Fluparoxan

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Fluparoxan
Fluparoxan.svg
Clinical data
Routes of
administration
Oral
Legal status
Legal status
  • Uncontrolled
Pharmacokinetic data
Bioavailability 85% oral from tablet formulation
Metabolism greater than 90% excreted as (sulphamic acid and carbamoyI glucuronide conjugates)
Biological half-life 6 hours
Excretion renal
Identifiers
Synonyms (+/-)-(trans)-5-fluoro-2,3,3a,9a-tetrahydro-1H-[1,4]benzodioxino[2,3-c]pyrrole hydrochloride hemihydrate
CAS Number (hydrochloride hemihydrate): 139679-54-2 101389-86-0 (free base)
(hydrochloride): 101389-87-1
Chemical and physical data
Formula C10H12ClFNO2.5
Molar mass 240.66 g·mol−1

Fluparoxan (GR50360A) (+/-)-(trans)-5-fluoro-2,3,3a,9a-tetrahydro-1H-[1,4]benzodioxino[2,3-c]pyrrole hydrochloride hemihydrate is a potent α2-adrenergic receptor antagonist (pKB = 7.9) with excellent α21 selectivity (2630 fold), and is the only well-studied a2 antagonist in its structural family which does not antagonize any variant of the imidazoline receptor.[1][2] It was shown to possess central α2-adrenoceptor antagonist activity after oral doses in man and was patented as an antidepressant by Glaxo in the early 1980s, but its development was discontinued when the compound failed to show a clear clinical advantage over existing therapies.[1]

Mechanism of action[edit]

Fluparoxan is a very selective α2-adrenergic blocker,[3] that readily cross the blood–brain barrier. Blockade of α2-adrenoreceptors, particularly presynaptic autoreceptors in noradrenergic neurons by fluparoxan, produces an increase in the synaptic concentrations of noradrenaline,[4] by blocking the autoinhibitory feedback mechanism. This release of noradrenaline has a potential value in the treatment of disorders which are associated with a deficiency of noradrenaline at postsynaptic adrenoreceptors, such as depression,[5] the early features of Alzheimer's disease and schizophrenia and other neurodevelopmental disorders associated with cognitive impairment.[6][7] Fluparoxan also exhibits no anticholinergic, antidopaminergic, alpha1-adrenergic, beta-adrenergic, muscarinic or 5-HT1-receptor-blocking effects.[3]

Pharmacology[edit]

Fluparoxan showed α2-adrenoceptors antagonist activity in vivo in several animal species.[3] In the conscious mouse, fluparoxan was effective by the oral route in preventing clonidine-induced hypothermia and antinociception. While in the rat the marked impairment of rotarod performance were prevented dose-dependently by fluparoxan. Fluparoxan, orally prevented agonist UK-14304 induced sedation and bradycardia in a dose-related fashion in the dog. Fluparoxan has been shown to possess central α2-adrenoceptor antagonist activity after both single and repeated oral doses in man, significantly attenuating all responses to the agonist clonidine (growth hormone secretion, bradycardia, hypotension, xerostomia) apart from the measures of sedation.[8]

Fluparoxan has shown positive effects in the treatment of cognitive dysfunction in schizophrenia patients when orally dosed with fluparoxan,[1] and in the treatment of central neurodegenerative disorders in models of Alzheimer's disease where it prevented age-related decline in spatial working memory in transgenic mice, although it had no effect in other memory tasks such as object recognition or the Morris water maze and occurred in the absence of obvious concomitant change in pathology such as β-amyloid plaque load and astrocytosis.[9]

The individual chiral isomers 7 (+) 3aR,9aR and 8 (-) 3aS,9aS of fluparoxan both had comparable levels of α2-adrenoceptors antagonist potency and α21 selectivity to racemic fluparoxan 6 (±) rel 3aR,9aR in vitro and a similar potency in vivo in reversing the hypothermia induced in mice by clonidine.[3]

