Biochanin-A has shown efficacy against different types of cancers.
Biochanin-A has shown efficacy against different types of cancers. a) breast cancer, b) prostate cancer, c) lung cancer, d) pancreatic cancer, e) colon cancer, f) osteosarcoma, g) glioma, h) leukaemia. The molecular structure of biochanin-A is depicted in the centre of diagram.
Breast cancer is the most widely reported form of cancer, presented with several subtypes and varying vulnerability to anti-cancer agents. Tumour cells have shown a unique pattern in terms of uncontrolled growth, dedifferentiated morphology, and resistance to apoptosis (
With the influence of biochanin-A, HER2 receptor activation is inhibited, resulting in blockade of downstream signalling pathways of cancer cell development, viability, and metastasis. In HER2-positive breast cancer, the transcriptional unit nuclear factor (NF)-κB is suppressed (
Biochanin-A dephosphorylates HER-2 receptor and MAPK or ERK1/2 causing blockade of cancer cell development, growth, metastasis, and mitogenesis. Biochanin-A inhibits Akt phosphorylation thereby downregulates mTOR signals and disrupts the cell cycle. It inhibits NFkB and interrupts transcription. It inhibits topoisomerase-ll and DNA replication (
Prostate cancer has been reported as a commonly found cancer in men and the second prominent death reason in western countries (
Biochanin-A elevates the level of testosterone-UDPGT (Uridine 5′-diphospho-glucuronosyltransferase) enzyme activity and disrupts the androgen metabolism in connection with UDP-glucuronic acid. PLK-1 (Polo-like kinase-1) is responsible for various cell cycles activities such as Cdc2 (Cyclin-dependent kinase) stimulation and mitosis. Biochanin-A induces p21 which is a negative regulator for PLK-1 leading to prostate cancer cell apoptosis (
Phytoestrogens have been predicted as compounds liable for chemoprotective activity on prolonged exposure. Prostatic cell proliferation in PC-3, LNCaP, and DU145 were inhibited by biochanin-A with variable mechanisms (
In
Biochanin-A inhibits aromatase enzyme and decreases estrogen levels. It activates p21 and antagonizes PLK-1 action. Increased level of testosterone UDGPT enzyme disrupts androgen metabolism with the treatment of biochanin-A. The level of tyrosine kinase is interrupted and inhibits signal transduction. It induces ER-β and E-cadherin and inhibits cell proliferation. Biochanin-A inhibits NF-kB and induced TRAIL associated apoptosis. It increased conversion of testosterone into glucuronide resulting low appearance of prostate-specific antigen (PSA) (
Cancer affecting the most vital body parts elucidate the difficulty of its therapy. Lung cancer has often been reported and is one of the supreme death causes in cancer patients. The fight against cancer with phytochemicals will benefit mankind greatly. Studies have been carried out on soy isoflavones, utilized as an integral system for the treatment and to boost the radiation viability on lung tumors (
The mechanism with which soy isoflavones boost radiation therapeutic effect is through inhibiting APE1/Ref-1 DNA repair in A549 cells, which leads to cell killing (
Biochanin-A cause apoptosis in lung cancer by increasing p21, caspase-3, and Bcl-2 levels. It lowers E-cadherin and blocks metastasis. Pro-inflammatory mediators such as TNF-α, IL-6, and cytokines are released to facilitate apoptosis. Soy isoflavones along with radiation therapy shows a synergistic effect in causing cell death by inhibiting APE/Ref-1 (
The low survival rate of pancreatic cancer with limited anti-cancer agents makes it difficult to manage the disease. It is also known to be the most aggressive one among other cancers (
The cluster formation ability of pancreatic cancer cells Panc1 was hindered by biochanin-A with dose-dependent toxicity. It inhibited mitosis, migration, and invasion of pancreatic cancer progression. EGFR, Akt, and MAPK pathways are deactivated resulting in apoptosis in Panc1 and AsPC-1 cell lines suggesting combination therapy with biochanin-A could be considered for treatment (
It is the most prevalent type of cancer in existence today. Statistics by the American Cancer Society, 2019, shows that colon cancer is the second leading source of mortality in cancer. As specified by American Institute for Cancer Research and World Cancer Research Fund reports dietary factors may elucidate the risk of having colorectal cancer. Intake of isoflavone-contained food like soy influences gastric cancer occurrence (
The synergism of biochanin-A with 5-fluorouracil evidenced in Caco-2 and HCT-116 cell lines indicates the modulatory influence of biochanin-A in colon cancer treatment. The biochanin-A on its own shows cytotoxicity in the cell lines. It blocked the “Akt and GSK3β phosphorylation and boosted the degradation of β-catenin” (
The inhibitory mechanism of biochanin-A on colon cancer is shown in
Biochanin-A boosted the anti-cancer effect exerted by 5-fluorouracil and gamma radiation when given in combination in colon cancer cells. Biochanin-A has inhibited Akt and GSK3β phosphorylation (
Glioblastoma multiforme (GBM), the most widely reported and destructive brain malignancy, has a high death rate. GBM tends to reappear since it displays both intra- and inter-tumoral heterogeneity (
In a dose-dependent manner, biochanin-A influenced the tumour invasion capacity by lowering matrix-degrading enzymes (MMP 2 and MMP 9) tested in U87MG cells (
Osteosarcoma (OS), a malignant bone tumour, is generally seen in children and adolescents. The low survival rate of OS is associated with drug resistance causing the poor response to chemotherapy. Hence, phytochemicals that can contribute to OS treatment are significant.
