Peringatan Keamanan

The median lethal dose of lovastatin is higher than 15 g/m2. Five healthy human volunteers have received up to 200 mg of lovastatin as a single dose without clinically significant adverse experiences. A few cases of accidental overdosage have been reported; no patients had any specific symptoms, and all patients recovered without sequelae. The maximum dose taken was 5 to 6 g.^F4661

In carcinogenic studies, there is an increase in the incidence of hepatocellular carcinomas and adenomas, pulmonary adenomas, papilloma in non-glandular mucose in stomach and thyroid neoplasms. However, with respect to effects on fertility, lovastatin has been reported to present testicular atrophy, decreased spermatogenesis, spermatocytic degeneration and giant cell formation which derived into decreased fertility in males. Lastly, there is no evidence of mutagenicity induced by lovastatin.^F4661

Lovastatin

DB00227

small molecule approved investigational

Deskripsi

Lovastatin, also known as the brand name product Mevacor, is a lipid-lowering drug and fungal metabolite derived synthetically from a fermentation product of Aspergillus terreus.^A174550 Originally named Mevinolin, lovastatin belongs to the statin class of medications, which are used to lower the risk of cardiovascular disease and manage abnormal lipid levels by inhibiting the endogenous production of cholesterol in the liver.^A174553 More specifically, statin medications competitively inhibit the enzyme hydroxymethylglutaryl-coenzyme A (HMG-CoA) Reductase,^A181421 which catalyzes the conversion of HMG-CoA to mevalonic acid and is the third step in a sequence of metabolic reactions involved in the production of several compounds involved in lipid metabolism and transport including cholesterol, low-density lipoprotein (LDL) (sometimes referred to as "bad cholesterol"), and very low-density lipoprotein (VLDL). Prescribing of statin medications is considered standard practice following any cardiovascular events and for people with a moderate to high risk of development of CVD, such as those with Type 2 Diabetes. The clear evidence of the benefit of statin use coupled with very minimal side effects or long term effects has resulted in this class becoming one of the most widely prescribed medications in North America.A181087, A181406

Lovastatin and other drugs from the statin class of medications including atorvastatin, pravastatin, rosuvastatin, fluvastatin, and simvastatin are considered first-line options for the treatment of dyslipidemia.A181087, A181406 Increasing use of the statin class of drugs is largely due to the fact that cardiovascular disease (CVD), which includes heart attack, atherosclerosis, angina, peripheral artery disease, and stroke, has become a leading cause of death in high-income countries and a major cause of morbidity around the world.^A181084 Elevated cholesterol levels, and in particular, elevated low-density lipoprotein (LDL) levels, are an important risk factor for the development of CVD.A181087,A181553 Use of statins to target and reduce LDL levels has been shown in a number of landmark studies to significantly reduce the risk of development of CVD and all-cause mortality.A181090,A181093,A181096,A181427,A181475,A181538 Statins are considered a cost-effective treatment option for CVD due to their evidence of reducing all-cause mortality including fatal and non-fatal CVD as well as the need for surgical revascularization or angioplasty following a heart attack.A181087, A181406 Evidence has shown that even for low-risk individuals (with <10% risk of a major vascular event occurring within 5 years) statins cause a 20%-22% relative reduction in major cardiovascular events (heart attack, stroke, coronary revascularization, and coronary death) for every 1 mmol/L reduction in LDL without any significant side effects or risks.A181397, A181403

While all statin medications are considered equally effective from a clinical standpoint, rosuvastatin is considered the most potent; doses of 10 to 40mg rosuvastatin per day were found in clinical studies to result in a 45.8% to 54.6% decrease in LDL cholesterol levels, while lovastatin has been found to have an average decrease in LDL-C of 25-40%.A174580,A181409,A181535,A181538,A1793 Potency is thought to correlate to tissue permeability as the more lipophilic statins such as lovastatin are thought to enter endothelial cells by passive diffusion, as opposed to hydrophilic statins such as pravastatin and rosuvastatin which are taken up into hepatocytes through OATP1B1 (organic anion transporter protein 1B1)-mediated transport.A181424,A181460 Despite these differences in potency, several trials have demonstrated only minimal differences in terms of clinical outcomes between statins.A181538, A181427

