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4. Biased receptor signalling and intracellular trafficking profiles of structurally distinct formylpeptide receptor 2 agonists.

Author

Peng, Cheng, Vecchio, Elizabeth A., Nguyen, Anh T. N., De Seram, Mia, Tang, Ruby, Keov, Peter, Woodman, Owen L., Chen, Yung‐Chih, Baell, Jonathan, May, Lauren T., Zhao, Peishen, Ritchie, Rebecca H., and Qin, Cheng Xue

Subjects
SECOND messengers (Biochemistry), TRAFFIC signs & signals, LIGANDS (Biochemistry), G proteins, MOLECULAR docking
Abstract

Background: There is increasing interest in developing FPR2 agonists (compound 43, ACT‐389949 and BMS‐986235) as potential pro‐resolving therapeutics, with ACT‐389949 and BMS‐986235 having entered phase I clinical development. FPR2 activation leads to diverse downstream outputs. ACT‐389949 was observed to cause rapid tachyphylaxis, while BMS‐986235 and compound 43 induced cardioprotective effects in preclinical models. We aim to characterise the differences in ligand‐receptor engagement and downstream signalling and trafficking bias profile. Experimental Approach: Concentration‐response curves to G protein dissociation, β‐arrestin recruitment, receptor trafficking and second messenger signalling were generated using FPR2 ligands (BMS‐986235, ACT‐389949, compound 43 and WKYMVm), in HEK293A cells. Log(τ/KA) was obtained from the operational model for bias analysis using WKYMVm as a reference ligand. Docking of FPR2 ligands into the active FPR2 cryoEM structure (PDBID: 7T6S) was performed using ICM pro software. Key Results: Bias analysis revealed that WKYMVm and ACT‐389949 shared a very similar bias profile. In comparison, BMS‐986235 and compound 43 displayed approximately 5‐ to 50‐fold bias away from β‐arrestin recruitment and trafficking pathways, while being 35‐ to 60‐fold biased towards cAMP inhibition and pERK1/2. Molecular docking predicted key amino acid interactions at the FPR2 shared between WKYMVm and ACT‐389949, but not with BMS‐986235 and compound 43. Conclusion and Implications: In vitro characterisation demonstrated that WKYMVm and ACT‐389949 differ from BMS‐986235 and compound 43 in their signalling and protein coupling profile. This observation may be explained by differences in the ligand‐receptor interactions. In vitro characterisation provided significant insights into identifying the desired bias profile for FPR2‐based pharmacotherapy. [ABSTRACT FROM AUTHOR]

Published
2024
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5. Novel formylpeptide receptor 1/2 agonist limits hypertension-induced cardiovascular damage.

Author

Singh, Jaideep, Jackson, Kristy L, Fang, Haoyun, Gumanti, Audrey, Claridge, Bethany, Tang, Feng Shii, Kiriazis, Helen, Salimova, Ekaterina, Parker, Alex M, Nowell, Cameron, Woodman, Owen L, Greening, David W, Ritchie, Rebecca H, Head, Geoffrey A, and Qin, Cheng Xue

Subjects
ANGIOTENSIN II, ARTERIAL calcification, CARDIAC hypertrophy, HEART fibrosis, INVECTIVE
Abstract

