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Ege Can Serefoglu, MD, FECSM
Bahceci Health Group, Istanbul, Turkey
Medipol University, School of Medicine, Istanbul, Turkey
Disclosures
 Consultant: Virility Medical Ltd., Haifa, Israel
Medical Devices in PE Treatment
Introduction
Current Treatments
New Treatments
Introduction
 Ejaculation is the expulsion of semen from the meatus
 Constituted by 2 phases
 Emmision: Ejection of the semen into the posterior urethra
Contraction of testes, epididymes, VD, SV, prostate
 Expulsion: Ejection of sperm from urethra
Rhythmic contractions of perineal muscles (BS/IC)
Giuliano and Clement. Annu. Rev. Sex Res. 2015
Saitz and Serefoglu. Nat Rev Urol, 2015
Premature Ejaculation
 Affects 3 to 30% of the male population
 according to the definition used
 Cited as“the most common male sexual dysfunction”
 Causes important psychological problems
 Diminished self-esteem
 Anxiety
 Embarrassment
 Relationship problems
Serefoglu et al J Sex Med 2012
Treatment Advantages Disadvantages
Behavioural therapy
• High reported initial success rate in
uncontrolled studies
• Limited long-term efficacy
Topical anaesthetics (creams and
sprays)
• Effective in majority of patients
• Penile and vaginal hypoesthesia
• Female anorgasmia
• Skin reactions
Clomipramine • Significant improvement in IELT
• Nausea
• Erectile dysfunction
• HSDD
• Reduced vigilance
• Rhythm disorders
Antidepressant SSRIs*
• Significant improvement in IELT
• Generally require daily dosing
• Limited data on patient-reported
outcomes
• SSRI withdrawal syndrome
• Poorly accepted by patients and
partners
PDE5 inhibitors • First line option in PE with concomitant ED
• Arguable efficacy in only PE
patients
Tramadol
• Significant improvement in IELT
• Suitable for on-demand dosing
• Limited clinical data
• Limited real-life clinical experience
• Risk of addiction?
Saitz and Serefoglu. Nat Rev Urol. 2015
Current PE Treatments
Saitz and Serefoglu. Nat Rev Urol, 2015
Botulinum Toxin Injection
 Long-Evans rats (33 males)
 ~2 weeks to adapt to the light–dark cycle
 Treatment
 Placebo: Saline injection (0.1 ml)
 Low Dose: Botulinum toxin-A (0.5 U in 0.1 ml)
 High Dose: Botulinum toxin-A (1 U in 0.1 ml)
Serefoglu EC et al. J Sex Med. 2012
Bulbospongiosus Muscle
The Effects of Btx-A Injection on
Male Rat Ejaculatory Behavior
p=0.53
P=0.04*
P=0.013*
PLACEBO LOW-DOSE HIGH-DOSE
* Paired-sample T-test
A Safety and Efficacy Study of OnabotulinumtoxinA in PE
ClinicalTrials.gov Identifier: NCT01917006
0
20
40
60
80
100
120
140
160
180
200
Baseline Week 2 Week 4 Week 6 Week 8 Week 10 Week 12
Average IELT(seconds)
OnabotulinumtoxinA Dose 1 OnabotulinumtoxinA Dose 2 OnabotulinumtoxinA Dose 3 OnabotulinumtoxinA Dose 4
OnabotulinumtoxinA Dose 5 OnabotulinumtoxinA Dose 6 Placebo
Can we inhibit rhythmic BS muscle
contractions w/o drugs?
 intermittent electrical stimuli
Neuromuscular electrical stimulation
(NMES)
 Application of intermittent electrical stimuli to
superficial muscles
 triggers muscle contractions
 via the activation of the intramuscular nerve branches
 common and well-recognized tx to improve muscle
function
 PFM training with NMES has been used in many urological
problems (e.g. LUTS, SUI, ED)
Herzig D et al. the journal of injury, function, and rehabilitation 7 (2015)
McClurg D et al Neurourology and urodynamics 27 (2008)
Eder SE Women's health (London, England) 10 (2014)
Lavoisier P et al. Physical therapy 94 (2014)
Pastore AL et al. Ther Adv Urol 6 (2014)
At a Glance
17
Technology
Development
Patent I
Application
Completed Safety
Clinical Study
Patent II
Application
2015 2016 2017 20182014
Article I
Publication
Prototype
Finalized
Completed Feasibility
Clinical Study
Article II
Publication
NMES
Wearable,
discrete and
non-painful
Immediate
effect
Single-use &
disposable
Drug free
18
Competitive Advantages
Parameter NMES Desensitizers SSRIs
Effect onset Immediate 15 mins. 2 – 4 hrs.
