Oral agents for the treatment of premature ejaculation: review of efficacy and safety in the context of the recent international society for sexual medicine criteria for lifelong premature ejaculation
Oral Agents for the Treatment of Premature Ejaculation: Review of Efficacy and Safety in the Context of the Recent International Society for Sexual Medicine Criteria for Lifelong Premature Ejaculationjsm_23862707.2725
Chris G. McMahon, MBBS, FAChSHM* and Hartmut Porst, MD†
*Australian Centre for Sexual Health, St. Leonards, NSW, Australia; †Private Urology and Andrology Practice andHospital, Hamburg, Germany
A B S T R A C T Introduction. New diagnostic criteria for lifelong premature ejaculation (PE) have been proposed by the Interna- tional Society of Sexual Medicine (ISSM), including an intravaginal ejaculatory latency time (IELT) of less than about 1 minute, lack of control over ejaculation, and PE-related distress or bother. Aim. The aim of this study was to review evidence supporting the efficacy and safety of oral agents for the treatment of PE in the context of the new ISSM criteria. Methods. The PubMed database was searched for randomized, double-blind, placebo-controlled studies of oral agents in PE that included stopwatch measurements of IELT. Main Outcome Measures. The main outcome measure used for this study was a review of the efficacy and safety data of oral agents for PE aligned with ISSM criteria. Results. Since the latest meta-analyses using similar criteria (conducted in 2004 and 2005 for selective serotonin reuptake inhibitors [SSRIs] and phosphodiesterase type 5 [PDE-5] inhibitors, respectively), eight studies evaluated SSRIs vs. placebo, one compared SSRIs, two evaluated PDE-5 inhibitors, and one evaluated an SSRI/PDE-5 inhibitor combination. New agents included dapoxetine (five studies) and tramadol (one study). Six studies enrolled men who met an approximation of the ISSM criteria. Although evidence suggests that most SSRIs, tramadol, and dapoxetine increase IELT to varying degrees, few studies included control over ejaculation and PE-related distress or bother as enrollment criteria or used validated patient-reported outcome instruments to evaluate these param- eters. Among studies that provided comprehensive adverse event data, safety and tolerability observations in men with PE were generally similar to those observed in other populations; however, with the exception of dapoxetine, known SSRI-class effects (e.g., withdrawal syndrome) were not evaluated in men with PE. Conclusions. This systematic review of well-controlled clinical trials in PE has demonstrated that while many oral agents, particularly SSRIs, tramadol, and dapoxetine, have proven effective and safe for the treatment of men with PE, few have been evaluated for their effects on the specific elements of the ISSM criteria. McMahon CG and Porst H. Oral agents for the treatment of premature ejaculation: Review of efficacy and safety in the context of the recent international society for sexual medicine criteria for lifelong premature ejaculation. J Sex Med 2011;8:2707–2725. Key Words. Premature Ejaculation; IELT; ISSM Criteria; Control over Ejaculation; Bother; Distress Introduction
inhibitor (SSRI) antidepressants [1–3], the tricyclicantidepressant clomipramine that blocks seroto-
C ommon treatment interventions for prema- nin, dopamine, and norepinephrine transporters
ture ejaculation (PE) include off-label use of
[4], phosphodiesterase (PDE)-5 inhibitors [1], or
oral agents, such as selective serotonin reuptake
topical anesthetic creams or sprays [1–3,5]. Other
2011 International Society for Sexual Medicine
agents, including a1-adrenoreceptor antagonists
were identified by searching for the keyword
[6,7] and the analgesic opioid receptor agonist and
“premature ejaculation” in the PubMed database.
noradrenaline reuptake inhibitor tramadol [8,9]
This search was then manually cross-referenced
have also been investigated for treating PE [2,10].
for all papers, and well-designed studies of oral
Psychotherapy and behavioral therapy also have a
agents were manually extracted. Well-designed
role, although well-designed, controlled trials that
studies were defined as randomized, double-blind,
use such approaches are lacking [3,5,10]. To date,
placebo-controlled trials that included stopwatch-
the largest trials of a treatment for PE have been
measured IELT as an outcome measure [17,18].