Biochanin-A and doxorubicin together suppressed the tumour development by promoting the release of apoptotic factors, damaging mitochondrial membrane potential, eliciting “the intrinsic mitochondrial pathway, caspase-9 and -3 activation” and increasing “Bax: Bcl-2/Bcl-XL ratio” (
Leukaemia or blood cancer affects the most important connective tissue of our body: blood, and the blood-forming tissue. It is considered a deadly and serious form of cancer (
Biochanin-A in JCS cells prompted monocytic differentiation to macrophages (markers “Mac-l and F4/80”) showing increased phagocytic activity. The cytokines production (“IL-la, IL-lo, IL-4 and TNF-α”) is regulated in the late stage of monocytic differentiation of JCS cells by biochanin-A (
Anti-cancer effects of biochanin-A substantiated through in vivo and in vitro experiments is summarized in
(
| Pharmacological Application | Study models | Dose used | Major findings\mechanisms | Reference |
|---|---|---|---|---|
| Breast cancer | HER-2 Positive breast cancer cell lines | 2–100 μM | NFκB ↓ Unique anticancer agent MAPK or ERK 1/2 phosphorylation × | (
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| MCF-7 human breast carcinoma cells | 10–50 μM | Cell cycle apoptotis + DMBA × | (
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| Human granular luteal cells | 10–100 nm | Cyp19 enzyme ↓ Have role in aromatase activity | (
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| MCF-7 breast cancer cell lines | 500 nm | Anti-oestrogenic property | (
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| CTLL-2 cells (Murine IL-2 dependent T cell clone | 5–50 μM | Topoisomerase II × | (
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| Prostate cancer | LNCaP cell lines | 0.5–50 μM | testosterone-UDPGT ↑ PSA ↓ Androgen metabolism × | (
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| PC-3 (p53 mutant) and LNCaP (p53 wild type) | 100 μM | p21 ↑ PLK-1 ↓ Cell apoptosis + | (
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| DU-145 and LNCaP | 8.0 μg/mL for LNCaP 9.0 μg/mL for DU-145 cells | EGF-stimulated growth × tyrosine kinase events × | (
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| Red clover diet Model (Isoflavones constitute 1.26% of the diet) | Biochanin A 5.74 mg isoflavone/g pellet | ER-β and E-cadherin levels ↑ Cancer formation × | (
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| LNCaP cells Athymic mice with LNCaP flank tumors | 10 μg/mL 400 μg for animal xenographs model | DNA fragmentation ↑ p21 and cyclin B ↓ Tumor size and incidence ↓ | (
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| Fibroblast cell | 100 μg/mL | 5 α-reductase isozymes × hormone-dependent tumours ↓ | (
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| LNCaP cells and DU145 cells, | 20–100 μM | TRAIL-associated cell death NF-κB × | (
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| PC-3, LnCaP, and DU145 | 100 μmol/L | Cell proliferation × Growth and metabolism × | (
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| Lung cancer | 95D and A549 cancer cells injected to male nude mice | Biochanin A IP 15,60 mg/kg group of A549 18,75 mg/kg group of 95D | Cell proliferation of lung cancer cells × | (
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| Human lung adenocarcinoma cell line(A427),Human monocyte leukaemia cell line (AML-193) | 5, 20, 40 μM | Hinderes proinflammatory effects triggered from leukaemia | (
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| New born mouse model | 65 mg/kg | Carcinogenesis × | (
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| Non-small cell lung cancer | Soy red clover isoflavones | Isoflavones combined with EGFR inhibitors improve NSCLC cell growth | (
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| Pancreatic cancer | Panc/AsPC-1 | 5 mg/mL | Cell proliferation × Apoptosis + | (