Racemic Fluparoxan as HCl hemi-hydrate, (+)Enantiomer HCl and (-)EnantiomerHCl
Adrenoceptors antagonist potency of racemic fluparoxan and enantiomers in vitro and in vivo [1]
Compound as HCl α2-Adrenoceptors
Vas deferens
UK14304
α1-Adrenoceptors
Anococcygeus muscle
Phenylephrine
Hypothermia
Clonidine
Mice po
Optical Rotation Melting Point
Measurement pKB pKB ED50mg/kg [α]20-23 mp°C
6 (+/-) rel 3aR,9aR 7.86 5.00 0.66 0 245
7 (+) 3aR,9aR 7.88 4.47 0.73 +159.6 235-236
8 (-) 3aS,9aS 7.68 4.95 0.46 -159.4 238-240

Pharmacokinetics[edit]

Fluparoxan has rat and human protein binding of 81-92% and 95% respectively. Fluparoxan shows high in vitro permeability in MCDK (Papp nm/s =2500) and Caco-2 (Papp nm/s =2000) cells which correlates well with the known high oral intestinal absorption (100%) in humans.[10] Fluparoxan is well absorbed following oral dosing in all animals. Clearance was largely metabolic, with both oral and intravenous doses being excreted mainly via the urine (> 90%, of administered dose), chiefly as phase II metabolites (sulphamic acid and carbamoyI glucuronide conjugates).[11] Fluparoxan has high oral bioavailability (100%) and a long duration of action (2hr) in the rat,[1] which accounts for its similar potency seen by both the oral and intravenous routes of administration in this species.[3] The excellent pharmacokinetics exhibited by fluparoxan in animals also translated into man [1] where it has a superior bioavailability (97%) and longer duration of action (6-7hrs).

Metabolism[edit]

Fluparoxan was not metabolised by human cytochrome P450 enzymes CYP 1A and CYP 2A, and was found not to be a mutagen in cultured human peripheral lymphocytes and did not cause gene mutation when administered to Chinese hamster fibroblasts in culture.[11] No mutagenic potential was identified in microbiological mutagenicity tests including a fluctuation test with S9 activation. No hydroxylated metabolites were identified after incubation with rat liver microsomes (S9) or in rat urine following oral dosing.[1] The compound was well tolerated on repeat oral administration to rat (≤ 200 mg /kg/day) and dog (≤ 80 mg/kg/day) for 12 months.

Chemistry[edit]

Racemic (±) fluparoxan 6 is a white crystalline powder as the hydrochloride hemihydrate m.p. 245 °C.[1] It is a mixture of two enantiomers and is moderately lipophilic (log P = 1.2) with good solubility 80 mg/mL in water at 25 °C. The compound is very stable in the solid state and its bioavailability from tablet formulation is 85% and absorption is rapid.[1]

Synthesis[edit]

Racemic (±) fluparoxan 6 was first synthesised by a convergent route,[1][2] which involved converting the bis-benzyl ether of cis-butene-l,4-diol 1 into its epoxide 2 followed by acid catalyzed ring opening to a racemic-diol which was then converted into the racemic trans bis-tosylate 3. Coupling 3-fluorocatechol 4 with the racemic trans bis-tosylate 3 in the presence base gave on deprotection the benzodioxan diol 5 which was converted to racemic 6 via coupling its bis-mesylate to benzylamine followed by deprotection.[1][2]

The Convergent Synthesis of Fluparoxan

The individual chiral isomers (+) 7 and (-) 8 of fluparoxan were originally prepared from the (+) and (-) isomers of diethyl tartrate via the corresponding chiral trans bis-tosylates in a convergent route similar to that shown in the synthesis of racemic fluparoxan.[1]

History[edit]

Although fluparoxan has been shown to possess central α2-adrenoceptor antagonist activity after both single and repeated oral doses in man, clinical evaluation in depression and its development for the treatment of male sexual dysfunction was discontinued in the early 1990s when the compound failed to show a clear clinical advantage over existing therapies. The same is true for other α2-adrenoceptor antagonists in depression and it is now generally agreed that the original hypothesis that blocking α2-presynaptic adrenoceptors to increase brain levels of noradrenalin is insufficient as a neurobiological basis for depressive disorders, with the true picture likely to be much more complex and heterogeneous, involving both monoaminergic and nonmonoaminergic players.[12] In contrast however, recent interest in fluparoxan has increased with its positive effects in treating cognitive dysfunction in central neurodegenerative diseases.[1]

See also[edit]

References[edit]

