Bosentan

C02K - Other antihypertensives ATC C02KX01 Small molecule approved 2001 Oral Natural product Black-box warning

JFDA label: Tracleer 62.5mg

⚠ Black-Box Warning

Distribution program:
Hepatotoxicity:
Embryo-fetal toxicity:

Mechanism of Action

Antagonist of Endothelin receptor, ET-A/ET-B — Endothelin receptor, ET-A/ET-B antagonist

Target	Action	Gene / class
Endothelin receptor, ET-A/ET-B efficacy	ANTAGONIST

Indications

Approved

Pulmonary arterial hypertension

Off-label

Prevention of digital ulcers in systemic sclerosis
Raynaud phenomenon in systemic sclerosis

Contraindications

Source: Lexicomp

Additional contraindications (not in US labeling): Moderate to severe hepatic impairment (eg, ALT or AST >3 times ULN, particularly when total bilirubin >2 times ULN) Absolute
Hypersensitivity to bosentan or any component of the formulation Absolute
concurrent use of cyclosporine or glyburide Absolute
use in women who are or may become pregnant Absolute

Adverse Reactions

Very Common >10%Common 1–10%Uncommon 0.1–1% Rare 0.01–0.1%Very Rare <0.01%Not Known

Cardiac disorders (6)

Very Common Edema

Common Chest pain · flushing · hypotension · palpitations · syncope

Nervous system disorders (1)

Very Common Headache

Hepatobiliary disorders (2)

Very Common Increased serum ALT · increased serum AST

Blood and lymphatic system disorders (1)

Common Anemia

Metabolism and nutrition disorders (1)

Common Fluid retention

Musculoskeletal and connective tissue disorders (1)

Common Arthralgia

Respiratory, thoracic and mediastinal disorders (2)

Very Common Respiratory tract infection

Common Sinusitis

Dosing

Source: Lexicomp

Pulmonary artery hypertension: Oral: ≥40 kg: Initial: 62.5 mg twice daily for 4 weeks; increase to maintenance dose of 125 mg twice daily. Doses >125 mg twice daily do not appear to confer additional clinical benefit but may increase risk of hepatotoxicity. Note: When discontinuing treatment, consider a reduction in dosage to 62.5 mg twice daily for 3 to 7 days (to avoid clinical deterioration). Coadministration with ritonavir: Oral: Dosage adjustment for concurrent use with ritonavir: Coadministration of bosentan in patients currently receiving ritonavir for at least 10 days: Begin with bosentan 62.5 mg once daily or every other day based on tolerability. Coadministration of ritonavir in patients currently receiving bosentan: Discontinue bosentan 36 hours prior to the initiation of ritonavir. After at least 10 days following the initiation of ritonavir, resume bosentan 62.5 mg once daily or every other day based on tolerability. Prevention of digital ulcers in systemic sclerosis (off-label use): Oral: 62.5 mg twice daily for 4 weeks followed by an increase to a maintenance dose of 125 mg twice daily; has been studied in clinical trials for up to 12 weeks (Korn 2004) Raynaud phenomenon in systemic sclerosis (off-label use): Oral: 62.5 mg twice daily for 4 weeks followed by an increase to a maintenance dose of 125 mg twice daily (Giordano 2010; Hettema 2007).

(For additional information see "Bosentan: Pediatric drug information") Pulmonary artery hypertension: Oral: Manufacturer’s labeling: Children 3 to ≤ 12 years: ≥4 to 8 kg: Initial and maintenance: 16 mg twice daily. >8 to 16 kg: Initial and maintenance: 32 mg twice daily. >16 to 24 kg: Initial and maintenance: 48 mg twice daily. >24 to 40 kg: Initial and maintenance: 64 mg twice daily. Alternate recommendations: Infants ≥7 months and Children ≤12 years: Limited data available (Barst 2003; Ivy 2004; Maiya 2006; Rosenzweig 2005): 5 to 10 to 20 kg: Initial: 31.25 mg daily for 4 weeks; increase to maintenance dose of 31.25 mg twice daily. >20 to 40 kg: Initial: 31.25 mg twice daily for 4 weeks; increase to maintenance dose of 62.5 mg twice daily. >40 kg: Initial: 62.5 mg twice daily for 4 weeks; increase to maintenance dose of 125 mg twice daily. Children >12 years and Adolescents (>40 kg): Refer to adult dosing.

