxycycline · Doxycyclinum · Efracea · Unidox 
Doxy-m · Doxyclycline · Doxycyclin · Doxycycline · Doxylets · Doxynord · Efracea · Vibratab 
Doxycyklin · Doxylin · Oracea 
Doximed · Doximycin · Doxitin · Oracea 
Doxitin · Doxy-M · Doxycyclin · Doxylan 
Doksiciklin · Dovicin · Vibramycin
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