Monograph
N01BB52 - Lidocaine, Combinations |
Propably not porphyrinogenic |
PNP |
Rationale
Limitations: This safety classification applies only to preparations containing a combination of the two drugs lidocaine and adrenaline (epinephrine). The same ATC-code (N01BB52) can in some countries be used for different combinations of lidocaine and other drugs which in theory may be porphyrinogenic. Please refer to the classification and monograph of each individual substance. If the combination contains a substance which is not classified (NC) or has been classified as porphyrinogenic (PRP or P), the safety classification of such a combination as PNP is no longer valid.
Lidocaine is metabolized by CYP1A2, with only a minor contribution from CYP 3A4.
Lidocaine is not listed as an inducer or as a mechanism-based inhibitor of CYP enzymes, nor is there any evidence of lidocaine capacity for Cyp-inhibition in clinical use.
Lidocaine is reported as used uneventfully by 68 patients, and thus strong clinical evidence points to lidocaine as probably not porphyrinogenic. There are two reports of possible activation of the disorder following the use of lidocaine, but the reports are poorly documented and are therefore not taken into account in the judgement of the porphyrinogenicity of lidocaine.
Lidocaine should be used with some caution in repeated high dosing because of lacking pharmacokinetic information during long term treatment. Lidocaine is classified PNP.
Adrenalin (epinephrine) is an endogenous catecholamine. The metabolism of adrenaline is not CYP-dependent and there are no data pointing to CYP-interaction. Epinephrine is classified NP.
Chemical description
Lidocaine hydrochloride is an amide derivative of diethyl amino acetic acid. Lidocaine has a lipophilic aromatic ring attached to a hydrophilic amino group by an amide linkage.
Adrenaline is a catecholamine added for longer duration of local anaesthesia.
Therapeutic characteristics
Lidocaine is a local anaesthetic with short duration. Lidocaine can be administered as an injection for use as nerve blockade, regional, infiltration and epidural anaesthesia. Administration in combination with vasoconstrictor such as adrenaline (epinephrine) (not porphyrinogenic) prolongs the effect of lidocaine, and reduces hepatic exposure and the risk of systemic reactions. Adverse effects are usually of short duration, and are dose related. Adverse reactions of lidocaine that can be confused with an acute porphyric attack are nausea, vomiting, confusion, paresthesia, tremors, seizures, numbness and respiratory depression.
Hepatic exposure
The plasma concentration of lidocaine is dependent on dose, administration method and vascularity of the site of injection. Intercostal blockade will produce a higher plasma concentration (about 5 uM for every 100 mg injected), than epidural anaesthesia and abdominal subcutaneous injection.
Metabolism and pharmacokinetics
The primary metabolic pathway of lidocaine is CYP1A2 and, to a minor extent, CYP3A4 mediated N-deethylation to the active monoethylglycinexylidide (MEGX). MEGX is further de-ethylated to 2,6-xylidine and glycinexylidide. 2,6-xylidine is hydrolysed by CYP 2A6 to 4-hydroxy-xylidine, which is the major metabolite found in urine.
In vitro studies suggest that CYP 3A4 may be an important contributor to the N-deethylation of lidocaine in high concentrations (above therapeutic concentrations) (Wang 2000). Found to be a week inhibitor of CYP 1A2 (Kobayashi 1998), and suggested as a competitive inhibitor of CYP1A2 by Wei (1999). In another study lidocaine was found to competitively inhibit N-monodesethylation of amioderone (with Ki = 120 µM) (Kobayashi 1998). Rendic (2002) reports that lidocaine is a substrate and an inhibitor of CYP1A2, a substrate for CYP2A6, CYP2B6, CYP2C8, CYP2C9, CYP2C18, CYP3A4 and an inhibitor and a substrate of CYP2D6. There is no evidence of lidocaine capacity for Cyp-inhibition in clinical use.
Some studies have shown an accumulation of lidocaine or/and MEGX in continued administration of lidocaine (Miyabe 1999, Thomson 1987, Bauer 1982, Ngo 1997).
One study report signs of CYP 3A4 TDI in rodent microsome experiments (Bensoussan 1994), but this has not been confirmed in human studies.
