Your search keyword '"Ginsenoside Rh2"' showing total 461 results

1. Ginsenoside Rh2 suppresses ferroptosis in ulcerative colitis by targeting specific protein 1 by upregulating microRNA-125a-5p.

Author

Zhao, Xun, Yuan, WenQiang, Yang, LiuChan, Yan, Fang, and Cui, DeJun

Subjects

ULCERATIVE colitis, GINSENOSIDES, FERRIC chloride, DEXTRAN sulfate, EPITHELIAL cells

Abstract

Background: Worldwide, ulcerative colitis (UC) is becoming increasingly fast growing. Ginsenoside Rh2 has been reported to alleviate UC. However, the latent biological mechanism of Rh2 in the treatment of UC remains uncertain. In this study, the goal was to determine the therapeutic effect of Rh2 on dextran sulfate sodium (DSS)-induced UC. Methods: A DSS-induced UC mouse model was established and divided into 7 groups for Rh2 gavage and/or miR-125a-5p lentivirus injection (n = 10 per group). Colonic specimens were collected for phenotypic and pathological analysis. miR-125a-5p and specific protein 1 (SP1) expression, inflammation-related factors IL-6 and IL-10, and apoptosis were detected in mice. Human normal colon epithelial cell line NCM460 was treated with H2O2 and ferric chloride hexahydrate to construct an in vitro cell model of colitis and induce ferroptosis. Independent sample t-test was used to compare cell proliferation, cell entry, apoptosis, and oxidative stress between the two groups. One way analysis of variance combined with the least significant difference t test was used for comparison between groups. Multiple time points were compared by repeated measurement analysis of variance. Results: DSS-induced UC mice had significantly decreased body weight, increased disease activity index, decreased colon length, and decreased miR-125a-5p expression (all P < 0.05). In the DSS-induced mouse model, the expression of miR-125a-5p rebounded and ferroptosis was inhibited after Rh2 treatment (all P < 0.05). Inhibition of miR-125a-5p or upregulation of SP1 expression counteracted the protective effects of Rh2 on UC mice and ferroptosis cell models (all P < 0.05). Conclusions: Rh2 mitigated DSS-induced colitis in mice and restrained ferroptosis by targeting miR-125a-5p. Downregulating miR-125a-5p or elevating SP1 could counteract the protective impacts of Rh2 on ferroptotic cells. The findings convey that Rh2 has a latent application value in the treatment of UC. Highlights: Rh2 mitigates DSS-induced ferroptosis in mice; MiR-125a-5p represses DSS-induced ferroptosis in mice. Rh2 has protective impacts on ferroptotic cells. MiR-125a-5p targets SP1; Repression of miR-125a-5p or elevation of SP1 can counteract the protective effects of Rh2 on ferroptotic cells. [ABSTRACT FROM AUTHOR]

Published

2024

2. Effects of ginsenoside Rh2 on cisplatin‐induced nephrotoxicity in renal tubular epithelial cells by inhibiting endoplasmic reticulum stress.

Author

Wang, Lianping, Hao, Xiaogang, Li, Xiangxin, Li, Qingjie, and Fang, Xuexun

Subjects

BLOOD urea nitrogen, GINSENG, ACUTE kidney failure, KIDNEY physiology, ENDOPLASMIC reticulum

Abstract

Nephrotoxicity remains a major adverse reaction of the anticancer drug cisplatin (CDDP) chemotherapy, which is an important risk factor for chronic renal disease. Ginsenoside Rh2 from Panax ginseng has been shown to protect against CDDP‐induced nephrotoxicity in vivo, but its pharmacological effect on renal tubular epithelial cells is not clearly understood. This study examined the molecular mechanisms underlying the nephroprotective effects of Rh2 on CDDP‐induced HK‐2 cells and acute kidney injury (AKI) mice. As a result of Rh2 treatment, CDDP‐induced HK‐2 cells showed increased cell viability and reduced lactate dehydrogenase release. Moreover, Rh2 ameliorated CDDP‐induced mitochondrial membrane potential, increased antioxidant enzyme activities, and reduced pro‐inflammatory cytokine expression to reduce damage. Rh2 inhibited apoptosis and enhanced the antioxidant capacity of HK‐2 cells by reducing proteins associated with endoplasmic reticulum (ER) stress, as well as by attenuating tunicamycin‐induced ER stress. In addition, treatment of CDDP‐induced AKI mice with Rh2 substantially reduced blood urea nitrogen and serum creatinine levels, attenuated histological damage of kidney. Further, Rh2 also improved kidney function by inhibiting ER stress to support in vitro findings. These results consistently demonstrated that Rh2 protects renal tubular epithelial cells from CDDP‐induced nephrotoxicity and apoptosis by restoring ER homeostasis, which might suggest a therapeutic potential and providing new insights into AKI alternative therapies. [ABSTRACT FROM AUTHOR]

Published

2024

3. Ginsenoside Rh2 suppresses ferroptosis in ulcerative colitis by targeting specific protein 1 by upregulating microRNA-125a-5p

Author

Xun Zhao, WenQiang Yuan, LiuChan Yang, Fang Yan, and DeJun Cui

Subjects

Ginsenoside Rh2, MicroRNA-125a-5p, Specific protein 1, Ulcerative colitis, Ferroptosis, Medicine

Abstract

Abstract Background Worldwide, ulcerative colitis (UC) is becoming increasingly fast growing. Ginsenoside Rh2 has been reported to alleviate UC. However, the latent biological mechanism of Rh2 in the treatment of UC remains uncertain. In this study, the goal was to determine the therapeutic effect of Rh2 on dextran sulfate sodium (DSS)-induced UC. Methods A DSS-induced UC mouse model was established and divided into 7 groups for Rh2 gavage and/or miR-125a-5p lentivirus injection (n = 10 per group). Colonic specimens were collected for phenotypic and pathological analysis. miR-125a-5p and specific protein 1 (SP1) expression, inflammation-related factors IL-6 and IL-10, and apoptosis were detected in mice. Human normal colon epithelial cell line NCM460 was treated with H2O2 and ferric chloride hexahydrate to construct an in vitro cell model of colitis and induce ferroptosis. Independent sample t-test was used to compare cell proliferation, cell entry, apoptosis, and oxidative stress between the two groups. One way analysis of variance combined with the least significant difference t test was used for comparison between groups. Multiple time points were compared by repeated measurement analysis of variance. Results DSS-induced UC mice had significantly decreased body weight, increased disease activity index, decreased colon length, and decreased miR-125a-5p expression (all P

Published

2024

4. Ginsenoside Rh2 Regulates the Calcium/ROS/CK1α/MLKL Pathway to Promote Premature Eryptosis and Hemolysis in Red Blood Cells.

Author

Alghareeb, Sumiah A, Alsughayyir, Jawaher, and Alfhili, Mohammad A

Subjects

*CASEIN kinase, *GINSENOSIDES, *VITAMIN C, *OXIDATIVE stress, *ANTINEOPLASTIC agents

Abstract

Ginsenoside Rh2 (GRh2) exhibits significant potential as an anticancer agent; however, progress in developing chemotherapeutic drugs is impeded by their toxicity toward off-target tissues. Specifically, anemia caused by chemotherapy is a debilitating side effect and can be caused by red blood cell (RBC) hemolysis and eryptosis. Cells were exposed to GRh2 in the antitumor range and hemolytic and eryptotic markers were examined under different experimental conditions using photometric and cytofluorimetric methods. GRh2 caused Ca2+-independent, concentration-responsive hemolysis in addition to disrupted ion trafficking with K+ and Cl– leakage. Significant increases in cells positive for annexin-V-fluorescein isothiocyanate, Fluo4, and 2,7-dichlorofluorescein were noted upon GRh2 treatment coupled with a decrease in forward scatter and acetylcholinesterase activity. Importantly, the cytotoxic effects of GRh2 were mitigated by ascorbic acid and by blocking casein kinase 1α (CK1α) and mixed lineage kinase domain-like (MLKL) signaling. In contrast, Ca2+ omission, inhibition of KCl efflux, and isosmotic sucrose aggravated GRh2-induced RBC death. In whole blood, GRh2 selectively targeted reticulocytes and lymphocytes. Altogether, this study identified novel mechanisms underlying GRh2-induced RBC death involving Ca2+ buildup, loss of membrane phospholipid asymmetry and cellular volume, anticholinesterase activity, and oxidative stress. These findings shed light on the hematologic toxicity of GRh2 which is crucial for optimizing its utilization in cancer treatment. [ABSTRACT FROM AUTHOR]

Published

2024

5. Ginsenoside Rh2 Alleviate Sepsis-related Encephalopathy via Up-regulating Nrf2/HO-1 Pathway and Apoptosis Inhibition

Author

Zhu, Yufeng, Li, Jinhang, Dai, Lijun, and Feng, Wei

Published

2024

6. Ginsenoside Rh2 shifts tumor metabolism from aerobic glycolysis to oxidative phosphorylation through regulating the HIF1-α/PDK4 axis in non-small cell lung cancer

Author

Xiyu Liu, Jingjing Li, Qingqing Huang, Mingming Jin, and Gang Huang

Subjects

Ginsenoside Rh2, NSCLC, PDK4, Glycolysis, Oxidative phosphorylation, Therapeutics. Pharmacology, RM1-950, Biochemistry, QD415-436

Abstract

Abstract Background Ginsenoside Rh2 (G-Rh2), a steroidal compound extracted from roots of ginseng, has been extensively studied in tumor therapy. However, its specific regulatory mechanism in non-small cell lung cancer (NSCLC) is not well understood. Pyruvate dehydrogenase kinase 4 (PDK4), a central regulator of cellular energy metabolism, is highly expressed in various malignant tumors. We investigated the impact of G-Rh2 on the malignant progression of NSCLC and how it regulated PDK4 to influence tumor aerobic glycolysis and mitochondrial function. Method We examined the inhibitory effect of G-Rh2 on NSCLC through I proliferation assay, migration assay and flow cytometry in vitro. Subsequently, we verified the ability of G-Rh2 to inhibit tumor growth and metastasis by constructing subcutaneous tumor and metastasis models in nude mice. Proteomics analysis was conducted to analyze the action pathways of G-Rh2. Additionally, we assessed glycolysis and mitochondrial function using seahorse, PET-CT, Western blot, and RT-qPCR. Result Treatment with G-Rh2 significantly inhibited tumor proliferation and migration ability both in vitro and in vivo. Furthermore, G-Rh2 inhibited the tumor’s aerobic glycolytic capacity, including glucose uptake and lactate production, through the HIF1-α/PDK4 pathway. Overexpression of PDK4 demonstrated that G-Rh2 targeted the inhibition of PDK4 expression, thereby restoring mitochondrial function, promoting reactive oxygen species (ROS) accumulation, and inducing apoptosis. When combined with sodium dichloroacetate, a PDK inhibitor, it complemented the inhibitory capacity of PDKs, acting synergistically as a detoxifier. Conclusion G-Rh2 could target and down-regulate the expression of HIF-1α, resulting in decreased expression of glycolytic enzymes and inhibition of aerobic glycolysis in tumors. Additionally, by directly targeting mitochondrial PDK, it elevated mitochondrial oxidative phosphorylation and enhanced ROS accumulation, thereby promoting tumor cells to undergo normal apoptotic processes.