conducted with dapoxetine [11–14], a short-acting
Studies of SSRIs and clomipramine published
SSRI that is the only oral agent approved for the
prior to 2004 were identified from a meta-analysis
treatment of PE in several European, Asia-Pacific,
and systematic review by Waldinger [19], and
studies evaluating PDE-5 inhibitors and SSRI/
Evidence-based criteria for the diagnosis of life-
PDE-5 inhibitor combination therapies published
long PE have recently been proposed by the Inter-
prior to 2005 were identified from a systematic
national Society for Sexual Medicine (ISSM) [15],
review by McMahon [20] and another recent study
including an intravaginal ejaculatory latency time
[21] (summarized in Table 2). Studies were
(IELT) of approximately 1 minute or less, lack of
selected for inclusion in this review after evalua-
control over ejaculation, and negative psycholo-
gical consequences such as distress, bother, fru-stration, and/or sexual avoidance. Consequently,recent proposals recommend that studies of PE
Evidence Synthesis
should include stopwatch assessments of IELT and
validated patient-reported outcome (PRO) mea-
The basis of ideal PE clinical trial design
sures for control over ejaculation and PE-related
involves adequately defining the trial population, a
cohort or case-study observational trial design, a
This systematic review qualitatively examines
double-blind placebo-controlled interventional
the efficacy and safety of oral agents evaluated
randomized clinical trial design, or a double-blind,
for the treatment of PE, including not only those
crossover randomized clinical intervention prefer-
agents for which data have accumulated over many
ence trial, and the use of sensitive, validated, and
years, but also on novel treatments for which data
have recently become available. The majority of
PROs can be assessed using validated single-
these data has been collected prior to the formal
item questions, validated multi-item multi-domain
inclusion of IELT in the definition of PE; there-
PE inventories, or validated omnibus sexual
fore, the purpose of this review was to reexamine
inventories. PROs for use in clinical trials of
how this evidence supports the use of these treat-
investigational drugs be have robust reliability,
ments in the context of the new ISSM criteria
reproducibility, and internal validity and should
conform to the guidelines of the relevant regula-tory agency [30]. Although each of the three PROs
Evidence Acquisition
of PE (IELT, control, and distress) has been opera-
All studies of oral treatments for PE published
tionalized, they may not be equally weighted, may
in peer-reviewed medical journals since 2004
vary in importance between subjects, and may have
Definition of approximations of the ISSM criteria for lifelong PE
Applied consensus criteria for elements of
ISSM = International Society for Sexual Medicine; PE = premature ejaculation; IELT = intravaginal ejaculatory latency time; PRO = patient-reported outcome. Efficacy and Safety of Oral Agents for PEEfficacy and Safety of Oral Agents for PE
differing meanings in different cultures where the
Impression-Improvement (CGI-I) scale. None
attitude of the partner and culturally determined
of these studies enrolled men who met an appro-
extent of emancipation may have an impact upon
ximation of the ISSM criteria. A meta-analysis
the subject’s subjective diagnosis of PE. Inven-
of published data suggests that daily dosing of
tories must be psychometrically validated to
paroxetine exerts the strongest ejaculation delay,
demonstrate reliability, convergent and divergent
increasing IELT approximately 8.8-fold over
validity, and sensitivity between individual items
and items within domains in order to provide areliable tool to detect changes in subjects with PE.
Many of the inventories used in contemporary PE
A 2005 systematic review [20] identified a single
observational and interventional trials have been
study of PDE-5 inhibitors that fulfilled the criteria
for a well-designed PE trial. This study [27]
showed that men (N = 144) who met an approxi-
measure in PE studies is IELT, reported as an
mation of the ISSM criteria for PE had a nonsig-
average (arithmetic mean) [11,12,14,31], geomet-
nificant (P = 0.3) increase in IELT (minutes) after
ric mean [12,14,31], or fold-increase (proportional
8 weeks of treatment with sildenafil (baseline, 1.04;
increase from baseline) [31]. Some studies do not
endpoint, 2.60) compared with placebo (baseline,
describe how IELT data were collected and/or
0.96; endpoint, 1.63). Subjects randomized to
analyzed [4,23–27], and those studies were not
sildenafil demonstrated significantly higher scores
for the IPE items of ejaculatory control (1.8 vs.