Adrenalin (epinephrine) is an endogenous compound. It is very rapidly inactivated by processes which include uptake into adrenergic neurones, diffusion, and enzymatic degradation in the liver and body tissues. Metabolism involves monoamine oxidase (MAO) and catechol-O-methyl transferase (COMT).
Preclinical data
Lidocaine was found to increase the activity of delta-aminolaevulinic acid synthase in a rat liver model (Parikh, R.K. & Moore, M.R., 1978). Lidocaine was found to induce delta-aminolaevulinic acid synthase and to cause accumulation of porphyrins and cytochrom P450 in chick embryo livers in ovo (de Verneuil, H., Deybach, J.C. et al, 1982).
Personal communication
Thunell, S., study to be published: 45 patients exposed without porphyric adverse reaction reported. After the completion of the study, one instance of possible activation of the disorder following the use of lidocaine for dental surgery in a middle-aged male carrier of AIP was reported (other precipitating factors can not be excluded).
IPNet drug reports
Uneventful use reported in 9 patients with acute porphyria. One report of an attack of acute porphyria following the use of lidocaine (N02BB01) in a male with active AIP, but the attack is poorly documented.
Uneventful use is also reported after use of lidocaine under other ATC codes; N02BB02 used in 9 patients, C01BB01 used in 1 patient, D04AB01 used in 3 patients and R02AD02 used in 1 patient.
References
# | Citation details | PMID |
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* | Scientific articles | |
1. | Continuous intercostal blockade with lidocaine after thoracic surgery - clinical and pharmacokinetic study. Anesth Analg1990;70: 345-9.
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2316876 |
2. | de Verneuil,H., Deybach,J.C. et al. Study of anaesthetic agents for their ability to elicit porphyrin biosynthesis in chick embryo liver. Biochem Pharmacol 1982; 32: 1011-18.
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3. | Miyabe M, Kakiuchi Y, et al, The plasma concentration of lidocaines principal metabolite increases during continuous epidural anesthesia in infants and children.
Anesth Analg. 1998 Nov;87(5):1056-7. |
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4. | Ngo LY, Tam YK, et al Effects of intravenous infusion of lidocaine on its pharmacokinetics in conscious instrumented dogs.
J Pharm Sci. 1997 Aug;86(8):944-52. |
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5. | Parikh, RK, Moore, MR. Effect of certain anaesthetic agents on the activity of rat hepatic delta-aminolaevulinate synthase. Br J Anaesth 1978; 50:1099-1103.
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718778 |
6. | Rendic, S. Summery of information on human CYP enzymes: human P450 metabolism. Drug metabolism reviews 2002; 34(1&2), 83-448.
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7. | Thunell, S. Evidence-based porphyrogenicity assessment of seven local anasthetics (2011, to be published).
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8. | Lidocaine metabolism in human liver microsomes by cytochrome P450IIIA4. Clin Pharmacol Ther 1989; 46(5):521-7.
Bargetzi MJ, Aoyama T et al. |
2582709 |
9. | Particular ability of cytochromes P450 3A to form inhibitory P450-iron-metabolite complexes upon metabolic oxidation of aminodrugs. Biochem Pharmacol 1995; 49(5):591-502.
Bensoussan M, delaforge M,et al. |
7887973 |
10. | Inhibitory effects of antiarrhythmic drugs on phenacetin O-deethylation catalysed by human CYP1A2.
Kobayashi K, Nakajima M, et al. Br J Clin Pharmacol. 1998 Apr;45(4):361-8. |
9578183 |
11. | Cytochrome P450 1A2 is a major determinant of lidocaine metabolism in vivo: effects of liver function.Clin Pharmacol Ther 2004;75(1):80-8.
Orlando R, Piccoli P et al. |
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12. | Changes in lignocaine disposition during long-term infusion in patients with acute ventricular arrhythmias.
Thomson AH, Kelman AW, et al. Ther Drug Monit. 1987 Sep;9(3):283-91. |
3672571 |
13. | Synthetic and natural compounds that interact with human cytochrome P450 1A2 and implications in drug development.
Wang B, Zhou SF. Curr Med Chem. 2009;16(31):4066-218. |
19754423 |
14. | Involvement of CYP1A2 and CYP3A4 in lidocaine N-deethylation and 3-hydroxylation in humans.
