Cymbalta� (duloxetine hydrochloride)
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About This Presentation
Cymbalta®� (duloxetine hydrochloride)
Generic name: Duloxetine HCl
Brand name: Cymbalta
FDA Approval: August 4, 2004
Selective serotonin and norepinephrine reuptake inhibitor (SSNRI)
Treatment for Major depressive Disorder
Slide Content
CymbaltaCymbalta
®®
(duloxetine hydrochloride) (duloxetine hydrochloride)
:: selective serotonin and selective serotonin and
norepinephrine reuptake inhibitor norepinephrine reuptake inhibitor
(SSNRI)(SSNRI)
®®
(duloxetine hydrochloride) (duloxetine hydrochloride)
:: selective serotonin and selective serotonin and
norepinephrine reuptake inhibitor norepinephrine reuptake inhibitor
(SSNRI)(SSNRI)
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Generic name:Generic name: D Duloxetine HCl uloxetine HCl
Brand name: Cymbalta Brand name: Cymbalta
FDA Approval: August 4, 2004FDA Approval: August 4, 2004
SSelective serotonin elective serotonin
andand norepinephrinenorepinephrine
reuptake inhibitor reuptake inhibitor
(SSNRI)(SSNRI)
Treatment forTreatment for Major depressive Disorder Major depressive Disorder
cymbaltacymbalta
IntroductionIntroduction
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Generic name:Generic name: D Duloxetine HCl uloxetine HCl
Brand name: Cymbalta Brand name: Cymbalta
FDA Approval: August 4, 2004FDA Approval: August 4, 2004
SSelective serotonin elective serotonin
andand norepinephrinenorepinephrine
reuptake inhibitor reuptake inhibitor
(SSNRI)(SSNRI)
Treatment forTreatment for Major depressive Disorder Major depressive Disorder
cymbaltacymbalta
IntroductionIntroduction
Major depressive DisorderMajor depressive Disorder ( (MDD)MDD)
MMD เป็นหนึ่งในกลุ่มโรคความผิดปกติ
ของอารมณ์ ( Mood Disorder)
Mood Disorder การแสดงอาการอาจมี
ลักษณะ
การซึมเศร้า
(Depression)
การคลุ้มคลั่ง
(Mania)
ทั้งสองแบบสลับกัน (Bipolar)
MDD คือภาวะที่ผู้ป่วยมีอาการซึม
เศร้า(depressive symptom)มากกว่าปกติ
จนเกิดการเสื่อมเสียหน้าที่
พบในหญิงมากกว่าชาย 2 เท่า โรคนี้พบ
มากในช่วงอายุ 25-40 ปี
IntroductionIntroduction
Unipolar
MMD เป็นหนึ่งในกลุ่มโรคความผิดปกติ
ของอารมณ์ ( Mood Disorder)
Mood Disorder การแสดงอาการอาจมี
ลักษณะ
การซึมเศร้า
(Depression)
การคลุ้มคลั่ง
(Mania)
ทั้งสองแบบสลับกัน (Bipolar)
MDD คือภาวะที่ผู้ป่วยมีอาการซึม
เศร้า(depressive symptom)มากกว่าปกติ
จนเกิดการเสื่อมเสียหน้าที่
พบในหญิงมากกว่าชาย 2 เท่า โรคนี้พบ
มากในช่วงอายุ 25-40 ปี
IntroductionIntroduction
Unipolar
• !
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EMOTIONAL SYMPTOMSEMOTIONAL SYMPTOMS
Sadness
Loss of interest or
pleasure in activities
Feeling overwhelmed
Anxiety
Poor concentration
Excessive or
inappropriate guilt
Recurrent thoughts of
death, suicidal
thoughts or attempts!" #• !
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PHYSICAL SYMPTOMSPHYSICAL SYMPTOMS
Headaches
Sleep disturbances
Fatigue
Back Pain
Changes in appetite
IntroductionIntroduction
Symptoms & Causes
of Depression
• !