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| Colon cancer | Caco-2,HCT-116 cell lines | 34 μM | Biochanin combination with 5 FU promotes management of colon cancer | (
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| HT29cells | 1–100 μM | Biochanin increases radiotoxicity | (
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| HCT-116 Sw-480 cell lines | 2.5–100 μM | Biochanin enhances genotoxYangiharaic effects and antitumor mechanism |
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| 320 DM cell line | 20 μM | Biochanin is a promising target for cancer | (
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| Glioblastoma multiforme | U87MG | 50 μM | MMP 2 and MMP 9 ↓ | (
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| Rat brain tumour (C6) Murine brain endothelial (bEnd.3) cells Ex-vivo chick chorioallantoic membrane model | 5, 35, and 70 μmol/L | Anti-angiogenic properties through ERK/AKT/mTOR dephosphorylation | (
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| U-87 MG, and T98 G | 70 μM | EGFR, p-ERK, p-AKT, c-myc, and MT-MMP1 activation ↓ cell survival * Synergism to anti-cancer ability of Temozolomide | (
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| U-87 human glioblastoma cell line | 20 μM and 70 μM | p-EGFR, p-ERK, uPAR, MMP-2 ↓ | (
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| Osteosarcoma | MG63 and U2OS Cells | 20±0.3 μg/mL | Bax: Bcl-2/Bcl-XL ratio ↑ caspase 9 & 3 + MMP ↓ | (
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| MG63 and U2OS Cells | 40 μM | Apoptosis + caspase-3 ↑ Cell proliferation and invasion × | (
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| Leukaemia | JCS | Monocytic differentiation to macrophages + Phagocytic activity ↑ | (
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Diabetes mellitus, an age-old metabolic disorder, has a high rate of occurrence around the world. It is described as “hyperglycaemia” caused by deformities in insulin secretion, insulin activity, or both (
Biochanin-A action in streptozotocin-induced diabetic rats displayed improved glucose digestion and dropped HbA1C levels. Serum visfatin amount was enhanced (
The influence of biochanin-A in diabetic neuropathy using an STZ-induced rat model revealed that, mechanical allodynia and hyperalgesia (paw withdrawal threshold) were reversed upon treatment. Hence, biochanin-A could be a drug of choice in diabetic neuropathy (
The anti-diabetic mechanism of biochanin-A is by decreasing oxidative stress. SIRT-1 influences the progression of insulin sensitivity. Biochanin-A act as a PPAR gamma receptor activator and produces anti-diabetic effect. The increased release of adiponectin and low resistin level to improve the diabetic condition is depicted in
Biochanin-A decreases the oxidative stress and helps in diabetes condition. It increases the expression of SIRT-1 and progresses insulin sensitivity. Biochanin-A is a PPAR-γ receptor activator producing an anti-diabetic effect. It increases the release of adiponectin and decreases the resistin level to improve the diabetic condition (
Dyslipidaemia or hyperlipidaemia is a very common metabolic disorder characterized by a high level of triglycerides and low-density lipoproteins, responsible for cardiovascular diseases (
Treatment with a moderate dose of biochanin-A in HFD mice has shown a substantial lowering of LDL and total cholesterol. Lipoprotein lipase and hepatic triglyceride lipase levels are increased. Molecular docking studies on biochanin-A displayed a noteworthy role in reducing cholesterol-ester transport (
Obesity has been the most serious global health concern that is rapidly turning into an outbreak, currently affecting both developing and developed countries to varying degrees. Despite the fact that obesity and overweight are on the rise in modern society, there are no pharmacological treatments available. As a result, both researchers and health-care systems must prioritise the development of safe and effective treatments for obesity.