Aims Formylpeptide receptors (FPRs) play a critical role in the regulation of inflammation, an important driver of hypertension-induced end-organ damage. We have previously reported that the biased FPR small-molecule agonist, compound17b (Cmpd17b), is cardioprotective against acute, severe inflammatory insults. Here, we reveal the first compelling evidence of the therapeutic potential of this novel FPR agonist against a longer-term, sustained inflammatory insult, i.e. hypertension-induced end-organ damage. The parallels between the murine and human hypertensive proteome were also investigated. Methods and results The hypertensive response to angiotensin II (Ang II, 0.7 mg/kg/day, s.c.) was attenuated by Cmpd17b (50 mg/kg/day, i.p.). Impairments in cardiac and vascular function assessed via echocardiography were improved by Cmpd17b in hypertensive mice. This functional improvement was accompanied by reduced cardiac and aortic fibrosis and vascular calcification. Cmpd17b also attenuated Ang II-induced increased cardiac mitochondrial complex 2 respiration. Proteomic profiling of cardiac and aortic tissues and cells, using label-free nano-liquid chromatography with high-sensitivity mass spectrometry, detected and quantified ∼6000 proteins. We report hypertension-impacted protein clusters associated with dysregulation of inflammatory, mitochondrial, and calcium responses, as well as modified networks associated with cardiovascular remodelling, contractility, and structural/cytoskeletal organization. Cmpd17b attenuated hypertension-induced dysregulation of multiple proteins in mice, and of these, ∼110 proteins were identified as similarly dysregulated in humans suffering from adverse aortic remodelling and cardiac hypertrophy. Conclusion We have demonstrated, for the first time, that the FPR agonist Cmpd17b powerfully limits hypertension-induced end-organ damage, consistent with proteome networks, supporting development of pro-resolution FPR-based therapeutics for treatment of systemic hypertension complications. [ABSTRACT FROM AUTHOR]

Published
2024
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6. The small‐molecule formyl peptide receptor biased agonist, compound 17b, is a vasodilator and anti‐inflammatory in mouse precision‐cut lung slices.

Author

Studley, William R., Lamanna, Emma, Martin, Katherine A., Nold‐Petry, Claudia A., Royce, Simon G., Woodman, Owen L., Ritchie, Rebecca H., Qin, Cheng Xue, and Bourke, Jane E.

Subjects
PEPTIDE receptors, PULMONARY arterial hypertension, NITRIC-oxide synthases, LUNGS, VASCULAR remodeling, G protein coupled receptors
Abstract

Background and Purpose: Pulmonary arterial hypertension (PAH), a rare fatal disorder characterised by inflammation, vascular remodelling and vasoconstriction. Current vasodilator therapies reduce pulmonary arterial pressure but not mortality. The G‐protein coupled formyl peptide receptors (FPRs) mediates vasodilatation and resolution of inflammation, actions possibly beneficial in PAH. We investigated dilator and anti‐inflammatory effects of the FPR biased agonist compound 17b in pulmonary vasculature using mouse precision‐cut lung slices (PCLS). Experimental Approach: PCLS from 8‐week‐old male and female C57BL/6 mice, intrapulmonary arteries were pre‐contracted with 5‐HT for concentration–response curves to compound 17b and 43, and standard‐of‐care drugs, sildenafil, iloprost and riociguat. Compound 17b‐mediated relaxation was assessed with FPR antagonists or inhibitors and in PCLS treated with TNF‐α or LPS. Cytokine release from TNF‐α‐ or LPS‐treated PCLS ± compound 17b was measured. Key Results: Compound 17b elicited concentration‐dependent vasodilation, with potencies of iloprost > compound 17b = riociguat > compound 43 = sildenafil. Compound 17b was inhibited by the FPR1 antagonist cyclosporin H but not by soluble guanylate cyclase, nitric oxide synthase or cyclooxygenase inhibitors. Under inflammatory conditions, the efficacy and potency of compound 17b were maintained, while iloprost and sildenafil were less effective. Additionally, compound 17b inhibited secretion of PAH‐relevant cytokines via FPR2. Conclusions and Implications: Vasodilation to compound 17b but not standard‐of‐care vasodilators, is maintained under inflammatory conditions, with additional inhibition of PAH‐relevant cytokine release. This provides the first evidence that targeting FPR, with biased agonist, simultaneously targets vascular function and inflammation, supporting the development of FPR‐based pharmacotherapy to treat PAH. LINKED ARTICLES: This article is part of a themed issue Therapeutic Targeting of G Protein‐Coupled Receptors: hot topics from the Australasian Society of Clinical and Experimental Pharmacologists and Toxicologists 2021 Virtual Annual Scientific Meeting. To view the other articles in this section visit http://onlinelibrary.wiley.com/doi/10.1111/bph.v181.14/issuetoc [ABSTRACT FROM AUTHOR]

Published
2024
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7. The pro‐resolving mediator, annexin A1 regulates blood pressure, and age‐associated changes in cardiovascular function and remodeling