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•
•
•
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EMOTIONAL SYMPTOMSEMOTIONAL SYMPTOMS
Sadness
Loss of interest or
pleasure in activities
Feeling overwhelmed
Anxiety
Poor concentration
Excessive or
inappropriate guilt
Recurrent thoughts of
death, suicidal
thoughts or attempts!" #• !
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PHYSICAL SYMPTOMSPHYSICAL SYMPTOMS
Headaches
Sleep disturbances
Fatigue
Back Pain
Changes in appetite
IntroductionIntroduction
Symptoms & Causes
of Depression
EtiologyEtiology
สาเหตุของโรค ปัจจุบันยังไม่ทราบแน่ชัด
แต่สาเหตุต่างๆที่ได้รับการกล่าวถึงได้แก่
Genetic factors
Psychosocial factors
Other biological factors
Catecholamine hypothesis
Down-regulation hypothesis
Cholinergic hypothesis
Major depressive DisorderMajor depressive Disorder
IntroductionIntroduction
สาเหตุของโรค ปัจจุบันยังไม่ทราบแน่ชัด
แต่สาเหตุต่างๆที่ได้รับการกล่าวถึงได้แก่
Genetic factors
Psychosocial factors
Other biological factors
Catecholamine hypothesis
Down-regulation hypothesis
Cholinergic hypothesis
Major depressive DisorderMajor depressive Disorder
IntroductionIntroduction
Many researchers believeMany researchers believe
depression is caused by an imbalance of two
naturally-occurring chemicals serotonin and norepin
ephrine in the brain and the body
Major depressive DisorderMajor depressive Disorder
IntroductionIntroduction
An imbalance in these chemicals may explain the
emotional and painful physical symptoms of depression
depression is caused by an imbalance of two
naturally-occurring chemicals serotonin and norepin
ephrine in the brain and the body
Major depressive DisorderMajor depressive Disorder
IntroductionIntroduction
An imbalance in these chemicals may explain the
emotional and painful physical symptoms of depression
Antidepressant Drugs•
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Monoamine oxidase inhibitor (MAOIs)
Tricyclic antidepressants (TCAs)
Atypical or second generation
•Serotonin reuptake inhibitors (SRI)
•Norepinephine reuptake inhibitors (NRI)
•Serotonin /Norepinephine reuptake
inhibitors (SNRI)
•Selective SRI (SSRI)
•Selective NRI (SNRI)
•Selective SNRI (SSNRI)
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Monoamine oxidase inhibitor (MAOIs)
Tricyclic antidepressants (TCAs)
Atypical or second generation
•Serotonin reuptake inhibitors (SRI)
•Norepinephine reuptake inhibitors (NRI)
•Serotonin /Norepinephine reuptake
inhibitors (SNRI)
•Selective SRI (SSRI)
•Selective NRI (SNRI)
•Selective SNRI (SSNRI)
CymbaltaCymbalta •
1"*222344
1"*222344
• molecular weight of 333.88molecular weight of 333.88•
5".
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•Each capsule contains enteric-coated pelletsEach capsule contains enteric-coated pellets
of 20, 30, or 60mg of duloxetineof 20, 30, or 60mg of duloxetine hydrochloridehydrochloride
1"*222344
1"*222344
• molecular weight of 333.88molecular weight of 333.88•
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•Each capsule contains enteric-coated pelletsEach capsule contains enteric-coated pellets
of 20, 30, or 60mg of duloxetineof 20, 30, or 60mg of duloxetine hydrochloridehydrochloride
Mechanism of actionMechanism of action
PharmacokineticsPharmacokinetics•
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Absorption Absorption
OralOrallyly duloxetine is well absorbed. duloxetine is well absorbed.
