Compounds > 7-3--dihydroxy-4--methoxyisoflavone

7-3--dihydroxy-4--methoxyisoflavone and Diabetes-Mellitus

7-3--dihydroxy-4--methoxyisoflavone has been researched along with Diabetes-Mellitus* in 2 studies

Other Studies

2 other study(ies) available for 7-3--dihydroxy-4--methoxyisoflavone and Diabetes-Mellitus

Article	Year
Calycosin plays a protective role in diabetic kidney disease through the regulation of ferroptosis. Pharmaceutical biology, 2022, Volume: 60, Issue:1 Diabetic kidney disease (DKD) is a devastating complication of diabetes. Renal functional deterioration caused by tubular injury is the primary change associated with this disease. Calycosin shows protective roles in various diseases.. This study explored the function and underlying mechanism of calycosin in DKD.. HG-induced decreased expression of glutathione (491.57 ± 33.56 to 122.6 ± 9.78 μmol/mL) and glutathione peroxidase 4 (inhibition rate 92.3%) and increased expression of lactate dehydrogenase (3.85 ± 0.89 to 16.84 ± 2.18 U/mL), malondialdehyde (3.72 ± 0.66 to 18.2 ± 1.58 nmol/mL), lipid ROS (4.31-fold increase) and NCOA4 (7.69-fold increase). The effects induced by HG could be blocked by calycosin. Moreover, calycosin alleviated the HG-induced decrease of cell viability and the increase of lipid ROS, but erastin could block the effects caused by calycosin. The. Calycosin has a protective effect on diabetic kidney disease; ferroptosis may be involved in this process. Topics: Animals; Diabetes Mellitus; Diabetic Nephropathies; Ferroptosis; Isoflavones; Lipids; Mice; Reactive Oxygen Species	2022
Bioinformatics and Frontiers in endocrinology, 2022, Volume: 13 Heart failure (HF) and diabetes mellitus (DM) are life-threatening diseases. However, existing clinical drugs to treat HF complicated with DM are relatively limited. In this study, we performed a viable bioinformatics strategy combining network pharmacology and molecular docking to identify potential anti-HF and -DM targets and therapeutic mechanisms of calycosin, a functional phytoestrogen.. Web-based databases were used to collect candidate genes/targets of calycosin and HF/DM and then identify the hub bio-targets of calycosin against HF/DM. Using the online-available database, all functional processes and signaling pathways of calycosin against HF/DM were screened and identified before further visualization.. All potential bio-targets of calycosin and HF/DM were collected, and 20 hub targets of calycosin against HF/DM were identified. Interestingly, molecular docking findings indicated that mitogen-activated protein kinase-1 (MAPK1), β-arrestin 1 (ARRB1), and homologue-1 (ABL1) may be potent pharmacological targets of calycosin against HF/DM. In addition, all primary molecular functions of calycosin against HF/DM were identified, including regulating protein binding, ubiquitination, and the metabolic process. Furthermore, the top molecular pathways of calycosin against HF/DM were revealed, including cardiomyocyte and chemokine signaling pathways. Topics: Computational Biology; Diabetes Mellitus; Heart Failure; Humans; Isoflavones; Molecular Docking Simulation	2022

Article

Year

Calycosin plays a protective role in diabetic kidney disease through the regulation of ferroptosis.

Pharmaceutical biology, 2022, Volume: 60, Issue:1

Diabetic kidney disease (DKD) is a devastating complication of diabetes. Renal functional deterioration caused by tubular injury is the primary change associated with this disease. Calycosin shows protective roles in various diseases.. This study explored the function and underlying mechanism of calycosin in DKD.. HG-induced decreased expression of glutathione (491.57 ± 33.56 to 122.6 ± 9.78 μmol/mL) and glutathione peroxidase 4 (inhibition rate 92.3%) and increased expression of lactate dehydrogenase (3.85 ± 0.89 to 16.84 ± 2.18 U/mL), malondialdehyde (3.72 ± 0.66 to 18.2 ± 1.58 nmol/mL), lipid ROS (4.31-fold increase) and NCOA4 (7.69-fold increase). The effects induced by HG could be blocked by calycosin. Moreover, calycosin alleviated the HG-induced decrease of cell viability and the increase of lipid ROS, but erastin could block the effects caused by calycosin. The. Calycosin has a protective effect on diabetic kidney disease; ferroptosis may be involved in this process.

Topics: Animals; Diabetes Mellitus; Diabetic Nephropathies; Ferroptosis; Isoflavones; Lipids; Mice; Reactive Oxygen Species

2022

Bioinformatics and

Frontiers in endocrinology, 2022, Volume: 13

Heart failure (HF) and diabetes mellitus (DM) are life-threatening diseases. However, existing clinical drugs to treat HF complicated with DM are relatively limited. In this study, we performed a viable bioinformatics strategy combining network pharmacology and molecular docking to identify potential anti-HF and -DM targets and therapeutic mechanisms of calycosin, a functional phytoestrogen.. Web-based databases were used to collect candidate genes/targets of calycosin and HF/DM and then identify the hub bio-targets of calycosin against HF/DM. Using the online-available database, all functional processes and signaling pathways of calycosin against HF/DM were screened and identified before further visualization.. All potential bio-targets of calycosin and HF/DM were collected, and 20 hub targets of calycosin against HF/DM were identified. Interestingly, molecular docking findings indicated that mitogen-activated protein kinase-1 (MAPK1), β-arrestin 1 (ARRB1), and homologue-1 (ABL1) may be potent pharmacological targets of calycosin against HF/DM. In addition, all primary molecular functions of calycosin against HF/DM were identified, including regulating protein binding, ubiquitination, and the metabolic process. Furthermore, the top molecular pathways of calycosin against HF/DM were revealed, including cardiomyocyte and chemokine signaling pathways.

Topics: Computational Biology; Diabetes Mellitus; Heart Failure; Humans; Isoflavones; Molecular Docking Simulation

2022