Author

Singh, Jaideep, primary, Jackson, Kristy L., additional, Tang, Feng Shii, additional, Fu, Ting, additional, Nowell, Cameron, additional, Salimova, Ekaterina, additional, Kiriazis, Helen, additional, Ritchie, Rebecca H., additional, Head, Geoffrey A., additional, Woodman, Owen L., additional, and Qin, Cheng Xue, additional

Published
2024
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10. Deep multi-omic profiling reveals extensive mitochondrial remodeling driven by glycemia in early diabetic kidney disease

Author

Granata, Cesare, primary, Thallas-Bonke, Vicki, additional, Caruana, Nikeisha j, additional, Huynh, Kevin, additional, Qin, Cheng Xue, additional, Laskowski, Adrienne, additional, Snelson, Matthew, additional, Anthonisz, Jarryd, additional, Jap, Edwina, additional, Ramm, Georg, additional, Cooper, Mark E, additional, Meikle, Peter, additional, Stroud, David A, additional, Ritchie, Rebecca H, additional, and Coughlan, Melinda T, additional

Published
2023
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12. Endothelium-dependent relaxation is impaired in Schlager hypertensive (BPH/2J) mice by region-specific mechanisms in conductance and resistance arteries

Author

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

Published
2023
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13. Novel Role for the AnxA1-Fpr2/ALX Signaling Axis as a Key Regulator of Platelet Function to Promote Resolution of Inflammation

Author

Senchenkova, Elena Y., Ansari, Junaid, Becker, Felix, Vital, Shantel A., Al-Yafeai, Zaki, Sparkenbaugh, Erica M., Pawlinski, Rafal, Stokes, Karen Y., Carroll, Jennifer L., Dragoi, Ana-Maria, Qin, Cheng Xue, Ritchie, Rebecca H., Sun, Hai, Cuellar-Saenz, Hugo H., Rubinstein, Mara R., Han, Yiping W., Orr, A. Wayne, Perretti, Mauro, Granger, D. Neil, and Gavins, Felicity N.E.

Published
2019
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14. A high-sucrose diet exacerbates the left ventricular phenotype in a high fat-fed streptozotocin rat model of diabetic cardiomyopathy

Author

Velagic, Anida, primary, Li, Mandy, additional, Deo, Minh, additional, Li, Jasmin Chendi, additional, Kiriazis, Helen, additional, Donner, Daniel G., additional, Anderson, Dovile, additional, De Blasio, Miles J., additional, Woodman, Owen L., additional, Kemp-Harper, Barbara K., additional, Qin, Cheng Xue, additional, and Ritchie, Rebecca H., additional

Published
2023
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18. Cardioprotective actions of nitroxyl donor Angeli's salt are preserved in the diabetic heart and vasculature in the face of nitric oxide resistance

Author

Velagic, Anida, primary, Li, Jasmin Chendi, additional, Qin, Cheng Xue, additional, Li, Mandy, additional, Deo, Minh, additional, Marshall, Sarah A., additional, Anderson, Dovile, additional, Woodman, Owen L., additional, Horowitz, John D., additional, Kemp‐Harper, Barbara K., additional, and Ritchie, Rebecca H., additional

Published
2022
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19. Endothelium-Dependent Relaxation is Impaired in Schlager Hypertensive (BPH/2J) Mice by Region-Specific Mechanisms in Conductance and Resistance Arteries

Author

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

Published
2022
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23. Corrigendum: Characterising an Alternative Murine Model of Diabetic Cardiomyopathy

Author

Tate, Mitchel, primary, Prakoso, Darnel, additional, Willis, Andrew M., additional, Peng, Cheng, additional, Deo, Minh, additional, Qin, Cheng Xue, additional, Walsh, Jesse L., additional, Nash, David M., additional, Cohen, Charles D., additional, Rofe, Alex K., additional, Sharma, Arpeeta, additional, Kiriazis, Helen, additional, Donner, Daniel G., additional, De Haan, Judy B., additional, Watson, Anna M. D., additional, De Blasio, Miles J., additional, and Ritchie, Rebecca H., additional

