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PSEUDO-EPHEDRIN
DRHerni Suprapti dr MKes
Mei 2022
1
Overview
Mei2022 2
◦ Theadrenergicdrugsaffectreceptorsthatarestimulatedbynorepinephrine
(noradrenaline)or epinephrine (adrenaline).
◦ Thesereceptorsareknownasadrenergicreceptorsoradrenoceptors.
◦ Adrenergicdrugsthatactivateadrenergicreceptorsaretermedsympathomimetics,
anddrugsthatblocktheactivationof adrenergicreceptorsaretermedsympatholytic.
◦ Somesympathomimeticsdirectlyactivateadrenergicreceptors(direct-acting
agonists),whileothersactindirectlybyenhancingreleaseorblockingreuptakeof
norepinephrine(indirect-acting agonists).
Adrenergicagonists (*):catecholamines.
Mei2022 3
DIRECT
-ACTINGAGENTS
◦ Albuterol
◦ Clonidine
◦ Dobutamine*
◦ Dopamine*
◦ Epinephrine*
◦ Fenoldopam
◦ Formoterol
◦ Isoproterenol*
◦ Mirabegron
◦ Norepinephrine*
◦ Phenylephrine
◦ Salmeterol
◦ Terbutaline
INDIRECT
-ACTINGAGENTS
◦ Amphetamine
◦ Cocaine
DIRECTANDINDIRECTACTING(mixedaction)
AGENTS
◦ Ephedrine
◦ Pseudoephedrine
Adrenergicreceptors (adrenoceptors)
Mei2022 4
◦ Inthesympatheticnervoussystem,severalclassesof adrenoceptorscanbedistinguished
pharmacologically
.
◦ Twomainfamiliesof receptors,designated andβ, areclassifiedonthebasisof theirresponses
to the adrenergicagonistsepinephrine, norepinephrine,and isoproterenol.
◦ Eachof thesemainreceptortypeshasanumberof specificreceptorsubtypesthathavebeen
identified.
◦ Alterationsin the primary structure of thereceptors influence their affinity for various agents.
Mei2022 5
A.Catecholamines
Mei2022 6
Sympathomimeticaminesthatcontainthe3,4-dihydroxybenzenegroup (suchasepinephrine,
norepinephrine,isoproterenol,anddopamine)arecalledcatecholamines.Thesecompoundsshare
thefollowing properties:
1. Highpotency:Catecholamines(with–OH groupsinthe3and4positionsonthebenzenering)
showthehighest potencyin directlyactivating α or β receptors.
2. Rapidinactivation:CatecholaminesaremetabolizedbyCOMTpostsynapticallyandbyMAO
intraneuronally,aswellasbyCOMTandMAO inthegutwall,andbyMAO intheliver.Thus,
catecholamineshaveonlyabrief period of actionwhengivenparenterally
,andtheyare
inactivated(ineffective)whenadministered orally
.
3. PoorpenetrationintotheCNS:Catecholaminesarepolarand,therefore,do notreadily
penetrateintotheCNS.Nevertheless,mostcatecholamineshavesomeclinicaleffects(anxiety
,
tremor,andheadaches)thatareattributabletoactiononthe CNS.
B.Non-catecholamines
Mei2022 7
◦ Compoundslackingthecatecholhydroxylgroupshavelongerhalf-lives,becausetheyarenot
inactivatedby COMT
.
◦ Theseincludephenylephrine,ephedrine,andamphetamine(Figure6.7).
◦ Theseagentsarepoor substratesfor MAO(animportantrouteof metabolism)and,thus,showa
prolongeddurationof action.
◦ Increasedlipid solubilityof manyof thenon-catecholamines(duetolackof polarhydroxyl
groups)permitsgreateraccesstothe CNS.