Published

2024

7. Differential antiangiogenic and anticancer activities of the active metabolites of ginsenoside Rg3

Author

Maryam Nakhjavani, Eric Smith, Kenny Yeo, Yoko Tomita, Timothy J. Price, Andrea Yool, Amanda R. Townsend, and Jennifer E. Hardingham

Subjects

Anticancer, Epimer, Ginsenoside Rh2, Ginsenoside Rg3, Protopanaxadiol, Botany, QK1-989

Abstract

Background: Epimers of ginsenoside Rg3 (Rg3) have a low bioavailability and are prone to deglycosylation, which produces epimers of ginsenoside Rh2 (S–Rh2 and R–Rh2) and protopanaxadiol (S-PPD and R-PPD). The aim of this study was to compare the efficacy and potency of these molecules as anti-cancer agents. Methods: Crystal violet staining was used to study the anti-proliferatory action of the molecules on a human epithelial breast cancer cell line, MDA-MB-231, and human umbilical vein endothelial cells (HUVEC) and compare their potency. Cell death and cell cycle were studied using flow cytometry and mode of cell death was studied using live cell imaging. Anti-angiogenic effects of the drug were studied using loop formation assay. Molecular docking showed the interaction of these molecules with vascular endothelial growth factor receptor-2 (VEGFR2) and aquaporin (AQP) water channels. VEGF bioassay was used to study the interaction of Rh2 with VEGFR2, in vitro. Results: HUVEC was the more sensitive cell line to the anti-proliferative effects of S–Rh2, S-PPD and R-PPD. The molecules induced necroptosis/necrosis in MDA-MB-231 and apoptosis in HUVEC. S–Rh2 was the most potent inhibitor of loop formation. In silico molecular docking predicted a good binding score between Rh2 or PPD and the ATP-binding pocket of VEGFR2. VEGF bioassay showed that Rh2 was an allosteric modulator of VEGFR2. In addition, SRh2 and PPD had good binding scores with AQP1 and AQP5, both of which play roles in cell migration and proliferation. Conclusion: The combination of these molecules might be responsible for the anti-cancer effects observed by Rg3.

Published

2024

8. Remodeling the tumor immune microenvironment through hydrogel encapsulated G-Rh2 in situ vaccine and systemic immunotherapy

Author

Chunhua Li, Dan Lei, Yudong Huang, Yuanhao Jing, Wanru Wang, Lanqi Cen, Zijian Wei, Anni Chen, Xiaoyu Feng, Yushu Wang, Lixia Yu, Ying Chen, and Rutian Li

Subjects

Ginsenoside Rh2, PD-1 monoclonal antibody, Hydrogel, In situ vaccination, Tumor microenvironment, Immune modulation, Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

Ginsenoside Rh2 (G-Rh2) is a vital bioactive compound in Traditional Chinese Medicine, celebrated for its strong pharmacological properties, particularly its potent antitumor effects. However, its poor water solubility and limited bioavailability have necessitated the development of a novel drug delivery method. In this study, we utilized an indocyanine green carboxylic acid-hydroxypropyl cellulose-abietic acid-bovine serum albumin hydrogel (ICG-HPC-AA/BSA hydrogel) as a tumor in situ vaccine to enhance the permeability, retention, and tumor-targeted therapeutic efficacy of G-Rh2. We examined the therapeutic impact of a G-Rh2-loaded hydrogel combined with systemic PD-1 antibody treatment in murine models of H22 liver cancer and CT26 colon cancer. Additionally, we explored the immune microenvironment of the tumors influenced by this in situ vaccination strategy.

Published

2024

9. Ginsenoside Rh2 shifts tumor metabolism from aerobic glycolysis to oxidative phosphorylation through regulating the HIF1-α/PDK4 axis in non-small cell lung cancer.

Author

Liu, Xiyu, Li, Jingjing, Huang, Qingqing, Jin, Mingming, and Huang, Gang

Subjects

*NON-small-cell lung carcinoma, *OXIDATIVE phosphorylation, *GINSENOSIDES, *AEROBIC metabolism, *PYRUVATE dehydrogenase kinase, *HEPATOCELLULAR carcinoma, *LACTATES, *ECULIZUMAB

Abstract

Background: Ginsenoside Rh2 (G-Rh2), a steroidal compound extracted from roots of ginseng, has been extensively studied in tumor therapy. However, its specific regulatory mechanism in non-small cell lung cancer (NSCLC) is not well understood. Pyruvate dehydrogenase kinase 4 (PDK4), a central regulator of cellular energy metabolism, is highly expressed in various malignant tumors. We investigated the impact of G-Rh2 on the malignant progression of NSCLC and how it regulated PDK4 to influence tumor aerobic glycolysis and mitochondrial function. Method: We examined the inhibitory effect of G-Rh2 on NSCLC through I proliferation assay, migration assay and flow cytometry in vitro. Subsequently, we verified the ability of G-Rh2 to inhibit tumor growth and metastasis by constructing subcutaneous tumor and metastasis models in nude mice. Proteomics analysis was conducted to analyze the action pathways of G-Rh2. Additionally, we assessed glycolysis and mitochondrial function using seahorse, PET-CT, Western blot, and RT-qPCR. Result: Treatment with G-Rh2 significantly inhibited tumor proliferation and migration ability both in vitro and in vivo. Furthermore, G-Rh2 inhibited the tumor's aerobic glycolytic capacity, including glucose uptake and lactate production, through the HIF1-α/PDK4 pathway. Overexpression of PDK4 demonstrated that G-Rh2 targeted the inhibition of PDK4 expression, thereby restoring mitochondrial function, promoting reactive oxygen species (ROS) accumulation, and inducing apoptosis. When combined with sodium dichloroacetate, a PDK inhibitor, it complemented the inhibitory capacity of PDKs, acting synergistically as a detoxifier. Conclusion: G-Rh2 could target and down-regulate the expression of HIF-1α, resulting in decreased expression of glycolytic enzymes and inhibition of aerobic glycolysis in tumors. Additionally, by directly targeting mitochondrial PDK, it elevated mitochondrial oxidative phosphorylation and enhanced ROS accumulation, thereby promoting tumor cells to undergo normal apoptotic processes. [ABSTRACT FROM AUTHOR]

Published

2024

10. 人参皂苷辛酸酯通过内质网应激诱导肝癌细胞免疫原性细胞死亡的机制 研究

Author

戴珍珍, 黄青昕, 胡淇睿, 吴汉城, 潘瑶, 邓泽元, and 陈芳

Abstract

Objective: To investigate whether octyl ester derivative of ginsenoside Rh2（ Rh2-O ） can induce immunogenic cell death of Huh-7 hepatocellular carcinoma cells and possible mechanism. Methods: Huh-7 cells were cultured in vitro, and divided into control group, Rh2-O group, positive control group （mitoxantrone treatment）. Viability and apoptosis of cells were detected by CCK-8 and flow cytometry, respectively. Concentrations of high mobility family protein 1 （HMGB1） and adenosine triphosphate （ATP） in supernatant were detected by ELISA and chemiluminescence assay, respectively. Membrane eversion of calreticulin （CRT） was detected by immunofluorescence assay. ROS level in cells was detected by fluorescence probe DCFH-DA, and expressions of proteins associated with endoplasmic reticulum stress signaling pathway were detected by Western blot. Results: Rh2-O treatment significantly reduced cell viability, promoted apoptosis, induced secretion of HMGB1, ATP, membrane eversion of CRT, increased accumulation of ROS in cells, and enhanced expressions of endoplasmic reticulum stress-related proteins PERK, eIF2α, p-eIF2α （all P<0.05）. After addition of endoplasmic reticulum stress inhibitor 4-phenylbutyric acid（ 4-PBA）, membrane eversion of CRT induced by Rh2-O was significantly inhibited （P<0.05）. Conclusion: Rh2-O can induce immunogenic cell death in hepatocellular carcinoma whose mechanism may be associated with activation of endoplasmic reticulum stress and promotion of CRT membrane eversion. [ABSTRACT FROM AUTHOR]

Published

2024

11. 装载人参皂苷Rh2外泌体的制备及其对肝癌细胞株 Huh7、PLC半数抑制浓度测算.

Author

李美乐, 赵梓粤, 金凯, 唐婷, 黄俊期, 王戈睿, and 谢裕安

Abstract

To prepare the exosomes loaded with ginsenoside Rh2 (Exos@G-Rh2), and to calculate the half-maximal inhibitory concentration (IC50) on hepatoma cell lines Huh7 and PLC. Methods Using exosome extraction kits to isolate and purify exosomes (Exos) from the culture supernatant of hepatoma Huh7 cells, the electroporation method was employed to prepare Exos@G-Rh2. Transmission electron microscopy was used to observe the morphology of Exos@GRh2 and Exos. The particle size of Exos@G-Rh2 and Exos was measured using nanoparticle tracking analysis. High-perfor⁃ mance liquid chromatography (HPLC) was utilized to determine the G-Rh2 content in Exos@G-Rh2, and the drug-loading capacity was calculated. The uptake of Exos@G-Rh2 by hepatoma cell lines Huh7 and PLC was observed using PKH-26 flu⁃ orescence staining. The IC50 of Exos@G-Rh2 and free G-Rh2 on Huh7 and PLC cells was measured using CCK-8. Re⁃ sults Under the transmission electron microscope, both Exos and Exos@G-Rh2 displayed the classic cup-shaped struc⁃ ture enveloped by a lipid membrane, with no significant morphological differences. The particle sizes of Exos@G-Rh2 and Exos were (156. 90±10. 23) nm and (143. 47±8. 62) nm, respectively, with no significant difference between them (P> 0. 05) . The drug-loading capacity of Exos@G-Rh2 was 24. 25%±0. 27%. In the cytoplasm of Huh7 and PLC cells, red fluo⁃ rescence was clearly visible, primarily within the cytoplasm. In the Huh7 cells, the IC50 value of free G-Rh2 was (34. 96± 1. 37）µg/mL, whereas the IC50 value of Exos@G-Rh2 was (29. 74±2. 83）µg/mL, showing a significant difference (P<0. 05) . In the PLC cells, the IC50 value of free G-Rh2 was (33. 41±1. 47）µg/mL, while the IC50 value of Exos@G-Rh2 was (30. 08±1. 12）µg/mL, also showing a significant difference (P<0. 05) . Conclusions Exos@G-Rh2 is successfully prepared, with its morphology and particle size showing no significant difference from Exos, and it can be taken up by Huh7 and PLC cells. Compared with free G-Rh2, Exos@G-Rh2 exhibits a lower IC50 for Huh7 and PLC cells. [ABSTRACT FROM AUTHOR]

Published

2024

12. Host-microbiota interactions in collagen-induced arthritis rats treated with human umbilical cord mesenchymal stem cell exosome and ginsenoside Rh2

Author

Zhongsheng Zhou, Yang Li, Shuhui Wu, Te Liu, and Jinlan Jiang

Subjects

Rheumatoid arthritis, Collagen-induced arthritis, Ginsenoside Rh2, Gut microbiota, Metabolites, Mesenchymal stem cell exosomes, Therapeutics. Pharmacology, RM1-950

Abstract

Mesenchymal stem cell exosome (MSCs-exo) is a class of products secreted by mesenchymal stem cells (MSCs) that contain various biologically active substances. MSCs-exo is a promising alternative to MSCs due to their lower immunogenicity and lack of ethical constraints. Ginsenoside Rh2 (Rh2) is a hydrolyzed component of the primary active substance of ginsenosides. Rh2 has a variety of pharmacological functions, including anti-inflammatory, anti-tumor, and antioxidant. Studies have demonstrated that gut microbiota and metabolites are critical in developing rheumatoid arthritis (RA). In this study, we constructed a collagen-induced arthritis (CIA) model in rats. We used MSCs-exo combined with Rh2 to treat CIA rats. To observe the effect of MSCs-exo combined with Rh2 on joint inflammation, rat feces were collected for 16 rRNA amplicon sequencing and untargeted metabolomics analysis. The results showed that the arthritis index score and joint swelling of CIA rats treated with MSCs-exo in combination with Rh2 were significantly lower than those of the model and MSCs-exo alone groups. MSCs-exo and Rh2 significantly ameliorated the disturbed gut microbiota in CIA rats. The regulation of Candidatus_Saccharibacteria and Clostridium_XlVb regulation may be the most critical. Rh2 enhanced the therapeutic effect of MSCs-exo compared with the MSCs-exo -alone group. Furthermore, significant changes in gut metabolites were observed in the CIA rat group, and these differentially altered metabolites may act as messengers for host-microbiota interactions. These differential metabolites were enriched into relevant critical metabolic pathways, revealing possible pathways for host-microbiota interactions.