Published
2021
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27. Current state and future perspective of cardiovascular medicines derived from natural products

Author

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

Published
2020
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30. Annexin‐A1 deficiency exacerbates pathological remodelling of the mesenteric vasculature in insulin‐resistant, but not insulin‐deficient, mice

Author

Jelinic, Maria, primary, Kahlberg, Nicola, additional, Leo, Chen Huei, additional, Ng, Hooi Hooi, additional, Rosli, Sarah, additional, Deo, Minh, additional, Li, Mandy, additional, Finlayson, Siobhan, additional, Walsh, Jesse, additional, Parry, Laura J., additional, Ritchie, Rebecca H., additional, and Qin, Cheng Xue, additional

Published
2020
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32. Nitric Oxide Resistance, Induced in the Myocardium by Diabetes, Is Circumvented by the Nitric Oxide Redox Sibling, Nitroxyl

Author

Qin, Cheng Xue, primary, Anthonisz, Jarryd, additional, Leo, Chen Huei, additional, Kahlberg, Nicola, additional, Velagic, Anida, additional, Li, Mandy, additional, Jap, Edwina, additional, Woodman, Owen L., additional, Parry, Laura J., additional, Horowitz, John D., additional, Kemp-Harper, Barbara K., additional, and Ritchie, Rebecca H., additional

Published
2020
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33. Characterising an Alternative Murine Model of Diabetic Cardiomyopathy

Author

Tate, Mitchel, primary, Prakoso, Darnel, additional, Willis, Andrew M., additional, Peng, Cheng, additional, Deo, Minh, additional, Qin, Cheng Xue, additional, Walsh, Jesse L., additional, Nash, David M., additional, Cohen, Charles D., additional, Rofe, Alex K., additional, Sharma, Arpeeta, additional, Kiriazis, Helen, additional, Donner, Daniel G., additional, De Haan, Judy B., additional, Watson, Anna M. D., additional, De Blasio, Miles J., additional, and Ritchie, Rebecca H., additional

Published
2019
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34. Substituted Pyridazin-3(2H)-ones as Highly Potent and Biased Formyl Peptide Receptor Agonists

Author

Deora, Girdhar Singh, primary, Qin, Cheng Xue, additional, Vecchio, Elizabeth A., additional, Debono, Aaron J., additional, Priebbenow, Daniel L., additional, Brady, Ryan M., additional, Beveridge, Julia, additional, Teguh, Silvia C., additional, Deo, Minh, additional, May, Lauren T., additional, Krippner, Guy, additional, Ritchie, Rebecca H., additional, and Baell, Jonathan B., additional

Published
2019
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35. Cardioprotective Actions of the Annexin-A1 N-Terminal Peptide, Ac2-26, Against Myocardial Infarction

Author

Qin, Cheng Xue, primary, Rosli, Sarah, additional, Deo, Minh, additional, Cao, Nga, additional, Walsh, Jesse, additional, Tate, Mitchel, additional, Alexander, Amy E., additional, Donner, Daniel, additional, Horlock, Duncan, additional, Li, Renming, additional, Kiriazis, Helen, additional, Lee, Man K. S., additional, Bourke, Jane E., additional, Yang, Yuan, additional, Murphy, Andrew J., additional, Du, Xiao-Jun, additional, Gao, Xiao Ming, additional, and Ritchie, Rebecca H., additional

Published
2019
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36. Author Correction: Endogenous Annexin-A1 Regulates Haematopoietic Stem Cell Mobilisation and Inflammatory Response Post Myocardial Infarction in Mice In Vivo

Author

Qin, Cheng Xue, primary, Finlayson, Siobhan B., additional, Al-Sharea, Annas, additional, Tate, Mitchel, additional, De Blasio, Miles J., additional, Deo, Minh, additional, Rosli, Sarah, additional, Prakoso, Darnel, additional, Thomas, Colleen J., additional, Kiriazis, Helen, additional, Gould, Eleanor, additional, Yang, Yuan H., additional, Morand, Eric F., additional, Perretti, Mauro, additional, Murphy, Andrew J., additional, Du, Xiao-Jun, additional, Gao, Xiao-Ming, additional, and Ritchie, Rebecca H., additional