Refer to adult dosing.

No dosage adjustment necessary. Bosentan is unlikely to be removed by dialysis (due to high molecular weight and extensive plasma protein binding).

Hepatic impairment at treatment initiation: Mild impairment (Child-Pugh class A): No dosage adjustment necessary. Moderate to severe impairment (Child-Pugh class B and C) and/or baseline transaminase >3 times ULN: Avoid use; systemic exposure is significantly increased in patients with moderate impairment (has not been studied in severe impairment). Hepatotoxicity during treatment: Modification based on transaminase elevation: Transaminase elevations accompanied by clinical symptoms of hepatotoxicity (unusual fatigue, nausea, vomiting, abdominal pain, fever, or jaundice) or a serum bilirubin ≥2 times ULN: Discontinue treatment. AST/ALT >3 times but ≤5 times ULN: Children 3 to ≤12 years: Confirm with additional test; if confirmed, interrupt treatment with no prior dose reduction. If transaminase levels return to pretreatment values, may reintroduce treatment at the dose used prior to treatment interruption. When reintroducing treatment, recheck transaminases within 3 days and at least every 2 weeks thereafter. Adolescents >12 years and Adults (>40 kg): Confirm with additional test; if confirmed, reduce dose to 62.5 mg twice daily or interrupt treatment and monitor at least every 2 weeks. If transaminase levels return to pretreatment values, may continue or reintroduce treatment (at the starting dose), as appropriate. When reintroducing treatment, recheck transaminases within 3 days and at least every 2 weeks thereafter. AST/ALT >5 times but ≤8 times ULN: Children 3 to ≤12 years: Confirm with additional test; if confirmed, stop treatment. Monitor transaminase levels at least every 2 weeks. If transaminase levels return to pretreatment values, consider reintroduction at the dose used prior to treatment interruption. When reintroducing treatment, recheck transaminases within 3 days and at least every 2 weeks thereafter. Adolescents >12 years and Adults (>40 kg): Confirm with additional test; if confirmed, stop treatment. Monitor transaminase levels at least every 2 weeks. If transaminase levels return to pretreatment values, may reintroduce treatment (at the starting dose) as appropriate. When reintroducing treatment, recheck transaminases within 3 days and at least every 2 weeks thereafter. AST/ALT >8 times ULN: Stop treatment and do not reintroduce.

Warnings & Precautions

Source: Lexicomp

Fluid retention/peripheral edema

Development of peripheral edema due to treatment and/or disease state (pulmonary arterial hypertension) may occur. There have also been postmarketing reports of fluid retention requiring treatment (eg, diuretics, fluid management, hospitalization) for heart failure. If clinically significant fluid retention develops (with or without weight gain), further evaluation is necessary to determine cause and appropriate treatment or discontinuation of therapy. Use with caution in patients with underlying heart failure due to potential complications from fluid retention. In a scientific statement from the American Heart Association, bosentan has been determined to be an agent that may exacerbate underlying myocardial dysfunction (magnitude: major) (AHA [Page 2016]).

Hematologic effects

Dose-related decreases in hematocrit/hemoglobin may be observed, usually within the first few weeks of therapy with subsequent stabilization of levels by 4 to 12 weeks of treatment. Monitor hemoglobin prior to treatment initiation, after 1 and 3 months, and every 3 months thereafter. Significant decreases in hemoglobin require further evaluation to determine the cause and specific management.

Hepatotoxicity

Bosentan is associated with transaminase elevations (ALT or AST ≥3 times ULN), and in a small number of cases may occur with elevations in bilirubin. Monitor transaminases at baseline then monthly thereafter. Adjust dosage if elevations in liver enzymes occur without symptoms of hepatic injury or elevated bilirubin. In the postmarketing surveillance (with close monitoring), there have been rare cases of unexplained hepatic cirrhosis after prolonged therapy (>12 months) in patients with multiple comorbidities and drug therapies. There have also been cases of hepatic failure. Treatment should be stopped in patients who develop elevated transaminases either in combination with symptoms of hepatic injury (unusual fatigue, jaundice, nausea, vomiting, abdominal pain, and/or fever) or elevated bilirubin (≥2 times ULN); safety of reintroduction is unknown. Avoid use in patients with baseline serum transaminases >3 times ULN at baseline (monitoring for hepatotoxicity may be more difficult) or moderate to severe hepatic impairment. The combination of hepatocellular injury (transaminase elevations >3 times ULN) and bilirubin increased ≥2 times ULN are a marker for potential serious hepatotoxicity. Transaminase elevations are dose dependent, generally asymptomatic, occur both early and late in therapy, progress slowly, and are usually reversible after treatment interruption or discontinuation. Transaminase elevations may also spontaneously reverse while continuing bosentan treatment. Con