Published

2024

13. Research Progress on the Antitumor Molecular Mechanism of Ginsenoside Rh2.

Author

Yang, Lan, Chen, Jenny Jie, Sheng-Xian Teo, Brian, Zhang, Jiong, and Jiang, Mingqiang

Subjects

*CHINESE medicine, *LIVER tumors, *NF-kappa B, *T cells, *ANTINEOPLASTIC agents, *BREAST tumors, *CELL proliferation, *APOPTOSIS, *CHALONES, *IMMUNE system, *COLON tumors, *CELL lines, *GLYCOSIDES, *MEDICAL research, *MOLECULAR structure, *LUNG tumors, *CELL death, *COMBINED modality therapy, *GINSENG, *CELL differentiation, *PHARMACODYNAMICS

Abstract

Cancer has evolved into a substantial public health concern as the second-leading cause of mortality globally. Radiotherapy and chemotherapy have been the two most widely used cancer therapies in recent years; however, both have drawbacks. Therefore, the focus has shifted to the creation of herbal medicines, the extraction of active ingredients, replacement therapy, and the adverse effects of these medications. Ginsenoside Rh2, which is extracted from ginseng, has been identified in many cancer cells. The immune system of the body is strengthened by ginsenoside Rh2, which can also cause the proliferation, death, and differentiation of tumor cells through various pathways. For instance, it inhibits the expression of the NF- κ B signaling pathway and induces cell apoptosis, affects the expression levels of mitochondrial apoptosis proteins Bcl-2 and Bax, and cooperates with the PD-1 blockade to reactivate T cells to promote an antitumor immune response. Furthermore, ginsenosides Rh2 has the effect of reversing the toxic effect of chemotherapy drugs on normal cells, reducing myocardial damage, and relieving bone marrow function suppression. For clinical applications, it is mainly used as an adjuvant drug for preoperative neoadjuvant chemotherapy, postoperative adjuvant chemotherapy, and rescue treatment of advanced cancer. This paper summarizes the pharmacological action and mechanism of ginsenosides Rh2 in all kinds of cancer and looks forward to its future development and application. [ABSTRACT FROM AUTHOR]

Published

2024

14. Ginsenoside Rh2 mitigates myocardial damage in acute myocardial infarction by regulating pyroptosis of cardiomyocytes.

Author

Hong Peng, Li Chen, Yi Deng, Xin Liao, and Yi Yang

Subjects

*GINSENOSIDES, *CARDIOVASCULAR diseases, *PYROPTOSIS, *MYOCARDIAL infarction, *PHOSPHATIDYLINOSITOL 3-kinases, *PI3K/AKT pathway

Abstract

Background: Acute myocardial infarction (AMI) is one of the most important causes of mortality among patients with cardiovascular disease. Ginsenoside Rh2 plays a protective role in cardiovascular diseases. Furthermore, pyroptosis reportedly participates in regulating the occurrence and development of AMI. However, whether ginsenoside Rh2 contributes to mitigating AMI by regulating cardiomyocyte pyroptosis remains unknown. Methods: In the present study, we established an AMI model in rats. Next, we determined the effects of ginsenoside Rh2 on AMI by examining the myocardial infarct area, while regulation of myocardial pyroptosis was determined by assessing related factors. We established a cardiomyocyte model using hypoxia/reoxygenation (H/R) treatment. The expression of pyroptosis-related factors was determined following ginsenoside Rh2 treatment. In addition, we evaluated the correlation between ginsenoside Rh2 and the phosphoinositide 3-kinase (PI3K)/protein kinase B (AKT) pathway at the mechanistic level. Results: Herein, we observed that ginsenoside Rh2 alleviated AMI in rats and cells. Notably, the expression levels of inflammatory factors were reduced in AMI rats and cells. Furthermore, AMI rats and cells exhibited high expression levels of cleaved caspase-1 and gasdermin D, which were downregulated following treatment with ginsenoside Rh2. Further analysis revealed that ginsenoside Rh2 could inhibit cardiomyocyte pyroptosis by regulating the PI3K/AKT signaling pathway. Conclusions: Collectively, the findings of the present study demonstrated that ginsenoside Rh2 regulates pyroptosis in cardiomyocytes to alleviate AMI in vivo and in vitro, thereby affording a novel therapeutic approach to treat AMI. [ABSTRACT FROM AUTHOR]

Published

2023

15. 基于人参皂苷 Rh2 反向筛选抗非小细胞肺癌靶点.

Author

黄雨杭, 陈靖峰, 唐 乾, 曹洪玉, and 郑学仿

Abstract

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Published

2023

16. Heterologous expression of Bacillus subtilis SL-44 glycosyltransferase catalyzed synthesis of ginsenoside Rh2

Author

Zhang Yufei, Liu Xiaochen, Li Zhiyan, Yue Junsong, and Pan Hong

Subjects

bacillus subtilis, glycosyltransferase, kinetic equation, ginsenoside rh2, 68t05, Mathematics, QA1-939

Abstract

In this paper, the synthesis of ginsenoside Rh2 was catalyzed by using heterologous expression of Bacillus subtilis SL-44 glycosyltransferase. The synthesis parameters of ginsenoside Rh2 were optimized by the selection of strains and chemical supplies, the establishment of kinetic equations for the respiration rate of UGT enzyme, the effect of storage temperature on the model, and the glycosylation reaction of ginsenoside PPD with UGT. The effect of Rh2 saturation on the thermal denaturation temperature of the protein was analyzed along with the kinetic properties of the enzyme GE02773 (GE03484) while varying the saturation of Rh2. The results showed that the conversion of ginsenoside Rh2 reached 84% at a temperature of 35℃, pH 8, 5% DMSO, 0.4 of M-UDPG, and 1M-PPD in reaction with GE02773. In this paper, we successfully achieved the efficient synthesis of ginsenoside Rh2, which provides new ways and ideas for the application and synthesis of ginsenoside Rh2, with important practical significance and scientific value.

Published

2024

17. Ginsenoside Rh2 augmented anti-PD-L1 immunotherapy by reinvigorating CD8+ T cells via increasing intratumoral CXCL10

Author

Mu-Yang Huang, Yu-Chi Chen, Wen-Yu Lyu, Xin-Yu He, Zi-Han Ye, Can-Yu Huang, Xin-Ling He, Xiuping Chen, Xiaobing Chen, Baoxian Zhang, Guoyin Kai, Xiaolei Zhang, Ting Li, Mingqing Huang, and Jin-Jian Lu

Subjects

PD-1/PD-L1, Ginsenoside Rh2, T cells, Tumor microenvironment, Combination treatment, Therapeutics. Pharmacology, RM1-950

Abstract

Profiting from the sustained clinical improvement and prolonged patient survival, immune checkpoint blockade of programmed cell death protein 1 (PD-1)/programmed death-ligand 1 (PD-L1) axis has emerged as a revolutionary cancer therapy approach. However, the anti-PD-1/PD-L1 antibodies only achieve a clinical response rate of approximately 20%. Herein, we identified a novel combination strategy that Chinese medicine ginseng-derived ginsenoside Rh2 (Rh2) markedly improved the anti-cancer efficacy of anti-PD-L1 antibody in mice bearing MC38 tumor. Rh2 combined with anti-PD-L1 antibody (combo treatment) further triggered the infiltration, proliferation and activation of CD8+ T cells in the tumor microenvironment (TME). Depletion of CD8+ T cells by mouse CD8 blocking antibody abolished the anti-cancer effect of combo treatment totally. Mechanistically, combo treatment further increased the expression of CXCL10 through activating TBK1-IRF3 signaling pathway, explaining the increased infiltration of T cells. Employing anti- CXC chemokine receptor 3 (CXCR3) blocking antibody prevented the T cells infiltration and abolished the anti-cancer effect of combo treatment. Meanwhile, combo treatment increased the percentage of M1-like macrophages and raised the ratio of M1/M2 macrophages in TME. By comparing the anti-cancer effect of combo treatment among MC38, CT26 and 4T1 tumors, resident T cells were considered as a prerequisite for the effectiveness of combo treatment. These findings demonstrated that Rh2 potentiated the anti-cancer effect of PD-L1 blockade via promoting the T cells infiltration and activation, which shed a new light on the combination strategy to enhance anti-PD-L1 immunotherapy by using natural product Rh2.

Published

2023

18. Evaluation of the Anti-Inflammatory Pain Effect of Ginsenoside-Conjugated O-Carboxymethyl Chitosan Particles.

Author

Lu, Huan-Jun, Cen, Jian-Ke, Ren, Yu, and Li, Mei-Xian

Subjects

*NUCLEAR magnetic resonance spectroscopy, *PROTON magnetic resonance, *CHITOSAN, *CHEMICAL shift (Nuclear magnetic resonance), *NUCLEAR magnetic resonance, *GINSENOSIDES, *DRUG delivery systems

Abstract

Nanoparticle delivery of functional molecules or vaccines is an effective method for the treatment of many diseases. This study aims to design ginsenoside Rh2-conjugated O-carboxymethyl chitosan (O-CMC/Rh2) as a drug delivery system and explore its anti-nociceptive effects. O-CMC/Rh2 was synthesized with an esterification reaction, and its chemical composition and morphology were evaluated using proton nuclear magnetic resonance (1H NMR), the attenuated total reflectance-Fourier transform infrared (ATR-FTIR) spectroscopy, and scanning electron microscopy (SEM). In addition, the in vitro cumulative release of Rh2 from the O-CMC/Rh2 was also evaluated under different pH conditions. The results showed that the ginsenoside Rh2 was successfully conjugated to the O-CMC matrix and exhibited a highly porous structure after conjugation, facilitating the release of Rh2 from O-CMC. Complete Freund's adjuvant (CFA) and burn injury-induced pain models were used to evaluate the anti-nociceptive effects of O-CMC/Rh2 on inflammatory pain. O-CMC/Rh2 reduced CFA-induced pain hypersensitivity in a dose-dependent manner and had a longer analgesic effect than Rh2. In addition, O-CMC/Rh2 also relieved the chronic pain induced by bury injury. These results indicated that O-CMC/Rh2 could be useful in reducing inflammatory pain, thus possessing a potential medicinal application in pain therapy. [ABSTRACT FROM AUTHOR]

Published

2023

19. Synergistic Effect of Ginsenoside Rh2 Combines with Ionizing Radiation on CT26/ luc Colon Carcinoma Cells and Tumor-Bearing Animal Model.

Author

Lee, Shan-Chih, Shen, Chao-Yu, Wang, Wei-Hsun, Lee, Yen-Po, Liang, Keng-Wei, Chou, Ying-Hsiang, Tyan, Yeu-Sheng, and Hwang, Jeng-Jong

Subjects

*IONIZING radiation, *GINSENOSIDES, *PROGRAMMED cell death 1 receptors, *ANIMAL models in research, *COLON (Anatomy), *DOSE-response relationship (Radiation)

Abstract

Background: The local tumor control rate of colon cancer by radiotherapy is unsatisfactory due to recurrence and radioresistance. Ginsenoside Rh2 (Rh2), a panoxadiol saponin, possesses various antitumor effects. Methods: CT26/luc murine colon carcinoma cells and a CT26/luc tumor-bearing animal model were used to investigate the therapeutic efficacy of Rh2 combined with ionizing radiation and the underlying mechanisms. Results: Rh2 caused cell cycle arrest at the G1 phase in CT26/luc cells; however, when combined with ionizing radiation, the cells were arrested at the G2/M phase. Rh2 was found to suppress the activity of NF-κB induced by radiation by inhibiting the MAPK pathway, consequently affecting the expression of effector proteins. In an in vivo study, the combination treatment significantly increased tumor growth delay time and overall survival. Furthermore, the combination treatment significantly reduced NF-κB and NF-κB-related effector proteins, along with PD-1 receptor expression. Additionally, Rh2 administration led to increased levels of interleukin-12, -18, and interferon-γ in the mice's sera. Importantly, biochemical analysis revealed no toxicities associated with Rh2 alone or combined with radiation. Conclusions: The combination of Rh2 with radiation may have potential as an alternative to improve the therapeutic efficacy of colorectal cancer. [ABSTRACT FROM AUTHOR]

Published

2023

20. 人参皂苷Rh2 对糖尿病肾病变大鼠肾损伤的保护作用及其机制.