Struktur Molekul 2D

Berat 404.5396

Wujud solid

Peta Jejaring Molekuler

Obat Target Gen Interaksi Enzim Transporter Carrier

Legenda: Obat • Target • Gen • Enzim • (Panah → menunjukkan arah efek / relasi) • Transporter • Carrier

1. Pendahuluan & Konsep

Fitur visualisasi ini dikembangkan menggunakan pendekatan Graph Theory untuk memetakan hubungan polifarmasi dan molekuler. Entitas (Obat, Target, Gen) direpresentasikan sebagai Simpul (Nodes), sedangkan hubungan biologisnya sebagai Sisi (Edges).

2. Sumber Data (Validasi)

Data Obat: Diekstraksi dari elemen drugbank-id dan name pada skema XML DrugBank.
Target Protein: Diambil dari elemen targets/target yang memuat polipeptida sasaran.
Genetik: Disinkronisasi dari sub-elemen gene-name dan varian snp-effects.
Genetik: Jumlah titik node dibatasi pada maksimal 10 (Slice=10) interaksi untuk menghindari tumpukan data.

3. Algoritma Visualisasi

Tata letak grafik menggunakan algoritma Force-Directed Graph (Barnes-Hut). Model fisika ini menerapkan gaya tolak-menolak antar simpul (Gravitasi: -3000) agar tidak tumpang tindih, serta gaya pegas (Spring: 0.04) pada garis penghubung untuk fleksibilitas interaksi.

4. Legenda Visual

Obat Utama (Pusat Analisis)

Target Protein (Mekanisme)

Gen (Faktor Genetik)

Metode ini mendukung analisis Precision Medicine dan evaluasi risiko Drug-Drug Interaction (DDI).

Profil Farmakokinetik

Waktu Paruh (Half-Life) Lovastatin half-life is reported to be of 13.37 hours.[F4664] The elimination half-life of the hydroxy acid form of lovastatin is reported to be of 0.7-3 hours.[A174583]

Volume Distribusi Lovastatin is able to cross the blood-brain barrier and placenta.[F4664]

Klirens (Clearance) -

Absorpsi

Lovastatin Cmax was found to be 3.013ng/mL with a Tmax of 3.36 hours.^F4664 Plasma concentrations of total radioactivity (lovastatin plus 14C-metabolites) peaked at 2 hours and declined rapidly to about 10% of peak by 24 hours postdose. Absorption of lovastatin, estimated relative to an intravenous reference dose, in each of four animal species tested, averaged about 30% of an oral dose. In animal studies, after oral dosing, lovastatin had high selectivity for the liver, where it achieved substantially higher concentrations than in non-target tissues. Lovastatin undergoes extensive first-pass extraction in the liver, its primary site of action, with subsequent excretion of drug equivalents in the bile. As a consequence of extensive hepatic extraction of lovastatin, the availability of drug to the general circulation is low and variable. In a single dose study in four hypercholesterolemic patients, it was estimated that less than 5% of an oral dose of lovastatin reaches the general circulation as active inhibitors. Following administration of lovastatin tablets the coefficient of variation, based on between-subject variability, was approximately 40% for the area under the curve (AUC) of total inhibitory activity in the general circulation.F4661,F4664 The peak concentrations of lovastatin when a dose of 10-40 mg is administered are reported to range from 1.04-4.03 ng/ml and an AUC of 14-53 ng.h/ml. This indicates that lovastatin presents a dose-dependent pharmacokinetic profile.^A174586 When lovastatin was given under fasting conditions, plasma concentrations of both active and total inhibitors were on average about two-thirds those found when lovastatin was administered immediately after a standard test meal.^F4664 Genetic differences in the OATP1B1 (Organic-Anion-Transporting Polypeptide 1B1) hepatic transporter encoded by the SCLCO1B1 gene (Solute Carrier Organic Anion Transporter family member 1B1) have been shown to impact lovastatin pharmacokinetics.^A181943 Evidence from pharmacogenetic studies of the c.521T>C single nucleotide polymorphism (SNP) showed that lovastatin Cmax and AUC were 340 and 286% higher, respectively, for individuals homozygous for 521CC compared to homozygous 521TT individuals.^A181946 The 521CC genotype is also associated with a marked increase in the risk of developing myopathy, likely secondary to increased systemic exposure.^A181955 Other statin drugs impacted by this polymorphism include rosuvastatin, pitavastatin, atorvastatin, simvastatin, and pravastatin.^A181460 While specific dosage instructions are not included in the available product monographs for lovastatin, individuals with the above-mentioned c.521CC OATP1B1 genotype should be monitored for development of adverse effects from increased exposure to the drug, such as muscle pain and risk of rhabdomyolysis, particularly at higher doses.