Hypersensitivity

Hypersensitivity reactions, including Drug Reaction with Eosinophilia and Systemic Symptoms (DRESS), anaphylaxis, rash and angioedema have been observed.

Spermatogenesis

Decreased sperm counts have been observed in men during treatment; bosentan may have an adverse effect on spermatogenesis.

Pulmonary veno-occlusive disease

If signs of pulmonary edema occur, consider possibility of pulmonary veno-occlusive disease; may require discontinuation of bosentan. Concurrent drug therapy issues:

Drug-drug interactions

Potentially significant interactions may exist, requiring dose or frequency adjustment, additional monitoring, and/or selection of alternative therapy. Consult drug interactions database for more detailed information. Special populations:

Pregnancy

Bosentan is likely to cause major birth defects if used by pregnant women based on animal data. Therefore, pregnancy must be excluded before the start of treatment with bosentan. Throughout treatment and for 1 month after stopping bosentan, women of childbearing potential must use 2 reliable methods of contraception unless the patient has an intrauterine device (IUD) or tubal sterilization in which case no other contraception is needed. Hormonal contraceptives, including oral, injectable, transdermal, and implantable contraceptives, should not be used as the sole means of contraception because these may not be effective in patients receiving bosentan. Obtain monthly pregnancy tests. Other warnings/precautions:

REMS program

Because of the risks of hepatotoxicity and birth defects, bosentan is only available through the Tracleer REMS Program. The Tracleer REMS Program is a component of the bosentan Risk Evaluation and Mitigation Strategy (REMS). Patients, prescribers, and pharmacies must enroll with the program. Call 1-866-228-3546 or visit http://www.tracleer.com/hcp/prescribing-tracleer.asp for more information.

Pregnancy & Lactation

Pregnancy

FDA category X Teratogenic Contraindicated

Contraindicated

Monthly pregnancy tests and two forms of contraception required due to teratogenic potential

Lactation

Avoid

It is not known if bosentan is present in breast milk. Due to the potential for serious adverse reactions in the breastfed infant, breastfeeding is not recommended by the manufacturer.

Monitoring

Clinical pearl	Serum transaminase (AST and ALT) and bilirubin (prior to treatment initiation and monthly thereafter, or more frequently if clinically necessary [every 2 weeks following transaminase elevations and 3 days after reintroducing therapy if withheld due to transaminase elevations]). Hemoglobin and hematocrit (at baseline, at 1 month and 3 months of treatment, and every 3 months thereafter [generally stabilizes after 4 to 12 weeks of treatment]). Pregnancy test in women of childbearing potential (prior to the initiation of therapy, monthly during treatment, and one month after stopping bosentan). Monitor for clinical signs/symptoms of liver injury (eg, abdominal pain, fatigue, fever, jaundice, nausea, vomiting) and fluid retention.

Clinical pearl

Serum transaminase (AST and ALT) and bilirubin (prior to treatment initiation and monthly thereafter, or more frequently if clinically necessary [every 2 weeks following transaminase elevations and 3 days after reintroducing therapy if withheld due to transaminase elevations]). Hemoglobin and hematocrit (at baseline, at 1 month and 3 months of treatment, and every 3 months thereafter [generally stabilizes after 4 to 12 weeks of treatment]). Pregnancy test in women of childbearing potential (prior to the initiation of therapy, monthly during treatment, and one month after stopping bosentan). Monitor for clinical signs/symptoms of liver injury (eg, abdominal pain, fatigue, fever, jaundice, nausea, vomiting) and fluid retention.

