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Sitaxentan

Summary

Sitaxentan sodium (TBC-11251) is a medication for the treatment of pulmonary arterial hypertension (PAH).[1] It was marketed as Thelin by Encysive Pharmaceuticals until Pfizer purchased Encysive in February 2008. In 2010, Pfizer voluntarily removed sitaxentan from the market due to concerns about liver toxicity.[2]

Sitaxentan
Clinical data
Other namesTBC-11251
AHFS/Drugs.comInternational Drug Names
License data
  • EU EMAby sitaxentan sodium
Routes of
administration		Oral
ATC code
Legal status
Legal status
  • Withdrawn
Pharmacokinetic data
Bioavailability70 to 100%
Protein binding>99%
MetabolismHepatic (CYP2C9- and CYP3A4-mediated)
Elimination half-life10 hours
ExcretionRenal (50 to 60%)
Fecal (40 to 50%)
Identifiers
  • N-(4-chloro-3-methyl-5-isoxazolyl)-2-[[4,5-(methylenedioxy)-o-tolyl]acetyl]-3-thiophenesulfonamide
CAS Number
  • 184036-34-8
    210421-64-0 (sodium salt)
PubChem CID
  • 216235
IUPHAR/BPS
  • 3950
DrugBank
  • DB06268
ChemSpider
  • 21106381
UNII
  • J9QH779MEM
KEGG
  • D07171
ChEMBL
  • ChEMBL282724
CompTox Dashboard (EPA)
  • DTXSID0057673 Edit this at Wikidata
Chemical and physical data
FormulaC18H15ClN2O6S2
Molar mass454.90 g·mol−1
3D model (JSmol)
  • Interactive image
  • Cc1cc2OCOc2cc1CC(=O)c3sccc3S(=O)(=O)Nc4onc(C)c4Cl

Mechanism of action edit

Sitaxentan is a small molecule that blocks the action of endothelin (ET) on the endothelin-A (ETA) receptor selectively (by a factor of 6000 compared with the ETB).[3] It is a sulfonamide class endothelin receptor antagonist (ERA) and is undergoing Food and Drug Administration (FDA) review for treating pulmonary hypertension. The rationale for benefit compared with bosentan, a nonselective ET blocker, is negligible inhibition of the beneficial effects of ETB stimulation, such as nitric oxide production and clearance of ET from circulation. In clinical trials, the efficacy of sitaxentan has been much the same as bosentan, but the hepatotoxicity of sitaxentan outweighs its benefits. Dosing is once daily, as opposed to twice daily for bosentan.

Regulatory status edit

On December 10, 2010 Pfizer announced it would be withdrawing sitaxentan worldwide (both from marketing and from all clinical study use), citing that it is a cause of fatal liver damage.[2]

Sitaxentan was approved for marketing in the European Union in 2006, in Canada in 2006[4] and in Australia in 2007. By February 2008 it had been launched commercially in Germany, Austria, The Netherlands, the United Kingdom, Ireland, France, Spain and Italy.

In March 2006, the FDA recommended an approvable status to sitaxentan but said it would not yet approve the product. In July 2006, sitaxentan received a second approvable letter stating that efficacy outcome issues raised in the context of the STRIDE-2 study were still unresolved. In July 2007, Encysive commenced a formal dispute resolution process in a preliminary meeting with the FDA. In September 2007 the company announced that it was making preparations for another phase III clinical trial (intended to be named STRIDE-5) to overcome the FDA's concerns.[5] The takeover by Pfizer resulted in a reconfiguration and extension of these plans, to include combination therapy with sildenafil. The Sitaxentan Efficacy and Safety Trial With a Randomized Prospective Assessment of Adding Sildenafil (SR-PAAS) was an ongoing program of three clinical trials conducted in the United States (ClinicalTtrials.gov identifiers: NCT00795639, NCT00796666 and NCT00796510) with anticipated completion dates between June 2010 and January 2014.

Adverse effects edit

Adverse effects observed with sitaxentan are class effects of endothelin receptor antagonists, and include :

Because sitaxentan inhibits metabolism of warfarin, a decreased dose of warfarin is needed when co-administered with sitaxentan. This is because warfarin acts to prevent blood from clotting, and if it remains unmetabolized, it can continue to thin the blood.

References edit

  1. ^ Barst RJ, Langleben D, Frost A, Horn EM, Oudiz R, Shapiro S, et al. (February 2004). "Sitaxsentan therapy for pulmonary arterial hypertension". American Journal of Respiratory and Critical Care Medicine. 169 (4): 441–447. doi:10.1164/rccm.200307-957OC. PMID 14630619.
  2. ^ a b Citing liver damage, Pfizer withdraws Thelin, Associated Press, December 12, 2010
  3. ^ Girgis RE, Frost AE, Hill NS, Horn EM, Langleben D, McLaughlin VV, et al. (November 2007). "Selective endothelin A receptor antagonism with sitaxsentan for pulmonary arterial hypertension associated with connective tissue disease". Annals of the Rheumatic Diseases. 66 (11): 1467–1472. doi:10.1136/ard.2007.069609. PMC 2111639. PMID 17472992.
  4. ^ "UPDATE 1-Encysive gets Canadian approval for hypertension drug". Reuters. 30 May 2007. Retrieved 2007-07-08.
  5. ^ "Encysive Pharmaceuticals to Conduct Phase III Study With Thelin (Sitaxsentan Sodium) in Pulmonary Arterial Hypertension". PrimeNewswire via COMTEX News Network. 29 September 2007. Retrieved 2007-12-12.

Further reading edit

  • Mucke HA (January 2009). "Sitaxentan for the oral treatment of pulmonary arterial hypertension: benefits from endothelin receptor subtype selectivity?". Clinical Medicine: Therapeutics. 1: 111–121. doi:10.4137/CMT.S2344. CMT-S2344.
  • Barst RJ, Rich S, Widlitz A, Horn EM, McLaughlin V, McFarlin J (June 2002). "Clinical efficacy of sitaxsentan, an endothelin-A receptor antagonist, in patients with pulmonary arterial hypertension: open-label pilot study". Chest. 121 (6): 1860–8. doi:10.1378/chest.121.6.1860. PMID 12065350.

External links edit

  • "Encysive Announces PDUFA Date for Thelin New Drug Application in Pulmonary Arterial Hypertension". July 2005.
  • "Primary or Unexplained Pulmonary Hypertension". American Heart Association.

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