Published
2018
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38. Diastolic dysfunction is more apparent in STZ-induced diabetic female mice, despite less pronounced hyperglycemia

Author

Chandramouli, Chanchal, primary, Reichelt, Melissa E., additional, Curl, Claire L., additional, Varma, Upasna, additional, Bienvenu, Laura A., additional, Koutsifeli, Parisa, additional, Raaijmakers, Antonia J. A., additional, De Blasio, Miles J., additional, Qin, Cheng Xue, additional, Jenkins, Alicia J., additional, Ritchie, Rebecca H., additional, Mellor, Kimberley M., additional, and Delbridge, Lea M. D., additional

Published
2018
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39. Endogenous Annexin-A1 Regulates Haematopoietic Stem Cell Mobilisation and Inflammatory Response Post Myocardial Infarction in Mice In Vivo

Author

Qin, Cheng Xue, primary, Finlayson, Siobhan B., additional, Al-Sharea, Annas, additional, Tate, Mitchel, additional, De Blasio, Miles J., additional, Deo, Minh, additional, Rosli, Sarah, additional, Prakoso, Darnel, additional, Thomas, Colleen J., additional, Kiriazis, Helen, additional, Gould, Eleanor, additional, Yang, Yuan H., additional, Morand, Eric F., additional, Perretti, Mauro, additional, Murphy, Andrew J., additional, Du, Xiao-Jun, additional, Gao, Xiao-Ming, additional, and Ritchie, Rebecca H., additional

Published
2017
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41. Small-molecule-biased formyl peptide receptor agonist compound 17b protects against myocardial ischaemia-reperfusion injury in mice

Author

Qin, Cheng Xue, primary, May, Lauren T., additional, Li, Renming, additional, Cao, Nga, additional, Rosli, Sarah, additional, Deo, Minh, additional, Alexander, Amy E., additional, Horlock, Duncan, additional, Bourke, Jane E., additional, Yang, Yuan H., additional, Stewart, Alastair G., additional, Kaye, David M., additional, Du, Xiao-Jun, additional, Sexton, Patrick M., additional, Christopoulos, Arthur, additional, Gao, Xiao-Ming, additional, and Ritchie, Rebecca H., additional

Published
2017
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42. Cardioprotective Actions of the Annexin-A1 N-Terminal Peptide, Ac2-26, Against Myocardial Infarction.

Author

Qin, Cheng Xue, Rosli, Sarah, Deo, Minh, Cao, Nga, Walsh, Jesse, Tate, Mitchel, Alexander, Amy E., Donner, Daniel, Horlock, Duncan, Li, Renming, Kiriazis, Helen, Lee, Man K. S., Bourke, Jane E., Yang, Yuan, Murphy, Andrew J., Du, Xiao-Jun, Gao, Xiao Ming, and Ritchie, Rebecca H.

Subjects
HEART fibrosis, PEPTIDE receptors, REPERFUSION, MYOCARDIAL infarction, CORONARY disease
Abstract

The anti-inflammatory, pro-resolving annexin-A1 protein acts as an endogenous brake against exaggerated cardiac necrosis, inflammation, and fibrosis following myocardial infarction (MI) in vivo. Little is known, however, regarding the cardioprotective actions of the N-terminal-derived peptide of annexin A1, Ac2-26, particularly beyond its anti-necrotic actions in the first few hours after an ischemic insult. In this study, we tested the hypothesis that exogenous Ac2-26 limits cardiac injury in vitro and in vivo. Firstly, we demonstrated that Ac2-26 limits cardiomyocyte death both in vitro and in mice subjected to ischemia-reperfusion (I-R) injury in vivo (Ac2-26, 1 mg/kg, i.v. just prior to post-ischemic reperfusion). Further, Ac2-26 (1 mg/kg i.v.) reduced cardiac inflammation (after 48 h reperfusion), as well as both cardiac fibrosis and apoptosis (after 7-days reperfusion). Lastly, we investigated whether Ac2-26 preserved cardiac function after MI. Ac2-26 (1 mg/kg/day s.c., osmotic pump) delayed early cardiac dysfunction 1 week post MI, but elicited no further improvement 4 weeks after MI. Taken together, our data demonstrate the first evidence that Ac2-26 not only preserves cardiomyocyte survival in vitro , but also offers cardioprotection beyond the first few hours after an ischemic insult in vivo. Annexin-A1 mimetics thus represent a potential new therapy to improve cardiac outcomes after MI. [ABSTRACT FROM AUTHOR]

Published
2019
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44. 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
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45. A high-sucrose diet exacerbates the left ventricular phenotype in a high fat-fed streptozotocin rat model of diabetic cardiomyopathy.