Control over ejaculation and PE-related dis-
1.5, respectively), ejaculatory confidence (2.2 vs.
tress or bother have not been as commonly evalu-
1.9, respectively), and overall sexual satisfaction
ated, and their assessment has been hampered by
(3.1 vs. 2.8, respectively) at the end of treatment
the array of instruments available. These PROs are
(P < 0.05 vs. placebo for all); PE-related distress or
assessed using single-item questions or as part of
bother were not evaluated. One additional well-
validated instruments, such as the Index of Prema-
designed study [21] was identified, in which 42
ture Ejaculation (IPE) [32], the Premature Ejacu-
potent men with lifelong PE (based on the ISSM
definition) were randomized to receive on-demand
Chinese Index of Premature Ejaculation (CIPE)
vardenafil or placebo. In this study, vardenafil was
[34], the Arabic Index of Premature Ejaculation
associated with a 7.5-fold increase in geometric
(AIPE) [35], and the Premature Ejaculation Profile
mean IELT (0.6 Ϯ 0.3 vs. 4.5 Ϯ 1.1 minute with
(PEP) [11,13,36,37]; other instruments, such
placebo; P < 0.01), and significant improvements
as the International Index of Erectile Function
in the IPE domains of ejaculatory control, confi-
(IIEF) [38,39] and Yonsei Sexual Function Inven-
dence, overall sexual satisfaction, and distress.
tory (YSFI) [40], have also been utilized. Studies
This study suggests that the role of PDE-5 inhibi-
that did not include PROs were not excluded from
tors should be further evaluated in additional
well-designed studies. A 2007 review of PDE-5inhibitors for PE considered preclinical and
Efficacy of Oral Agents in the Treatment of PE
clinical data to understand potential central and
Table 3 summarizes the efficacy results from
peripheral mechanisms of action of these agents
well-designed studies (randomized, double-blind,
and their overall effectiveness in PE [42]. The
placebo-controlled trials that included stopwatch-
authors concluded that data were limited but
measured IELT) of oral agents in the treatment of
encouraging, and emphasized the need for large,
studies of these agents in men with PE.
This review identified five well-designed studies
Sexual Dysfunction (ICSD) and International
of SSRIs and clomipramine for the treatment
Society for Sexual Medicine’s Guidelines for the
of PE. Compared with placebo, daily fluoxetine
Diagnosis and Treatment of Premature Ejacula-
[22,24], citalopram [26], duloxetine [25], and clo-
tion have assigned level 4d evidence to support the
mipramine [4] significantly increased IELT. Few
efficacy and safety of off-label on-demand or daily
validated PROs were reported, although duloxet-
dosing of PDE-5 inhibitors in the treatment of
ine [25] and citalopram [26] were associated with
lifelong PE in men with normal erectile function.
improvements in PE based on the Clinical Global
Treatment of lifelong PE with PDE-5 inhibitors in
Efficacy and Safety of Oral Agents for PEEfficacy and Safety of Oral Agents for PE
men with normal erectile function is not recom-
mended and further evidence-based research is
Sexual Dysfunction (ICSD) and International
encouraged to understand conflicting data [43,44].
Society for Sexual Medicine’s Guidelines for theDiagnosis and Treatment of Premature Ejacula-
tion have assigned level 2d evidence to support
No well-designed studies of a1-receptor antago-
the efficacy and safety of daily dosing of
nists in treating PE were identified, although two
a1-adrenoceptor antagonists and tramadol in the
studies were found that evaluated measures of sat-
treatment of PE and their use as a treatment for
isfaction and subjective feelings of improvement
[6,7]. In the first study [6], subjects received tera-
zosin, alfuzosin, and placebo for 2 months each,
One well-designed study [23] compared the effi-
and approximately 50% of the subjects reported
cacy of fluoxetine and tadalafil alone and in com-
that their ejaculation time had been sufficiently
bination in men who met an approximation of
prolonged to satisfy both partners following active
the ISSM criteria for lifelong PE. Mean IELT
treatment (vs. 24% with placebo, P < 0.05 for
increased from 51.3 seconds across groups at base-
both). In the second study [7], 35% of men with
line to 233.6 seconds with fluoxetine, 186.5
PE and lower urinary tract symptoms (without
seconds with tadalafil, and 336.1 seconds with flu-
chronic prostatitis or benign prostatic hyperplasia
oxetine plus tadalafil (vs. 67.8 seconds with
[BPH]) treated with terazosin for 1 month were
placebo; P Յ 0.001 for all). Assessments of control
able to delay their ejaculation until their partner
over ejaculation or ejaculation-related distress or
reached orgasm, and 33.3% were able to increase
their time to ejaculation; however, it is unclearhow time to ejaculation was measured. Both
studies were limited by the use of nonvalidated
Dapoxetine was evaluated in five large random-
endpoints of patient impression of change and
ized, double-blind, placebo-controlled phase III
sexual satisfaction, and they did not evaluate actual
trials including >6,000 men in >25 countries; four
of these trials met the criteria for a well-designedstudy [11,12,14], while one study was conducted
primarily to evaluate safety [13]. Dapoxetine is the
While no studies met the criteria for a well-
only SSRI for which well-designed studies in PE
designed study, tramadol has been evaluated in a
populations have included on-demand dosing.