Metabolisme

Lovastatin is given as a lactone prodrug and thus, in order to produce its mechanism of action, it is required to be converted to the active beta-hydroxy form. This drug activation process does not seem to be related to CYP isoenzyme activity^A414 but rather to be controlled by the activity of serum paraoxonase.^A15320 Lovastatin is metabolized by the microsomal hepatic enzyme system (Cytochrome P-450 isoform 3A4). The major active metabolites present in human plasma are the ?-hydroxy acid of lovastatin, its 6'-hydroxy, 6'-hydroxymethyl, and 6'-exomethylene derivatives.^F4664 The uptake of lovastatin by the liver is enhanced by the activity of OATP1B1.^A35026

Rute Eliminasi

Following an oral dose of 14C-labeled lovastatin to man, 10% of the dose was excreted in urine and 83% in feces. The latter represents absorbed drug excreted in bile, together with unabsorbed drug.^F4664

Interaksi Makanan

2 Data

1. Avoid grapefruit products. Grapefruit products may increase the risk for lovastatin related adverse effects such as myopathy and rhabdomyolysis.
2. Take with food. Food increases bioavailability.

Interaksi Obat

568 Data

Reserpine	The metabolism of Lovastatin can be increased when combined with Reserpine.
Nifedipine	The metabolism of Nifedipine can be decreased when combined with Lovastatin.
Cyclosporine	The serum concentration of Lovastatin can be increased when it is combined with Cyclosporine.
Acipimox	Acipimox may increase the myopathic rhabdomyolysis activities of Lovastatin.
Bezafibrate	Bezafibrate may increase the myopathic rhabdomyolysis activities of Lovastatin.
Ciprofibrate	The risk or severity of myopathy, rhabdomyolysis, and myoglobinuria can be increased when Ciprofibrate is combined with Lovastatin.
Daptomycin	The risk or severity of myopathy can be increased when Lovastatin is combined with Daptomycin.
Gemfibrozil	The risk or severity of rhabdomyolysis, myoglobinuria, and elevated creatine kinase (CPK) can be increased when Gemfibrozil is combined with Lovastatin.
Raltegravir	The risk or severity of myopathy and rhabdomyolysis can be increased when Raltegravir is combined with Lovastatin.
Trabectedin	The risk or severity of myopathy and rhabdomyolysis can be increased when Lovastatin is combined with Trabectedin.
Everolimus	The metabolism of Lovastatin can be decreased when combined with Everolimus.
Ibrutinib	The metabolism of Ibrutinib can be decreased when combined with Lovastatin.
Fluconazole	The metabolism of Lovastatin can be decreased when combined with Fluconazole.
Avanafil	The serum concentration of Avanafil can be increased when it is combined with Lovastatin.
Eplerenone	The metabolism of Eplerenone can be decreased when combined with Lovastatin.
Erythromycin	The serum concentration of Lovastatin can be increased when it is combined with Erythromycin.
Cilostazol	The serum concentration of Lovastatin can be increased when it is combined with Cilostazol.
Colchicine	Colchicine may increase the myopathic rhabdomyolysis activities of Lovastatin.
Fentanyl	The metabolism of Fentanyl can be decreased when combined with Lovastatin.
Vardenafil	The metabolism of Vardenafil can be decreased when combined with Lovastatin.
Boceprevir	The risk or severity of myopathy and rhabdomyolysis can be increased when Boceprevir is combined with Lovastatin.
Bosentan	The serum concentration of Lovastatin can be decreased when it is combined with Bosentan.
Clarithromycin	The risk or severity of myopathy and rhabdomyolysis can be increased when Clarithromycin is combined with Lovastatin.
