Delving into the Latest Updates on Diosmin with Synapse

Overview

Basic Info

Drug Type

Small molecule drug

Synonyms

3',5,7-trihydroxy-4'-methoxyflavone 7-rhamnoglucoside, 3',5,7-trihydroxy-4'-methoxyflavone-7-rutinoside, Citrus Bioflavonoids

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Target-

Action-

Mechanism-

Therapeutic Areas

Cardiovascular DiseasesDigestive System DisordersUrogenital Diseases

Active Indication

Chronic venous insufficiencyHemorrhoidsRenal fibrosis

Inactive Indication-

Originator Organization-

Active Organization

Les Laboratoires Servier SASThe Second Affiliated Hospital of Anhui Medical University

Inactive Organization-

License Organization-

Drug Highest PhaseApproved

First Approval Date

China (04 Jun 2004),

Chronic venous insufficiencyHemorrhoids

RegulationOrphan Drug (United States)

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Structure/Sequence

Molecular FormulaC28H32O15

InChIKeyGZSOSUNBTXMUFQ-YFAPSIMESA-N

CAS Registry520-27-4

This study is performed to consider the safety and healing ability of diosmin in patients with systemic sclerosis (scleroderma) and open sores on their fingers (digital ulcers). Two (2) out of three (3) participants will receive active product. The participants will have four (4) visits over eight (8) weeks. Physical exams and photos will be performed. A variety of questions will be asked describing level of pain and lifestyle changes.

Start Date15 Dec 2024

Sponsor / Collaborator

Primus Pharmaceuticals, Inc.

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NCT06584799

/ RecruitingPhase 3IIT

Comparative Assessment of the Efficacy and Safety of Venoactive Drug Treatment of Pelvic Venous Disorders

Venoactive drug (VAD) therapy is one of the most effective methods of treating chronic venous diseases (CVD). Numerous studies have proven its high efficacy in relieving symptoms of CVD, such as leg pain and swelling, leg heaviness and fatigue. Pelvic venous disorders (PeVDs) represent a group of pathological conditions including varicose veins of the pelvis and vulva, and compression stenoses of the left renal and common iliac veins. Although PeVDs are associated with venous lesions of the pelvis and retroperitoneum and have specific clinical manifestations, they are one of the forms of CVD and constitute a separate cohort. A number of studies on the VAD usage in PeVD indicate the wide possibilities of this type of treatment in eliminating chronic pelvic pain (CPP), the most dramatic symptom of PeVD, which is the main cause of disability and decreased quality of life, social and daily activity in women with PeVD. Currently, a variety of VADs are presented on the pharmaceutical market, which, according to the product labels, provide effects not only on the venous outflow from the lower extremities, but also on venous hemodynamics in the pelvis. At the same time, a literature analysis shows that micronized purified flavonoid fraction (MPFF) has the greatest evidence base obtained in the efficacy and safety studies of VADs in PeVD. Nevertheless, patients are rarely interested in the scientific dossier of drugs, and in the real practice the patients with PeVD and CPP most often ask: "What is the best drug to use for the CPP relief?" This is quite understandable, as it is CPP in PeVD that results not only in disability, but also in family conflicts, psycho-emotional stress and depressive states. In this regard, patients seek to get rid of pain as soon as possible and strive to use the most effective drug. An extensive scientific base of comparative studies on the use of various VADs in patients with CVD and PeVD has been accumulated to date. However, the literature is lack of any data on the comparative efficacy and safety of VADs in the treatment of patients with PeVD. This, in turn, makes not possible for doctors and patients to choose the optimal and most effective drug based on the objective research data. All the above has predetermined the purpose of the planned study as evaluating the efficacy and safety of different VADs in the treatment of female patients with PeVD.