single-blind, placebo-controlled study, and in an
Results summarized in Table 3 report each manu-
open-label study. On-demand tramadol (25 mg)
script individually; data below are from an inte-
significantly increased IELT vs. placebo in 60 men
grated analysis [31] and is the only study where
with lifelong PE (P < 0.0001) [8,9]. In the open-
results are reported separately for men with IELTs
label crossover comparator study of daily paroxet-
of Յ1 minute and Յ0.5 minute, as well as for the
ine (20 mg) and on-demand tramadol (50 mg) in
overall study population. In the four studies that
35 subjects with lifelong PE, superior IELT fold-
evaluated IELT, increases in IELT were signifi-
increases and PRO responses were demonstrated
cantly (P < 0.001) greater with dapoxetine vs.
with paroxetine (22-fold vs. fivefold for tramadol)
placebo beginning with the first dose, which was
after 12 weeks of treatment [9]. Although this
maintained at all subsequent time points [31].
study was limited by the use of the Diagnostic and
Dapoxetine 30 and 60 mg on-demand significantly
Statistical Manual of Mental Disorders Fourth
increased arithmetic and geometric mean IELT
Edition Text Revision (DSM-IV-TR) definition
compared with placebo (1.9 and 1.2 minutes for
to diagnose PE, 66% of men had an IELT of
placebo, 3.1 and 2.0 minutes for dapoxetine 30 mg,
Յ1 minute at baseline, suggesting that the overall
and 3.6 and 2.3 minutes for dapoxetine 60 mg,
population is reasonably representative of the
respectively). This represents a 1.6-, 2.5-, and 3.0-
ISSM definition. A large, international, prospec-
fold increase over baseline geometric mean IELT
tive, randomized, placebo-controlled, double-
for placebo, dapoxetine 30 mg, and dapoxetine
blind trial of tramadol for the treatment of PE
60 mg, respectively. IELT increases with dapoxet-
(NCT00983151) was recently stopped prema-
ine were significantly (P < 0.001) greater than
turely, although no reason has been provided;
placebo beginning with the first dose, which was
maintained at all subsequent time points. Similar
stopped because of recruitment difficulties.
results were observed in men with IELTs Յ1
minute and Յ0.5 minute at baseline. Progressively
lation at Week 12 (vs. 41.9% with placebo,
greater fold-increases were observed with decreas-
P < 0.001) and to 34.9% and 28.8% with dapoxet-
ing baseline average IELTs. Subjects with baseline
ine 30 and 60 mg, respectively, among men with
average IELTs of 1.5–2 minutes, 1–1.5 minutes,
IELT values of <1 minute at baseline (vs. 50.7%
0.5–1 minute, and less than 0.5 minute showed
with placebo, P < 0.001). Approximately, one-
geometric mean fold-increases of 1.5, 1.6, 1.6, and
third of the subjects reported “quite a bit” or
1.7, respectively, with placebo treatment; 2.2, 2.3,
“extremely” for their level of ejaculation-related
2.4, and 3.4, respectively, with dapoxetine 30 mg;
interpersonal difficulty at baseline; by Week 12,
and 2.6, 2.5, 3.0, and 4.3 with dapoxetine 60 mg.
this decreased among the overall population to
The PEP [45] or individual PEP items were
16.0% and 12.3% with dapoxetine 30 and 60 mg,
used to evaluate control over ejaculation (five
respectively (vs. 23.8% with placebo, P < 0.001)
trials), satisfaction with sexual intercourse (five
and to 17.7% and 13.9% with dapoxetine 30 and
trials), and ejaculation-related personal distress
60 mg, respectively, among men with IELT values
and interpersonal difficulty (three trials). Clinical
of <1 minute at baseline (vs. 28.2% with placebo,
global impression of change (CGI) in PE was
P < 0.001). Significantly more men receiving
also measured on a 7-point scale (five trials). Two
dapoxetine 30 or 60 mg reported that their PE was
studies [12,14] included stopwatch-measured
at least “better” at Week 12 (30.7% and 38.3%,
IELT and all four PEP items and enrolled men
respectively, among the overall population and
based on an IELT of Յ2 minutes on 75% of
25.2% and 34.9% for men with IELT values of <1
occasions, low control over ejaculation, and
minute at baseline, respectively) compared with
placebo (13.9% and 9.4% among the overall popu-
varied populations in each study, and the use of the
lation and for men with IELT values of <1 minute
DSM-IV-TR definition to diagnose PE, the
at baseline, respectively; P Յ 0.05 for all).
