Your search keyword '"Qin, Cheng Xue"' showing total 8 results

1. Antioxidant activity contributes to flavonol cardioprotection during reperfusion of rat hearts

Author

Qin, Cheng Xue, Williams, Spencer J., and Woodman, Owen L.

Subjects

*ANTIOXIDANTS, *FLAVONOIDS, *CARDIOTONIC agents, *REPERFUSION, *LABORATORY rats, *FREE radicals, *MYOCARDIAL infarction, *LACTATE dehydrogenase

Abstract

Abstract: The mechanism of flavonol-induced cardioprotection is unclear. We compared the protective actions of a flavonol that inhibits calcium utilization and has antioxidant activity, 3′,4′-dihydroxyflavonol (DiOHF); a flavonol that affects only calcium activity, 4′-OH-3′-OCH3-flavonol (4′-OH-3′-OCH3F); and a water-soluble flavonol with selective antioxidant activity, DiOHF-6-succinamic acid (DiOHF-6-SA), in isolated, perfused rat hearts. Hearts were subjected to global ischemia for 20min followed by 30min reperfusion and were treated with vehicle (0.05% DMSO), DiOHF, 4′-OH-3′-OCH3F, or DiOHF-6-SA (all 10μM, n =5–8 per group). Flavonols were infused for 10min before ischemia and during reperfusion. In vehicle-treated hearts, left-ventricular (LV) + dP/dt was reduced by 60% at the end of reperfusion compared to the preischemic level. Lactate dehydrogenase (LDH) release was elevated and endothelial NO synthase (eNOS) expression was lower in vehicle-treated hearts compared to shams. In comparison, DiOHF treatment improved LV function upon reperfusion, decreased LDH, and preserved eNOS expression. The antioxidant DiOHF-6-SA also preserved contractility, reduced LDH, and preserved eNOS expression. In contrast, hearts treated with 4′-OH-3′-OCH3F showed a degree of contractile impairment similar to that of the vehicle group. DiOHF and DiOHF-6-SA also exerted cardioprotection when given only during reperfusion and not when administered only before ischemia. Flavonol-induced cardioprotection relies on antioxidant activity and is mainly exerted during reperfusion. [Copyright &y& Elsevier]

Published

2011

2. 2-Morpholinoisoflav-3-enes as flexible intermediates in the synthesis of phenoxodiol, isophenoxodiol, equol and analogues: Vasorelaxant properties, estrogen receptor binding and Rho/RhoA kinase pathway inhibition

Author

Tilley, Andrew J., Zanatta, Shannon D., Qin, Cheng Xue, Kim, In-Kyeom, Seok, Young-Mi, Stewart, Alastair, Woodman, Owen L., and Williams, Spencer J.

Subjects

*CARDIOVASCULAR disease treatment, *ISOFLAVONES, *FLAVONOIDS, *CHEMICAL synthesis, *ESTROGEN receptors, *ENZYME inhibitors, *DRUG metabolism

Abstract

Abstract: Isoflavone consumption correlates with reduced rates of cardiovascular disease. Epidemiological studies and clinical data provide evidence that isoflavone metabolites, such as the isoflavan equol, contribute to these beneficial effects. In this study we developed a new route to isoflavans and isoflavenes via 2-morpholinoisoflavenes derived from a condensation reaction of phenylacetaldehydes, salicylaldehydes and morpholine. We report the synthesis of the isoflavans equol and deoxygenated analogues, and the isoflavenes 7,4′-dihydroxyisoflav-3-ene (phenoxodiol, haganin E) and 7,4′-dihydroxyisoflav-2-ene (isophenoxodiol). Vascular pharmacology studies reveal that all oxygenated isoflavans and isoflavenes can attenuate phenylephrine-induced vasoconstriction, which was unaffected by the estrogen receptor antagonist ICI 182,780. Furthermore, the compounds inhibited U46619 (a thromboxane A2 analogue) induced vasoconstriction in endothelium-denuded rat aortae, and reduced the formation of GTP RhoA, with the effects being greatest for equol and phenoxodiol. Ligand displacement studies of rat uterine cytosol estrogen receptor revealed the compounds to be generally weak binders. These data are consistent with the vasorelaxation activity of equol and phenoxodiol deriving at least in part by inhibition of the RhoA/Rho-kinase pathway, and along with the limited estrogen receptor affinity supports a role for equol and phenoxodiol as useful agents for maintaining cardiovascular function with limited estrogenic effects. [Copyright &y& Elsevier]

Published

2012

3. The formyl peptide receptors FPR1 and FPR2 as targets for inflammatory disorders: recent advances in the development of small-molecule agonists.