Wang JS, Backman JT, et al. Drug Metab Dispos. 2000 Aug;28(8):959-65. |
10901707 |
15. | Inhibition of human liver cytochrome P450 1A2 by the class IB antiarrhythmics mexiletine, lidocaine, and tocainide. J Pharmacol Exsperim Ther 1999 May;289(2):853-8
Wei X, Dai R, et al. |
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* | Drug reference publications | |
16. | McEvoy GK, editor. Lidocaine Hydrochloride. The AHFS Drug Information 2008. Bethesda, MD: American Society of Health-System Pharmacists; 2009. Electronic version (February 2009).
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17. | Sweetman SC, editor. Martindale: The complete drug reference. Lidocaine Hydrochloride. Pharmaceutical Press 2009.
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* | Summary of Product Characteristics | |
18. | Norwegian medicines agency. Summary of Product Characteristics (SPC). Xylocain adrenalin.
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19. | Swedish medicines agency. Summary of Product Characteristics (SPC) Xylocard.
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Netherlands
Cathejell · Cathejell 20 mg/0,5 mg gel · Instillagel · Instillagel, gel · Lignospan · Lignospan 2% Special, injectievloeistof · Pliaglis · Pliaglis 70 mg/g + 70 mg/g crème · Rapydan · Rapydan 70 mg/70 mg medicinale pleister · Xylocaine / Adrenaline · Xylocaine 1% - Adrenaline, injectievloeistof 10 mg/ml + 0,005 mg/ml · Xylocaine 1% - Adrenaline, injectievloeistof 10 mg/ml + 5 microgram/ml · Xylocaine 1% - adrenaline, oplossing voor injectie 10 mg/ml + 5ug/ml · Xylocaine 10 mg/ml + 5 microgram/ml adrenaline oplossing voor injectie · Xylocaine 10 mg/ml + 5 microgram/ml adrenaline, oplossing voor injectie · Xylocaine 2% - Adrenaline 1:80.000 DENTAL, oplossing voor injectie · Xylocaine 2% - Adrenaline, injectievloeistof 20 mg/ml + 5 µg/ml · Xylocaine 2% - adrenaline, oplossing voor injectie 20 mg/ml + 5ug/ml · Xylocaine 2%- Adrenaline, injectievloeistof 20 mg/ml + 5 microgram/ml · Xylocaine 20 mg/ml + 5 microgram/ml adrenaline oplossing voor injectieBelgium
Lignospan · Lignospan 20 mg/ml - 0.013 mg/ml sol. inj. cart. · Pliaglis · Pliaglis 70 mg/g - 70 mg/g crème · Rapydan · Rapydan 70 mg - 70 mg emplâtre médic. sachet · Xogel · Xogel Adulte 50 mg - 1.5 mg/g gel gingiv. · Xogel Enfants 50 mg - 1.5 mg/g gel gingiv. · Xylonor · Xylonor Pellets 5 g - 0.15 g tampon impr. · Xylonor Spray 15 g - 0.15 g sol. pulv. bucc. flac. pulv.United Kingdom
. · Boots Mouth Ulcer gel · Anbesol · Anbesol liquid · Bonjela · Bonjela Junior gel · Bonjela Teething gel · Bradosol Plus · Bradosol Plus lozenges · Calgel · Calgel teething gel · Children's 3 Months Plus · Children's 3 Months Plus teething gel sugar free · Covonia · Covonia Sore Throat 0.2%/0.05% oromucosal spray lemon · Covonia Sore Throat · Covonia Sore Throat 0.2%/0.05% oromucosal spray menthol · Denela · Denela 5% cream · Dentinox · Dentinox teething gel · Emla · Emla 5% cream · Emla 5% cream pre-medication pack · Iglu · Iglu oromucosal gel · Iglu Rapid Relief oromucosal gel · Instillagel · Instillagel gel · Lidocaine · Lidocaine 1% / Hydrocortisone 0.1% mouthwash · Lidocaine 5% / Phenylephrine 0.5% nasal spray · Lidocaine / Adrenaline · Lidocaine 100mg/10ml (1%) / Adrenaline (base) 50micrograms/10ml (1 in 200,000) solution for injection ampoules · Lidocaine 2% / Adrenaline (base) 0.05% nasal spray · Lidocaine 200mg/10ml (2%) / Adrenaline (base) 50micrograms/10ml (1 in 200,000) solution for injection ampoules · Lidocaine 4% / Adrenaline (base) 0.02% nasal solution · Lidocaine 4% / Tetracaine 0.5% / Adrenaline (base) 0.1% gel · Lidocaine 400mg/20ml (2%) / Adrenaline (base) 100micrograms/20ml (1 in 200,000) solution for injection vials · Lidocaine 50mg/10ml (0.5%) / Adrenaline (base) 50micrograms/10ml (1 in 200,000) solution for injection ampoules · Lidocaine / Chlorhexidine · Lidocaine 1% and Chlorhexidine gel · Lidocaine 2% and Chlorhexidine gel · Lidocaine / Prilocaine · Lidocaine 2.5% / Prilocaine 2.5% cream · Lignospan · Lignospan Special 20mg/ml / 12.5micrograms/ml solution for injection 1.8ml cartridges · Lignospan Special 20mg/ml / 12.5micrograms/ml solution for injection 2.2ml cartridges · Lignostab-A · Lignostab-A 2% 1 in 80,000 injection 2.2ml cartridges · Medijel · Medijel oromucosal gel · Medijel pastilles · Minims lidocaine and fluorescein · Minims lidocaine and fluorescein eye drops 0.5ml unit dose · Nulbia · Nulbia 5% cream · Pliaglis · Pliaglis 70mg/g / 70mg/g cream · Rapydan · Rapydan 70mg/70mg medicated plasters · Rexocaine · Rexocaine 2% injection 2.2ml cartridges · Rinstead · Rinstead teething gel · Woodward's · Woodward's teething gel · Xylocaine / Adrenaline · Xylocaine 0.5% with Adrenaline 100micrograms/20ml (1 in 200,000) solution for injection vials · Xylocaine 1% with Adrenaline 100micrograms/20ml (1 in 200,000) solution for injection vials · Xylocaine 2% with Adrenaline 1 in 80,000 Dental injection 2.2ml cartridges · Xylocaine 2% with Adrenaline 100micrograms/20ml (1 in 200,000) solution for injection vials · Xylonor · Xylonor 50mg/g / 1.5mg/g gel · Xylonor 150mg/g / 1.5mg/g oromucosal spray · Xylotox · Xylotox 2% E80 Dental injection 2.2ml cartridgesDenmark
Instillagel · Lidocaine / Adrenaline · Lidokain-adrenalin "SAD" · Lidokain-noradrenalin "SAD" · Pliapel · Ralydan · Xion · Xylocaine / Adrenaline · Xylocain-adrenalin · Xyloplyin Dental AdrenalinNorway
Pliaglis · Rapydan · Xylanaest mit Epinephrin · Xylocaine / Adrenaline · Xylocain Adrenalin · Xylocain Dental Adrenalin · Xylocain-Adrenalin · Xylocaine with adrenaline aspen · Xylocaine-Adrenaline · Xylocaine with epinephrinePoland
Anesderm · Calgel · EMLA · Emla Plaster · Lignocainum 2% c. noradrenalino 0,00125% WZF · Pliaglis · Rapydan · Xylodont 2% z adrenalina 1:100.000 · Xylodont 2% z adrenalina 1:50.000 · Xylodont 2% z adrenalina 1:80.000Luxembourg
EMLA · EMLA-PATCH · LIGNOSPAN · ORAQIX · Pliaglis · RAPYDAN · Xylocaine / Adrenaline · XYLOCAINE 1% ADRENALINE 1:200.000 · XYLOCAINE 2% ADRENALINE 1:200.000Iceland
Lident · Xylocaine / Adrenaline · Xylocain adrenalin · Xylocain Dental adrenalinFinland
Lidocaine / Adrenaline · Lidocain C Adrenalin · Xylocaine / Adrenaline · Xylocain Dental AdrenalinLatvia
Cathejell Lidocaine · Cathejell with Lidocaine · Cessolute · Emla · InstillagelSerbia
Calgel · Calgel® · Lidocaine / Adrenaline · LIDOKAIN 2%-ADRENALIN GALENIKA
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