Mei2022 8
D.Mechanismof actionof adrenergic agonists
Mei2022 9
1. Direct-actingagonists:Thesedrugsactdirectlyon orβ receptors,producingeffectssimilar to
thosethatoccurfollowingstimulationof sympatheticnervesor releaseof epinephrinefrom the
adrenalmedulla(Figure6.8).Examplesof direct-actingagonistsincludeepinephrine,
norepinephrine,isoproterenol,and phenylephrine.
2. Indirect-actingagonists:Theseagentsmayblockthereuptakeof norepinephrineorcausethe
releaseof norepinephrinefromthecytoplasmicpoolsorvesiclesof theadrenergicneuron
(Figure6.8).Thenorepinephrinethentraversesthesynapseandbindsto or β receptors.
Examplesof reuptakeinhibitorsandagentsthatcausenorepinephrinereleaseincludecocaine
andamphetamines, respectively
.
3. Mixed-actionagonists:Ephedrineanditsstereoisomer,pseudoephedrine,bothstimulate
adrenoceptorsdirectly and releasenorepinephrinefrom the adrenergicneuron (Figure 6.8).
Mei2022 10
MIXED-ACTIONADRENERGICAGONISTS(1/2)
Mei2022 11
◦ Ephedrineandpseudoephedrinearemixed-actionadrenergic agents.
◦ Theynotonlyreleasestorednorepinephrinefromnerveendings(Figure6.8)butalsodirectlystimulateboth  and
β receptors.
◦ Thus,awidevarietyof adrenergicactionsensuethataresimilartothoseof epinephrine, althoughlesspotent.
◦ Ephedrineandpseudoephedrinearenotcatecholsandarepoor substratesfor COMTandMAO.
◦ Therefore,thesedrugshavealongdurationofaction.
◦ EphedrineandpseudoephedrinehaveexcellentabsorptionorallyandpenetrateintotheCNS,but
pseudoephedrine hasfewerCNSeffects.
◦ Ephedrineiseliminatedlargelyunchangedinurine,andpseudoephedrine undergoesincompletehepatic
metabolismbeforeeliminationin urine.
◦ Ephedrineraisessystolicanddiastolicblood pressuresbyvasoconstrictionandcardiacstimulationandcanbeused to
treat hypotension.
◦ Ephedrineproducesbronchodilation,butitislesspotentandsloweractingthanepinephrineor isoproterenol.
◦ Itwaspreviouslyusedtopreventasthmaattacksbuthasbeenreplacedbymoreeffectivemedications.
MIXED-ACTIONADRENERGICAGONISTS(2/2)
Mei2022 12
◦ Ephedrineproducesamildstimulationof theCNS.
◦ Thisincreasesalertness,decreasesfatigue,andpreventssleep.
◦ Italsoimprovesathleticperformance.
◦ [Note:Theclinicaluseof ephedrineisdecliningbecauseof theavailabilityof better,morepotent
agentsthatcausefeweradverseeffects.Ephedrine-containingherbalsupplements(mainlyephedra-
containingproducts)havebeenbannedbytheU.S.FoodandDrug Administrationbecauseof life-
threateningcardiovascular reactions.]
◦ Pseudoephedrineisprimarilyusedorallytotreatnasalandsinuscongestion.
◦ Pseudoephedrinehasbeenillegallyusedtoproducemethamphetamine.
◦ Therefore,productscontainingpseudoephedrinehavecertainrestrictionsandmustbekeptbehind
thesalescounterintheUnited States.
◦ Importantcharacteristicsof theadrenergicagonistsaresummarizedinFigures 6.15–6.17.
Mei2022 13
Mei2022 14
Mei2022 15
Mei2022 16
Pharmacology
Mei2022 17
◦ Pseudoephedrinecausesvasoconstrictionwhichleadstoadecongestanteffect.
◦ Ithasashortdurationof actionunlessformulatedasanextendedreleaseproduct.
◦ Riskof centralnervoussystemstimulation.
◦ Pseudoephedrineisaphenethylamineandadiastereomerof ephedrinewithsympathomimetic
property.