Author

Yi, Xiangyan, Tran, Eric, Odiba, Jephthah O., Qin, Cheng Xue, Ritchie, Rebecca H., and Baell, Jonathan B.

Subjects

*PEPTIDE receptors, *PATTERN perception receptors, *PHARMACEUTICAL chemistry, *BIOLOGICAL assay, *STRUCTURE-activity relationships

Abstract

Formyl peptide receptors (FPRs) comprise a class of chemoattractant pattern recognition receptors, for which several physiological functions like host-defences, as well as the regulation of inflammatory responses, have been ascribed. With accumulating evidence that agonism of FPR1/FPR2 can confer pro-resolution of inflammation, increased attention from academia and industry has led to the discovery of new and interesting small-molecule FPR1/FPR2 agonists. Focused attention on the development of appropriate physicochemical and pharmacokinetic profiles is yielding synthesis of new compounds with promising in vivo readouts. This review presents an overview of small-molecule FPR1/FPR2 agonist medicinal chemistry developed over the past 20 years, with a particular emphasis on interrogation in the increasingly sophisticated bioassays which have been developed. [Display omitted] • Targeting formyl peptide receptors (FPRs) is an emerging therapeutic approach for inflammatory disorders. • Current understanding of FPRs related structural biology and biased signalling pharmacology. • This review summarised small-molecule FPR1/FPR2 agonists development over the past 20 years from both academia and industry. • We highlighted specific bioassays and several characterisations of each chemotype. • A constructive perspective of future FPRs agonists development was proposed. [ABSTRACT FROM AUTHOR]

Published

2024

4. Relaxin elicits renoprotective actions accompanied by increasing bile acid levels in streptozotocin-induced diabetic mice.

Author

Leo, Chen Huei, Ou, Jamie Li Min, Ong, Eng Shi, Qin, Cheng Xue, Ritchie, Rebecca H., Parry, Laura J., and Ng, Hooi Hooi

Subjects

*STREPTOZOTOCIN, *BILE acids, *KIDNEY cortex, *RELAXIN, *RENAL fibrosis

Abstract

The peptide hormone relaxin has potent anti-fibrotic and anti-inflammatory properties in various organs, including the kidneys. However, the protective effects of relaxin in the context of diabetic kidney complications remain controversial. Here, we aimed to evaluate the effects of relaxin treatment on key markers of kidney fibrosis, oxidative stress, and inflammation and their subsequent impact on bile acid metabolism in the streptozotocin-induced diabetes mouse model. Male mice were randomly allocated to placebo-treated control, placebo-treated diabetes or relaxin-treated diabetes groups (0.5 mg/kg/d, final 2 weeks of diabetes). After 12 weeks of diabetes or sham, the kidney cortex was harvested for metabolomic and gene expression analyses. Diabetic mice exhibited significant hyperglycaemia and increased circulating levels of creatine, hypoxanthine and trimethylamine N-oxide in the plasma. This was accompanied by increased expression of key markers of oxidative stress (Txnip), inflammation (Ccl2 and Il6) and fibrosis (Col1a1, Mmp2 and Fn1) in the diabetic kidney cortex. Relaxin treatment for the final 2 weeks of diabetes significantly reduced these key markers of renal fibrosis, inflammation, and oxidative stress in diabetic mice. Furthermore, relaxin treatment significantly increased the levels of bile acid metabolites, deoxycholic acid and sodium glycodeoxycholic acid, which may in part contribute to the renoprotective action of relaxin in diabetes. In summary, this study shows the therapeutic potential of relaxin and that it may be used as an adjunctive treatment for diabetic kidney complications. [ABSTRACT FROM AUTHOR]

Published

2023

5. Capadenoson, a clinically trialed partial adenosine A1 receptor agonist, can stimulate adenosine A2B receptor biased agonism.

Author

Baltos, Jo-Anne, Vecchio, Elizabeth A., Harris, Matthew A., Qin, Cheng Xue, Ritchie, Rebecca H., Christopoulos, Arthur, White, Paul J., and May, Lauren T.