Author

曲萌, 姜雨竹, 黄睿, 马振卓, 夏吉辰, 张媛, and 董志恒

Subjects

*RENAL fibrosis, *INTRAPERITONEAL injections, *HIGH-fat diet, *GINSENOSIDES, *KIDNEY physiology

Abstract

Objective To discuss the protective effect of ginsenoside Rh2 on kidney injury in the rats with diabetic kidney lesions (DKL), and to clarify its mechanism. Methods The DKL rat model was established by using the high-fat and high-energy diet combined with intraperitoneal injection of streptozotocin (STZ) .Thirty SD model rats were randomly divided into model group, low dose (10 mg·kg-1) of Rh2 group and high dose (20 mg·kg-1) of Rh2 group, and there were 10 rats in each group; other ten SD rats were regared as normal control group. The body weights and kidney weights of the rats in various groups were detected，and the kidney index was caculated; after intervented for 8 weeks, automatic analyzer was used to detect the levels of serum creatinine (Scr), urea nitrogen (BUN) and 24 h urinary protein (UP) in serum of the rats in various groups; enzyme linked immunosorbent assay (ELISA) method was used to detect the levels of collagen type Ⅳ (Col Ⅳ) in kidney tissue of the rats in various groups; Western blotting method was used to detect the expression levels of transforming growth factor-β1 (TGF-β1), Smad3 and Smad7 proteins in kidney tissue of the rats in various groups. Results Compared with normal control group, the body weight of the rats in model group was decreased (P<0.01), the kidney weight and kidney index were significantly increased (P<0.01), the levels of Scr, BUN and 24 h UP in serum were increased (P<0.01), the level of Col Ⅳ in kidney tissue was increased (P<0.01), the expression levels of TGF-β1 and Smad3 proteins in kidney tissue were increased (P<0.01), and the expression level of Smad7 protein in renal tissue was decreased (P<0.01) . Compared with model group，the body weight of the rats in low and high doses of Rh2 groups were inecreased (P<0.05 or P<0.01), the kidney weight and kidney index were decreased (P<0.05 or P<0.01), the levels of Scr, BUN and 24 h UP in serum were significantly decreased (P<0.05 or P<0.01), the level of Col Ⅳ in kidney tissue was decreased (P<0.01), the expression levels of TGF-β1 and Smad3 proteins in kidney tissue were decreased (P<0.01), and the expression level of Smad7 protein in kidney tissue was increased (P<0.01) . Conclusion Ginsenoside Rh2 can inhibit the kidney fibrosis and improves the kidney function in the DKL rats, and has a protective effect on the kidney of DKL rats; its mechanism may be related to regulating the expression of TGF-β1/Smads signaling pathway. [ABSTRACT FROM AUTHOR]

Published

2023

21. Ginsenoside Rh2 suppresses colon cancer growth by targeting the miR-150-3p/SRCIN1/Wnt axis

Author

Li Shipeng, Han Wenfeng, He Qichen, Wang Yang, Jin Gang, and Zhang Youcheng

Subjects

ginsenoside Rh2, colon cancer, miR-150-3p, SRCIN1, Wnt pathway, Biochemistry, QD415-436, Genetics, QH426-470

Abstract

Ginsenoside Rh2, which is extracted from ginseng, exerts antitumor activity. Recent studies suggest that Rh2 may suppress the growth of colon cancer (CC) in vitro. However, the underlying mechanism remains unclear. In this study, we identified the relative levels of miR-150-3p in CC tissues and cells by a comprehensive strategy of data mining, computational biology, and real-time reverse transcription PCR (qRT-PCR) experiments. The regulatory effects of miR-150-3p/SRCIN1 on the proliferative and invasive abilities of CC cells are evaluated by CCK-8, EdU, wound healing, and transwell assays. Cell cycle- and apoptosis-related protein levels are assessed by western blot analysis. An in vivo tumor formation assay was conducted to explore the effects of miR-150-3p on tumor growth. Furthermore, bioinformatics and dual luciferase reporter assays are applied to determine the functional binding of miRNA to mRNA of the target gene. Finally, the relationship between Rh2 and miR-150-3p was further verified in SW620 and HCT-116 cells. miR-150-3p is downregulated in CC tissues and cell lines. Functional assays indicate that the upregulation of miR-150-3p inhibits tumor growth both in vivo and in vitro. In addition, SRCIN1 is upregulated in CC and predicts a poor prognosis, and it is the direct target for miR-150-3p. Moreover, the miR-150-3p mimic decreases Topflash/Fopflash-dependent luciferase activity, resulting in the inhibition of Wnt pathway activity. Rh2 can suppress the growth of CC by increasing miR-150-3p expression. Rh2 alleviates the accelerating effect on Wnt pathway activity, cell proliferation/migration, and colony formation caused by miR-150-3p inhibition. Rh2 inhibits the miR-150-3p/SRCIN1/Wnt axis to suppress colon cancer growth.

Published

2023

22. The ways for ginsenoside Rh2 to fight against cancer: the molecular evidences in vitro and in vivo.

Author

Qi-rui Hu, Yao Pan, Han-cheng Wu, Zhen-zhen Dai, Qing-xin Huang, Ting Luo, Jing Li, Ze-yuan Deng, and Fang Chen

Subjects

ginsenoside Rh2, anticancer, apoptosis, anti-proliferation, Botany, QK1-989

Abstract

Cancer is a global public health issue that becomes the second primary cause of death globally. Considering the side effects of radio- or chemo-therapy, natural phytochemicals are promising alternatives for therapeutic interventions to alleviate the side effects and complications. Ginsenoside Rh2 (GRh2) is the main phytochemical extracted from Panax ginseng C.A. Meyer with anticancer activity. GRh2 could induce apoptosis and autophagy of cancer cells and inhibit proliferation, metastasis, invasion, and angiogenesis in vitro and in vivo. In addition, GRh2 could be used as an adjuvant to chemotherapeutics to enhance the anticancer effect and reverse the adverse effects. Here we summarized the understanding of the molecular mechanisms underlying the anticancer effects of GRh2 and proposed future directions to promote the development and application of GRh2.

Published

2023

23. Multiple ingredients of a Chinese medicine formula Sheng-Mai-San coordinately attenuate doxorubicin-induced cardiotoxicity

Author

Meng Wang, Dongfang Xie, Meng Zhang, and Xiu-Jie Wang

Subjects

Cardiotoxicity, Doxorubicin, Ginsenoside Rh2, Ophiopogonin D, Schisandrin B, Sheng-Mai-San, Other systems of medicine, RZ201-999, Therapeutics. Pharmacology, RM1-950

Abstract

Background: Doxorubicin (DOX) is one of the most widely used antitumor drugs. However, continuous DOX treatment would cause crucial cardiotoxicity side effect, accompanied with the accumulation of reactive oxygen species (ROS), impaired mitochondrial functions and increased cardiomyocyte death. Sheng-Mai-San (SMS), a traditional Chinese medicine widely used for cardiovascular diseases, has been clinically used to counteract cardiotoxicity of DOX, yet the underlying mechanism is largely unknown. Methods: We utilized JC-1 assay to examine the effects of SMS and its components under DOX treatment in rat cardiomyocytes (H9c2 cells), and further investigated the functional mechanisms of active components in SMS formula via transcriptome sequencing, bioinformatics analysis and molecular experiments. Results: We identified three functional components of SMS in protecting cardiomyocytes from DOX-induced damages and revealed the coordinated regulatory mechanisms of these components, namely ginsenoside Rh2 (Rh2), Ophiopogonin D (OpD) and Schisandrin B (SchB). We found that Rh2 mainly acts to restore mitochondrial functions and to decrease ROS generation by enhancing fatty acid metabolism and antioxidant activity, OpD has assistive roles in mitochondrial function repair, and SchB mainly functions by inhibiting cell death, as well as activating cytoskeleton and ECM organization. Conclusion: This study provides supporting evidence for the clinical application of SMS to reduce the cardiotoxicity effects of DOX treatment, and also sheds light for the mechanistic studies of traditional Chinese medicine.

Published

2023

24. 人参皂苷 Rh2 对大鼠 C6 胶质瘤细胞 Siah-1、Synaptophysin、MMP9 及 VEGF 表达的影响.

Author

吴国玉, 杨 俊, 熊绍权, 祝 捷, and 李建梅

Subjects

*VASCULAR endothelial growth factors, *GINSENOSIDES, *GENE expression, *MOLECULAR cloning, *SYNAPTOPHYSIN

Abstract

Objective: To investigate the impacts of ginsenoside Rh2 on the Siah-1, synaptophysin, matrix metalloproteinase-9 (MMP-9) and vascular endothelial growth factor (VEGF) expression in rat C6 glioma cells. Methods: Rat C6 glioma cells were grouped into control group, low-dose ginsenoside Rh2 group (16 μg/mL), medium dose ginsenoside Rh2 group (32 μg/mL), and high-dose ginsenoside Rh2 group (48 μg/mL), cell proliferation was detected by CCK-8 method and plate cloning test. Cell apoptosis was detected by flow cytometry. Cell invasion was detected by Transwell. The VEGF, Siah-1, Synaptophysin and MMP-9 mRNA expression in C6 glioma cells was detected by real-time fluorescence quantitation-polymerase chain reaction (qRT-PCR); and Western blot was used to detect the protein VEGF, Siah-1, Synaptophysin and MMP-9 expression in C6 glioma cells. Results: Compared with the control group, the OD450 value (24 h, 48 h), clone formation rate, cell invasion number, VEGF, Synaptophysin, MMP-9 mRNA and protein expression in C6 glioma cells in the low-dose ginsenoside Rh2 group, the medium dose ginsenoside Rh2 group, and the high-dose ginsenoside Rh2 group were decreased, the cell apoptosis rate and the Siah-1 mRNA and protein expression were increased, which were dose dependent (P<0.05). Conclusions: Ginsenoside Rh2 may inhibit the proliferation and invasion of rat C6 glioma cells and promote cell apoptosis by up-regulating Siah-1 and down-regulating the VEGF, Synaptophysin and MMP-9 expression. [ABSTRACT FROM AUTHOR]

Published

2023

25. In vivo study of anticancer activity of ginsenoside Rh2-containing arginine-reduced graphene in a mouse model of breast cancer

Author

Shervindokht Farhangfar, Farzaneh Fesahat, Hadi Zare-Zardini, Mahdi Dehghan-Manshadi, Fateme Zare, Seyed Mohsen Mirsmaeili, Maryam Vajihinejad, and Hossein Soltaninejad

Subjects

arginine, breast cancer, genes, ginsenoside rh2, graphene, tumor, Medicine

Abstract

Objective(s): This study aims to evaluate the in vivo anticancer activity of arginine-reduced graphene (Gr-Arg) and ginsenoside Rh2-containing arginine-reduced graphene (Gr-Arg-Rh2). Materials and Methods: Thirty-two mice with breast cancer were divided into four groups and treated every three days for 32 days: Group 1, PBS, Group 2, Rh2, Group 3, Gr-Arg, and Group 4, Gr-Arg-Rh2. The tumor size and weight, gene expression (IL10, INF-γ, TGFβ, and FOXP3), and pathological properties of the tumor and normal tissues were assessed. Results: Results showed a significant decrease in TGFβ expression for all drug treatment groups compared with the controls (P=0.04). There was no significant difference among the groups regarding IL10 and FOXP3 gene expression profiles (P>0.05). Gr-Arg-Rh2 significantly inhibited tumor growth (size and weight) compared with Rh2 and control groups. The highest survival rate and the highest percentage of tumor necrosis (87.5%) belonged to the Gr-Arg-Rh2 group. Lungs showed metastasis in the control group. No metastasis was observed in the Gr-Arg-Rh2 group. Gr-Arg-Rh2 showed partial degeneration of hepatocytes and acute cell infiltration in the portal spaces and around the central vein. The Gr-Arg group experienced a moderate infiltration of acute cells into the port spaces and around the central vein. The Rh2 group also showed a mild infiltration of acute and chronic cells in portal spaces. Conclusion: Based on the results, Gr-Arg-Rh2 can reduce tumor size, weight, and growth, TGF-β gene expression, and increase tumor necrosis and survival time in mice with cancer.