◦ Pseudoephedrinedisplacesnorepinephrinefromstoragevesiclesinpresynapticneurones,thereby
releasingnorepinephrineintotheneuronalsynapseswhereitstimulatesprimarilyalpha-adrenergic
receptors.
◦ Pseudoephedrineisanalpha-AdrenergicAgonist.
◦ Italsohasweakdirectagonistactivityatalpha-andbeta- adrenergicreceptors.
◦ Receptorstimulationresultsinvasoconstrictionanddecreasesnasalandsinuscongestion.
PharmacologicalClassification
Mei2022 18
◦ NasalDecongestants
◦ Drugsdesignedtotreatinflammationof thenasalpassages,generallytheresultof aninfection(more
often than not the commoncold) or anallergy related condition, e.g., hayfever.
◦ Theinflammationinvolvesswellingof themucousmembranethatlinesthenasalpassagesandresultsin
inordinatemucusproduction.
◦ Theprimaryclassof nasaldecongestantsarevasoconstrictoragents.
◦ Bronchodilator Agents
◦ Agentsthatcauseanincreasein theexpansionof abronchusor bronchialtubes.
WHO AnatomicalTherapeuticChemical(ATC)
Classification
Mei2022 19
◦ R- Respiratorysystem
◦ R01- Nasalpreparations
◦ R01B- Nasaldecongestantsfor systemicuse
◦ R01BA- Sympathomimetics
◦ R01BA02- Pseudoephedrine
Pharmacokinetic
Absorption,Distributionand Excretion
Mei2022 20
◦ Absorption
◦ A240mgoraldoseof pseudoephedrinereachesaCmaxof 246.3±10.5ng/mL fedand272.5±13.4ng/mLfasted,witha
T
maxof 6.60±1.38hfedand11.87±0.72hfasted,withanAUCof 6862.0±334.1ng*h/mL fedand7535.1±333.0ng*h/mL
fasted.
◦ Routeof Elimination
◦ 55-75%of anoraldoseisdetectedintheurineasunchangedpseudoephedrine.
◦ Renal.About55to75%of adoseisexcretedunchange.Therateof excretionisacceleratedinacidicurine.
◦ Drugreleaseappearedtofollowfirstorder kinetics.
◦ Volumeof Distribution
◦ Theapparentvolumeof distributionof pseudoephedrinis2.6-3.3L/kg.
◦ Clearance
◦ A60mgoraldoseof pseudoephedrinehasaclearanceof 5.9±1.7mL/min/kg.
◦ Onlythreedrugsarecommonlyusedasoraldecongestants:phenylpropanolamine(PP
A),
pseudoephedrine(PDE),andphenylephrine (PE).
◦ BothPP
AandPDEarereadilyandcompletelyabsorbed,whereasPE,withabioavailabilityof
onlyapproximately38%,issubjecttogutwallmetabolismandisthoughttobeabsorbed
erratically
.
◦ Peakconcnarereachedbetween0.5and2hrafteradmin.
◦ Allthreedrugsareextensivelydistributedintoextravascularsites(apparentvolumeof
distributionbetween2.6and5.0 L/kg).
◦ No proteinbinding datainhumansare available.
Mei2022 21
Metabolism/Metabolites
Mei2022 22
◦ Pseudoephedrineis<1%N-demethylated toaninactive metabolite.
◦ Themajorityof pseudoephedrineiseliminatedunmetabolizedinthe urine.
◦ Pseudoephedrineisincompletelymetabolized(lessthan1%)intheliverbyN-demethylationtoaninactivemetabolite.
◦ Thedruganditsmetaboliteareexcretedinurine;55-96%of adoseisexcreted unchanged.
◦ WhereasPP
AandPDEarenotsubstantiallymetabolized,PEundergoesextensivebiotransformationinthegutwallandtheliver.