Subjects

*ADENOSINES, *CARDIOVASCULAR disease treatment, *VENTRICULAR remodeling, *HEART cells, *CLINICAL trials

Abstract

The adenosine A 2B receptor (A 2B AR) has been identified as an important therapeutic target in cardiovascular disease, however in vitro and in vivo targeting has been limited by the paucity of pharmacological tools, particularly potent agonists. Interestingly, 2-((6-amino-3,5-dicyano-4-(4-(cyclopropylmethoxy)phenyl)-2-pyridinyl)thio)acetamide (BAY60-6583), a potent and subtype-selective A 2B AR agonist, has the same core structure as 2-amino-6-[[2-(4-chlorophenyl)-1,3-thiazol-4-yl]methylsulfanyl]-4-[4-(2-hydroxyethoxy)phenyl]pyridine-3,5-dicarbonitril (capadenoson). Capadenoson, currently classified as an adenosine A 1 receptor (A 1 AR) partial agonist, has undergone two Phase IIa clinical trials, initially in patients with atrial fibrillation and subsequently in patients with stable angina. Capadenoson has also been shown to decrease cardiac remodeling in an animal model of advanced heart failure and a capadenoson derivative, neladenoson bialanate, recently entered clinical development for the treatment of chronic heart failure. The therapeutic effects of capadenoson are currently thought to be mediated through the A 1 AR. However, the ability of capadenoson to stimulate additional adenosine receptor subtypes, in particular the A 2B AR, has not been rigorously assessed. In this study, we demonstrate that capadenoson does indeed have significant A 2B AR activity in physiologically relevant cells, cardiac fibroblasts and cardiomyocytes, which endogenously express the A 2B AR. Relative to the non-selective adenosine receptor agonist NECA, capadenoson was a biased A 2B AR agonist with a preference for cAMP signal transduction over other downstream mediators in cells with recombinant and endogenous A 2B AR expression. These findings suggest the reclassification of capadenoson as a dual A 1 AR/A 2B AR agonist. Furthermore, a potential A 2B AR contribution should be an important consideration for the future clinical development of capadenoson-like therapeutics, as the A 2B AR can promote cardioprotection and modulate cardiac fibrosis in heart disease. [ABSTRACT FROM AUTHOR]

Published

2017

6. Endothelium-dependent relaxation is impaired in Schlager hypertensive (BPH/2J) mice by region-specific mechanisms in conductance and resistance arteries.

Author

Jelinic, Maria, Jackson, Kristy L., O'Sullivan, Kelly, Singh, Jaideep, Giddy, Thomas, Deo, Minh, Parry, Laura J., Ritchie, Rebecca H., Woodman, Owen L., Head, Geoffrey A., Leo, Chen Huei, and Qin, Cheng Xue

Subjects

*ENDOTHELIUM, *VASCULAR resistance, *ANGIOTENSIN receptors, *BLOOD pressure, *MESENTERIC artery, *HYPERTENSION, *ARTERIAL diseases

Abstract

Endothelial dysfunction and arterial stiffness are hallmarks of hypertension, and major risk factors for cardiovascular disease. BPH/2J (Schlager) mice are a genetic model of spontaneous hypertension, but little is known about the vascular pathophysiology of these mice and the region-specific differences between vascular beds. Therefore, this study compared the vascular function and structure of large conductance (aorta and femoral) and resistance (mesenteric) arteries of BPH/2J mice with their normotensive BPN/2J counterparts. Blood pressure was measured in BPH/2J and BPN/3J mice via pre-implanted radiotelemetry probes. At endpoint, vascular function and passive mechanical wall properties were assessed using wire and pressure myography, qPCR and histology. Mean arterial blood pressure was elevated in BPH/2J mice compared to BPN/3J controls. Endothelium-dependent relaxation to acetylcholine was attenuated in both the aorta and mesenteric arteries of BPH/2J mice, but through different mechanisms. In the aorta, hypertension reduced the contribution of prostanoids. Conversely, in the mesenteric arteries, hypertension reduced the contribution of both nitric oxide and endothelium-dependent hyperpolarization. Hypertension reduced volume compliance in both femoral and mesenteric arteries, but hypertrophic inward remodelling was only observed in the mesenteric arteries of BPH/2J mice. This is the first comprehensive investigation of vascular function and structural remodelling in BPH/2J mice. Overall, hypertensive BPH/2J mice exhibited endothelial dysfunction and adverse vascular remodelling in the macro- and microvasculature, underpinned by distinct region-specific mechanisms. This highlights BPH/2J mice as a highly suitable model for evaluating novel therapeutics to treat hypertension-associated vascular dysfunction. Schlager (BPH/2J) mice are a robust model of hypertensive vascular disease. The aorta, femoral and mesenteric arteries of hypertensive BPH/2J mice were compared to those of normotensive BPN/3J controls. In the aorta, hypertension reduced endothelium-dependent relaxation (reduced contribution of prostanoids (PGs)) and increased contraction to phenylephrine (PE; with reduced α 1 -adrenoreceptor (Adra1a) and increased α 2 -adrenoreceptor (Adra2a) gene expression). In femoral arteries, hypertension reduced volume compliance and elastin content without geometric remodelling. In mesenteric arteries, hypertension reduced endothelium-dependent relaxation (reduced contribution of nitric oxide (NO) and endothelium-dependent hyperpolarization (EDH)), increased contraction to angiotensin II (Ang II; with reduced angiotensin receptor type 1a (Agtr1a) expression), increased axial stiffness and reduced volume compliance (associated with hypertrophic inward remodelling). [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2023