Published

2022

26. Tumor cell membrane-camouflaged responsive nanoparticles enable MRI-guided immuno-chemodynamic therapy of orthotopic osteosarcoma

Author

Liwen Fu, Weiying Zhang, Xiaojun Zhou, Jingzhong Fu, and Chuanglong He

Subjects

Ginsenoside Rh2, Hollow manganese dioxide, Magnetic resonance imaging, Chemodynamic therapy, Immunotherapy, Materials of engineering and construction. Mechanics of materials, TA401-492, Biology (General), QH301-705.5

Abstract

Osteosarcoma is a refractory bone disease in young people that needs the updating and development of effective treatment. Although nanotechnology is widely applied in cancer therapy, poor targeting and inadequate efficiency hinder its development. In this study, we prepared alendronate (ALD)/K7M2 cell membranes-coated hollow manganese dioxide (HMnO2) nanoparticles as a nanocarrier to load Ginsenoside Rh2 (Rh2) for Magnetic Resonance imaging (MRI)-guided immuno-chemodynamic combination osteosarcoma therapy. Subsequently, the ALD and K7M2 cell membranes were successively modified on the surface of HMnO2 and loaded with Rh2. The tumor microenvironment (TME)-activated Rh2@HMnO2-AM nanoparticles have good bone tumor-targeting and tumor-homing capabilities, excellent GSH-sensitive drug release profile and MRI capability, and attractive immuno-chemodynamic combined therapeutic efficiency. The Rh2@HMnO2-AM nanoparticles can effectively trigger immunogenic cell death (ICD), activate CD4+/CD8+ T cells in vivo, and upregulate BAX, BCL-2 and Caspase-3 in cellular level. Further results revealed that Rh2@HMnO2-AM enhanced the secretion of IL-6, IFN-γ and TNF-α in serum and inhibited the generation of FOXP3+ T cells (Tregs) in tumors. Moreover, the Rh2@HMnO2-AM treatment significant restricted tumor growth in-situ tumor-bearing mice. Therefore, Rh2@HMnO2-AM may serve as an effective and bio-friendly nanoparticle platform combined with immunotherapy and chemodynamic therapy to provide a novel approach to osteosarcoma therapy.

Published

2022

27. Facile approach for surfactant-free synthesis of Au@ginsenoside Rh2 nanoparticles and researches on anticancer activity

Author

Hua Yao, Xupeng Mu, Zhenhong Wei, Xiuying Li, Liya Wu, Yongri Jin, Xuwen Li, Jing Li, and Jinlan Jiang

Subjects

Ginsenoside Rh2, Au nanoparticles, Drug-modified nanocomposite, Facile synthesis, Anticancer activity, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Inorganic nanocomposites especially Au nanostructures have exhibited outstanding physicochemical properties in biomedical fields. For further clinical applications on theranostics, especially drug delivery, numerous explorations of green and facile synthesis methods combining with pharmacoactive natural components have been investigated to construct safe and multifunctional bioactive Au nanoparticles (NPs). Ginsenoside Rh2 is protopanaxadiol type compound isolated from plants of genus Panax, with excellent anticancer effect and antioxidant activity. In this research, we prepared the novel Au nanoparticles using ginsenoside Rh2 as both reducing and stabilizing agents. Results The synthesized Au@ginsenoside Rh2 NPs were proved to exhibit desirable inhibitory effect on different cancer cell lines, which benefited from the inherent anticancer effect of the ginsenoside Rh2. Investigations in vitro indicated that Au@ginsenoside Rh2 NPs inhibited cell proliferation, cell migration and invasion, induced cell cycle arrest, enhanced the reactive oxygen species (ROS) generation, and regulated the protein expressions of caspase-3, 8, 9 to trigger cell apoptosis as well. Conclusions Because of the absence of toxic chemical surfactants, the eco-friendly synthesis method of Au NPs modified by natural phytochemicals avoided tedious separation and modification processes. On the other hand, Au@ginsenoside Rh2 NPs also improved water solubility and bioavailability of the hydrophobic drug ginsenoside Rh2. It broadened minds for preparation and application of traditional Chinese medicines (TCMs) modified metal nanoparticles and deserved further study.

Published

2022

28. The ginsenoside Rh2 protects porcine oocytes against aging and oxidative stress by regulating SIRT1 expression and mitochondrial activity.

Author

Liu, Hongye, An, Zhi-Yong, Li, Zhou-Yan, Yang, Liu-Hui, Zhang, Xiu-Li, Lv, Yan-Tong, Yin, Xi-Jun, Quan, Lin-Hu, and Kang, Jin-Dan

Subjects

*GINSENOSIDES, *GENE expression, *OXIDATIVE stress, *SIRTUINS, *OVUM

Abstract

Post-ovulatory aging, a major problem faced by oocytes cultured in vitro, causes oxidative damage and mitochondrial dysfunction in oocytes. The ginsenoside Rh2 is one of the main monomeric components of ginseng, but its effects on porcine oocytes are unknown. In the present study, in vitro aging (IVA) and accelerated induction of aging using H 2 O 2 resulted in DNA damage and an increased incidence of abnormal spindle formation in porcine oocytes. Rh2 supplementation increased the antioxidant capacity, reduced the occurrence of early apoptosis, and improved the development of in vitro fertilized blastocysts. It also rescued the abnormal aggregation of mitochondria and the decrease of the mitochondrial membrane potential under mitochondrial dysfunction. Meanwhile, Rh2 enhanced mRNA expression of the anti-aging and mitochondrial biogenesis-related genes silent information regulator of transcription 1 (SIRT1) and peroxisome proliferator-activated receptor coactivator 1-α (PGC-1α), and the antioxidant gene superoxide dismutase 1 (SOD1). The protection of porcine oocytes against aging and oxidative stress by Rh2 was confirmed using the SIRT1-specific inhibitor EX-527. Our results reveal that Rh2 upregulates SIRT1/PGC-1α to enhance mitochondrial function in porcine oocytes and improve their quality. Our study indicates that Rh2 can be used to prevent mitochondrial dysfunction in oocytes. • Rh2 increases the antioxidant capacity of oocytes and reduces the accumulation of ROS caused by aging and oxidative stress. • Rh2 reduced early apoptosis, spindle abnormalities, and abnormal mitochondrial distribution caused by oxidative damage. • Rh2 regulates the SIRT1-PGC-1α pathway to improve mitochondrial activity and enhance oocyte quality. [ABSTRACT FROM AUTHOR]

Published

2023

29. 人参皂苷 RH2 通过 BCL2L1/PI3K/AKT 信号通路逆转环磷酰胺诱导的卵巢颗粒细胞损伤.

Author

王文芳 and 曲婷

Abstract

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Published

2023

30. Ginsenoside Rh2 inhibits breast cancer cell growth viaERβ-TNFα pathway

Author

Peng Kunjian, Luo Tiao, Li Jijia, Huang Jingjia, Dong Zizeng, Liu Jia, Pi Chaoqiong, Zou Zizeng, Gu Qin, Liu Ousheng, Zhang Jian-Ting, and Luo Zhi-Yong

Subjects

ginsenoside Rh2, estrogen receptor, TNFα, breast cancer, apoptosis, Biochemistry, QD415-436, Genetics, QH426-470

Abstract

Ginsenoside Rh2 is one of rare panaxidiols extracted from Panax ginseng and a potential estrogen receptor ligand that exhibits moderate estrogenic activity. However, the effect of Rh2 on growth inhibition and its underlying molecular mechanism in human breast cells are not fully understood. In this study, we tested cell viability by MTT and colony formation assays. Cell growth and cell cycle were determined to investigate the effect of ginsenoside Rh2 by flow cytometry. The expressions of estrogen receptors (ERs), TNFα, and apoptosis-related proteins were detected by qPCR and western blot analysis. The mechanisms of ERα and ERβ action were determined using transfection and inhibitors. Antitumor effect of ginsenoside Rh2 against MCF-7 cells was investigated in xenograft mice. Our results showed that ginsenoside Rh2 induced apoptosis and G1/S phase arrest in MCF-7 cells. Treatment of cells with ginsenoside Rh2 down-regulated protein levels of ERα, and up-regulated mRNA and protein levels of ERβ and TNFα. We also found that ginsenoside Rh2-induced TNFα over-expression is through up-regulation of ERβ initiated by ginsenoside Rh2. Furthermore, ginsenoside Rh2 induced MCF-7 cell apoptosis via estrogen receptor β-TNFα pathway in vivo. These results demonstrate that ginsenoside Rh2 promotes TNFα-induced apoptosis and G1/S phase arrest via regulation of ERβ.

Published

2022

31. In vivo study of anticancer activity of ginsenoside Rh2-containing arginine-reduced graphene in a mouse model of breast cancer.

Author

Farhangfar, Shervin Dokht, Fesahat, Farzaneh, Zare-Zardini, Hadi, Dehghan-Manshadi, Mahdi, Zare, Fateme, Miresmaeili, Seyed Mohsen, Vajihinejad, Maryam, and Soltaninejad, Hossein

Subjects

*GINSENOSIDES, *ANTINEOPLASTIC agents, *LABORATORY mice, *GENE expression profiling, *BREAST cancer

Abstract

Objective(s): This study aims to evaluate the in vivo anticancer activity of arginine-reduced graphene (Gr-Arg) and ginsenoside Rh2-containing arginine-reduced graphene (Gr-Arg-Rh2). Materials and Methods: Thirty-two mice with breast cancer were divided into four groups and treated every three days for 32 days: Group 1, PBS, Group 2, Rh2, Group 3, Gr-Arg, and Group 4, Gr-Arg-Rh2. The tumor size and weight, gene expression (IL10, INF-γ, TGFß, and FOXP3), and pathological properties of the tumor and normal tissues were assessed. Results: Results showed a significant decrease in TGFß expression for all drug treatment groups compared with the controls (P=0.04). There was no significant difference among the groups regarding IL10 and FOXP3 gene expression profiles (P>0.05). Gr-Arg-Rh2 significantly inhibited tumor growth (size and weight) compared with Rh2 and control groups. The highest survival rate and the highest percentage of tumor necrosis (87.5%) belonged to the Gr-Arg-Rh2 group. Lungs showed metastasis in the control group. No metastasis was observed in the Gr-Arg-Rh2 group. Gr-Arg-Rh2 showed partial degeneration of hepatocytes and acute cell infiltration in the portal spaces and around the central vein. The Gr-Arg group experienced a moderate infiltration of acute cells into the port spaces and around the central vein. The Rh2 group also showed a mild infiltration of acute and chronic cells in portal spaces. Conclusion: Based on the results, Gr-Arg-Rh2 can reduce tumor size, weight, and growth, TGF-ß gene expression, and increase tumor necrosis and survival time in mice with cancer. [ABSTRACT FROM AUTHOR]

Published

2022

32. Potential of ginsenoside Rh2and its derivatives as anti-cancer agents.

Author

LI, Keke, LI, Zhongyu, Men, Lei, LI, Wei, and GONG, Xiaojie

Abstract

As a steroid skeleton-based saponin, ginsenoside Rh 2 (G-Rh 2) is one of the major bioactive ginsenosides from the plants of genus Panax L. Many studies have reported the notable pharmacological activities of G-Rh 2 such as anticancer, antiinflammatory, antiviral, antiallergic, antidiabetic, and anti-Alzheimer's activities. Numerous preclinical studies have demonstrated the great potential of G-Rh 2 in the treatment of a wide range of carcinomatous diseases in vitro and in vivo. G-Rh 2 is able to inhibit proliferation, induce apoptosis and cell cycle arrest, retard metastasis, promote differentiation, enhance chemotherapy and reverse multi-drug resistance against multiple tumor cells. The present review mainly summarizes the anticancer effects and related mechanisms of G-Rh 2 in various models as well as the recent advances in G-Rh 2 delivery systems and structural modification to ameliorate its anticancer activity and pharmacokinetics characteristics. [ABSTRACT FROM AUTHOR]

Published

2022

33. Ginsenoside Rh2 Induces HeLa Apoptosis through Upregulating Endoplasmic Reticulum Stress-Related and Downstream Apoptotic Gene Expression.