◦ Eliminationof PP
AandPDEispredominantlyrenal,withurinaryexcretionbeingpHdependent.
◦ Elimination of PP
AandPDEmayberapid in children, andthe agentsshould beusedwith cautionin patients with renalimpairment.
◦ Inaddition,PP
Aincrcaffeineplasmalevelsanddecrtheophylline clearance.
◦ Reducedmetabolismof PEoccurswithconcurrentadminof monoamineoxidaseinhibitors.
◦ No directrelationshipbetweennasaldecongestanteffectandplasmaconcentrationhasbeenestablished.
Biological Half-Life
Mei2022 23
◦ Half-livesarerelativelyshort,approximately2.5hrfor PE,4hrfor PP
A,and6hrforPDE.
◦ UrinarypHcanaffecttheeliminationhalf-life of pseudoephedrine,prolonging itwhenalkaline
(pH8)andreducingitwhenacidic(pH 5).
◦ Theeliminationhalf-life of pseudoephedrinerangesfrom3-6 or 9-16 hourswhenurinarypHis
5or8,respectively
,whilewhenurinarypHis5.8,theeliminationhalf-life of thedrugranges
from5-8 hours.
◦ Inonestudyinchildren6-12 yearsof age,theeliminationhalf-life of pseudoephedrine
averagedabout3hourswhenurinarypHw
as6.5.
Mechanismof Action
Mei2022 24
◦ Pseudoephedrineactsmainlyasanagonistof alphaadrenergicreceptorsandlessstronglyasan
agonistof betaadrenergic receptors.
◦ Thisagonismof adrenergicreceptorsproducesvasoconstrictionwhichisusedasa
decongestantandasatreatmentof priapism.
◦ Pseudoephedrineisalsoaninhibitorof norepinephrine,dopamine,andserotonin transporters.
◦ Thesympathomimeticeffectsof pseudoephedrineincludeanincreaseinmeanarterialpressure,
heart rate,and chronotropic responseof theright atria.
◦ Pseudoephedrineisalsoapartialagonistof theanococcygeal muscle.
◦ PseudoephedrinealsoinhibitsNF-kappa-B,NF
A
T
,and AP-1.
◦ Thepharmacologicalpropertiesof theephedrinederivativepseudoephedrinewereinvestigatedat
thenuclear level.
◦ Followingintraperitonealinjectionof SpragueDawleyratswithpseudoephedrine,Fosinductionw
as
measuredinvariousbrainareasbyWesternblotsand immunocytochemistry
.
◦ PseudoephedrineinducedFos-likeimmunoreactivityinthenucleusaccumbensandstriatuminatime
andconcentration-dependentmannerwithmaximaleffectat60mg/kg 2hrafter injection.
◦ Immunocytochemicalstudiesconfirmedthatthemajorityof thesignalw
asdetectableinthenucleus
accumbensandstriatum.
◦ Pre-injectionwiththeD1dopaminereceptorantagonistSCH23390partiallyandcompletelyblocked
pseudoephedrine-inducedFos-likeimmunoreactivityinthestriatumandnucleusaccumbens,
respectively
,suggestingthattheactionof pseudoephedrineismediatedviadopaminereleaseand
resultsintheactivationof D1dopamine receptors.
◦ Withtheexceptionof thehigherdosesrequired,theactionsof pseudoephedrineweresimilarto
thosepreviouslydescribedfor thepsychostimulant amphetamine.
Mei2022 25
◦ Becausepseudoephedrinehasbeenusedintheclandestinesynthesisof methamphetamineand
methcathinone,bothCNSstimulantswithgreatpotentialfor habituationandphysicaland/or
psychicdependence,theUSenactedtheComprehensiveMethamphetamineControlActof 1996
(USPublicLaw104-237)andlatertheMethamphetamineAnti-ProliferationAct(MAP
A(US Public
Law106-310),titleXXXVIof theChildren'sHealthActof 2000)toreducethepotentialfor misuse
(diversion)of pseudoephedrine.