In HFD-induced obesity, oral treatment of biochanin-A significantly reduced the physiological changes that have occurred during trace element metabolism. This could be due to the inhibition of pathological mechanisms that derange trace elements, possibly by reverting hyperglycemia and insulin resistance and changing hepcidin and HO-1 levels. These findings strongly suggest that biochanin-A has therapeutic potential in the treatment of obesity and the prevention of cardiovascular disease (
Biochanin-A promotes AMPK signalling in C3H10T1/2 MSCs, leading to upregulation of brown fat adipocyte. According to the findings, biochanin-A treatment improves mitochondrial biogenesis and lipolysis, modulating the thermogenic process. Biochanin-A improves energy expenditure by boosting mitochondrial respiration while preserving the functional mitochondria. These data imply that biochanin A might be a new antiobesity drug (
Asian countries usually presented lower cardiovascular disease (CVD) mortality rates as it has very different dietary patterns from that of Western countries. Benefits over cardiovascular disease risk is an appreciated capability of soy protein and isoflavones. Isoflavones restore the disrupted endothelial function (
Biochanin-A mitigated myocardial injury by inhibiting the anti-inflammatory pathway, TLR4/NF-kB/NLRP3 signalling. It perfected the injury area and stopped the release of aspartate transaminase (AST), creatine kinase (CK-MB) and lactic dehydrogenase (LDH) enzyme. Biochanin-A further decreased inflammatory cytokines and protected rats from myocardial infarction (
In the 19th and 20th centuries, people were drinking red clover tea or tincture (ethanolic extract) as an antispasmodic to give relief in whooping cough, measles, bronchitis, laryngitis, and tuberculosis (
It has been proven that biochanin-A diminishes airway resistance and improves respiratory health in methacholine (MCh) induced mice. Inflammatory mediators released were under control and ovalbumin (OVA)-specific immunoglobulin E (IgE) levels were low, hence, evidencing significant effect in allergic asthma and COPD (
Osteoarthritis is a condition that affects articular cartilage and synovial joints with structural and functional failure and diminishes the quality of life (
Biochanin-A controlled the cartilage damage by deactivating the expression of MMP, NF-κB, and activation of TIMP-1, hence effective in OA cases (
Inflammation, biological feedback of the human body to damaging stimuli, is also associated with a wide range of diseases such as “obesity, atherosclerosis, rheumatoid arthritis, and even cancer”. Isoflavones are famous for their anti-inflammatory properties. Underlining the evidence for isoflavones is required in managing chronic diseases in which inflammation plays a vital role. Isoflavones that are an assured agent in various inflammatory diseases, show exciting anti-inflammatory effects proven in animal and human studies through better anti-oxidant properties, reduced pro-inflammatory enzymes, and NF-κB regulation (
Biochanin-A repressed LPS induced TNF-α and IL-8 production, NF-κB. Through PPAR-γ activation, biochanin-A displayed an anti-inflammatory effect hence, can be considered as an agent in the therapeutic management of inflammatory cardiovascular disease (
Antioxidant rich foods may lower the chance of developing a number of ailments including heart disease and certain cancers. Free radicals are removed from cells by antioxidants, which minimizes oxidation related damage in the body. Biochanin
Water-soluble urban particulate matter is a major lung toxicant shown to induce oxidative damage in human alveolar basal-epithelial cells. Biochanin-A tested in this model produced a protective effect by increasing anti-oxidant markers such as catalase, superoxide dismutase and glutathione. The malondialdehyde (MDA) and nitric oxide (NO) levels were found to be reduced and mitigated the lung injury by regulating MEK5/extracellular signal-related kinase 5 (ERK5) nuclear factor-erythroid factor 2-related factor 2 (Nrf-2) pathway (
The hepatoprotective abilities of biochanin-A were explored in carbon-tetrachloride hepatotoxicity animal model. The anti-oxidant and anti-inflammatory capacity of biochanin-A influence the elevated hepatic enzyme level, such as AST, ALP, ALT, bilirubin, etc., and found to be a promising molecule in hepatotoxicity models (