Author

Liu, Ying, Wang, Xinran, Qiao, Juhui, Wang, Jiawen, Jiang, Leilei, Wang, Chenxi, Yu, Shiting, Zhang, Peiguang, Zhao, Daqing, Fan, Meiling, and Liu, Meichen

Subjects

*ENDOPLASMIC reticulum, *GINSENOSIDES, *GENE expression, *APOPTOSIS, *GINSENG, *CERVICAL cancer, *HELA cells

Abstract

Cervical cancer is a common gynecological malignancy afflicting women all over the world. Ginsenoside Rh2 (GRh2), especially 20(S)-GRh2, is a biologically active component in the natural plant ginseng, which can exhibit anticancer effects. Here, we aimed to investigate the effect of 20(S)-GRh2 on cervical cancer and elucidate the underlying mechanism through RNA-seq. In this study, the CCK-8 assay showed that 20(S)-GRh2 inhibited HeLa cell viability in a time- and dose-dependent manner. Caspase 3 activity and Annexin V staining results showed that 20(S)-GRh2 induced apoptosis of HeLa cells. Gene function enrichment analysis revealed that the biological process gene ontology (GO) terms were associated with the apoptotic signaling pathway. Biological process GO terms' similarity network indicated that apoptosis might be from endoplasmic reticulum stress (ERs). Kyoto Encyclopedia of Genes and Genomes enrichment analysis revealed that 20(S)-GRh2 primarily modulates apoptosis pathway genes. Combined protein–protein interaction network, hub gene screening, and qPCR validation data showed that ERs-related genes (ATF4 and DDIT3) and the downstream apoptotic genes (JUN, FOS, BBC3, and PMAIP1) were potential novel targets of 20(S)-GRh2-inducing cervical cancer cell apoptosis. Differential transcript usage analysis indicated that DDIT3 is also a differential transcript and its usage of the isoform (ENST00000552740.5) was reduced by 20(S)-GRh2. Molecular docking suggested that 20(S)-GRh2 binds to the targets (ATF4, DDIT3, JUN, FOS, BBC3, and PMAIP1) with high affinity. In conclusion, our findings indicated that 20(S)-GRh2 might promote ERs-related apoptosis of cervical cancer cells by regulating the DDIT3-based targets' signal pathway. The role of 20(S)-GRh2 at the transcriptome level provides novel targets and evidence for the treatment of cervical cancer. [ABSTRACT FROM AUTHOR]

Published

2022

34. c-MYC-mediated TRIB3/P62+ aggresomes accumulation triggers paraptosis upon the combination of everolimus and ginsenoside Rh2

Author

Min-Xia Su, Yu-Lian Xu, Xiao-Ming Jiang, Mu-Yang Huang, Le-Le Zhang, Luo-Wei Yuan, Xiao-Huang Xu, Qi Zhu, Jian-Li Gao, Jia-Hong Lu, Xiuping Chen, Ming-Qing Huang, Yitao Wang, and Jin-Jian Lu

Subjects

Everolimus, Ginsenoside Rh2, Paraptosis, Aggresomes, P62, TRIB3, Therapeutics. Pharmacology, RM1-950

Abstract

The mammalian target of rapamycin (mTOR) pathway is abnormally activated in lung cancer. However, the anti-lung cancer effect of mTOR inhibitors as monotherapy is modest. Here, we identified that ginsenoside Rh2, an active component of Panax ginseng C. A. Mey., enhanced the anti-cancer effect of the mTOR inhibitor everolimus both in vitro and in vivo. Moreover, ginsenoside Rh2 alleviated the hepatic fat accumulation caused by everolimus in xenograft nude mice models. The combination of everolimus and ginsenoside Rh2 (labeled Eve-Rh2) induced caspase-independent cell death and cytoplasmic vacuolation in lung cancer cells, indicating that Eve-Rh2 prevented tumor progression by triggering paraptosis. Eve-Rh2 up-regulated the expression of c-MYC in cancer cells as well as tumor tissues. The increased c-MYC mediated the accumulation of tribbles homolog 3 (TRIB3)/P62+ aggresomes and consequently triggered paraptosis, bypassing the classical c-MYC/MAX pathway. Our study offers a potential effective and safe strategy for the treatment of lung cancer. Moreover, we have identified a new mechanism of TRIB3/P62+ aggresomes-triggered paraptosis and revealed a unique function of c-MYC.

Published

2022

35. Efficient production of ginsenoside Rh2 from xylose by remodeling metabolism in Saccharomyces cerevisiae.

Author

Zhang, Wanze, Zhang, Jiale, Zhao, Xiaomeng, Zhang, Zhanwei, He, Shifan, Bian, Xueke, Wang, Haibin, Zhang, Chuanbo, and Lu, Wenyu

Subjects

*GINSENOSIDES, *SACCHAROMYCES cerevisiae, *XYLOSE, *GINSENG, *CANDIDA tropicalis, *LIGNOCELLULOSE, *METABOLISM

Abstract

[Display omitted] • The optimization of the XR-XDH pathway almost eliminates the generation of xylitol. • The highest Rh2 production of 209.5 mg/L was obtained in shake-flask fermentation. • Transcriptomic analysis reveals the reason for Rh2 efficient production. • The titer of Rh2 achieved 1.47 g/L in a 5 L bioreactor fed-batch fermentation. Ginsenoside Rh2, a promising candidate for cancer prevention and therapy, has applications in the fields of health products and pharmaceuticals. However, the current production of Rh2 through the extraction of Panax ginseng is not sustainable and cannot meet the increasing market demand. Here, we increased the Rh2 production in Saccharomyces cerevisiae by engineering the heterologous xylose metabolic pathway. The Candida tropicalis derived xylose reductase-xylitol dehydrogenase pathway was successfully constructed in in the previously engineered protopanaxadiol (PPD)-producing strain. A PPD high-yield strain with strong xylose utilization capacity was optimized to reduce the generation of byproduct xylitol with the expression of a soluble pyridine nucleotide transhydrogenase. The new yeast chassis produced 494.0 mg/L PPD in xylose medium, which could provide sufficient precursors for Rh2. The Rh2 production strain was then constructed by integrating the glycosyltransferases UGTPg45 overexpression module and further optimized through systematic enhancement of its mevalonic acid (MVA) pathway, resulting in a Rh2 titer of 209.5 mg/L in xylose medium. In addition, we confirmed that the engineered strain also exhibited good fermentation performance in the lignocellulose hydrolysate mimic glucose-xylose mixed medium, and we further elucidated the reasons of higher Rh2 production in xylose fermentation stage through transcriptomic and metabolic analysis. Taken all strategies together, the resulting strain produced 1.47 g/L Rh2 in a 5 L bioreactor with mixed sugar medium, making it possible for a green and sustainable biotechnology to produce ginsenoside Rh2 using xylose efficiently. This is the first report on the use of xylose for high-value chemical ginsenoside Rh2 production, which will pave the way for the future industrial production of ginsenoside Rh2 from a renewable carbon source such as lignocellulose. [ABSTRACT FROM AUTHOR]

Published

2024

36. Evaluation of the Anti-Inflammatory Pain Effect of Ginsenoside-Conjugated O-Carboxymethyl Chitosan Particles

Author

Huan-Jun Lu, Jian-Ke Cen, Yu Ren, and Mei-Xian Li

Subjects

O-carboxymethyl chitosan, ginsenoside Rh2, anti-nociception, inflammatory pain, Organic chemistry, QD241-441

Abstract

Nanoparticle delivery of functional molecules or vaccines is an effective method for the treatment of many diseases. This study aims to design ginsenoside Rh2-conjugated O-carboxymethyl chitosan (O-CMC/Rh2) as a drug delivery system and explore its anti-nociceptive effects. O-CMC/Rh2 was synthesized with an esterification reaction, and its chemical composition and morphology were evaluated using proton nuclear magnetic resonance (1H NMR), the attenuated total reflectance-Fourier transform infrared (ATR-FTIR) spectroscopy, and scanning electron microscopy (SEM). In addition, the in vitro cumulative release of Rh2 from the O-CMC/Rh2 was also evaluated under different pH conditions. The results showed that the ginsenoside Rh2 was successfully conjugated to the O-CMC matrix and exhibited a highly porous structure after conjugation, facilitating the release of Rh2 from O-CMC. Complete Freund’s adjuvant (CFA) and burn injury-induced pain models were used to evaluate the anti-nociceptive effects of O-CMC/Rh2 on inflammatory pain. O-CMC/Rh2 reduced CFA-induced pain hypersensitivity in a dose-dependent manner and had a longer analgesic effect than Rh2. In addition, O-CMC/Rh2 also relieved the chronic pain induced by bury injury. These results indicated that O-CMC/Rh2 could be useful in reducing inflammatory pain, thus possessing a potential medicinal application in pain therapy.

Published

2023

37. Synergistic Effect of Ginsenoside Rh2 Combines with Ionizing Radiation on CT26/luc Colon Carcinoma Cells and Tumor-Bearing Animal Model

Author

Shan-Chih Lee, Chao-Yu Shen, Wei-Hsun Wang, Yen-Po Lee, Keng-Wei Liang, Ying-Hsiang Chou, Yeu-Sheng Tyan, and Jeng-Jong Hwang

Subjects

colorectal cancer, ginsenoside Rh2, radiotherapy, immunomodulation, Medicine, Pharmacy and materia medica, RS1-441

Abstract

Background: The local tumor control rate of colon cancer by radiotherapy is unsatisfactory due to recurrence and radioresistance. Ginsenoside Rh2 (Rh2), a panoxadiol saponin, possesses various antitumor effects. Methods: CT26/luc murine colon carcinoma cells and a CT26/luc tumor-bearing animal model were used to investigate the therapeutic efficacy of Rh2 combined with ionizing radiation and the underlying mechanisms. Results: Rh2 caused cell cycle arrest at the G1 phase in CT26/luc cells; however, when combined with ionizing radiation, the cells were arrested at the G2/M phase. Rh2 was found to suppress the activity of NF-κB induced by radiation by inhibiting the MAPK pathway, consequently affecting the expression of effector proteins. In an in vivo study, the combination treatment significantly increased tumor growth delay time and overall survival. Furthermore, the combination treatment significantly reduced NF-κB and NF-κB-related effector proteins, along with PD-1 receptor expression. Additionally, Rh2 administration led to increased levels of interleukin-12, -18, and interferon-γ in the mice’s sera. Importantly, biochemical analysis revealed no toxicities associated with Rh2 alone or combined with radiation. Conclusions: The combination of Rh2 with radiation may have potential as an alternative to improve the therapeutic efficacy of colorectal cancer.