overall population was reasonably representative
The dapoxetine phase III study populations of
of the ISSM definition of lifelong PE (64.9% had
>6,000 men represented a heterogeneous popula-
lifelong PE; 58% had an IELT <1 minute).
tion with both lifelong and acquired PE and
Overall, subjects reported significant improve-
included some men with mild erectile dysfunction
ments in all PEP items with dapoxetine (P Յ 0.001
(ED). In a post-hoc analysis of data from three
vs. placebo for all), and results were similar for
phase 3 clinical trials [46], study-end dapoxetine
men with IELT values of <1 minute at baseline
mean IELT and PRO responses were superior
[31]. “Good” or “very good” control over ejacula-
to placebo and dose-dependent, with a similar
tion was reported by <1% across groups at baseline
pattern for men with lifelong and acquired PE.
However, the presence of mild ED diminished
tion (26.2% with dapoxetine 30 mg and 30.2%
PRO responsiveness in both subtypes, particularly
with dapoxetine 60 mg vs. 11.2% with placebo;
P < 0.001 for both) and among men with IELT
Female partners also reported improvements in
values of <1 minute at baseline (19.7% with dapox-
sexual functioning [31], including their perception
etine 30 mg and 26.0% with dapoxetine 60 mg vs.
of the male subject’s control over ejaculation
7.2% with placebo; P < 0.001 for both) at 12
and CGIC and their own satisfaction with sexual
weeks. Similarly, “good” or “very good” satisfac-
intercourse in three studies [11,12], and their
tion with sexual intercourse was reported by
own ejaculation-related interpersonal difficulty
approximately 15.0% of men across groups at
and personal distress in one study [12]. Significant
baseline and increased among the overall popula-
improvements in partner perception of the man’s
tion (37.9% with dapoxetine 30 mg and 42.8%
control over ejaculation and CGIC were observed
with dapoxetine 60 mg vs. 24.4% with placebo;
at Week 12; 26.7% and 34.3% reported the man’s
P < 0.001 for both) and among men with IELT
control over ejaculation as “good” or “very good”
values of <1 minute at baseline (32.9% with dapox-
with dapoxetine 30 and 60 mg, respectively, vs.
etine 30 mg and 40.0% with dapoxetine 60 mg vs.
11.9% with placebo (P < 0.0001 for both) [31].
32.9% with placebo; P < 0.001 for both) at 12
Female partners of men treated with dapoxetine
weeks. At baseline, ~70% of subjects across groups
also reported significant improvements in their
reported their level of ejaculation-related personal
own satisfaction with sexual intercourse, with
distress as “quite a bit” or “extremely,” which
37.5% and 44.7% reporting “good” or “very
decreased to 28.2% and 22.2% with dapoxetine 30
good” satisfaction with sexual intercourse with
and 60 mg, respectively, among the overall popu-
dapoxetine 30 and 60 mg, respectively, vs. 24.0%
Efficacy and Safety of Oral Agents for PE
with placebo at Week 12 (P < 0.001 for both). Sig-
that withdrawal-like symptoms following abrupt
nificant improvements in female partner-rated
discontinuation of citalopram are mild and tran-
ejaculation-related personal distress and interper-
sient, and are likely associated with the re-
sonal difficulty related to ejaculation were also
emergence of depression [51]. None of the
observed with dapoxetine vs. placebo.
well-designed studies of SSRIs in men withPE specifically evaluated class-related effects,
although improvements in psychometric assess-
The safety and tolerability findings from well-
ments, including Symptom Checklist 90-R scores,
designed studies of oral agents for PE are summa-
Dyadic Adjustment Scale scores, and measures of
anxiety were reported with clomipramine [4].
