🧬 BDNF Extraction Viewer

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Lack of sustained improvements in erectile function following low-intensity extracorporeal shockwave therapy correlate with decreases in corporal brain-derived neurotropic factor: a pilot study and prospective clinical trial.

PMID: 41583708 · DOI: 10.1093/sexmed/qfaf107 · Sexual medicine, 2025 · Skye Coffey, Vy Nguyen, Ashley N Matthew, Bridget S Kastelberg, Maria E Teves, Mina Ghatas, Adam P Klausner, Ryan P Smit
📄 Abstract

Low-intensity extracorporeal shockwave therapy (Li-ESWT) is thought to treat erectile dysfunction (ED) by stimulating neovascularization and nerve regeneration as demonstrated in animal models by histologically increased angiogenesis and neuronal-related growth factors, though corresponding human studies are limited. We hypothesized that Li-ESWT results in appreciable increases in growth factors in human tissues, and in this proof-of-concept study we aimed to determine whether markers for neovascularization and nerve regeneration can be detected in the corporal blood of men following Li-ESWT treatment. Patients were prospectively enrolled in a clinical trial of Li-ESWT for ED. Patients received 12 bi-weekly Li-ESWT treatments of 0.2 mJ/mm eNOS, nNOS, VEGF, and BDNF were detectable and demonstrated changes in cavernosal plasma samples following Li-ESWT treatment. Twenty-five patients completed all five study visits. Mean patient age was 63. Mean baseline International Index of Erectile Function-Erectile Function score prior to treatment was 14.24 (±1.21). Corporal plasma samples were analyzed for eNOS, nNOS, VEGF, and BDNF using the enzyme-linked immunosorbent assay. Levels of eNOS, nNOS, and VEGF showed an upward trend following treatment but did not reach significance. BDNF levels were noted to decrease. Corporal blood aspirates may function as surrogates for histological studies to understand effects of Li-ESWT at the tissue level in humans. To our knowledge, this is first the molecular study in human tissues to attempt to quantify neurogenesis and neovascularization in penile tissue following Li-ESWT for ED. Although our sample size is small, we believe this represents a promising first step in understanding the effect of Li-ESWT at a tissue level in men. The clinical significance of our findings is currently unknown, but markers of neovascularization and neurogenesis are detectable in corporal plasma and may change following Li-ESWT. ClinicalTrials.gov

Confidence: 0.19 · 10 полей извлечено
Идентификация (6 полей)
Target
Brain-derived neurotrophic factor
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Alt. target
BDNF
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Protein family
Neurotrophin family
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Functional class
Growth factor
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Subcellular loc.
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Isoforms (metab/obesity)
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Механизм действия (21 полей)
Mechanism
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Mutations (obesity/lean)
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Activity (obesity)
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Activity temporal
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Energy balance
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Appetite
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Fat metabolism
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Lipolysis
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Thermogenesis
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Muscle metabolism
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Inflammation
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Glucose metabolism
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AA metabolism
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Hormonal pathways
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Cell death
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Adipocyte fibrosis
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Upstream (biochem)
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Upstream (physiol)
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Downstream (biochem)
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Downstream (physiol)
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PTMs
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Экспрессия (8 полей)
Tissue expression
eNOS, nNOS, VEGF, and BDNF were detectable in cavernosal plasma samples
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In vitro
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In vivo
Prospective clinical trial of Li-ESWT for ED in 25 patients; corporal plasma samples analyzed for eNOS, nNOS, VEGF, BDNF
0.95
In silico
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Genetic association
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Ex vivo
Corporal blood aspirates may function as surrogates for histological studies
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Animal model
Animal models mentioned in background: Li-ESWT stimulates neovascularization and nerve regeneration in animal models
0.70
Diet/model
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Клиника (11 полей)
Drug
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Indication
erectile dysfunction
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Patient subgroups
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Safety concerns
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Off-target
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Trial stage
pilot study; prospective clinical trial
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Pharma competitors
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AE severity
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MOA weight loss
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Endpoints
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Approved
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