Published

2023

38. Ginsenoside Rh2 reduces depression in offspring of mice with maternal toxoplasma infection during pregnancy by inhibiting microglial activation via the HMGB1/TLR4/NF-κB signaling pathway

Author

Xiang Xu, Yu-Nan Lu, Jia-Hui Cheng, Hui-Wen Lan, Jing-Mei Lu, Guang-Nan Jin, Guang-Hua Xu, Cheng-Hua Jin, Juan Ma, Hu-Nan Piao, Xuejun Jin, and Lian-Xun Piao

Subjects

Ginsenoside Rh2, Microglia, Offspring, Psychiatric disorders, Toxoplasma gondii, Botany, QK1-989

Abstract

Background: Maternal Toxoplasma gondii (T. gondii) infection during pregnancy has been associated with various mental illnesses in the offspring. Ginsenoside Rh2 (GRh2) is a major bioactive compound obtained from ginseng that has an anti-T. gondii effect and attenuates microglial activation through toll-like receptor 4 (TLR4)/nuclear factor-kappa B (NF-κB) signaling pathway. GRh2 also alleviated tumor-associated or lipopolysaccharide-induced depression. However, the effects and potential mechanisms of GRh2 on depression-like behavior in mouse offspring caused by maternal T. gondii infection during pregnancy have not been investigated. Methods: We examined GRh2 effects on the depression-like behavior in mouse offspring, caused by maternal T. gondii infection during pregnancy, by measuring depression-like behaviors and assaying parameters at the neuronal and molecular level. Results: We showed that GRh2 significantly improved behavioral measures: sucrose consumption, forced swim time and tail suspended immobility time of their offspring. These corresponded with increased tissue concentrations of 5-hydroxytryptamine and dopamine, and attenuated indoleamine 2,3-dioxygenase or enhanced tyrosine hydroxylase expression in the prefrontal cortex. GRh2 ameliorated neuronal damage in the prefrontal cortex. Molecular docking results revealed that GRh2 binds strongly to both TLR4 and high mobility group box 1 (HMGB1). Conclusion: This study demonstrated that GRh2 ameliorated the depression-like behavior in mouse offspring of maternal T. gondii infection during pregnancy by attenuating the excessive activation of microglia and neuroinflammation through the HMGB1/TLR4/NF-κB signaling pathway. It suggests that GRh2 could be considered a potential therapy in preventing and treating psychiatric disorders in the offspring mice of mothers with prenatal exposure to T. gondii infection.

Published

2022

39. Ginsenoside Rh2 upregulates long noncoding RNA STXBP5-AS1 to sponge microRNA-4425 in suppressing breast cancer cell proliferation

Author

Jae Eun Park, Hyeon Woo Kim, Sung Hwan Yun, and Sun Jung Kim

Subjects

Breast cancer, ceRNA, Ginsenoside Rh2, Long noncoding RNA, microRNA, Botany, QK1-989

Abstract

Background: Ginsenoside Rh2, a major saponin derivative in ginseng extract, is recognized for its anticancer activities. Compared to coding genes, studies on long noncoding RNAs (lncRNAs) and microRNAs (miRNAs) that are regulated by Rh2 in cancer cells, especially on competitive endogenous RNA (ceRNA) are sparse. Methods: LncRNAs whose promoter DNA methylation level was significantly altered by Rh2 were screened from methylation array data. The effect of STXBP5-AS1, miR-4425, and RNF217 on the proliferation and apoptosis of MCF-7 breast cancer cells was monitored in the presence of Rh2 after deregulating the corresponding gene. The ceRNA relationship between STXBP5-AS1 and miR-4425 was examined by measuring the luciferase activity of a recombinant luciferase/STXBP5-AS1 plasmid construct in the presence of mimic miR-4425. Results: Inhibition of STXBP5-AS1 decreased apoptosis but stimulated growth of the MCF-7 cells, suggesting tumor-suppressive activity of the lncRNA. MiR-4425 was identified to have a binding site on STXBP5-AS1 and proven to be downregulated by STXBP5-AS1 as well as by Rh2. In contrast to STXBP5-AS1, miR-4425 showed pro-proliferation activity by inducing a decrease in apoptosis but increased growth of the MCF-7 cells. MiR-4425 decreased luciferase activity from the luciferase/STXBP5-AS1 construct by 26%. Screening the target genes of miR-4425 and Rh2 revealed that Rh2, STXBP5-AS1, and miR-4425 consistently regulated tumor suppressor RNF217 at both the RNA and protein level. Conclusion: LncRNA STXBP5-AS1 is upregulated by Rh2 via promoter hypomethylation and acts as a ceRNA, sponging the oncogenic miR-4425. Therefore, Rh2 controls the STXBP5-AS1/miR-4425/RNF217 axis to suppress breast cancer cell growth.

Published

2021

40. Ginsenoside Rh2 reduces m6A RNA methylation in cancer via the KIF26B-SRF positive feedback loop

Author

Chunmei Hu, Linhan Yang, Yi Wang, Shijie Zhou, Jing Luo, and Yi Gu

Subjects

ginsenoside Rh2, KIF26B, SRF, m6A RNA methylation, Cancer, Botany, QK1-989

Abstract

Background: The underlying mechanisms of the potential tumor-suppressive effects of ginsenoside Rh2 are complex. N6-methyladenosine (m6A) RNA methylation is usually dysregulated in cancer. This study explored the regulatory effect of ginsenoside Rh2 on m6A RNA methylation in cancer.Methods: m6A RNA quantification and gene-specific m6A RIP-qPCR assays were applied to assess total and gene-specific m6A RNA levels. Co-immunoprecipitation, fractionation western blotting, and immunofluorescence staining were performed to detect protein interactions and distribution. QRT-PCR, dual-luciferase, and ChIP-qPCR assays were conducted to check the transcriptional regulation. Results: Ginsenoside Rh2 reduces m6A RNA methylation and KIF26B expression in a dose-dependent manner in some cancers. KIF26B interacts with ZC3H13 and CBLL1 in the cytoplasm of cancer cells and enhances their nuclear distribution. KIF26B inhibition reduces m6A RNA methylation level in cancer cells. SRF bound to the KIF26B promoter and activated its transcription. SRF mRNA m6A abundance significantly decreased upon KIF26B silencing. SRF knockdown suppressed cancer cell proliferation and growth both in vitro and in vivo, the effect of which was partly rescued by KIF26B overexpression.Conclusion: ginsenoside Rh2 reduces m6A RNA methylation via downregulating KIF26B expression in some cancer cells. KIF26B elevates m6A RNA methylation via enhancing ZC3H13/CBLL1 nuclear localization. KIF26B-SRF forms a positive feedback loop facilitating tumor growth.

Published

2021

41. Facile approach for surfactant-free synthesis of Au@ginsenoside Rh2 nanoparticles and researches on anticancer activity.

Author

Yao, Hua, Mu, Xupeng, Wei, Zhenhong, Li, Xiuying, Wu, Liya, Jin, Yongri, Li, Xuwen, Li, Jing, and Jiang, Jinlan

Subjects

*CELL cycle, *ANTINEOPLASTIC agents, *CELL migration, *GOLD nanoparticles, *POISONS, *GINSENOSIDES, *METAL nanoparticles

Abstract

Background: Inorganic nanocomposites especially Au nanostructures have exhibited outstanding physicochemical properties in biomedical fields. For further clinical applications on theranostics, especially drug delivery, numerous explorations of green and facile synthesis methods combining with pharmacoactive natural components have been investigated to construct safe and multifunctional bioactive Au nanoparticles (NPs). Ginsenoside Rh2 is protopanaxadiol type compound isolated from plants of genus Panax, with excellent anticancer effect and antioxidant activity. In this research, we prepared the novel Au nanoparticles using ginsenoside Rh2 as both reducing and stabilizing agents. Results: The synthesized Au@ginsenoside Rh2 NPs were proved to exhibit desirable inhibitory effect on different cancer cell lines, which benefited from the inherent anticancer effect of the ginsenoside Rh2. Investigations in vitro indicated that Au@ginsenoside Rh2 NPs inhibited cell proliferation, cell migration and invasion, induced cell cycle arrest, enhanced the reactive oxygen species (ROS) generation, and regulated the protein expressions of caspase-3, 8, 9 to trigger cell apoptosis as well. Conclusions: Because of the absence of toxic chemical surfactants, the eco-friendly synthesis method of Au NPs modified by natural phytochemicals avoided tedious separation and modification processes. On the other hand, Au@ginsenoside Rh2 NPs also improved water solubility and bioavailability of the hydrophobic drug ginsenoside Rh2. It broadened minds for preparation and application of traditional Chinese medicines (TCMs) modified metal nanoparticles and deserved further study. [ABSTRACT FROM AUTHOR]

Published

2022

42. (20S) Ginsenoside Rh2-Activated, Distinct Apoptosis Pathways in Highly and Poorly Differentiated Human Esophageal Cancer Cells.

Author

Li, He, Han, Chunxiao, Chen, Chen, Han, Guanghong, and Li, Yang

Subjects

*ESOPHAGEAL cancer, *GINSENOSIDES, *CANCER cells, *BCL-2 proteins, *DEATH receptors, *MITOCHONDRIAL proteins, *APOPTOSIS

Abstract

Ginsenoside Rh2 (G-Rh2), a rare ginsenoside isolated from red ginseng, has considerable anti-cancer activity and induces apoptosis in a variety of cancer cells, but its activity in esophageal cancer cells is unclear. In this study, we examined the cytotoxic activity of (20S) G-Rh2 in highly differentiated esophageal squamous ECA109 cells and poorly differentiated esophageal squamous TE-13 cells. (20S) G-Rh2 exerted intense cytotoxicity in ECA109 and TE-13 cells with an IC50 of 2.9 and 3.7 μg/mL, respectively. After treatment with G-Rh2, Bcl-2, and Bcl-xL, the two main anti-apoptosis Bcl-2 family proteins upregulated, and Bax and Bak, the two key pro-apoptosis proteins translocated to mitochondria in both cell lines. At the same time, cytochrome c and Smac released from mitochondria, followed by caspase-9 activation, indicating that a mitochondria-mediated intrinsic apoptosis pathway was activated in both cell lines upon treatment with (20S) G-Rh2. It is noteworthy that (20S) G-Rh2 upregulated the transcription and protein expression of two death receptors, Fas and DR5, and subsequently activated Caspase-8 in the TE-13 cells but not in the ECA109 cells. Taken together, we demonstrated the potent anti-esophageal cancer cell activity of (20S) G-Rh2 and showed its working mechanism in two differentiated esophageal cancer cells, which can provide important evidence for developing an effective strategy for anti-esophageal cancer treatment. [ABSTRACT FROM AUTHOR]

Published

2022

43. Ginsenoside Rh2 administration produces crucial antidepressant‐like effects in a CUMS‐induced mice model of depression.

Author

Shi, Lin‐Sheng, Ji, Chun‐Hui, Liu, Yue, Gu, Jiang‐Hong, Tang, Wen‐Qian, Zhang, Wei, and Guan, Wei

Subjects

*GINSENOSIDES, *SADNESS, *ANIMAL disease models, *LABORATORY mice, *GINSENG, *MENTAL depression

Abstract

Introduction: The most striking feature of depression is sadness and a loss of interest in activities, which represents a major cause of disability globally. Therefore, it is necessary to identify novel antidepressants for clinical practice. Ginsenoside Rh2 (Rh2) is one of the major bioactive ginsenosides that can be extracted from Panax ginseng and has been demonstrated to improve both memory and learning. The purpose of this study was to provide broad insight into the mechanisms underlying depression and gain greater insights into antidepressant therapy. Methods: In this study, we first established an effective and feasible depression animal model of chronic unpredictable mild stress (CUMS) and behavioral testing was evaluated by the forced swim test (FST), the tail suspension test (TST) and the sucrose preference test. Following pretreatment with Rh2 (10 and 20 mg/kg), the immobility time of mice was reduced without affecting locomotor activity in both the FST and TST. Western blotting and immunofluorescence were used to investigate the activation of the hippocampal BDNF signaling pathway and hippocampal neurogenesis. Results: Different concentrations of Rh2 significantly reduced depressive‐like symptoms in CUMS‐induced mice and downregulated the effects of the BDNF signaling cascade and neurogenesis in the hippocampus. Furthermore, the administration of K252a completely prevented the antidepressant‐like activity of Rh2 in mice. Conclusion: The results indicated that Rh2 possesses the antidepression action via the positive regulation of the BDNF‐TrkB pathway. [ABSTRACT FROM AUTHOR]

Published

2022

44. Network Pharmacology-Based Study on the Mechanism of Ginsenoside Rh2 in Glioma Treatment.

Author

Wu, Xue, Qin, Xiujiao, and Dong, Han

Subjects

GINSENOSIDES, GLIOMAS, GINSENG, CELLULAR signal transduction, GENE ontology, CELL migration