Natural isoflavones have exposed anti-microbial activity in various studies. The specific inhibitory action of biochanin-A was explored against possible
Neurological disorders hampering the brain and nervous system are associated with a wide group of disorders as well as varying pathophysiology and symptoms. Inflammation is thought to be one important pathogenesis to cause peripheral (neuropathic pain, fibromyalgia) and central nervous systems disorders (e.g., Parkinson's disease, ischaemia, and traumatic brain injury, etc.) (
Two key pathways in the development of cerebral ischaemia/reperfusion damage are oxidative stress and neuroinflammation. Biochanin-A pretreatment on experimental animals induced with stroke, showed that the neurological deficiency is improved and the size of neural infarct and brain oedema was reduced. Biochanin-A reduced oxidative stress in the brain by augmenting SOD (superoxide dismutase) and GSH-Px (glutathione peroxidase) and repressing MDA (malondialdehyde) levels. The neuroprotective effects of biochanin-A might be attributed to the activation of the Nrf2 pathway and suppression of the NF-κB pathway (
Parkinson’s disease (PD) is related to the degeneration of dopaminergic neurons in the SNpc. Oxidative stress in connection with the neurodegenerative symptoms has been found in this condition. Studies on lipopolysaccharide (LPS)-injected animals revealed that treatment with O-methylated biochanin-A amended the behavioural patterns of animals, stopped the dopamine neuronal loss, and prevented the harmful microglia activation. Biochanin-A additionally blocked the activation of NADPH-oxidase, MDA formation, SOD, and GPx actions in the brain preferring its choice as an anti-oxidant in PD management (J. Wang
The neuroprotective efficacy of various phytoestrogenic isoflavones including biochanin-A was screened against oxidative stress-induced cell death in the HCN 1-A (human cortical cell line) maintained in culture using the Alzheimer's disease-associated hydrogen peroxide (H
2O
2) model. Due to the anti-oxidant efficacy of isoflavones, the concentration-reliant reduction in neuron viability by H
2O
2 was prevented (
The neuroprotective effects of biochanin-A on LPS-induced dopaminergic neuron injury in in vivo and in vitro models, as well as the molecular processes involved were explored. Biochanin-A therapy for 21 days substantially reduced behavioural impairment in PD rats, lowered dopaminergic neuronal loss, and suppressed microglia activation in LPS-induced PD rats. Biochanin-A protects LPS-induced PD rats, and the mechanisms are thought to be related to the suppression of the inflammatory response and the MAPK signalling pathway. Biochanin-A prevented primary microglial activation and protected dopaminergic neurons, reduced the amount of nitric oxide, IL-1, and TNF-α in supernatants, and suppressed the formation of reactive oxygen species (
The behavioural and neurochemical effects of biochanin-A among cognitive-impaired animals in scopolamine-induced amnesia and naturally occurring aged animal amnesia models were assessed. In exteroceptive behavioural paradigms such as the elevated plus maze and the passive shock avoidance paradigm, biochanin-A decreased the transfer latency and increased the step through latency considerably in scopolamine-treated and natural aged mice. Acetylcholinesterase activity was found decreased in a dose-reliant manner amongst biochanin-A treated animals. A high level of GSH suppressed the pyknotic neurons formation, noradrenalin and dopamine expression thereby revealed the protective ability of biochanin-A against Alzheimer's disease (
In postmenopausal women, oestrogen insufficiency is a major risk factor for Alzheimer's disease. In the Morris water-maze test, chronic treatment with biochanin-A replicated the capacity of β-estradiol (E2) to restore learning and memory deficits in ovariectomized (OVX) rats. Biochanin-A also lowered MDA levels and increased SOD and GSH-Px enzyme levels eventually produced neuro-protective effect and can be used to treat memory loss in postmenopausal women who are suffering from an oestrogen imbalance (
The several pharmacological models explained in the review are collectively summarized in
(↑increase, ↓decrease, × inhibit, + activation).