Mei2022 26
Mei 2022 27
Terimakasih

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Pseudo-ephedrine

  • 2. Overview Mei2022 2 ◦ Theadrenergicdrugsaffectreceptorsthatarestimulatedbynorepinephrine (noradrenaline)or epinephrine (adrenaline). ◦ Thesereceptorsareknownasadrenergicreceptorsoradrenoceptors. ◦ Adrenergicdrugsthatactivateadrenergicreceptorsaretermedsympathomimetics, anddrugsthatblocktheactivationof adrenergicreceptorsaretermedsympatholytic. ◦ Somesympathomimeticsdirectlyactivateadrenergicreceptors(direct-acting agonists),whileothersactindirectlybyenhancingreleaseorblockingreuptakeof norepinephrine(indirect-acting agonists).
  • 3. Adrenergicagonists (*):catecholamines. Mei2022 3 DIRECT -ACTINGAGENTS ◦ Albuterol ◦ Clonidine ◦ Dobutamine* ◦ Dopamine* ◦ Epinephrine* ◦ Fenoldopam ◦ Formoterol ◦ Isoproterenol* ◦ Mirabegron ◦ Norepinephrine* ◦ Phenylephrine ◦ Salmeterol ◦ Terbutaline INDIRECT -ACTINGAGENTS ◦ Amphetamine ◦ Cocaine DIRECTANDINDIRECTACTING(mixedaction) AGENTS ◦ Ephedrine ◦ Pseudoephedrine
  • 4. Adrenergicreceptors (adrenoceptors) Mei2022 4 ◦ Inthesympatheticnervoussystem,severalclassesof adrenoceptorscanbedistinguished pharmacologically . ◦ Twomainfamiliesof receptors,designated andβ, areclassifiedonthebasisof theirresponses to the adrenergicagonistsepinephrine, norepinephrine,and isoproterenol. ◦ Eachof thesemainreceptortypeshasanumberof specificreceptorsubtypesthathavebeen identified. ◦ Alterationsin the primary structure of thereceptors influence their affinity for various agents.
  • 6. A.Catecholamines Mei2022 6 Sympathomimeticaminesthatcontainthe3,4-dihydroxybenzenegroup (suchasepinephrine, norepinephrine,isoproterenol,anddopamine)arecalledcatecholamines.Thesecompoundsshare thefollowing properties: 1. Highpotency:Catecholamines(with–OH groupsinthe3and4positionsonthebenzenering) showthehighest potencyin directlyactivating α or β receptors. 2. Rapidinactivation:CatecholaminesaremetabolizedbyCOMTpostsynapticallyandbyMAO intraneuronally,aswellasbyCOMTandMAO inthegutwall,andbyMAO intheliver.Thus, catecholamineshaveonlyabrief period of actionwhengivenparenterally ,andtheyare inactivated(ineffective)whenadministered orally . 3. PoorpenetrationintotheCNS:Catecholaminesarepolarand,therefore,do notreadily penetrateintotheCNS.Nevertheless,mostcatecholamineshavesomeclinicaleffects(anxiety , tremor,andheadaches)thatareattributabletoactiononthe CNS.
  • 7. B.Non-catecholamines Mei2022 7 ◦ Compoundslackingthecatecholhydroxylgroupshavelongerhalf-lives,becausetheyarenot inactivatedby COMT . ◦ Theseincludephenylephrine,ephedrine,andamphetamine(Figure6.7). ◦ Theseagentsarepoor substratesfor MAO(animportantrouteof metabolism)and,thus,showa prolongeddurationof action. ◦ Increasedlipid solubilityof manyof thenon-catecholamines(duetolackof polarhydroxyl groups)permitsgreateraccesstothe CNS.