Range of
effect
localized localized systemic
Duration of
effect
specific to
intercourse
exceeds intercourse
Adverse
events
minor
Numbness of
penis,
transference to
partner
nausea
ED
reduced libido
headaches
drowsiness
January 2019 19
NMESDevice
Clinical Feasibility Studies
21Shechter et al. WMSM Lisbon 2018.
Regulatory Status
February 19 22
US – Class II
• FDA approval planned
for Q4 2019
• Positive feedback from
FDA following pre-sub
meeting
• De-Novo pathway
EU – Class IIa
• CE approval planned
for Q4 2019
• Notified Body – BSI
• ISO13485:2016
compliance
Roadmap
February 19 23
2019 2020 20212018
Clinical
Initiated pivotal
study
Q1 2018
Product Dev
Device optimization completion
Q1 2019
Clinical
Pivotal study
completion
Q3 2019
Marketing
Initial sales
Q1 2020
Clinical
EU post marketing
study completion
Q1 2018
Regulatory
FDA and CE
mark approvals
Q4 2019
Clinical
Initiate post marketing
studies
Q1 2020
Clinical
US post marketing
study completion
Q1 2021
BizDev
Series A
Q1 2019
Other Devices
 Transcutaneous Posterior Tibial Nerve Stimulation
(TPTNS)
 Neuromodulation device (Morari®)
Transcutaneous Posterior Tibial
Nerve Stimulation (TPTNS)
 TPTNS is an effective therapy for controlling urinary
incontinence.
 Its efficacy in inhibiting the ejaculatory reflex is evaluated
 Phase II clinical trial, 26 pts
 3 TPTNS therapies per week for 12 weeks
 Frequency 20 HZ, pulse width of 200 microseconds, for 30 mins.
 The IELT and the PEDT scale was evaluated
Saffon et al. ESSM 2019
TPTNS
 52.9% of patients had at least tripled their baseline IELT
(p=0.019)
 mean IELT had increased 5.4 times (CI 95% 2.3 - 8.4)
 PEDT score decreased 5.7 points on average
 1 episode of constipation, 1 pt reported a sensation of heat in
the leg during one therapy session.
2.9
5.2
6.3
0
2
4
6
8
10
6 weeks End of therapy 3 months follow-up
Times the IELT increased
Saffon et al. ESSM 2019
Transdermal, non-invasive wearable device
using neuromodulation to delay ejaculation
Thank you…
egecanserefoglu@hotmail.com

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Mechanical Devices for the Treatment of Premature Ejaculation

  • 1. Ege Can Serefoglu, MD, FECSM Bahceci Health Group, Istanbul, Turkey Medipol University, School of Medicine, Istanbul, Turkey
  • 2. Disclosures  Consultant: Virility Medical Ltd., Haifa, Israel
  • 3. Medical Devices in PE Treatment Introduction Current Treatments New Treatments
  • 4. Introduction  Ejaculation is the expulsion of semen from the meatus  Constituted by 2 phases  Emmision: Ejection of the semen into the posterior urethra Contraction of testes, epididymes, VD, SV, prostate  Expulsion: Ejection of sperm from urethra Rhythmic contractions of perineal muscles (BS/IC) Giuliano and Clement. Annu. Rev. Sex Res. 2015
  • 5. Saitz and Serefoglu. Nat Rev Urol, 2015
  • 6. Premature Ejaculation  Affects 3 to 30% of the male population  according to the definition used  Cited as“the most common male sexual dysfunction”  Causes important psychological problems  Diminished self-esteem  Anxiety  Embarrassment  Relationship problems Serefoglu et al J Sex Med 2012
  • 7. Treatment Advantages Disadvantages Behavioural therapy • High reported initial success rate in uncontrolled studies • Limited long-term efficacy Topical anaesthetics (creams and sprays) • Effective in majority of patients • Penile and vaginal hypoesthesia • Female anorgasmia • Skin reactions Clomipramine • Significant improvement in IELT • Nausea • Erectile dysfunction • HSDD • Reduced vigilance • Rhythm disorders Antidepressant SSRIs* • Significant improvement in IELT • Generally require daily dosing • Limited data on patient-reported outcomes • SSRI withdrawal syndrome • Poorly accepted by patients and partners PDE5 inhibitors • First line option in PE with concomitant ED • Arguable efficacy in only PE patients Tramadol • Significant improvement in IELT • Suitable for on-demand dosing • Limited clinical data • Limited real-life clinical experience • Risk of addiction? Saitz and Serefoglu. Nat Rev Urol. 2015 Current PE Treatments
  • 8. Saitz and Serefoglu. Nat Rev Urol, 2015
  • 10.  Long-Evans rats (33 males)  ~2 weeks to adapt to the light–dark cycle  Treatment  Placebo: Saline injection (0.1 ml)  Low Dose: Botulinum toxin-A (0.5 U in 0.1 ml)  High Dose: Botulinum toxin-A (1 U in 0.1 ml) Serefoglu EC et al. J Sex Med. 2012
  • 12. The Effects of Btx-A Injection on Male Rat Ejaculatory Behavior p=0.53 P=0.04* P=0.013* PLACEBO LOW-DOSE HIGH-DOSE * Paired-sample T-test
  • 13.