Chemistry & Properties

Formula	C27H29N5O6S
Molecular weight	551.63 g/mol
IUPAC name	4-tert-butyl-N-[6-(2-hydroxyethoxy)-5-(2-methoxyphenoxy)-2-pyrimidin-2-ylpyrimidin-4-yl]benzenesulfonamide
CAS	147536-97-8
PubChem CID	104865
InChIKey	`GJPICJJJRGTNOD-UHFFFAOYSA-N`
logP	4.2 (XLogP 3.8)
Polar surface area	145.65 Å²
H-bond acceptors / donors	10 / 2
Drug-likeness (QED)	0.29
Lipinski violations	1

SMILES

COc1ccccc1Oc1c(NS(=O)(=O)c2ccc(C(C)(C)C)cc2)nc(-c2ncccn2)nc1OCCO

Biology & Pharmacokinetics

Pharmacokinetics

BBB penetrant	No

Enzyme interactions

Enzyme	Role	Detail
CYP2C19	Inhibitor	—
CYP2C8	Inhibitor	—
CYP2C9	Inhibitor	—
CYP2C9	Substrate	—
CYP3A4	Inhibitor	—
CYP3A4	Substrate	—

Receptor binding (top 1)

Target	Action	Affinity
ETB receptor (EDNRB)	Antagonist	pKi 7.1

Transporters

BCRP (Inhibitor)BSEP (Inhibitor)BSEP (Inhibitor)MDR1 (Inhibitor)MRP1 (Inhibitor)MRP2 (Inhibitor)MRP3 (Inhibitor)MRP4 (Inhibitor)NTCP (Inhibitor)OAT (Inhibitor)OATP (Inhibitor)OATP1B1 (Inhibitor)OATP1B1 (Inhibitor)OATP1B3 (Inhibitor)OATP1B3 (Inhibitor)P-gp (Inhibitor)Transporter(unspecified) (Inhibitor)MDR1 (Substrate)OATP (Substrate)OATP1B1 (Substrate)OATP1B3 (Substrate)OATP2B1 (Substrate)P-gp (Substrate)Transporter(unspecified) (Substrate)

Drug–drug interactions (100+, DDInter)

Interacting drug	Severity	Management
Axitinib	major
Bosutinib	major
Brigatinib	major
Cobicistat	major
Cobimetinib	major
Cyclosporine	major
Deflazacort	major
Encorafenib	major
Entrectinib	major
Ethinylestradiol	major
Fedratinib	major
Glasdegib	major
Glyburide	major
Hydrocodone	major
Leflunomide	major
Lorlatinib	major
Medroxyprogesterone acetate	major
Neratinib	major
Olaparib	major
Siponimod	major
Sonidegib	major
Teriflunomide	major
Venetoclax	major
Abemaciclib	moderate
Acalabrutinib	moderate
Acetohexamide	moderate
Albendazole	moderate
Alpelisib	moderate
Apalutamide	moderate
Apixaban	moderate
Apremilast	moderate
Aprepitant	moderate
Artemether	moderate
Asparaginase Escherichia coli	moderate
Astemizole	moderate
Betamethasone	moderate
Brentuximab vedotin	moderate
Brimonidine (ophthalmic)	moderate
Brimonidine (topical)	moderate
Busulfan	moderate

Showing 40 of 100+.

Registered Products (9)

Brand	Form / strength	Pack	Agent	Citizen (JOD)
Bosentas 62.5	Tablet 62.5 mg	14 tab	ORIENT DRUG STORE CO	9.830
Bosentas 125	Tablet 125 mg	14 tab	ORIENT DRUG STORE CO	16.120
Gonista	Film-Coated Tablet 125.0 mg	56 F.C Tab pack varies	UNITED PHARM.MFG.CO.LTD(UPM)/JORDAN	—
Gonista	Film-Coated Tablet 62.5 mg	60 F.C Tab	UNITED PHARM.MFG.CO.LTD(UPM)/JORDAN	—
Gonista	Film-Coated Tablet 125.0 mg	60 F.C Tab pack varies	UNITED PHARM.MFG.CO.LTD(UPM)/JORDAN	—
Pahex	Tablet 62.5 mg	56 tab	Sun Set Drug Store	—
Pahex	Tablet 125 mg	56 tab	Sun Set Drug Store	—
Tracleer	Tablet 62.5 mg	56 tab	Shawi & Rushedat Drug Store	—
Tracleer	Tablet 125 mg	56 tab	Shawi & Rushedat Drug Store	—