  • 9. D.Mechanismof actionof adrenergic agonists Mei2022 9 1. Direct-actingagonists:Thesedrugsactdirectlyon orβ receptors,producingeffectssimilar to thosethatoccurfollowingstimulationof sympatheticnervesor releaseof epinephrinefrom the adrenalmedulla(Figure6.8).Examplesof direct-actingagonistsincludeepinephrine, norepinephrine,isoproterenol,and phenylephrine. 2. Indirect-actingagonists:Theseagentsmayblockthereuptakeof norepinephrineorcausethe releaseof norepinephrinefromthecytoplasmicpoolsorvesiclesof theadrenergicneuron (Figure6.8).Thenorepinephrinethentraversesthesynapseandbindsto or β receptors. Examplesof reuptakeinhibitorsandagentsthatcausenorepinephrinereleaseincludecocaine andamphetamines, respectively . 3. Mixed-actionagonists:Ephedrineanditsstereoisomer,pseudoephedrine,bothstimulate adrenoceptorsdirectly and releasenorepinephrinefrom the adrenergicneuron (Figure 6.8).
  • 11. MIXED-ACTIONADRENERGICAGONISTS(1/2) Mei2022 11 ◦ Ephedrineandpseudoephedrinearemixed-actionadrenergic agents. ◦ Theynotonlyreleasestorednorepinephrinefromnerveendings(Figure6.8)butalsodirectlystimulateboth  and β receptors. ◦ Thus,awidevarietyof adrenergicactionsensuethataresimilartothoseof epinephrine, althoughlesspotent. ◦ Ephedrineandpseudoephedrinearenotcatecholsandarepoor substratesfor COMTandMAO. ◦ Therefore,thesedrugshavealongdurationofaction. ◦ EphedrineandpseudoephedrinehaveexcellentabsorptionorallyandpenetrateintotheCNS,but pseudoephedrine hasfewerCNSeffects. ◦ Ephedrineiseliminatedlargelyunchangedinurine,andpseudoephedrine undergoesincompletehepatic metabolismbeforeeliminationin urine. ◦ Ephedrineraisessystolicanddiastolicblood pressuresbyvasoconstrictionandcardiacstimulationandcanbeused to treat hypotension. ◦ Ephedrineproducesbronchodilation,butitislesspotentandsloweractingthanepinephrineor isoproterenol. ◦ Itwaspreviouslyusedtopreventasthmaattacksbuthasbeenreplacedbymoreeffectivemedications.
  • 12. MIXED-ACTIONADRENERGICAGONISTS(2/2) Mei2022 12 ◦ Ephedrineproducesamildstimulationof theCNS. ◦ Thisincreasesalertness,decreasesfatigue,andpreventssleep. ◦ Italsoimprovesathleticperformance. ◦ [Note:Theclinicaluseof ephedrineisdecliningbecauseof theavailabilityof better,morepotent agentsthatcausefeweradverseeffects.Ephedrine-containingherbalsupplements(mainlyephedra- containingproducts)havebeenbannedbytheU.S.FoodandDrug Administrationbecauseof life- threateningcardiovascular reactions.] ◦ Pseudoephedrineisprimarilyusedorallytotreatnasalandsinuscongestion. ◦ Pseudoephedrinehasbeenillegallyusedtoproducemethamphetamine. ◦ Therefore,productscontainingpseudoephedrinehavecertainrestrictionsandmustbekeptbehind thesalescounterintheUnited States. ◦ Importantcharacteristicsof theadrenergicagonistsaresummarizedinFigures 6.15–6.17.