| Pharmacological application | Study model | Dose and route used | Findings | Reference |
|---|---|---|---|---|
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STZ-rat model | 10 mg/kg bodyweight per os (p/o) | HbAIc level ↓ Glucose tolerance, Insulin resistance ↓ | (
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| 10–15 mg/kg p/o | Glucose digestion ↑ HbA1C levels ↓ Serum visfatin amount ↑ | (
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| 10–15 mg/kg p/o | FBS ↓ hyperglycemia-induced free radicals | (
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| 15 mg/kg p/o | Nesfatin-1 ↑ Insulin ↑ FBG level ↓ | (
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| 10–15 mg/kg p/o | Adiponectin ↑ insulin ↑ serum resistin ↓ serum adiponectin ↑ | (
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| 0.1, 1 and 5 mg/kg intraperitonial (i/p) | Mechanical allodynia ↓ Hyperalgesia ↓ | (
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| 10–15 mg/kg p/o | The concentrations of VEGF, TNF-α and IL-1β in retina ↓ blood sugar ↓ inflammation ↓ angiogenesis ↓ | (
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| 10–20 mg/kg/day p/o | Diabetic nephropathy × Renal TGF-β expression↑ | (
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| db/db diabetic mice model | 10–50 mg/kg/day red clover extract (Red clover extract containing 9.6% biochanin-A) p/o | Hepatic PPARα/γ stimulation ↑ Hepatic fatty acid synthase levels ↓ | (
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| STZ-diabetic C57BL/6 mice | 1 mg/kg/day p/o | Hepatic PPARα ↑ Lipid profile ↓ Glucose levels ↓ | (
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| High fat diet + streptozotocin | 10, 20 and 40 mg/kg | Glucose tolerance ↓ Insulin resistance ↓ Insulin sensitivity, SIRT-1 expression ↑ | (
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| Streptozotocin- Nicotinamide rat model | 5 mg/kg | Fasting blood glucose ↓ Body weight ↑ | (
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HFD Mice model | 30mg/kg/day,60mg/kg/day, and 120mg/kg/day | LDL,total cholesterol ↓ Lipoprotein lipase and hepatic triglyceride lipase ↑ | (
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HFD-induced obese rats. | p/o | HFD induced trace elements metabolism ↓ Glucose, insulin, ferritin, total cholesterol, phospholipids, free fatty acids ↓ | (
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| C57BL/6 mice HFD | 0.05% biochanin-A p/o | PPAR ↑ glucose 6-phosphatase and pyruvate kinase × Obesity-induced hepatic steatosis and insulin resistance × | (
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Transient coronary ligation in Sprague-Dawley rats | 12.5, 25 and 50 mg/kg intragastrically | TLR4/NF-kB/NLRP3 signalling × AST, CK-MB, LDH enzyme releases ↓ | (
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| apoE-/- mice fed with Western diet. | 50 mg/kg intragastrically | pro-inflammatory cytokines ↓ | (
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| isoproterenol-induced MI rats | 10 mg/kg body weight subcutaneously | antioxidant levels ↑ lipid peroxidation and detoxifying enzyme systems ↓ |
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Ovalbumin-Induced Airway Hyperresponsiveness BABL/c mice model | 100 μmol/kg, p/o | Total inflammatory cells ↓ Eosinophils ↓ Neutrophils ↓ Th1-released IL-2 & TNF-α ↓ Th2-released IL-4 & IL-5 ↓ | (
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| Male Hartley guinea pigs | 10–30 μm | baseline tension and cumulative OVA-induced contractions in isolated sensitized guinea pig tracheal × degranulation of mast cells× inflammation ↓ | (
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| PM2.5-induced lung toxicity in SD rats | 5, 50,100 mg/kg intragastric administration | cell death ↓ release of pro-inflammatory mediators, MDA, LDH, AKP ↑ antioxidant enzymes levels ↑ | (
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Osteoarthritis rabbit model | 5–25 mM intra-articular injection | Cartilage damage ↓ MMP, NF-κB × TIMP-1 + | (
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BALB/c mice+ intragastric administration of
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2 μg/mL | Salmonella infection × AMPK/ULK1/mTOR pathway |
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| Cerebral ischemia: | C57BL/6 male mice middle cerebral artery occlusion induced Focal cerebral ischemia | 5,10 mg/kg intraperitoneal | GOT protein expression ↑ stroke lesion volume ↓ | (
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| Ischemic stroke Rat model | 10, 20, or 40 mg/kg/day | infarct size and brain edema ↓ SOD,GSH-Px ↑ MDA,NF-κB × Nrf2 nuclear translocation, HO-1 + |
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| Middle cerebral artery occlusion (MCAO) rat model | 10, 20, or 40 mg/kg/day | inflammatory response TNF-α and IL-1β levels, MPO activity↓ p38 signalling ↓ | (
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| Parkinson’s disease | SD Rats with Iron and Rotenone Co-treatment | 30 mg/kg | malondialdehyde ↓ glutathione levels ↑ striatal dopamine depletion↓ behavioural impairments ↓ maintains redox equilibrium | (
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| C57BL/6 with enhanced neonatal Iron and MPTP co-treatment | 10–60 mg/kg | microglial p38 MAPK activation × behavioral and neurochemical deficits ↑ | (
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| Alzheimer's disease | LPS-induced PD rats | 12.5, 25, 50 mg/kg | inflammatory response ↓ MAPK signalling pathway × nitric oxide, IL-1, and TNF-α | (
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| scopolamine-treated mice and natural aged cognitive deficit mice | 40 mg/kg | AchE activity ↓ GSH ↑ thiobarbituric acid, ROS ↓ pyknotic neurons ↓ | (
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| ovariectomized (OVX) rats | 5,20,60 mg/kg | restore learning and memory deficits, MDA ↓ SOD and GSH-Px ↑ | (
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(↑increase, ↓decrease, × inhibit, + activation).