Author

Velagic A, Li M, Deo M, Li JC, Kiriazis H, Donner DG, Anderson D, De Blasio MJ, Woodman OL, Kemp-Harper BK, Qin CX, and Ritchie RH

Subjects
Rats, Male, Animals, Streptozocin adverse effects, Rats, Sprague-Dawley, Diet, High-Fat adverse effects, Phenotype, Diabetic Cardiomyopathies, Diabetes Mellitus, Type 2 chemically induced, Diabetes Mellitus, Experimental chemically induced, Ventricular Dysfunction, Left, Heart Failure
Abstract

Left ventricular (LV) dysfunction is an early, clinically detectable sign of cardiomyopathy in type 2 diabetes mellitus (T2DM) that precedes the development of symptomatic heart failure. Preclinical models of diabetic cardiomyopathy are essential to develop therapies that may prevent or delay the progression of heart failure. This study examined the molecular, structural, and functional cardiac phenotype of two rat models of T2DM induced by a high-fat diet (HFD) with a moderate- or high-sucrose content (containing 88.9 or 346 g/kg sucrose, respectively), plus administration of low-dose streptozotocin (STZ). At 8 wk of age, male Sprague-Dawley rats commenced a moderate- or high-sucrose HFD. Two weeks later, rats received low-dose STZ (35 mg/kg ip for 2 days) and remained on their respective diets. LV function was assessed by echocardiography 1 wk before end point. At 22 wk of age, blood and tissues were collected postmortem. Relative to chow-fed sham rats, diabetic rats on a moderate- or high-sucrose HFD displayed cardiac reactive oxygen species dysregulation, perivascular fibrosis, and impaired LV diastolic function. The diabetes-induced impact on LV adverse remodeling and diastolic dysfunction was more apparent when a high-sucrose HFD was superimposed on STZ. In conclusion, a high-sucrose HFD in combination with low-dose STZ produced a cardiac phenotype that more closely resembled T2DM-induced cardiomyopathy than STZ diabetic rats subjected to a moderate-sucrose HFD. NEW & NOTEWORTHY Left ventricular dysfunction and adverse remodeling were more pronounced in diabetic rats that received low-dose streptozotocin (STZ) and a high-sucrose high-fat diet (HFD) compared with those on a moderate-sucrose HFD in combination with STZ. Our findings highlight the importance of sucrose content in diet composition, particularly in preclinical studies of diabetic cardiomyopathy, and demonstrate that low-dose STZ combined with a high-sucrose HFD is an appropriate rodent model of cardiomyopathy in type 2 diabetes.

Published
2023
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46. Therapeutic Potential of Lipoxin A 4 in Chronic Inflammation: Focus on Cardiometabolic Disease.

Author

Fu T, Mohan M, Brennan EP, Woodman OL, Godson C, Kantharidis P, Ritchie RH, and Qin CX