  • 17. Pharmacology Mei2022 17 ◦ Pseudoephedrinecausesvasoconstrictionwhichleadstoadecongestanteffect. ◦ Ithasashortdurationof actionunlessformulatedasanextendedreleaseproduct. ◦ Riskof centralnervoussystemstimulation. ◦ Pseudoephedrineisaphenethylamineandadiastereomerof ephedrinewithsympathomimetic property. ◦ Pseudoephedrinedisplacesnorepinephrinefromstoragevesiclesinpresynapticneurones,thereby releasingnorepinephrineintotheneuronalsynapseswhereitstimulatesprimarilyalpha-adrenergic receptors. ◦ Pseudoephedrineisanalpha-AdrenergicAgonist. ◦ Italsohasweakdirectagonistactivityatalpha-andbeta- adrenergicreceptors. ◦ Receptorstimulationresultsinvasoconstrictionanddecreasesnasalandsinuscongestion.
  • 18. PharmacologicalClassification Mei2022 18 ◦ NasalDecongestants ◦ Drugsdesignedtotreatinflammationof thenasalpassages,generallytheresultof aninfection(more often than not the commoncold) or anallergy related condition, e.g., hayfever. ◦ Theinflammationinvolvesswellingof themucousmembranethatlinesthenasalpassagesandresultsin inordinatemucusproduction. ◦ Theprimaryclassof nasaldecongestantsarevasoconstrictoragents. ◦ Bronchodilator Agents ◦ Agentsthatcauseanincreasein theexpansionof abronchusor bronchialtubes.
  • 19. WHO AnatomicalTherapeuticChemical(ATC) Classification Mei2022 19 ◦ R- Respiratorysystem ◦ R01- Nasalpreparations ◦ R01B- Nasaldecongestantsfor systemicuse ◦ R01BA- Sympathomimetics ◦ R01BA02- Pseudoephedrine
  • 20. Pharmacokinetic Absorption,Distributionand Excretion Mei2022 20 ◦ Absorption ◦ A240mgoraldoseof pseudoephedrinereachesaCmaxof 246.3±10.5ng/mL fedand272.5±13.4ng/mLfasted,witha T maxof 6.60±1.38hfedand11.87±0.72hfasted,withanAUCof 6862.0±334.1ng*h/mL fedand7535.1±333.0ng*h/mL fasted. ◦ Routeof Elimination ◦ 55-75%of anoraldoseisdetectedintheurineasunchangedpseudoephedrine. ◦ Renal.About55to75%of adoseisexcretedunchange.Therateof excretionisacceleratedinacidicurine. ◦ Drugreleaseappearedtofollowfirstorder kinetics. ◦ Volumeof Distribution ◦ Theapparentvolumeof distributionof pseudoephedrinis2.6-3.3L/kg. ◦ Clearance ◦ A60mgoraldoseof pseudoephedrinehasaclearanceof 5.9±1.7mL/min/kg.
  • 21. ◦ Onlythreedrugsarecommonlyusedasoraldecongestants:phenylpropanolamine(PP A), pseudoephedrine(PDE),andphenylephrine (PE). ◦ BothPP AandPDEarereadilyandcompletelyabsorbed,whereasPE,withabioavailabilityof onlyapproximately38%,issubjecttogutwallmetabolismandisthoughttobeabsorbed erratically . ◦ Peakconcnarereachedbetween0.5and2hrafteradmin. ◦ Allthreedrugsareextensivelydistributedintoextravascularsites(apparentvolumeof distributionbetween2.6and5.0 L/kg). ◦ No proteinbinding datainhumansare available. Mei2022 21
  • 22. Metabolism/Metabolites Mei2022 22 ◦ Pseudoephedrineis<1%N-demethylated toaninactive metabolite. ◦ Themajorityof pseudoephedrineiseliminatedunmetabolizedinthe urine. ◦ Pseudoephedrineisincompletelymetabolized(lessthan1%)intheliverbyN-demethylationtoaninactivemetabolite. ◦ Thedruganditsmetaboliteareexcretedinurine;55-96%of adoseisexcreted unchanged. ◦ WhereasPP AandPDEarenotsubstantiallymetabolized,PEundergoesextensivebiotransformationinthegutwallandtheliver. ◦ Eliminationof PP AandPDEispredominantlyrenal,withurinaryexcretionbeingpHdependent. ◦ Elimination of PP AandPDEmayberapid in children, andthe agentsshould beusedwith cautionin patients with renalimpairment. ◦ Inaddition,PP Aincrcaffeineplasmalevelsanddecrtheophylline clearance. ◦ Reducedmetabolismof PEoccurswithconcurrentadminof monoamineoxidaseinhibitors. ◦ No directrelationshipbetweennasaldecongestanteffectandplasmaconcentrationhasbeenestablished.