| Pharmacological application | Study model | Dose and route used | Findings | Reference |
|---|---|---|---|---|
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Cervical carcinoma (HeLa) cells | EC 50 = 1–4 mmol/L | PPAR receptor activator | (
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C3H10T1/2 cells | _ | Mitochondrial respiration ↑ AMPK signalling + | (
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| Neuronal cells | _ | ER stress ↓ leptin signalling × | (
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OVA-Induced Tracheal Contractions In Vitro. | 10–30 μm | anti-spasmodic agent | (
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IL-1β induced rabbit chondrocytes | 5, 25, 50 μM | Cartilage damage ↓ MMP, NF-κB × TIMP-1 + | (
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| Primary Rat Adipose-Derived Stem Cells (ADSCs). | 0.3 μM | Adipocyte differentiation × PPARγ, LPL, OPN and leptin ↓ OPG ↑ osteoblast differentiation ↑ adipogenesis × |
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ADSCs | 0.1–1 μM | cytoplasmic lipid droplet accumulation × PPAR-γ × Runx2, OPG, RhoA protein, OCN ↑ | (
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| RAW 264.7 and HT-29 cell lines | 100 μM and 50 μM | NO production, LPS, IKK activity × NF-κB + IL-6, IL-1β, and TNF-α production in RAW264.7 cells ↓ cell proliferation in HT-29 cell line × | (
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Potential bacterial pathogens of the human digestive system | 0.13mM 0.26–0.51 mM | Clostridium tertium, clostridium clostridioforme × | (
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| in vitro antibacterial activity | 16 to 128 μg/mL | Growth inhibitory effect to gram-positive and gram-negative bacteria | (
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12 μM & 6.5 μM buccal formulation | Chlamydia growth × Antichlamydial action + | (
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| HeLa cells/Macrophages | _ | Salmonella infection × AMPK/ULK1/mTOR pathway |
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| Cerebral ischemia: | Mouse hippocampal HT4 neural cells or primary cortical neurons | 25 and 50 μM | GOT mRNA expression ↑ glutamate-induced cell death × | (
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| L-glutamate-induced cytotoxic PC12 cell line | 1, 10, 50, and 100 μM | cytotoxicity ↓ glutathione ↑ LDH, caspase-3 | (
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| Parkinson’s disease | Rat mesencephalic neuron-glia cultures | 12.5, 25, 50 mg/kg
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NADPH-oxidase, MDA formation, SOD, and GPx × dopamine neuronal loss ↓ | (
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| BV2 microglial cells | 1.25, 2.5, 5 μM | LPS related microglia activation × TNFα, IL-1β, nitric-oxide, and ROS ↓ |
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| LPS treated mice BV 2 microglial cells | 1.25, 2.5, 5 μM | TNFα, IL-1β, nitric oxide, and ROS ↓ MAPK signalling × | (
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| BV2 Microglia | 5, 10, 20 μM | PPAR-γ levels ↑ NF-κB release × | (
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| Alzheimer's disease | HCN 1-A cell line with H2O2 model | 0.5, 1 and 2 μg/mL | H2O2 induced neurotoxicity ↓ | (
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| PC12 cells with β-Amyloid-Induced Neurotoxicity | 100 μM | Amyloid beta induced cell toxicity ↓ cytochrome-c and Puma Bcl-2/Bax ↓ | (
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| Microglial cells | 1.25, 2.5, 5, 10, 15, 20, 25, 30 μM | microglial activation × nitric oxide, IL-1b, and TNF-α ↓ ROS × MAPK signaling pathway × | (
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| In-vitro BACE-1 activity assay | 28 μM | BACE1 × strong binding between the chemical and the allosteric site of BACE1 |