In well-designed studies of SSRI antidepressants
In the two well-designed studies of PDE-5 inhibi-
in PE subjects, adverse events (AEs) were reported
tors (sildenafil and vardenafil) identified in this
by 3 of 13 men receiving citalopram [25,26] and 3
review, the overall incidence of AEs was not
of 10 men receiving duloxetine, but AE incidence
reported; however, the most common AEs included
was not reported in every study (Table 4). The
headache (10–15%), flushing (12–15%), dyspepsia
most common AEs included nausea, dry mouth,
(5–10%), abnormal vision (5%), and rhinitis (5%),
headache, and insomnia. Two of nine men receiv-
which tended to attenuate and disappear with con-
ing fluoxetine discontinued because of AEs (nausea
tinued use [21,27]. These data are similar to those
and insomnia) [24]. None of these studies reported
reported in a recent systematic review [52] of the
the incidence of serious AEs. It is important to
use of PDE-5 inhibitors in men with ED. In that
note that these studies used chronic daily dosing,
analysis, overall AE rates were 50% with sildenafil
based on the dosing schedule used in the approved
and 47% with tadalafil; the overall AE rate for
indications. However, these agents may be taken as
needed or continuously [47], which may alter the
included headache (13–17%), dyspepsia (3.8–
incidence of AEs and may influence patient pref-
10%), flushing (4.8–13%), and rhinitis (3.1–7.9%).
erence for a particular dosing schedule [48].
The rate of serious AEs was low (1.2–2.5%).
The majority of safety and AE information for
SSRIs is derived from studies in subjects with
In the study [6] by Cavallini comparing alfuzosin
depression and other psychiatric/behavioral disor-
and terazosin with placebo, hypotension was the
ders. In a meta-analysis [49] of studies in patients
most common AE leading to discontinuation (four
with major depressive disorder, the incidence of
patients [4.4%]; two each with terazosin and alfu-
AEs with SSRIs ranged from 8.5% to 16.3% and
zosin). Other AEs included headache (one patient
included dry mouth, nausea, dizziness, head-
with alfuzosin) and headache with epigastralgia
ache, fatigue, constipation, diarrhea, somnolence,
(one patient with terazosin), neither of which
insomnia, nervousness, sweating, and anorexia.
resulted in discontinuation. In the study by Bas¸ar
SSRIs have several class-related effects, includ-
and coworkers of terazosin vs. placebo daily for 1
ing agitation, irritability, unusual changes in
month [6], published safety data were limited to
behavior, anxiety, impulsivity, akathisia, hypoma-
the finding that none of the patients discontinued
nia, mania, and the potential for suicidality in chil-
treatment because of AEs. These data in men with
dren, adolescents, and young adults. Abrupt
PE are comparable to what has been observed
discontinuation of SSRIs may result in SSRI with-
in men with hypertension or BPH. The most
drawal syndrome (typically characterized by head-
common AEs with terazosin include postural
ache, diarrhea, nausea, vomiting, chills, dizziness,
hypotension (3.9%), dizziness (9.1%), somnolence
or fatigue). One retrospective study [50] of
(3.6%), nasal congestion/rhinitis (1.9%), and
patients (N = 352) who were treated with SSRIs
impotence (1.6%) [53]. With alfuzosin, common
reported that 30.8%, 20.0%, and 2.2% of subjects
AEs in men with BPH include dizziness (5.7%),
who discontinued treatment with clomipramine,
upper respiratory infections (3.0%), headache
paroxetine, and sertraline, respectively, experi-
enced withdrawal symptoms; no subjects reportedsymptoms following discontinuation of fluoxetine.
Data on SSRI withdrawal symptoms with citalo-
In the single-blind, placebo-controlled study, eight
pram are limited; however, it has been reported
(13.3%) men experienced mild dyspepsia (n = 5)
Efficacy and Safety of Oral Agents for PEEfficacy and Safety of Oral Agents for PE
and mild somnolence (n = 3) with tramadol [8].
and 60 mg, respectively, most commonly because
Tramadol was generally tolerated in the open-label
of nausea, dizziness, and diarrhea. Syncope
study, with gastric upset being the most common
(including loss of consciousness), which appeared
AE [9]. No serious AEs or AE-related discontinu-
to be vasovagal in nature and generally occurred
ations were reported in either study. These AEs
within 3 hours of the first dose, was reported in
are similar to what has been reported with trama-
0.05%, 0.06% and 0.23% of subjects with placebo,
dol in other populations. A recent meta-analysis
dapoxetine 30 mg, and dapoxetine 60 mg, respec-
[54] of 11 controlled studies of tramadol in more
tively [31]. Syncope occurred more frequently
than 1,000 patients with osteoarthritis reported
when dapoxetine was administered at one of the
that the most common AEs were nausea, vomiting,
study sites (onsite [0.31%] vs. offsite [0.08%]),
dizziness, somnolence, tiredness, and headache,
appeared to be related to syncope-associated
and approximately 20% of patients receiving tra-
onsite study procedures (e.g., blood draws or
madol or tramadol/acetaminophen experienced
orthostatic maneuvers) and occurred almost exclu-
nonserious AEs. Although tramadol is reported to
sively with dapoxetine 60 mg, with only one
have a lower risk of dependence than traditional
reported episode with the 30-mg dose. Similar
opioids, its use as an on-demand treatment for PE
observations have been reported with other SSRIs,
is limited by the potential risk of addiction [55]. In
and these events resolved without sequelae.