C max of duloxetine occurring 6 hoursC max of duloxetine occurring 6 hours
FoodFood
•not affect the Cmaxnot affect the Cmax
•but delays the time to reach peak but delays the time to reach peak
concentration from 6 to 10 hoursconcentration from 6 to 10 hours
•decreases the extent of absorption (AUC) by decreases the extent of absorption (AUC) by
about 10%about 10%
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Absorption Absorption
OralOrallyly duloxetine is well absorbed. duloxetine is well absorbed.
C max of duloxetine occurring 6 hoursC max of duloxetine occurring 6 hours
FoodFood
•not affect the Cmaxnot affect the Cmax
•but delays the time to reach peak but delays the time to reach peak
concentration from 6 to 10 hoursconcentration from 6 to 10 hours
•decreases the extent of absorption (AUC) by decreases the extent of absorption (AUC) by
about 10%about 10%
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DistributionDistribution
volume of distribution averages about volume of distribution averages about
1640 L1640 L
highly bound (>90%) to proteins in highly bound (>90%) to proteins in
human plasmahuman plasma
•albumin albumin
•α1-acid glycoproteinα1-acid glycoprotein
PharmacokineticsPharmacokinetics
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MetabolismMetabolism
extensive metabolism to numerousextensive metabolism to numerous
metabolitesmetabolites
major biotransformation pathways major biotransformation pathways
•conjugation and oxidationconjugation and oxidation
•Both CYP2D6 and CYP1A2 catalyze the Both CYP2D6 and CYP1A2 catalyze the
oxidation of the naphthyl ring oxidation of the naphthyl ring in vitroin vitro
MetabolitesMetabolites found in plasma includefound in plasma include
• 4-hydroxy duloxetine glucuronide 4-hydroxy duloxetine glucuronide
• 5-hydroxy, 6-methoxy duloxetine5-hydroxy, 6-methoxy duloxetine sulfatesulfate
PharmacokineticsPharmacokinetics
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MetabolismMetabolism
extensive metabolism to numerousextensive metabolism to numerous
metabolitesmetabolites
major biotransformation pathways major biotransformation pathways
•conjugation and oxidationconjugation and oxidation
•Both CYP2D6 and CYP1A2 catalyze the Both CYP2D6 and CYP1A2 catalyze the
oxidation of the naphthyl ring oxidation of the naphthyl ring in vitroin vitro
MetabolitesMetabolites found in plasma includefound in plasma include
• 4-hydroxy duloxetine glucuronide 4-hydroxy duloxetine glucuronide
• 5-hydroxy, 6-methoxy duloxetine5-hydroxy, 6-methoxy duloxetine sulfatesulfate
PharmacokineticsPharmacokinetics
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EliminationElimination
Only trace(<1% of the dose) amounts Only trace(<1% of the dose) amounts
of unchanged duloxetine are present in of unchanged duloxetine are present in
the urinethe urine
Most (about 70%) of the duloxetine Most (about 70%) of the duloxetine
dose appears in the urine as metabolitdose appears in the urine as metabolit
es of duloxetinees of duloxetine
about 20% is excreted in the feces.about 20% is excreted in the feces.
elimination half-life of about 12 hourselimination half-life of about 12 hours
PharmacokineticsPharmacokinetics
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EliminationElimination
Only trace(<1% of the dose) amounts Only trace(<1% of the dose) amounts
of unchanged duloxetine are present in of unchanged duloxetine are present in
the urinethe urine
Most (about 70%) of the duloxetine Most (about 70%) of the duloxetine
dose appears in the urine as metabolitdose appears in the urine as metabolit
es of duloxetinees of duloxetine
about 20% is excreted in the feces.about 20% is excreted in the feces.
