Botox Penile Injections for Erectile Dysfunction

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madman

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Abstract

Background:
Erectile dysfunction (ED) is a socio-economic problem.There are several options for its management including intra-cavernosal injection (ICI).

Objective: To compare the safety, efficacy, and durability of ICI of onabotulinum toxin-A (BTX) in different doses (50 and 100 U) against placebo (saline) in the management of vasculogenic ED non-responding to pharmacological therapy (phosphodiesterase type 5 inhibitors or/and ICI of trimix).

Materials and Methods: A prospective randomized double-blind placebo-controlled trial was conducted between July 2016 and February 2019. A total of 176 patients were randomly assigned (1:1:1) to one of the treatment sequences: Botox 100 U group (BTX-100; 62 patients), Botox 50 U group (BTX-50; 59 patients), or placebo group (55 patients). All patients were followed up for 6 months.

Results: Significant improvement in all parameters, that is, SHIM score & Erection Hardness Score (EHS), Sexual Encounter Profile (SEP), Global Assessment Score (GAS), and Doppler parameters (p < 0.001) was observed in patients of BTX-100 and BTX-50 groups with maximum improvement at the 3rd month of treatment. Around 40% of patients were responders and were able to engage in sexual intercourse. Patients in placebo group did not experience significant improvement (p = 0.264). It was noted that at the 2nd week and 3rd months after treatment, there was no statistically significant difference in the improvement of these parameters in BTX-100 and BTX-50 groups (p > 0.05). In the 6th month, there was a statistically significant difference between the aforementioned groups in favor of BTX-100 (p < 0.01).

Conclusions: Only one-time ICI of BTX (50 U and 100 U) is effective and safe for the treatment of refractory ED. This agent has a considerably long duration of action, particularly BTX-100U seems to be more durable.




1  | INTRODUCTION

Erectile dysfunction (ED), which is defined as a persistent inability to achieve or maintain a penile erection sufficient to permit satisfactory sexual performance, represents a significant medical challenge with an immense sociomedical and economical burden.1

The prevalence of ED is usually associated with other medical comorbidities such as cardiometabolic syndrome, neuropsychological disorders, and depression. The prevalence of ED is anticipated to affect about 1/3 billion patients by the year 20252 with an actual increase in its incidence among juniors.3

Several treatment modalities for ED are available including penile prosthesis, intra-cavernous injection (ICI), intra-urethral therapy, and oral phosphodiesterase type 5 inhibitors (PDE5Is). Despite the advances in oral and intra-urethral treatments, ICI remains a viable and effective second-line therapy for many patients.4-7 Recently, the application of stem cells and gene therapy for ED treatment has shown some early promise but disappointing clinical outcomes.8

Although the current modalities for ED treatment demonstrate some degree of clinical success, many of these modalities suffer from inherent disadvantages such as modest efficacy, lack of durability, and short-term efficacy, and sometimes debilitating side effects.8 Thus, the development of effective, safe, and durable treatment of ED, particularly the refractory vasculogenic erectile dysfunction, is a pressing and unmet medical need.

Approximately four out of five patients with ED are attributed to organic etiologies with multiple signal transduction pathways converge to endothelial dysfunction.9 Thus, effective therapy of vasculogenic ED should be directed toward this factor.

Onabotulinum toxin-A (BTX) is widely used for the treatment of various medical conditions.8,10
BTX exerts multiple pharmacological effects, which may qualify BTX as a therapeutic candidate for the treatment of ED. For instance, it blocks the release of acetylcholine and norepinephrine-mediated sympathetic pathway and increases the expression of vascular endothelial growth factor and CD31.11 The expression of these factors and the activation of its downstream signaling cascades enhance vasodilation and endothelial cell proliferation and thus are involved in the pathophysiology of ED. These findings represent the theoretical and molecular rationale for the potential effects of BTX in the treatment of vasculogenic ED. Indeed, several reported a durable efficacy of BTX in the treatment of several vasospastic disorders such as Raynaud's phenomenon.12


*Indeed, until now, there is no well-conducted human study that investigated a suitable dose of BTX-A as an ICI for the treatment of ED. Thus, we carried out this prospective, randomized, double-blinded, and controlled trial to test the hypothesis that treatment with BTX-A (50 or 100 U) can exert a durable, safe, and beneficial therapeutic effect for management of drugs non-responders ED patients.