community practice, dependence does occur, but
Dapoxetine is the only agent for which studies
appears to be minimal [56]. Adams and colleagues
have been adequately powered and designed to
[57] reported abuse rates of 0.7% for tramadol
assess SSRI class-related effects in a PE popu-
compared with 0.5% for nonsteroidal anti-
lation. Dapoxetine was not associated with
inflammatory drugs and 1.2% for hydrocodone,
treatment-emergent anxiety (measured by the
based on application of a dependency algorithm as
Hamilton Anxiety Scale), depression (measured by
a measure of persistence of drug use.
the Montgomery-Åsberg Depression Rating Scaleand the Beck Depression Inventory II), or suicid-
ality [31]. Abrupt discontinuation of dapoxetine
There are limited data regarding the safety and
was not associated with an increased incidence
tolerability of combination treatments for PE. In
of withdrawal syndrome compared with placebo
the study that evaluated fluoxetine, tadalafil, and
fluoxetine plus tadalafil, the overall incidence of
Discontinuation-emergent Signs and Symptoms
AEs was higher with the combination (40%) com-
pared with either drug alone (fluoxetine, 33%; tad-alafil, 26%) or placebo (12%); common AEs withfluoxetine plus tadalafil included somnolence,
Discussion
nausea, palpitation, and muscle soreness [23].
This review is limited by the author’s attempt to
retrospectively apply the contemporary ISSM
Similar AE profiles have been reported across the
definition of lifelong PE to previously conducted
phase III trials of dapoxetine [20]. In the integrated
intervention studies that employed differing
analysis of these studies [31], AEs occurred in 651/
inclusion/exclusion criteria and study endpoints.
1,857 (35.1%), 760/1,616 (47.0%), 1,270/2,106
The attempt to approximate data from studies
(60.3%), and 341/502 (67.9%) subjects with
enrolling a heterogenous population of both life-
placebo, dapoxetine 30 mg prn, dapoxetine 60 mg
long and acquired PE to the ISSM definition of
prn, and dapoxetine 60 mg qd, respectively. The
lifelong PE is somewhat balanced by the recently
published post-hoc analysis of dapoxetine phase 3
nausea, diarrhea, headache, dizziness, insomnia,
baseline and treatment outcome data suggesting
somnolence, fatigue, and nasopharyngitis. Nausea
that there are substantial similarities in baseline
was the most common AE associated with discon-
IELT, PROs and response to dapoxetine between
tinuation. Sexual function AEs occurred in a low
percentage of subjects across groups.
While many of the well-designed studies of oral
Severe or serious AEs occurred infrequently
agents in PE included in this review may be con-
(~3% and Յ1%, respectively), and most AEs were
sidered to have at least partially met the ISSM
of mild to moderate severity [31]. Across trials,
criteria for lifelong PE for their study populations,
AE-related discontinuation occurred in 1.7–4.0%
few used validated PRO measures for control over
and 5.1–10.0% of subjects receiving dapoxetine 30
ejaculation and PE-related distress or bother, or
included detailed prospective reporting of SSRI
Administration schedules also varied among
class-related AEs. All of these studies were con-
studies. As mentioned above, in the studies of
ducted prior to the existence of the ISSM defini-
SSRI antidepressants included in this review,
tion of lifelong PE and the development of PE
chronic daily dosing was used. SSRIs were devel-
inventories; however, these elements have been
oped for daily use in chronic diseases, and their
included in most earlier criteria, such as those pro-
pharmacokinetic profiles are characteristic of
posed by the DSM-IV-TR [58], the American
agents intended to remain at therapeutic concen-
Urological Association [59], and the International
trations for extended periods of time. Daily
Consultation on Urological Diseases [60].
