INTRODUCTION•Mometasonefuroateisapotentsyntheticcorticosteroidwithminimalbioavailabilitywhenadministeredtopically(dermatitis)orviainhalation(allergy,asthma)

•Maximumplasmaconcentrationsnear50pg/mLareexpectedfollowinginhalationof100-400µg,andasensitivemethodisrequiredtomeasureanadequatenumberofdatapointsforcalculatingpharmacokineticparameters

• Apost-extractionderivatizationprocedurecoupledwithadual-columnLC-MS/MSset-upprovidedsufficientsensitivitytovalidateanLLOQof0.250pg/mL

Figure 1. Mometasone furoate and hydrazone reaction products

ThetargetLLOQof0.25pg/mLwaschallengingtoachieveastheneutralsteroidtendstoformadductsinpositiveESIandthesignalisdilutedbythepresenceof2chlorineatoms.Derivatizationwithseveralhydrazinecompoundsordansylchloridewasinvestigatedtoincreaseandstabilizetheresponse.Twoisomericproductswereoftenobservedwithreversedphasechromatography.

Figure 2. Reversed phase chromatography of derivatised mometasone furoate.

Thereactionproductspresentedthemselvesasasinglepeakusingcationexchangechromatographywithmoderateretention.

A Sub-Picogram LC-MS/MS Method for the Analysis of Mometasone Furoate in Human Plasma.Lapko, V; Dzerk, A; Linderholm, K; Coe, R; Retke, B; Merrill, M; Sheldon, CCelerion, Lincoln, NE, USA

Figure 3. Mometasone furoate derivative SCX chromatography

SAMpLE pREpARATIONSeveralsolventsweretestedacrossthepHrangeandn-butylchlorideat alkaline pHwas chosen to provide the cleanest baseline andadequaterecoveryfrom1.0mLofEDTAplasmapriortoderivatization.

1mL Sample /IS + 1mL 2% NH4OH + 4.5 mL ButylChloride

Mix/Separate & evaporate organic

Derivatize/Evaporate/reconstitute

Severematrixsuppressionwasobservedforallderivativesincludingseveralhighlyretainedspeciesthatnearlyeliminatedthesignalfromsubsequentinjections.

Figure 4. Post column infusion experiment, mometasone furoate retention time ca. 1.6 minutes under typical (not final) SCX conditions.

INSTRUMENTATIONAdual-columnback-flushmethodwasadopted.Inthisapproach,2columnsareusedunderisocraticconditionswithonebeingrinsedofflineinthereversedirectionwhiletheanalysiscolumniselutingtothemassspec.Alternatingcolumnsviaavalveswitcheliminatesdownfieldelutionofsuppressivecompounds.•MobilePhase:Acetonitrile:Methanol:15mMammoniumformate,pH2.5;AnalyticalFlowRate0.9mL/min,Back-flushFlowRate1.0mL/min

• Column:SCX3x50mm5µm,50°C• Detection:Electrosprayionization(ESI)datawasacquiredbymultiplereaction-monitoring(MRM)inpositivemodeonanABSCIEX5500Q-TRAP®massspectrometer.Acquisitiontime2.0minutes

Figure 5. Dual column backflush LC-MS/MS design.

Mometasonechromatographyunderthefinalconditions,LLOQ,BlankandPostColumnInfusion. Figure 6. Final conditions for mometasone furoate derivative

O

CH3

HO

Cl

H

H

CH3

OCl

O

O

O

CH3

NN

CH3

Cl

H

H

CH3HO

OCl

O

O

O

R

H

CH3

N NH2

H

R

N

CH3

Cl

H

H

CH3HO

OCl

O

O

O

CH3

N

R

H

H+

Mometasone d3-37Cl-Mometasone

MS

Autosampler

Position 1

MS

Position 2

PC COLUMN

COLUMNPC

Waste

PC COLUMN

PUMP B

WASTE

MassSpec

Pump A

Position 1

Position 2

PC Column A

PC COLUMNPC Column A

Autosampler

Pump A

Column BPC

PC Column B

Pump B

Waste

Pump B

MassSpec

RESULTS• Thevalidatedanalyticalrangewas0.25to25.0pg/mLofmometasonefuroateusing1.0mLofhumanEDTAplasma

• Theinter-batchprecision(%C.V.)andaccuracy(%Bias)ofqualitycontrolsamplesisshowninTable1

• Theextractionrecoveryofmometasonefuroatewas87–93%• SelectivityandmatrixeffectdatawereacceptableforhealthyandhemolyzedhumanEDTAplasma

•MometasonefuroatewasstableinhumanEDTAplasmathrough6freeze/thawcycles,inclusiveof53hoursatambienttemperatureunderwhitelightingandforupto57dayswhenstoredat-20°C

•Derivatizedmometasonefuroateintegritywasmaintainedupto78hrspostextraction

Table 1. Validation Interday Reproducibility

Abioequivalencestudyofa200ugmometasonenasalspraygeneratedover3000samplesforanalysis.Reanalysisof262samplesconfirmed97%oftheoriginalresultsusingestablishedindustry-widecriteriaforincurredsamplereproducibility.Theaveragedifferencebetweenallreassayresultswas4.1%.

CONCLUSIONSArobustmethodforanalysisofmometasonefuroateinhumanplasmahasbeendevelopedandvalidated.Despitesub-picogramsensitivityrequirements,therelativelysimplemethodovercomesextremematrixeffectstoaccuratelyandreproduciblyquantifymometasonefuroateforpharmacokineticcharacterizationofverylowdosageintranasalandtopicalformulations.

ACKNOwLEDgMENTTheauthorsthankAlyssaPerry,ChrisKafonek,MarzukiMohamed,andJosephSilvafortheircontributions.

a. Lower Limit of Quantitation 0.25 pg/mL

b. Blank Control Plasma

c. Post Column Infusion

Quality Control Samples Precision (% CV) Accuracy (% Bias) Inter-Batch LLOQ 0.25 pg/mL

Low 0.75 pg/mL Medium 5.0 pg/mL High 20.0 pg/mL

16.9 7.6 2.3 2.3

4.4 2.8 5.8 1.5