  • 14. A Safety and Efficacy Study of OnabotulinumtoxinA in PE ClinicalTrials.gov Identifier: NCT01917006 0 20 40 60 80 100 120 140 160 180 200 Baseline Week 2 Week 4 Week 6 Week 8 Week 10 Week 12 Average IELT(seconds) OnabotulinumtoxinA Dose 1 OnabotulinumtoxinA Dose 2 OnabotulinumtoxinA Dose 3 OnabotulinumtoxinA Dose 4 OnabotulinumtoxinA Dose 5 OnabotulinumtoxinA Dose 6 Placebo
  • 15. Can we inhibit rhythmic BS muscle contractions w/o drugs?  intermittent electrical stimuli
  • 16. Neuromuscular electrical stimulation (NMES)  Application of intermittent electrical stimuli to superficial muscles  triggers muscle contractions  via the activation of the intramuscular nerve branches  common and well-recognized tx to improve muscle function  PFM training with NMES has been used in many urological problems (e.g. LUTS, SUI, ED) Herzig D et al. the journal of injury, function, and rehabilitation 7 (2015) McClurg D et al Neurourology and urodynamics 27 (2008) Eder SE Women's health (London, England) 10 (2014) Lavoisier P et al. Physical therapy 94 (2014) Pastore AL et al. Ther Adv Urol 6 (2014)
  • 17. At a Glance 17 Technology Development Patent I Application Completed Safety Clinical Study Patent II Application 2015 2016 2017 20182014 Article I Publication Prototype Finalized Completed Feasibility Clinical Study Article II Publication
  • 19. Competitive Advantages Parameter NMES Desensitizers SSRIs Effect onset Immediate 15 mins. 2 – 4 hrs. Range of effect localized localized systemic Duration of effect specific to intercourse exceeds intercourse Adverse events minor Numbness of penis, transference to partner nausea ED reduced libido headaches drowsiness January 2019 19
  • 21. Clinical Feasibility Studies 21Shechter et al. WMSM Lisbon 2018.
  • 22. Regulatory Status February 19 22 US – Class II • FDA approval planned for Q4 2019 • Positive feedback from FDA following pre-sub meeting • De-Novo pathway EU – Class IIa • CE approval planned for Q4 2019 • Notified Body – BSI • ISO13485:2016 compliance
  • 23. Roadmap February 19 23 2019 2020 20212018 Clinical Initiated pivotal study Q1 2018 Product Dev Device optimization completion Q1 2019 Clinical Pivotal study completion Q3 2019 Marketing Initial sales Q1 2020 Clinical EU post marketing study completion Q1 2018 Regulatory FDA and CE mark approvals Q4 2019 Clinical Initiate post marketing studies Q1 2020 Clinical US post marketing study completion Q1 2021 BizDev Series A Q1 2019
  • 24. Other Devices  Transcutaneous Posterior Tibial Nerve Stimulation (TPTNS)  Neuromodulation device (Morari®)
  • 25. Transcutaneous Posterior Tibial Nerve Stimulation (TPTNS)  TPTNS is an effective therapy for controlling urinary incontinence.  Its efficacy in inhibiting the ejaculatory reflex is evaluated  Phase II clinical trial, 26 pts  3 TPTNS therapies per week for 12 weeks  Frequency 20 HZ, pulse width of 200 microseconds, for 30 mins.  The IELT and the PEDT scale was evaluated Saffon et al. ESSM 2019
  • 26. TPTNS  52.9% of patients had at least tripled their baseline IELT (p=0.019)  mean IELT had increased 5.4 times (CI 95% 2.3 - 8.4)  PEDT score decreased 5.7 points on average  1 episode of constipation, 1 pt reported a sensation of heat in the leg during one therapy session. 2.9 5.2 6.3 0 2 4 6 8 10 6 weeks End of therapy 3 months follow-up Times the IELT increased Saffon et al. ESSM 2019
  • 27.
  • 28.
  • 29. Transdermal, non-invasive wearable device using neuromodulation to delay ejaculation

Notes de l'éditeur

  1. This slide summarizes the range of commonly used treatment options utilised to treat PE, including the advantages and disadvantages of each Over the past 20-30 years, the PE treatment paradigm has shifted from psychotherapy to drug treatment
  2. Spontaneous – the intensity of stimulation can be predetermined before the patch is applied. The patch can be applied even hours before intercourse. Addressing population variability - by allowing the user to precisely determine the intensity of the stimulation (contrary to oral pharmaceutical dosage)
  3. Using a hand-held TENS device