Start Date01 Dec 2024

Sponsor / Collaborator

Russian National Research Medical University

NCT06546111

/ RecruitingPhase 1/2IIT

Clinical Study to Evaluate the Possible Efficacy and Safety of Diosmin and Hesperidin Combined Therapy in Patients With Helicobacter Pylori Infection

This study intends to assess the possible effectiveness and safety of Diosmin and Hesperidin combination in patients with Helicobacter pylori Infection through evaluating its effect on stool antigen test and serum levels of inflammatory biomarkers as(TNF-A and MDA).

Start Date01 Oct 2024

Sponsor / Collaborator

University of Sadat City

100 Clinical Results associated with Diosmin

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100 Translational Medicine associated with Diosmin

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100 Patents (Medical) associated with Diosmin

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2,092

Literatures (Medical) associated with Diosmin

01 Dec 2025·Molecular Biology Reports

A review of six bioactive compounds from preclinical studies as potential breast cancer inhibitors

Review

Author: Rampogu, Shailima ; Oh, Tae Hwan ; Al-Antari, Mugahed A ; Shaik, Baji

Breast cancer is one of the predominant causes of mortality in women worldwide. Although therapeutics such as surgery, chemotherapy, hormonal therapy, and radiotherapy have been used, they are associated with adverse effects or multidrug resistance. The use of natural compounds is a promising strategy, owing to their abundance and medicinal value. This review focuses on six natural compounds, namely cinnamaldehyde, diosmin, taxifolin, phloretin, arctigenin, and eugenol, and details their mechanisms of breast cancer inhibition based on in vitro and in vivo studies. These compounds generally promote apoptosis and cell cycle arrest, hinder metastasis and invasion, and decrease tumor growth. This review reinforces the use of natural compounds as therapeutics for breast cancer from their preclinical studies. These compounds might be promising for drug development due to their abundance, high reliability, and safety.

01 Jun 2025·Phytomedicine

Diosmin attenuates UUO-induced renal ferroptosis and fibrosis by inhibiting the HIF-1α/FABP4 signaling axis

Article

Author: Zhu, Jun-Xing ; Liu, Meng-Qian ; Zhu, Yuyu ; Li, Xun-Liang ; Shi, Rui ; Wei, Jie ; Wang, Xue-Rong ; Zhu, Jia-Xin ; Zhao, Wen-Man ; Wang, De-Guang ; Chu, Fan ; Zhu, Yu-Ke ; Wang, Zhi-Juan

BACKGROUND AND PURPOSERenal fibrosis is a major pathological feature of chronic kidney disease (CKD) that poses significant therapeutic challenges owing to its irreversible nature. In this study, we aimed to investigate the effects of diosmin, a polyphenolic flavonoid with anti-inflammatory, antioxidant, and antifibrotic properties, on renal fibrosis and to explore the underlying mechanisms.STUDY DESIGN AND METHODSMouse renal fibrosis model induced by UUO surgery and an HK-2 cell fibrosis model stimulated by TGF-β1 were established to evaluate the effects of diosmin treatment on cell injury, inflammatory response, and ferroptosis. Changes in the expression of related genes in the kidney tissues were analyzed using RNA-seq. In addition, the effects of fatty acid-binding protein 4 (FABP4) on the efficacy of diosmin were explored by knockdown and overexpression of FABP4. Double luciferase reporter gene assay, Chip-qPCR, molecular docking, surface plasmon resonance, and cellular thermal shift experiments were performed to explore this mechanism.RESULTSDiosmin mitigated renal tubular injury and collagen deposition in the UUO model by modulating fibrotic markers, such as fibronectin, Col I α1, and α-SMA. It also reduces iron accumulation, decreases the expression of MDA, ASCL4, and inflammatory cytokines, and increases the expression of GPX4 and SOD2, thereby attenuating ferroptosis and enhancing the cellular response to oxidative stress. In vitro, diosmin counteracted TGF-β1-induced cellular damage and ferroptosis. RNA-seq analysis revealed that diosmin intervention suppressed the expression of FABP4 induced by UUO and targeted silencing of FABP4 attenuated cellular damage and ferroptosis. Conversely, FABP4 overexpression in vivo compromised the renoprotective effects of diosmin. Mechanically, diosmin was found to bind to HIF-1α and reduce its nuclear translocation, thereby inhibiting FABP4 transcription, resulting in reduced inflammation, collagen deposition, and ferroptosis. Furthermore, the overexpression of HIF-1α reversed the protective effects of diosmin.CONCLUSIONDiosmin potentially attenuates renal ferroptosis and fibrosis through the inhibition of the HIF-1α/FABP4 axis, offering a promising therapeutic approach for renal fibrosis.