elimination half-life of about 12 hourselimination half-life of about 12 hours
PharmacokineticsPharmacokinetics
Inhibitors of CYP1A2Inhibitors of CYP1A2
co-administered with fluvoxamineco-administered with fluvoxamine
((a potent CYP1A2 inhibitor)a potent CYP1A2 inhibitor)
•AUC was increased approximately 6-foldAUC was increased approximately 6-fold
•Cmax was increased about 2.5-foldCmax was increased about 2.5-fold
•t1/2 was increased approximately 3-foldt1/2 was increased approximately 3-fold
Other drugs that inhibit CYP1A2 Other drugs that inhibit CYP1A2
metabolismmetabolism
•include cimetidine and quinolone include cimetidine and quinolone
antimicrobials such as ciprofloxacin and enoxantimicrobials such as ciprofloxacin and enox
acinacin
Drug interactionsDrug interactions
co-administered with fluvoxamineco-administered with fluvoxamine
((a potent CYP1A2 inhibitor)a potent CYP1A2 inhibitor)
•AUC was increased approximately 6-foldAUC was increased approximately 6-fold
•Cmax was increased about 2.5-foldCmax was increased about 2.5-fold
•t1/2 was increased approximately 3-foldt1/2 was increased approximately 3-fold
Other drugs that inhibit CYP1A2 Other drugs that inhibit CYP1A2
metabolismmetabolism
•include cimetidine and quinolone include cimetidine and quinolone
antimicrobials such as ciprofloxacin and enoxantimicrobials such as ciprofloxacin and enox
acinacin
Drug interactionsDrug interactions
Inhibitors of CYP2D6Inhibitors of CYP2D6
Concomitant use of duloxetine with
potent inhibitors of CYP2D6 would be
expected to, and does, result in higher
concentrations of duloxetine
Paroxetine (20 mg QD)
•increased the concentration of duloxetine
(40 mg QD) by about 60%
•and greater degrees of inhibition are
expected with higher doses of paroxetine
DrugDrug interactionsinteractions
Concomitant use of duloxetine with
potent inhibitors of CYP2D6 would be
expected to, and does, result in higher
concentrations of duloxetine
Paroxetine (20 mg QD)
•increased the concentration of duloxetine
(40 mg QD) by about 60%
•and greater degrees of inhibition are
expected with higher doses of paroxetine
DrugDrug interactionsinteractions
Drugs Highly Bound to PlasmaDrugs Highly Bound to Plasma
ProteinProtein
Because duloxetine is highly bound to Because duloxetine is highly bound to
plasma proteinplasma protein
•may cause increased free concentrationsmay cause increased free concentrations
of the other drug, potentially resulting in of the other drug, potentially resulting in
adverse eventsadverse events
Drug interactionsDrug interactions
ProteinProtein
Because duloxetine is highly bound to Because duloxetine is highly bound to
plasma proteinplasma protein
•may cause increased free concentrationsmay cause increased free concentrations
of the other drug, potentially resulting in of the other drug, potentially resulting in
adverse eventsadverse events
Drug interactionsDrug interactions
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ContraindicationsContraindications
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ContraindicationsContraindications
In clinical studiesIn clinical studies
TThehe most common side effectmost common side effect waswas nauseanausea
•the nausea was mild to moderate, and the nausea was mild to moderate, and
usually subsided within one to two weeksusually subsided within one to two weeks
Other most common side effects included Other most common side effects included
(listed in order of frequency):(listed in order of frequency):
•Dry mouthDry mouth
•ConstipationConstipation
•Decreased appetiteDecreased appetite
•FatigueFatigue
•SleepinessSleepiness
•Increased sweatingIncreased sweating
Side EffectsSide Effects
TThehe most common side effectmost common side effect waswas nauseanausea