Diltiazem	The serum concentration of Lovastatin can be increased when it is combined with Diltiazem.
Etoposide	The metabolism of Lovastatin can be decreased when combined with Etoposide.
Aldesleukin	The metabolism of Lovastatin can be decreased when combined with Aldesleukin.
Octreotide	The metabolism of Lovastatin can be decreased when combined with Octreotide.
Fluvoxamine	The metabolism of Lovastatin can be decreased when combined with Fluvoxamine.
Citalopram	The metabolism of Lovastatin can be decreased when combined with Citalopram.
Ziprasidone	The metabolism of Lovastatin can be decreased when combined with Ziprasidone.
Cabergoline	The metabolism of Lovastatin can be decreased when combined with Cabergoline.
Diethylstilbestrol	The metabolism of Lovastatin can be decreased when combined with Diethylstilbestrol.
Isradipine	The metabolism of Lovastatin can be decreased when combined with Isradipine.
Valproic acid	The metabolism of Lovastatin can be decreased when combined with Valproic acid.
Acetaminophen	The metabolism of Lovastatin can be decreased when combined with Acetaminophen.
Dihydroergotamine	The metabolism of Lovastatin can be decreased when combined with Dihydroergotamine.
Methadone	The metabolism of Lovastatin can be decreased when combined with Methadone.
Methylergometrine	The metabolism of Lovastatin can be decreased when combined with Methylergometrine.
Mefloquine	The metabolism of Lovastatin can be decreased when combined with Mefloquine.
Clozapine	The metabolism of Lovastatin can be decreased when combined with Clozapine.
Mirtazapine	The metabolism of Lovastatin can be decreased when combined with Mirtazapine.
Sorafenib	The metabolism of Lovastatin can be decreased when combined with Sorafenib.
Nitric Oxide	The metabolism of Lovastatin can be decreased when combined with Nitric Oxide.
Cerivastatin	The metabolism of Lovastatin can be decreased when combined with Cerivastatin.
Teniposide	The metabolism of Lovastatin can be decreased when combined with Teniposide.
Chloramphenicol	The metabolism of Lovastatin can be decreased when combined with Chloramphenicol.
Lansoprazole	The metabolism of Lovastatin can be decreased when combined with Lansoprazole.
Quinine	The metabolism of Lovastatin can be decreased when combined with Quinine.
Raloxifene	The metabolism of Lovastatin can be decreased when combined with Raloxifene.
Cimetidine	The metabolism of Lovastatin can be decreased when combined with Cimetidine.
Haloperidol	The metabolism of Lovastatin can be decreased when combined with Haloperidol.
Ciprofloxacin	The metabolism of Lovastatin can be decreased when combined with Ciprofloxacin.
Zafirlukast	The metabolism of Lovastatin can be decreased when combined with Zafirlukast.
Vinblastine	The metabolism of Lovastatin can be decreased when combined with Vinblastine.
Fluticasone propionate	The metabolism of Lovastatin can be decreased when combined with Fluticasone propionate.
Thiopental	The metabolism of Lovastatin can be decreased when combined with Thiopental.
Imatinib	The metabolism of Lovastatin can be decreased when combined with Imatinib.
Nicardipine	The metabolism of Lovastatin can be decreased when combined with Nicardipine.
Astemizole	The metabolism of Lovastatin can be decreased when combined with Astemizole.
Dextropropoxyphene	The metabolism of Lovastatin can be decreased when combined with Dextropropoxyphene.
Epinephrine	The metabolism of Lovastatin can be decreased when combined with Epinephrine.