  • 23. Biological Half-Life Mei2022 23 ◦ Half-livesarerelativelyshort,approximately2.5hrfor PE,4hrfor PP A,and6hrforPDE. ◦ UrinarypHcanaffecttheeliminationhalf-life of pseudoephedrine,prolonging itwhenalkaline (pH8)andreducingitwhenacidic(pH 5). ◦ Theeliminationhalf-life of pseudoephedrinerangesfrom3-6 or 9-16 hourswhenurinarypHis 5or8,respectively ,whilewhenurinarypHis5.8,theeliminationhalf-life of thedrugranges from5-8 hours. ◦ Inonestudyinchildren6-12 yearsof age,theeliminationhalf-life of pseudoephedrine averagedabout3hourswhenurinarypHw as6.5.
  • 24. Mechanismof Action Mei2022 24 ◦ Pseudoephedrineactsmainlyasanagonistof alphaadrenergicreceptorsandlessstronglyasan agonistof betaadrenergic receptors. ◦ Thisagonismof adrenergicreceptorsproducesvasoconstrictionwhichisusedasa decongestantandasatreatmentof priapism. ◦ Pseudoephedrineisalsoaninhibitorof norepinephrine,dopamine,andserotonin transporters. ◦ Thesympathomimeticeffectsof pseudoephedrineincludeanincreaseinmeanarterialpressure, heart rate,and chronotropic responseof theright atria. ◦ Pseudoephedrineisalsoapartialagonistof theanococcygeal muscle. ◦ PseudoephedrinealsoinhibitsNF-kappa-B,NF A T ,and AP-1.
  • 25. ◦ Thepharmacologicalpropertiesof theephedrinederivativepseudoephedrinewereinvestigatedat thenuclear level. ◦ Followingintraperitonealinjectionof SpragueDawleyratswithpseudoephedrine,Fosinductionw as measuredinvariousbrainareasbyWesternblotsand immunocytochemistry . ◦ PseudoephedrineinducedFos-likeimmunoreactivityinthenucleusaccumbensandstriatuminatime andconcentration-dependentmannerwithmaximaleffectat60mg/kg 2hrafter injection. ◦ Immunocytochemicalstudiesconfirmedthatthemajorityof thesignalw asdetectableinthenucleus accumbensandstriatum. ◦ Pre-injectionwiththeD1dopaminereceptorantagonistSCH23390partiallyandcompletelyblocked pseudoephedrine-inducedFos-likeimmunoreactivityinthestriatumandnucleusaccumbens, respectively ,suggestingthattheactionof pseudoephedrineismediatedviadopaminereleaseand resultsintheactivationof D1dopamine receptors. ◦ Withtheexceptionof thehigherdosesrequired,theactionsof pseudoephedrineweresimilarto thosepreviouslydescribedfor thepsychostimulant amphetamine. Mei2022 25
  • 26. ◦ Becausepseudoephedrinehasbeenusedintheclandestinesynthesisof methamphetamineand methcathinone,bothCNSstimulantswithgreatpotentialfor habituationandphysicaland/or psychicdependence,theUSenactedtheComprehensiveMethamphetamineControlActof 1996 (USPublicLaw104-237)andlatertheMethamphetamineAnti-ProliferationAct(MAP A(US Public Law106-310),titleXXXVIof theChildren'sHealthActof 2000)toreducethepotentialfor misuse (diversion)of pseudoephedrine. Mei2022 26