4  | DISCUSSION


Our findings suggest that BTX might provide a safe, effective, and relatively durable improvement of ED. Several mechanisms are proposed for the potential therapeutic effect of BTX in the treatment of many vasculogenic disorders, including ED. For instance, BTX inhibits sympathetic adrenergic or cholinergic vasoconstriction, sensory nerves, and/or endothelial exocytosis of endothelin 1, which are involved in the pathophysiology of erectile dysfunction.8,17 Mounting evidence suggests that the effects BTX are mediated by non–nitric-oxide-mediated mechanism. Instead, it inhibits the neuronal membrane fusion with the synaptic vesicles that contain norepinephrine neurotransmitters. So, preventing the release of norepinephrine rather than nitric oxide.8 These effects might lead to a decrease in the tone of resistance penile vessels, an increase in resting blood flow, and a reduction in persistent cavernosal smooth muscle tone. BTX-A injection induces sinusoidal dilatation of cavernous tissue which seems to be mediated by smooth muscle relaxation.18,19

*Ultimately, these effects are responsible for, at least in part, facilitating an erectile response to sexual stimulation through its modulatory effect on the erectile tissue8,20




5  |  CONCLUSIONS


Treatment of refractory ED by single ICI of BTX was found to be effective, durable, and safe. All noted complications were related to ICI of vasoactive agents during subsequent follow-up penile Doppler studies. While ICI of BTX helped around 40% of patients to restart their sexual activities, around 60% of patients were still not able to complete intercourse.

This novel application of ICI BTX demonstrated a considerable long duration of action, which lasts at least 3–6 months. Although both 50 U and 100 U are effective and safe, BTX-100 appears to be more durable. Further studies with different doses are warranted to confirm current results.
 

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TABLE 1 Baseline characteristics of study patients
Screenshot (7520).png
 
FIGURE 2 SEP Questions 2 and 3 of study groups during follow-up visits. Data expressed as Number & percent *: significance ≤0.05 (chi square test), A: significance vs BTX-100 IU, B: significance vs BTX50 IU a: significance vs baseline, b: significance vs 2weeks, c: significance vs 3 months SEP = Sexual Encounter Profile
Screenshot (7521).png

Screenshot (7522).png
 
FIGURE 3 GAS Questions 1 and 2 of study groups during follow-up visits. Data expressed as Number & percent *: significance ≤0.05 (chi-square test), A: significance vs BTX-100 IU, B: significance vs BTX50 IU; a: significance vs baseline, b: significance vs 2weeks, c: significance vs 3 months. GAS = Global Assessment Score
Screenshot (7523).png

Screenshot (7524).png
 
*Approximately four out of five patients with ED are attributed to organic etiologies with multiple signal transduction pathways converge to endothelial dysfunction.9 Thus, effective therapy of vasculogenic ED should be directed toward this factor

*Onabotulinum toxin-A (BTX) is widely used for the treatment of various medical conditions.8,10 BTX exerts multiple pharmacological effects, which may qualify BTX as a therapeutic candidate for the treatment of ED. For instance, it blocks the release of acetylcholine and norepinephrine-mediated sympathetic pathway and increases the expression of vascular endothelial growth factor and CD31.11 The expression of these factors and the activation of its downstream signaling cascades enhance vasodilation and endothelial cell proliferation and thus are involved in the pathophysiology of ED. These findings represent the theoretical and molecular rationale for the potential effects of BTX in the treatment of vasculogenic ED
 
wow thats amazing. I'd be willing to try it. Looking for a dr in my area but not sure what to search.

Botox procedures commonly done in plastic surgeon and dermatologist offices, even some dentists do it. Should make for an interesting inquiry, that's for sure.
 
If I understand the study correctly (just skimmed), the test subjects didn't respond to either PDE5 inhibitors (e.g., Cialis, Viagra) or Trimix. So they are truly "hard cases." And yet 40% of them responded to Botox - and for months.

I'm in the camp of (1) PDE5 inhibitors no longer work well and (2) Trimix works spectacularly, as it does for most men. But imagine a Trimix-like product that you only have to inject every few months!
 
That would be freaking awesome! I have searched for it in my area, Dallas, but I can't seem to find anyone that does it. Hopefully it gets offered at some point.
 
Cool that the effects last "several months." However, the response rate of 54% is nowhere near the response rate for Trimix, which I understand is around 90%.
 
I spoke with one of the offices I linked earlier and they said the treatment is about 3K. Include the cost of the flight/hotel into that and it just adds up alot. I could drive to Houston though. Best medical city in the world.
 
Interesting that it costs $3K, when my wife can get a few injections of Botox in her forehead for $150 from an licensed nurse.

That being said, it would be great if it becomes a realistic treatment, because of what I mention above. The product itself is already plentiful and relatively cheap.
 
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Interesting that it costs $3K, when my wife can get a few injections of Botox in her forehead for $150 from an licensed nurse.

That being said, it would be great if it becomes a realistic treatment, because of what I mention above. The product itself is already plentiful and relatively cheap.
Has anyone tried this? I see there are now more studies confirming Botox, and it’s similar competitors, can help ED. The studies indicate it lasts for 3 months or more and is even more effective coupled with Viagra/Cialis or injections.
 
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