Abstract

Several studies have shown that failure to resolve inflammation may contribute to the progression of many chronic inflammatory disorders. It has been suggested targeting the resolution of inflammation might be a novel therapeutic approach for chronic inflammatory diseases, including inflammatory bowel disease, diabetic complications, and cardiometabolic disease. Lipoxins [LXs] are a class of endogenously generated mediators that promote the resolution of inflammation. Biological actions of LXs include inhibition of neutrophil infiltration, promotion of macrophage polarization, increase of macrophage efferocytosis, and restoration of tissue homeostasis. Recently, several studies have demonstrated that LXs and synthetic analogues protect tissues from acute and chronic inflammation. The mechanism includes down-regulation of pro-inflammatory cytokines and chemokines (e.g., interleukin-1β and tumor necrosis factor-α), inhibition of the activation of the master pro-inflammatory pathway (e.g., nuclear factor κ-light-chain-enhancer of activated B cells pathway) and increased release of the pro-resolving cytokines (e.g., interleukin-10). Three generations of LXs analogues are well described in the literature, and more recently a fourth generation has been generated that appears to show enhanced potency. In this review, we will briefly discuss the potential therapeutic opportunity provided by lipoxin A 4 as a novel approach to treat chronic inflammatory disorders, focusing on cardiometabolic disease and the current drug development in this area., Competing Interests: The authors declare no competing financial interest., (Copyright © 2020 American Chemical Society.)

Published
2020
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47. Substituted Pyridazin-3(2 H)-ones as Highly Potent and Biased Formyl Peptide Receptor Agonists.

Author

Deora GS, Qin CX, Vecchio EA, Debono AJ, Priebbenow DL, Brady RM, Beveridge J, Teguh SC, Deo M, May LT, Krippner G, Ritchie RH, and Baell JB

Subjects
Blood Proteins metabolism, Calcium Signaling drug effects, Drug Discovery, HL-60 Cells, Humans, Inflammation drug therapy, Inflammation metabolism, MAP Kinase Signaling System drug effects, Phosphorylation drug effects, Protein Binding, Receptors, Lipoxin, Structure-Activity Relationship, Pyrazines chemical synthesis, Pyrazines pharmacology, Receptors, Formyl Peptide agonists
Abstract

Herein we describe the development of a focused series of functionalized pyridazin-3(2 H)-one-based formyl peptide receptor (FPR) agonists that demonstrate high potency and biased agonism. The compounds described demonstrated biased activation of prosurvival signaling, ERK1/2 phosphorylation, through diminution of the detrimental FPR1/2-mediated intracellular calcium (Ca i 2+ ) mobilization. Compound 50 showed an EC 50 of 0.083 μM for phosphorylation of ERK1/2 and an approximate 20-fold bias away from Ca i 2+ mobilization at the hFPR1.

Published
2019
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48. Cardioprotective Actions of the Annexin-A1 N-Terminal Peptide, Ac 2-26 , Against Myocardial Infarction.

Author

Qin CX, Rosli S, Deo M, Cao N, Walsh J, Tate M, Alexander AE, Donner D, Horlock D, Li R, Kiriazis H, Lee MKS, Bourke JE, Yang Y, Murphy AJ, Du XJ, Gao XM, and Ritchie RH

Abstract

The anti-inflammatory, pro-resolving annexin-A1 protein acts as an endogenous brake against exaggerated cardiac necrosis, inflammation, and fibrosis following myocardial infarction (MI) in vivo . Little is known, however, regarding the cardioprotective actions of the N-terminal-derived peptide of annexin A1, Ac 2-26 , particularly beyond its anti-necrotic actions in the first few hours after an ischemic insult. In this study, we tested the hypothesis that exogenous Ac 2-26 limits cardiac injury in vitro and in vivo. Firstly, we demonstrated that Ac 2-26 limits cardiomyocyte death both in vitro and in mice subjected to ischemia-reperfusion (I-R) injury in vivo (Ac 2-26, 1 mg/kg, i.v. just prior to post-ischemic reperfusion). Further, Ac 2-26 (1 mg/kg i.v.) reduced cardiac inflammation (after 48 h reperfusion), as well as both cardiac fibrosis and apoptosis (after 7-days reperfusion). Lastly, we investigated whether Ac 2-26 preserved cardiac function after MI. Ac 2-26 (1 mg/kg/day s.c., osmotic pump) delayed early cardiac dysfunction 1 week post MI, but elicited no further improvement 4 weeks after MI. Taken together, our data demonstrate the first evidence that Ac 2-26 not only preserves cardiomyocyte survival in vitro , but also offers cardioprotection beyond the first few hours after an ischemic insult in vivo . Annexin-A1 mimetics thus represent a potential new therapy to improve cardiac outcomes after MI.

Published
2019
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