7. Novel strategies to promote resolution of inflammation to treat lower extremity artery disease.

Author

Zhang, Qian, Li, Fengyang, Ritchie, Rebecca H., Woodman, Owen L., Zhou, Xiaojun, and Qin, Cheng Xue

Subjects

*ARTERIAL diseases, *TISSUE remodeling, *G protein coupled receptors, *ATHEROSCLEROTIC plaque, *INFLAMMATION, *HEALING

Abstract

Lower extremity artery disease (LEAD) is a chronic inflammatory disease that occurs when atherosclerotic plaques form in the lower extremities, which may lead to amputation if not manged properly. Given clinical standardcare (pharmacological and surgical) have limited efficacy in LEAD, developing novel strategies to manage LEAD remains an unmet clinical need. Given that active resolution of inflammation is essential to facilitate tissue healing and repair, failure to resolve inflammation may lead to chronic inflammation, dysregulated cellular homeostasis and adverse tissue remodeling. Several studies have demonstrated the importance of the balance between endogenous pro-resolving mediators and pro-inflammatory factors. There is growing evidence to suggest endogenous pro-resolving mediators engage with pro-resolving G-protein-coupled receptors to reduce the initiation and progression of inflammatory responses and to increase therapeutic angiogenesis in LEAD. Here, we highlight the mechanisms and the consequences of resolved inflammation, and the therapeutic potential of endogenous pro-resolving mediators-based strategy for this devastating disease. [ABSTRACT FROM AUTHOR]

Published

2022

8. Current state and future perspective of cardiovascular medicines derived from natural products.

Author

Zhao, Chunhui, Li, Sen, Zhang, Junhong, Huang, Yuanyun, Zhang, Luoqi, Zhao, Feng, Du, Xia, Hou, Jinli, Zhang, Tong, Shi, Chenjing, Wang, Ping, Huo, Ruili, Woodman, Owen L., Qin, Cheng Xue, Xu, Haiyu, and Huang, Luqi

Subjects

*NATURAL products, *CHINESE medicine, *CARDIOVASCULAR agents, *SYNTHETIC biology, *BIODIVERSITY, *DRUGS

Abstract

The contribution of natural products (NPs) to cardiovascular medicine has been extensively documented, and many have been used for centuries. Cardiovascular disease (CVD) is the leading cause of morbidity and mortality worldwide. Over the past 40 years, approximately 50% of newly developed cardiovascular drugs were based on NPs, suggesting that NPs provide essential skeletal structures for the discovery of novel medicines. After a period of lower productivity since the 1990s, NPs have recently regained scientific and commercial attention, leveraging the wealth of knowledge provided by multi-omics, combinatorial biosynthesis, synthetic biology, integrative pharmacology, analytical and computational technologies. In addition, as a crucial part of complementary and alternative medicine, Traditional Chinese Medicine has increasingly drawn attention as an important source of NPs for cardiovascular drug discovery. Given their structural diversity and biological activity NPs are one of the most valuable sources of drugs and drug leads. In this review, we briefly described the characteristics and classification of NPs in CVDs. Then, we provide an up to date summary on the therapeutic potential and the underlying mechanisms of action of NPs in CVDs, and the current view and future prospect of developing safer and more effective cardiovascular drugs based on NPs. Unlabelled Image • Characteristics and classification of natural products in cardiovascular medicine • Therapeutic applications and mechanisms of actions of natural product-derived cardiovascular medicine. • Integrative pharmacology approach of Traditional Chinese Medicine against cardiovascular diseases. • Geographical distribution and biosynthesis of key natural product for cardiovascular medicine. [ABSTRACT FROM AUTHOR]

Published

2020