•the nausea was mild to moderate, and the nausea was mild to moderate, and
usually subsided within one to two weeksusually subsided within one to two weeks
Other most common side effects included Other most common side effects included
(listed in order of frequency):(listed in order of frequency):
•Dry mouthDry mouth
•ConstipationConstipation
•Decreased appetiteDecreased appetite
•FatigueFatigue
•SleepinessSleepiness
•Increased sweatingIncreased sweating
Side EffectsSide Effects
Cymbalta should be administeredCymbalta should be administered
•at a at a total dose of 40 mg/daytotal dose of 40 mg/day (given as 20(given as 20
mg BID)mg BID)
•to 60 mg/dayto 60 mg/day (given either once a day or as (given either once a day or as
30 mg BID) without regard to meals30 mg BID) without regard to meals
Dosage and Dosage and
administrationadministration
•at a at a total dose of 40 mg/daytotal dose of 40 mg/day (given as 20(given as 20
mg BID)mg BID)
•to 60 mg/dayto 60 mg/day (given either once a day or as (given either once a day or as
30 mg BID) without regard to meals30 mg BID) without regard to meals
Dosage and Dosage and
administrationadministration
Clinical studies Clinical studies
European Psychiatry (2006)European Psychiatry (2006)
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major depressive major depressive disorder:disorder:
a placebo- and paroxetine-controlled triala placebo- and paroxetine-controlled trial
By By D.G.S. Perahia , F. Wang , C.H. Mallinckrodt ,D.G.S. Perahia , F. Wang , C.H. Mallinckrodt ,
D.J. Walker , M.J. Detke D.J. Walker , M.J. Detke
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Duloxetine doses of 80 and 120 mg/Duloxetine doses of 80 and 120 mg/
day were assessed for efficacy and sday were assessed for efficacy and s
afety in the treatment of major depreafety in the treatment of major depre
ssive disorderssive disorder (MDD)(MDD)
Objective:Objective:
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ssive disorderssive disorder (MDD)(MDD)
Objective:Objective:
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patients age patients age ≥≥ 18 18
DSM-IV criteria for MDDDSM-IV criteria for MDD
CGI-S rating CGI-S rating ≥≥ 4 and HAMD17 total score 4 and HAMD17 total score
≥≥ 15 at the screening and baseline study 15 at the screening and baseline study
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Study designStudy design
multi-site, randomized, double-blind, multi-site, randomized, double-blind,
placebo and paroxetine-controlled stuplacebo and paroxetine-controlled stu
dydy
randomly assigned in a 1:1:1:1 ratio randomly assigned in a 1:1:1:1 ratio
•placeboplacebo
•duloxetine 80 mg/dayduloxetine 80 mg/day
•duloxetine 120 mg/day duloxetine 120 mg/day
•paroxetine 20 mg/day paroxetine 20 mg/day
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Study designStudy design
multi-site, randomized, double-blind, multi-site, randomized, double-blind,
placebo and paroxetine-controlled stuplacebo and paroxetine-controlled stu
dydy
randomly assigned in a 1:1:1:1 ratio randomly assigned in a 1:1:1:1 ratio
•placeboplacebo
•duloxetine 80 mg/dayduloxetine 80 mg/day
•duloxetine 120 mg/day duloxetine 120 mg/day
•paroxetine 20 mg/day paroxetine 20 mg/day
Patients and methodsPatients and methods
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Patients Screened
n=48064
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n=392(
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acute phase
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HAMD
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20mg
n=70
completed
continuation ph
n=62
completed
continuation ph
n=58
completed
continuation ph
n=62
completed
continuation ph
n=61
5.