Aprepitant	The metabolism of Lovastatin can be decreased when combined with Aprepitant.
Tamoxifen	The metabolism of Lovastatin can be decreased when combined with Tamoxifen.
Daunorubicin	The metabolism of Lovastatin can be decreased when combined with Daunorubicin.
Paroxetine	The metabolism of Lovastatin can be decreased when combined with Paroxetine.
Tranylcypromine	The metabolism of Lovastatin can be decreased when combined with Tranylcypromine.
Tetracycline	The metabolism of Lovastatin can be decreased when combined with Tetracycline.
Roxithromycin	The metabolism of Lovastatin can be decreased when combined with Roxithromycin.
Phenelzine	The metabolism of Lovastatin can be decreased when combined with Phenelzine.
Propofol	The metabolism of Lovastatin can be decreased when combined with Propofol.
Acetazolamide	The metabolism of Lovastatin can be decreased when combined with Acetazolamide.
Diazepam	The metabolism of Lovastatin can be decreased when combined with Diazepam.
Clofazimine	The metabolism of Lovastatin can be decreased when combined with Clofazimine.
Tacrolimus	The metabolism of Lovastatin can be decreased when combined with Tacrolimus.
Ethanol	The metabolism of Lovastatin can be decreased when combined with Ethanol.
Quinidine	The metabolism of Lovastatin can be decreased when combined with Quinidine.
Metronidazole	The metabolism of Lovastatin can be decreased when combined with Metronidazole.
Buprenorphine	The metabolism of Lovastatin can be decreased when combined with Buprenorphine.
Isoniazid	The metabolism of Lovastatin can be decreased when combined with Isoniazid.
Dirithromycin	The metabolism of Lovastatin can be decreased when combined with Dirithromycin.
Doxorubicin	The metabolism of Lovastatin can be decreased when combined with Doxorubicin.
Metyrapone	The metabolism of Lovastatin can be decreased when combined with Metyrapone.
Sulfamethoxazole	The metabolism of Lovastatin can be decreased when combined with Sulfamethoxazole.
Glyburide	The metabolism of Lovastatin can be decreased when combined with Glyburide.
Irbesartan	The metabolism of Lovastatin can be decreased when combined with Irbesartan.
Topotecan	The metabolism of Lovastatin can be decreased when combined with Topotecan.
Norfloxacin	The metabolism of Lovastatin can be decreased when combined with Norfloxacin.
Oxybutynin	The metabolism of Lovastatin can be decreased when combined with Oxybutynin.
Mequitazine	The metabolism of Lovastatin can be decreased when combined with Mequitazine.
Primaquine	The metabolism of Lovastatin can be decreased when combined with Primaquine.
Dimethyl sulfoxide	The metabolism of Lovastatin can be decreased when combined with Dimethyl sulfoxide.
Fluvastatin	The metabolism of Lovastatin can be decreased when combined with Fluvastatin.
Pimozide	The metabolism of Lovastatin can be decreased when combined with Pimozide.
Miconazole	The metabolism of Lovastatin can be decreased when combined with Miconazole.
Bicalutamide	The metabolism of Lovastatin can be decreased when combined with Bicalutamide.
Rabeprazole	The metabolism of Lovastatin can be decreased when combined with Rabeprazole.
Desipramine	The metabolism of Lovastatin can be decreased when combined with Desipramine.
Candicidin	The metabolism of Lovastatin can be decreased when combined with Candicidin.
Orphenadrine	The metabolism of Lovastatin can be decreased when combined with Orphenadrine.
Ifosfamide	The metabolism of Lovastatin can be decreased when combined with Ifosfamide.