01 Jun 2025·Separation and Purification Technology

Recovery of essential oils, polyphenols, fermentable sugars, and pectin from orange residues: Evaluation of extraction methodologies and characterization of value-added bioactive compounds

Author: Sierra, R. ; Lopez, G. D. ; Villabona, L. C. ; Mussatto, S. I. ; Posada, J. A. ; Duran-Aranguren, D. D. ; Carazzone, C.

Residues from orange processing are being continuously generated in vast amounts due to the increasing demand for this fruit and its byproducts worldwide.The valorization of Orange Residues is challenging in contrast to conventional "lignocellulosic residues" since this fruit-derived biomass contains high amounts of pectin and an extractive fraction rich in sugars, essential oils, and polyphenols.The relative amounts of these fractions are highly influenced by the juice/pulp extraction process.Even though several studies have explored how to produce added value from this biomass, it is necessary to compare how different techniques and operating conditions influence the bioactive compounds that can be recovered and the remnant biomass after processing.This study compares essential oil extraction, solvent extraction, and acid hydrolysis for fermentable sugar and pectin production to elucidate a feasible sequence for a biorefinery from Orange Residues.From our results, it was proposed a tech. feasible sequence that maximizes the yields of i) essential oils (0.70 ± 0.05 g/ 100 g DM) from steam distillation (4 h, 1500 W), ii) naringin (0.19 g/100 g DM), hesperidin (1.27 g/100 g DM), and glucose (3.9 g/100 g DM) from solid-liquid extraction (Ethanol 61.6% (w/v), 45.8°C, 155.5 min, and 5% (w/v) biomass load), iii) pectin (25.24 g/100 g DM) from citric acid hydrolysis (pH 1.5, 90°C, 82.1 min, and 5% (w/v) biomass load), and iv) glucose (12.41 g/100 g DM) and xylose (10.13 g/100 g DM) from sulfuric acid hydrolysis (Sulfuric acid 0.68% (w/v), 121°C, 24.1 min, and 7.32% (w/v) biomass load), in a biorefinery scheme.

100 Deals associated with Diosmin

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External Link

KEGG	Wiki	ATC	Drug Bank
D07858	Diosmin	C05CA03	DB08995

R&D Status

Approved

10 top approved records.

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Indication	Country/Location	Organization	Date
Chronic venous insufficiency	China	Les Laboratoires Servier SAS	04 Jun 2004
Hemorrhoids	China	Les Laboratoires Servier SAS	04 Jun 2004

Developing

10 top R&D records.

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Indication	Highest Phase	Country/Location	Organization	Date
Renal fibrosis	Preclinical	China	The Second Affiliated Hospital of Anhui Medical University	09 Jan 2024

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Clinical Result

Indication

Phase

Evaluation

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Study	Phase	Population	Analyzed Enrollment	Group	Results	Evaluation	Publication Date


NCT03413618 (RIDILOTT-DVT, CTgov)	Phase 4	Postthrombotic Syndrome	90	compression stockings+rivaroxaban+Diosmin (Experimental: Rivaroxaban + Diosmin + Stockings)	dommpzqrca(hednaxcwfi) = tcyhqjmrwu eanwbcmexp (chdrynfirt, ktqovovgpl - svbkzdeagv) View more	-	27 Jan 2020
				compression stockings+rivaroxaban (Control: Rivaroxaban + Stockings Only)	dommpzqrca(hednaxcwfi) = vsumgokjzj eanwbcmexp (chdrynfirt, rakhmhhvfe - gsdqnvtkuq) View more