Patients Screened
n=48064
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Duloxetine
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Paroxetine
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n=62
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continuation ph
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continuation ph
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Efficacy measures
primary measures
•HAMD17 total score
Secondary measures
•HAMD17 subscales
•(anxiety/somatization, core factor,Maier, sleep, and retardation)
•The Montgomery Asberg depression rating scale (MADRS)
•The Hamilton anxiety rating scale (HAMA)
•Patient global impression of improvement scales(PGI-I)
•The Sheehan disability scale (SDS)
•Visual analog scales (VAS) for pain
•The somatic symptom inventory (SSI)
Patients and methodsPatients and methods
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Efficacy measures
primary measures
•HAMD17 total score
Secondary measures
•HAMD17 subscales
•(anxiety/somatization, core factor,Maier, sleep, and retardation)
•The Montgomery Asberg depression rating scale (MADRS)
•The Hamilton anxiety rating scale (HAMA)
•Patient global impression of improvement scales(PGI-I)
•The Sheehan disability scale (SDS)
•Visual analog scales (VAS) for pain
•The somatic symptom inventory (SSI)
Patients and methodsPatients and methods
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Safety and tolerability assessmentsSafety and tolerability assessments
RReported adverse eventseported adverse events
RRecorded at each visitecorded at each visit
•vital signs, and weight vital signs, and weight
•Supine blood pressure Supine blood pressure
• heart rate heart rate
Laboratory tests (hematology, clinical Laboratory tests (hematology, clinical
chemistry, and urinalysis)chemistry, and urinalysis)
The Arizona sexual experiences scale The Arizona sexual experiences scale
(ASEX)(ASEX)
Patients and methodsPatients and methods
*
•
•
•
•
•
•
•
•
•
!
!
Safety and tolerability assessmentsSafety and tolerability assessments
RReported adverse eventseported adverse events
RRecorded at each visitecorded at each visit
•vital signs, and weight vital signs, and weight
•Supine blood pressure Supine blood pressure
• heart rate heart rate
Laboratory tests (hematology, clinical Laboratory tests (hematology, clinical
chemistry, and urinalysis)chemistry, and urinalysis)
The Arizona sexual experiences scale The Arizona sexual experiences scale
(ASEX)(ASEX)
Patients and methodsPatients and methods
Results: Efficacy Results: Efficacy (acute ph.)(acute ph.)• !"
#$%% &'!()*+#$%, &'!()*+#$) &
()*+#$% !--
"-!
Fig. 2. (a) HAMD17 change over the 8-week treatment period. Effect of placebo
(N = 99), duloxetine 80 mg/day (N = 93), duloxetine 120 mg/day (N = 102),
and paroxetine 20 mg/day (N = 97) on HAMD17 total scores (mean change
from baseline
#$%% &'!()*+#$%, &'!()*+#$) &
()*+#$% !--
"-!
Fig. 2. (a) HAMD17 change over the 8-week treatment period. Effect of placebo
(N = 99), duloxetine 80 mg/day (N = 93), duloxetine 120 mg/day (N = 102),
and paroxetine 20 mg/day (N = 97) on HAMD17 total scores (mean change
from baseline
Results: Results: Summary of primary efficacy outcomes (acute ph.)Summary of primary efficacy outcomes (acute ph.)
HAMD17: 17-item Hamilton rating scale for depression; MADRS: Montgomery Asberg depression rating
scale; HAMA: Hamilton anxiety rating scale; CGI-S:
clinical global impression of severity; PGI-I: patient global impression of improvement; LS mean: least-
square mean; S.E.: standard error. Items from the
HAMD17 scale used in the following subscales include: anxiety/somatization (items 10–13, 15, 17), core
factor (items 1–3, 7, 8), Maier (items 1, 2, 7–10); retardation
(items 1, 7, 8, 14), and sleep (items 4–6). *P ≤ 0.05 vs. placebo; **P ≤ 0.01.
a Results from MMRM analysis: mean change from baseline to week 8 ± S.E. Mean at week 8 for PGI-I.
b Administered as 40 mg twice daily (BID).
c Administered as 60 mg twice daily (BID).
d Administered once daily.