Abstract

Glioma, originated from the neuroectoderm, is one of the prevalent tumors. It is reported that ginsenoside Rh2, a compound extracted from Panax ginseng, shows pharmacological activity in inhibiting the proliferation and metastasis of glioma cells. However, the precise underlying mechanism has not been completely clarified. In this study, the molecular mechanism of ginsenoside Rh2 in glioma treatment was investigated using network pharmacology, through which the target of ginsenoside Rh2 in glioma treatment was screened, and further the biological functions were analyzed by gene ontology biological annotation and Kyoto Encyclopedia of Genes and Genomes pathway enrichment. In total, 80 potential targets of ginsenoside Rh2 for glioma treatment were screened. Biological functions analysis revealed that ginsenoside Rh2 was associated with several cancer-related signaling pathways such as VEGF signaling pathway, thereby regulating cell processes, including cell migration and cell proliferation, which suggests that ginsenoside Rh2 targets multiple genes, further mediating indicated signaling network in anti-glioma and providing a potential mechanism of ginsenoside Rh2 in glioma treatment. [ABSTRACT FROM AUTHOR]

Published

2022

45. Ginsenoside Rh2 administration produces crucial antidepressant‐like effects in a CUMS‐induced mice model of depression

Author

Lin‐Sheng Shi, Chun‐Hui Ji, Yue Liu, Jiang‐Hong Gu, Wen‐Qian Tang, Wei Zhang, and Wei Guan

Subjects

brain‐derived neurotrophic factor, chronic unpredictable mild stress, depression, ginsenoside Rh2, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Abstract Introduction The most striking feature of depression is sadness and a loss of interest in activities, which represents a major cause of disability globally. Therefore, it is necessary to identify novel antidepressants for clinical practice. Ginsenoside Rh2 (Rh2) is one of the major bioactive ginsenosides that can be extracted from Panax ginseng and has been demonstrated to improve both memory and learning. The purpose of this study was to provide broad insight into the mechanisms underlying depression and gain greater insights into antidepressant therapy. Methods In this study, we first established an effective and feasible depression animal model of chronic unpredictable mild stress (CUMS) and behavioral testing was evaluated by the forced swim test (FST), the tail suspension test (TST) and the sucrose preference test. Following pretreatment with Rh2 (10 and 20 mg/kg), the immobility time of mice was reduced without affecting locomotor activity in both the FST and TST. Western blotting and immunofluorescence were used to investigate the activation of the hippocampal BDNF signaling pathway and hippocampal neurogenesis. Results Different concentrations of Rh2 significantly reduced depressive‐like symptoms in CUMS‐induced mice and downregulated the effects of the BDNF signaling cascade and neurogenesis in the hippocampus. Furthermore, the administration of K252a completely prevented the antidepressant‐like activity of Rh2 in mice. Conclusion The results indicated that Rh2 possesses the antidepression action via the positive regulation of the BDNF‐TrkB pathway.

Published

2022

46. Network Pharmacology-Based Prediction and Verification of Ginsenoside Rh2-Induced Apoptosis of A549 Cells via the PI3K/Akt Pathway.

Author

Song, Chao, Yuan, Yue, Zhou, Jing, He, Ziliang, Hu, Yeye, Xie, Yuan, Liu, Nan, Wu, Lei, and Zhang, Ji

Subjects

PI3K/AKT pathway, GINSENOSIDES, WESTERN immunoblotting, GINSENG, CANCER cells, INHIBITION of cellular proliferation

Abstract

Ginsenoside Rh2 (G-Rh2), a rare protopanaxadiol (PPD)-type triterpene saponin, from Panax ginseng has anti-proliferation, anti-invasion, and anti-metastatic activity. However, the mechanisms by which G-Rh2 induces apoptosis of lung cancer cells are unclear. In the present work, a G-Rh2 target-lung cancer network was constructed and analyzed by the network pharmacology approach. A total of 91 compound-targets of G-Rh2 was obtained based on the compound-target network analysis, and 217 targets were identified for G-Rh2 against lung cancer by PPI network analysis. The 217 targets were significantly enriched in 103 GO terms with FDR <0.05 as threshold in the GO enrichment analysis. In KEGG pathway enrichment analysis, all the candidate targets were significantly enriched in 143 pathways, among of which PI3K-Akt signaling pathway was identified as one of the top enriched pathway. Besides, G-Rh2 induced apoptosis in human lung epithelial (A549) cells was verified in this work. G-Rh2 significantly inhibited the proliferation of A549 cells in a dose-dependent manner, and the apoptosis rate significantly increased from 4.4% to 78.7% using flow cytometry. Western blot analysis revealed that the phosphorylation levels of p85, PDK1, Akt and IκBα were significantly suppressed by G-Rh2. All the experimental findings were consistent with the network pharmacology results. Research findings in this work will provide potential therapeutic value for further mechanism investigations. [ABSTRACT FROM AUTHOR]

Published

2022

47. Network Pharmacology-Based Prediction and Verification of Ginsenoside Rh2-Induced Apoptosis of A549 Cells via the PI3K/Akt Pathway

Author

Chao Song, Yue Yuan, Jing Zhou, Ziliang He, Yeye Hu, Yuan Xie, Nan Liu, Lei Wu, and Ji Zhang

Subjects

ginsenoside Rh2, network pharmacology, lung cancer, A549 cells, PI3K-Akt signaling pathway, Therapeutics. Pharmacology, RM1-950

Abstract

Ginsenoside Rh2 (G-Rh2), a rare protopanaxadiol (PPD)-type triterpene saponin, from Panax ginseng has anti-proliferation, anti-invasion, and anti-metastatic activity. However, the mechanisms by which G-Rh2 induces apoptosis of lung cancer cells are unclear. In the present work, a G-Rh2 target-lung cancer network was constructed and analyzed by the network pharmacology approach. A total of 91 compound-targets of G-Rh2 was obtained based on the compound-target network analysis, and 217 targets were identified for G-Rh2 against lung cancer by PPI network analysis. The 217 targets were significantly enriched in 103 GO terms with FDR

Published

2022

48. Study on synthesis of rare ginsenoside Rh2 by one-step purification and immobilization of glycosyltransferase from magnetic Ni-based MOF.

Author

Yue, Junsong, Liu, Xiaochen, Wu, Zhansheng, Li, Zhiyan, Wang, Jianwen, Tu, Min, and Shi, Huaiqi

Subjects

*METAL-organic frameworks, *GLYCOSYLTRANSFERASES, *ENCAPSULATION (Catalysis), *MAGNETIC nanoparticles, *MAGNETIC separation

Abstract

• Preparation of a magnetic MOF with superior materials and high enzyme load. • The immobilized material has a specific adsorption effect on UGT containing His-tag. • Simultaneous purification and immobilization of the enzyme onto the material. • Immobilization improved the stability of enzyme molecules. • The immobilized enzyme is easy to separate and can be reused. To solve the problem that free glycosyltransferase is difficult to isolate and reuse in ginsenoside Rh2 catalysis and synthesis. In this study, we developed a magnetic nickel-based metal-organic framework (MOF) material (Fe 3 O 4/ PDA@MOF) to enable the separation of recombinant glycosyl transferase (UGT) directly from crude enzyme solutions, while simultaneously immobilizing it by utilizing the specific adsorption of Ni2+ ions to His-tag. Our investigations demonstrated that the Fe 3 O 4 /PDA@MOF@UGT was successfully prepared, which not only maintained enzyme activity, but was reused by low-cost magnetic separation and exhibited enhanced enzyme loading and stability. Following thorough research and optimization, the immobilized enzyme achieved a rare ginsenoside Rh2 concentration of 69.68 µg/mL under optimal conditions, with an initial activity of 61.99 % after six cycles. This cost-effective, efficient, and sustainable biocomposite holds significant promise for industrial applications in enzyme purification and catalytic synthesis of ginsenoside. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

49. Host-microbiota interactions in collagen-induced arthritis rats treated with human umbilical cord mesenchymal stem cell exosome and ginsenoside Rh2.

Author

Zhou, Zhongsheng, Li, Yang, Wu, Shuhui, Liu, Te, and Jiang, Jinlan

Subjects

*MESENCHYMAL stem cells, *COLLAGEN-induced arthritis, *GINSENOSIDES, *UMBILICAL cord, *RHEUMATOID arthritis, *JOINT diseases

Abstract

Mesenchymal stem cell exosome (MSCs-exo) is a class of products secreted by mesenchymal stem cells (MSCs) that contain various biologically active substances. MSCs-exo is a promising alternative to MSCs due to their lower immunogenicity and lack of ethical constraints. Ginsenoside Rh2 (Rh2) is a hydrolyzed component of the primary active substance of ginsenosides. Rh2 has a variety of pharmacological functions, including anti-inflammatory, anti-tumor, and antioxidant. Studies have demonstrated that gut microbiota and metabolites are critical in developing rheumatoid arthritis (RA). In this study, we constructed a collagen-induced arthritis (CIA) model in rats. We used MSCs-exo combined with Rh2 to treat CIA rats. To observe the effect of MSCs-exo combined with Rh2 on joint inflammation, rat feces were collected for 16 rRNA amplicon sequencing and untargeted metabolomics analysis. The results showed that the arthritis index score and joint swelling of CIA rats treated with MSCs-exo in combination with Rh2 were significantly lower than those of the model and MSCs-exo alone groups. MSCs-exo and Rh2 significantly ameliorated the disturbed gut microbiota in CIA rats. The regulation of Candidatus_Saccharibacteria and Clostridium_XlVb regulation may be the most critical. Rh2 enhanced the therapeutic effect of MSCs-exo compared with the MSCs-exo -alone group. Furthermore, significant changes in gut metabolites were observed in the CIA rat group, and these differentially altered metabolites may act as messengers for host-microbiota interactions. These differential metabolites were enriched into relevant critical metabolic pathways, revealing possible pathways for host-microbiota interactions. [Display omitted] • The combination of MSCs-exo and Rh2 significantly sweetened joint inflammation in CIA rats. • MSCs-exo and Rh2 significantly ameliorated the disturbed gut microbiota in CIA rats. • Vitamin digestion, absorption, and arachidonic acid pathways could be pivotal in CIA rat pathogenesis. [ABSTRACT FROM AUTHOR]

Published

2024

50. c-MYC-mediated TRIB3/P62+ aggresomes accumulation triggers paraptosis upon the combination of everolimus and ginsenoside Rh2.

Author

Su, Min-Xia, Xu, Yu-Lian, Jiang, Xiao-Ming, Huang, Mu-Yang, Zhang, Le-Le, Yuan, Luo-Wei, Xu, Xiao-Huang, Zhu, Qi, Gao, Jian-Li, Lu, Jia-Hong, Chen, Xiuping, Huang, Ming-Qing, Wang, Yitao, and Lu, Jin-Jian

Subjects

GINSENOSIDES, EVEROLIMUS, ANTINEOPLASTIC agents, GINSENG, MTOR inhibitors, LUNG cancer

Abstract

The mammalian target of rapamycin (mTOR) pathway is abnormally activated in lung cancer. However, the anti-lung cancer effect of mTOR inhibitors as monotherapy is modest. Here, we identified that ginsenoside Rh2, an active component of Panax ginseng C. A. Mey., enhanced the anti-cancer effect of the mTOR inhibitor everolimus both in vitro and in vivo. Moreover, ginsenoside Rh2 alleviated the hepatic fat accumulation caused by everolimus in xenograft nude mice models. The combination of everolimus and ginsenoside Rh2 (labeled Eve-Rh2) induced caspase-independent cell death and cytoplasmic vacuolation in lung cancer cells, indicating that Eve-Rh2 prevented tumor progression by triggering paraptosis. Eve-Rh2 up-regulated the expression of c-MYC in cancer cells as well as tumor tissues. The increased c-MYC mediated the accumulation of tribbles homolog 3 (TRIB3)/P62+ aggresomes and consequently triggered paraptosis, bypassing the classical c-MYC/MAX pathway. Our study offers a potential effective and safe strategy for the treatment of lung cancer. Moreover, we have identified a new mechanism of TRIB3/P62+ aggresomes-triggered paraptosis and revealed a unique function of c-MYC. Eve-Rh2 up-regulates the expression of c-MYC, which mediates the accumulation of TRIB3/P62+ aggresomes bypassing the classical c-MYC/MAX pathway, thereby triggering paraptosis and ultimately inhibiting tumor progression. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2022