  1. ^ a b c d e f g h i j k l m Borthwick AD (March 2016). "Fluparoxan: A Comprehensive Review of its Discovery, Adrenergic and CNS activity and treatment of Cognitive Dysfunction in central Neurodegenerative diseases". Mini reviews in medicinal chemistry. doi:10.2174/1389557516666160321115041. PMID 26996616. 
  2. ^ a b c Kitchin J, Borthwick AD, Brodie AC, Cherry PC, Crame AJ, Pipe AJ, Procopiou PA, Seaman MA, Turnbull JP (December 1995). "Synthesis of Benzodioxinopyrroles as selective α 2-adrenoceptor antagonists". Bioorganic & Medicinal Chemistry. 3 (12): 1595–1603. doi:10.1016/0968-0896(95)00143-3. PMID 8770384. 
  3. ^ a b c d e Halliday CA, Jones BJ, Skingle M, Walsh DM, Wise H, Tyers MB (April 1991). "The pharmacology of fluparoxan: a selective α2‐adrenoceptor antagonist". British Journal of Pharmacology. 102 (4): 887–895. doi:10.1111/j.1476-5381.1991.tb12272.x. PMC 1917968Freely accessible. PMID 1677298. 
  4. ^ Fernández-Pastor B, Meana JJ (May 2002). "In vivo tonic modulation of the noradrenaline release in the rat cortex by locus coeruleus somatodendritic α2-adrenoceptors". European Journal of Pharmacology. 442 (3): 225–229. doi:10.1016/S0014-2999(02)01543-1. PMID 12065075. 
  5. ^ Cottingham C, Wang Q (November 2012). "α2 Adrenergic receptor dysregulation in depressive disorders: implications for the neurobiology of depression and antidepressant therapy". Neuroscience & Biobehavioral Reviews. 36 (10): 2214–2225. doi:10.1016/j.neubiorev.2012.07.011. PMC 3508310Freely accessible. PMID 22910678. 
  6. ^ Marien MR, Colpaert FC, Rosenquist AC (April 2004). "Noradrenergic mechanisms in neurodegenerative diseases: a theory". Brain Research Reviews. 45 (1): 38–78. doi:10.1016/j.brainresrev.2004.02.002. PMID 15063099. 
  7. ^ Gibbs AA, Naudts KH, Azevedo RT, David AS (April 2010). "Deletion variant of α2b-adrenergic receptor gene moderates the effect of COMT val 158 met polymorphism on episodic memory performance". European Neuropsychopharmacology. 20 (4): 272–275. doi:10.1016/j.euroneuro.2009.12.007. PMID 20110158. 
  8. ^ Johnson MA, Blackwell CP, Smith J (May 1995). "Antagonism of the effects of clonidine by the alpha 2‐adrenoceptor antagonist, fluparoxan". British Journal of Clinical Pharmacology. 39 (5): 477–483. doi:10.1111/j.1365-2125.1995.tb04483.x. PMC 1365053Freely accessible. PMID 7669482. 
  9. ^ Scullion GA, Kendall DA, Marsden CA, Sunter D, Pardon MC (March 2011). "Chronic treatment with the α 2-adrenoceptor antagonist fluparoxan prevents age-related deficits in spatial working memory in APP× PS1 transgenic mice without altering β-amyloid plaque load or astrocytosis". Neuropharmacology. 60 (2): 223–234. doi:10.1016/j.neuropharm.2010.09.002. PMID 20850464. 
  10. ^ Gristwood WE (December 1990). "Determination of fluparoxan (GR50360) in plasma by gas chromatography". Journal of Chromatography B. 527: 436–440. doi:10.1016/S0378-4347(00)82128-3. PMID 2387889. 
  11. ^ a b Beresford AP, Ellis WJ, Ayrton J, Johnson MA, Lewis DF (January 1997). "Cytochrome P4501A (CYP1A) induction in rat and man by the benzodioxino derivative, fluparoxan". Xenobiotica. 27 (2): 159–173. doi:10.1080/004982597240668. PMID 9058530. 
  12. ^ Belmaker RH, Agam G (January 2008). "Major depressive disorder". New England Journal of Medicine. 358 (1): 55–68. doi:10.1056/NEJMra073096. PMID 18172175.