Mechanism of Huoxue Tongluo Decoction in treatment of erectile dysfunction caused by ischemic stroke based on network pharmacology

Ji-sheng Wang; Heng-heng Dai; Kai-ge Zhang; Sheng Deng; Bing-hao Bao; Jun-long Feng; Fan-chao Meng; Ji-sheng Wang; Heng-heng Dai; Kai-ge Zhang; Ke-gang Cao; Sheng Deng; Bing-hao Bao; Jun-long Feng; Fan-chao Meng; Hai-song LI; Bin Wang; Ke-gang Cao

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Mechanism of Huoxue Tongluo Decoction in treatment of erectile dysfunction caused by ischemic stroke based on network pharmacology

Author: Ji-sheng WANG ¹ ; Heng-heng DAI ¹ ; Kai-ge ZHANG ¹ ; Sheng DENG ¹ ; Bing-hao BAO ¹ ; Jun-long FENG ¹ ; Fan-chao MENG ¹ ; Ji-sheng WANG ² ; Heng-heng DAI ² ; Kai-ge ZHANG ² ; Ke-gang CAO ² ; Sheng DENG ² ; Bing-hao BAO ² ; Jun-long FENG ² ; Fan-chao MENG ² ; Hai-song LI ² ; Bin WANG ² ; Ke-gang CAO ³
Author Information

1. First Clinical School of Medicine, Beijing University of Chinese Medicine
2. Dongzhimen Hospital Affiliated to Beijing University of Traditional Chinese Medicine
3. China Tibetology Research Center, Beijing Tibetan Hospital
Publication Type:Journal Article
Keywords: erectile dysfunction; Huoxue Tongluo Decoction; ischemic stroke; network pharmacology
From: Chinese Herbal Medicines 2021;13(3):351-358
CountryChina
Language:Chinese
Abstract: Objective: To study the therapeutic effect of Huoxue Tongluo Decoction (HXTLD) on erectile dysfunction caused by ischemic stroke and identify the mechanisms involved. Methods: Network pharmacology was used to predict the key active ingredients and targets of HXTLD. Surgical methods were used to create a rat model of ischemic stroke. The rats were then given a suspension of HXTLD by ig administration. Erectile function was evaluated by Apomorphine (APO) induction. Real-time fluorescence quantitative reverse transcription-polymerase chain reaction (Real-time PCR) and Western blotting were used to detect the expression of related mRNAs and proteins in rat penile corpus cavernous tissue and brain tissue. Hematoxylin & Eosin (HE) staining was used to investigate structural changes in the penile cavernous tissue. Results: Network pharmacology showed that tumor necrosis factor (TNF), nitric oxide synthase 3 (eNOS), and vascular endothelial growth factor (VEGF) were the key targets of HXTLD in the treatment of erectile dysfunction caused by ischemic stroke. Experimental studies showed that HXTLD improved erectile dysfunction caused by ischemic stroke. HE results showed that HXTLD improved the structure of the corpus cavernosa. HXTLD also inhibited the expression of TNF and VEGF proteins in penile tissue (P < 0.05) and enhanced the expression of eNOS protein in penile tissue (P < 0.05). Conclusion: HXTLD improved the erectile function of rats with erectile dysfunction caused by ischemic stroke by regulating the mRNA and protein levels of TNF, eNOS and VEGF.