administration of these agents results in the
There is a wide disparity in AE reporting
chronic blockade of serotonin transport, leading to
amongst studies of oral agents. By convention,
the desensitization of presynaptic 5-HT1A autore-
AEs are reported retrospectively by the subject at
the next trial visit, and are recorded and rated by
receptors and resultant greater increases in 5-HT
the investigator using Medical Dictionary for
neurotransmission [62–65], a principal factor
Regulatory Activities [61] coding by their relation
thought to contribute to both the therapeutic and
to the trial drug. However, trial visits may be up to
adverse effects of these agents. Daily dosing also
4 weeks apart, prompting concerns regarding the
results in significant accumulation (approximately
reliability of subject recall of the AE frequency,
eightfold with paroxetine [66] and twofold with
severity, duration and/or temporal relation to
sertraline [67]. PDE-5 inhibitors, tramadol, and
administration. Prospective reporting of AEs
dapoxetine are all intended for and evaluated with
within 24 hours in a subject diary using a validated
on-demand administration. In contrast to long-
questionnaire, such as the Udvalg for Kliniske
acting SSRIs, dapoxetine has a rapid pharmacoki-
Undersogelser (UKU) side effect rating scale
netic profile; maximum plasma concentrations are
for psychotropic/neuroleptic drugs, has been
reached approximately 1 hour after oral adminis-
tration and fall to less than 5% of this peak within
A wide range of diagnostic criteria were used for
PE in these clinical trials. Few trials enrolled men
Current understanding of the safety and toler-
who approximately met the ISSM criteria. While
ability of SSRIs, PDE-5 inhibitors, a1-antagonists,
all of the studies included here implemented an
and tramadol in the treatment of PE relies heavily
IELT threshold in their enrollment criteria, differ-
on results from studies in other patient popula-
ent thresholds were applied (i.e., <1 minute, Յ2
tions (e.g., depression, ED, BPH, and chronic,
minutes); differences in baseline IELT may have a
severe musculoskeletal pain). In addition, men
profound impact on the apparent magnitude of
with many of the approved indications for these
IELT increases with treatment. Further, no more
treatments are excluded from PE trials, despite the
than a handful of studies incorporated both an
fact that men with PE frequently have comorbid
IELT threshold and PRO measures for control
conditions such as depression or ED. Further
over ejaculation and PE-related distress or bother
study is necessary to determine the safety and tol-
[11,12,14,21,27], leaving only IELT as the main
erability of these agents in a PE population and in
outcome measure for contrasting efficacy results
men with PE and comorbid conditions.
The ISSM criteria for lifelong PE provide an
The wide variability among PE study designs
evidence-based definition of PE that can be used as
also complicates their comparison and interpreta-
a standard in future trial design; in contrast, no
tion. Studies have ranged in length from 4 to 24
evidence-based definition of acquired PE has been
weeks, and the impact of treatment duration
put forth. The ISSM was unable to define acquired
on outcomes is unclear. Various methods were
PE because of a lack of sufficient normative data
used for reporting IELT outcomes, including
[15]. As noted recently by Jannini [69], clinical trials
arithmetic mean, geometric mean, or fold-increase
of dapoxetine contained men with acquired PE as
from baseline. Further, a wide range of validated
well as men with lifelong PE, and dapoxetine was
and unvalidated PRO instruments have been used,
shown to be effective in both groups. These trials
complicating the comparison of PRO results
typically included stopwatch-measured IELT and
between studies. There is a need for consensus on
validated PRO measures of control over ejaculation
the appropriate use and application of PRO mea-
and distress or bother related to PE; therefore,
sures to ensure interpretability of results across
information from these trials may provide some
insight into the clinical picture of acquired PE. Efficacy and Safety of Oral Agents for PEConclusions Statement of Authorship
Improvements in PE with treatment should be
evaluated based on the characteristics that define
(a) Conception and Design
the condition. According to the new ISSM cri-
teria, the parameters of importance are IELT,
(b) Acquisition of Data
control over ejaculation, and negative psychologi-
cal consequences such as distress, bother, fru-
(c) Analysis and Interpretation of Data
stration, and sexual avoidance. This systematic
review of well-designed trials in PE demonstratedthat many agents, particularly SSRI antidepres-
sants and dapoxetine, are effective and well tol-
(a) Drafting the Article
erated for the treatment of men with PE. (b) Revising It for Intellectual Content
Evidence for the effectiveness of PDE-5 inhibi-
tors, a1-receptor antagonists, and tramadol iscurrently weak and none are currently recom-
mended as treatment for PE with the exception
(a) Final Approval of the Completed Article
acquired PE. While most studies now reportstopwatch-measured IELT, the ISSM lifelong PEcriteria of control-over-ejaculation and PE-
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