Target Protein

3-hydroxy-3-methylglutaryl-coenzyme A reductase HMGCR

Integrin alpha-L ITGAL

Histone deacetylase 2 HDAC2

Referensi & Sumber

Synthesis reference: Donald F. Gerson, Xinfa Xiao, "Process for the production of lovastatin using Coniothyrium fuckelii." U.S. Patent US5409820, issued January, 1984.

Artikel (PubMed)

PMID: 28102516
Boruta T, Bizukojc M: Production of lovastatin and itaconic acid by Aspergillus terreus: a comparative perspective. World J Microbiol Biotechnol. 2017 Feb;33(2):34. doi: 10.1007/s11274-017-2206-9. Epub 2017 Jan 19.
PMID: 6933445
Alberts AW, Chen J, Kuron G, Hunt V, Huff J, Hoffman C, Rothrock J, Lopez M, Joshua H, Harris E, Patchett A, Monaghan R, Currie S, Stapley E, Albers-Schonberg G, Hensens O, Hirshfield J, Hoogsteen K, Liesch J, Springer J: Mevinolin: a highly potent competitive inhibitor of hydroxymethylglutaryl-coenzyme A reductase and a cholesterol-lowering agent. Proc Natl Acad Sci U S A. 1980 Jul;77(7):3957-61.
PMID: 15531285
Endo A: The origin of the statins. 2004. Atheroscler Suppl. 2004 Oct;5(3):125-30. doi: 10.1016/j.atherosclerosissup.2004.08.033.
PMID: 7890038
Chiloeches A, Lasa M, Brihuega F, Montes A, Toro MJ: Effects of lovastatin on adenylyl cyclase activity and G proteins in GH4C1 cells. FEBS Lett. 1995 Mar 13;361(1):46-50.
PMID: 3069436
Henwood JM, Heel RC: Lovastatin. A preliminary review of its pharmacodynamic properties and therapeutic use in hyperlipidaemia. Drugs. 1988 Oct;36(4):429-54. doi: 10.2165/00003495-198836040-00003.
PMID: 9160173
Lennernas H, Fager G: Pharmacodynamics and pharmacokinetics of the HMG-CoA reductase inhibitors. Similarities and differences. Clin Pharmacokinet. 1997 May;32(5):403-25. doi: 10.2165/00003088-199732050-00005.
PMID: 22992668
Whirl-Carrillo M, McDonagh EM, Hebert JM, Gong L, Sangkuhl K, Thorn CF, Altman RB, Klein TE: Pharmacogenomics knowledge for personalized medicine. Clin Pharmacol Ther. 2012 Oct;92(4):414-7. doi: 10.1038/clpt.2012.96.
PMID: 12015788
Lamson M, Phillips G, Shen J, Lukacsko P, Friedhoff L, Niecestro RM: Pharmacokinetics of lovastatin extended-release dosage form (Lovastatin XL) in healthy volunteers. Biopharm Drug Dispos. 2002 May;23(4):143-9. doi: 10.1002/bdd.304.

Menampilkan 8 dari 38 artikel.

Textbook

Acton A. (2013). Advances in Lovastatin Research and Application. ScholarlyBrief.
ISBN: 0-7432-9925-6
Loughlin K. and Generali J. (2006). Prescription Drugs: Alternative Uses, Alternative Cures. Free Press.

Link

Attachment

Contoh Produk & Brand

Produk: 330 • International brands: 1

Produk

Act Lovastatin

Tablet • 20 mg • Oral • Canada • Approved
Act Lovastatin

Tablet • 40 mg • Oral • Canada • Approved
Advicor

Tablet, extended release • - • Oral • US • Approved
Advicor

Tablet, extended release • - • Oral • US • Approved
Advicor

Tablet, extended release • - • Oral • US • Approved
Advicor

Tablet, extended release • - • Oral • US • Approved
Advicor

Tablet, extended release • - • Oral • US • Approved
Advicor

Tablet, extended release • - • Oral • US • Approved

Menampilkan 8 dari 330 produk.

International Brands

Altocor — Andrx

Sekuens Gen/Protein (FASTA)

Sekuens dimuat saat dibutuhkan agar halaman tetap ringan.