HAMD17: 17-item Hamilton rating scale for depression; MADRS: Montgomery Asberg depression rating
scale; HAMA: Hamilton anxiety rating scale; CGI-S:
clinical global impression of severity; PGI-I: patient global impression of improvement; LS mean: least-
square mean; S.E.: standard error. Items from the
HAMD17 scale used in the following subscales include: anxiety/somatization (items 10–13, 15, 17), core
factor (items 1–3, 7, 8), Maier (items 1, 2, 7–10); retardation
(items 1, 7, 8, 14), and sleep (items 4–6). *P ≤ 0.05 vs. placebo; **P ≤ 0.01.
a Results from MMRM analysis: mean change from baseline to week 8 ± S.E. Mean at week 8 for PGI-I.
b Administered as 40 mg twice daily (BID).
c Administered as 60 mg twice daily (BID).
d Administered once daily.
Results: Results: Safety and tolerabilitySafety and tolerability
(acute ph.)(acute ph.)
(acute ph.)(acute ph.)
Summary of primary and secondary efficacy
outcomes: continuation ph.
outcomes: continuation ph.
Results: Results: Safety and tolerability (continuation ph.)Safety and tolerability (continuation ph.)
ConclusionsConclusions
This study reinforces previous evidence
for the efficacy and safety of duloxetine in
the treatment of MDD in acute therapy.
Long-term efficacy cannot be
unequivocally concluded from this trial
Because neither duloxetine dose differed
significantly from placebo in maintenance
of effect during the continuation phase.
This study reinforces previous evidence
for the efficacy and safety of duloxetine in
the treatment of MDD in acute therapy.
Long-term efficacy cannot be
unequivocally concluded from this trial
Because neither duloxetine dose differed
significantly from placebo in maintenance
of effect during the continuation phase.
Cymbalta เป็นยาตัวแรกในกลุ่มSSelective elective
serotonin andserotonin and norepinephrinenorepinephrine reuptake inhibreuptake inhib
itor (SSNRI)itor (SSNRI)
ออกฤทธิ์ยับยั้งการ
ออกฤทธิ์ยับยั้งการ
reuptakereuptake
ของ
ของ
serotonin serotonin
และและNE NE
ทำาให้ระดับของสารทั้ง
ทำาให้ระดับของสารทั้ง
2 2
ตัวในบริเวณ
ตัวในบริเวณ
synapsesynapseมากขึ้นมากขึ้น
ที่ใช้ในการรักษา
ที่ใช้ในการรักษา
Major depressive DisorderMajor depressive Disorder
ขนาดที่แนะนำาให้ใช้คือ
ขนาดที่แนะนำาให้ใช้คือ
40-60 40-60 mg/daymg/day
SE SE
ของยาไม่รุนแรงที่พบได้บ่อยคือ อาการ
ของยาไม่รุนแรงที่พบได้บ่อยคือ อาการ
คลื่นไส้และอาการจะลดลงหลังได้ยา
คลื่นไส้และอาการจะลดลงหลังได้ยา
1-1-
22อาทิตย์อาทิตย์
summary
serotonin andserotonin and norepinephrinenorepinephrine reuptake inhibreuptake inhib
itor (SSNRI)itor (SSNRI)
ออกฤทธิ์ยับยั้งการ
ออกฤทธิ์ยับยั้งการ
reuptakereuptake
ของ
ของ
serotonin serotonin
และและNE NE
ทำาให้ระดับของสารทั้ง
ทำาให้ระดับของสารทั้ง
2 2
ตัวในบริเวณ
ตัวในบริเวณ
synapsesynapseมากขึ้นมากขึ้น
ที่ใช้ในการรักษา
ที่ใช้ในการรักษา
Major depressive DisorderMajor depressive Disorder
ขนาดที่แนะนำาให้ใช้คือ
ขนาดที่แนะนำาให้ใช้คือ
40-60 40-60 mg/daymg/day
SE SE
ของยาไม่รุนแรงที่พบได้บ่อยคือ อาการ
ของยาไม่รุนแรงที่พบได้บ่อยคือ อาการ
คลื่นไส้และอาการจะลดลงหลังได้ยา
คลื่นไส้และอาการจะลดลงหลังได้ยา
1-1-
22อาทิตย์อาทิตย์
summary
The
end
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