Your search keyword '"Julie R. McMullen"' showing total 199 results

1. Sex-specific regulation of the cardiac transcriptome by the protein phosphatase 2A regulatory subunit B55α

Author

Nicola M. Sergienko, Adam J. Trewin, Helen Kiriazis, Antonia J. A. Raaijmakers, Daniel G. Donner, Victoria C. Garside, Kelly A. Smith, James R. Bell, Kimberley M. Mellor, Lea M. D. Delbridge, Julie R. McMullen, and Kate L. Weeks

Subjects

Specialties of internal medicine, RC581-951

Abstract

Abstract Protein phosphatase 2A (PP2A) regulatory subunit B55α has been implicated in the transcriptional regulation of cardiac growth and fibrosis by suppressing HDAC5/MEF2 signalling in cardiomyocytes. We created and characterised two mouse models with global or cardiomyocyte-specific disruption of the gene encoding B55α (Ppp2r2a) to conduct the first detailed exploration of B55α in the heart. Global homozygous B55α knockout mice died in utero, while heterozygous mice had thinner left ventricular walls at 12 months, an effect more pronounced in males. At 10–12 weeks of age, cardiomyocyte-specific B55α knockout mice displayed normal cardiac morphology with increased left ventricular collagen deposition, identifying B55α as a negative regulator of cardiac fibrosis. Gene expression analyses demonstrated extensive remodelling of the cardiac transcriptome in male but not female mice, revealing a sexually dimorphic role for B55α in cardiac transcriptional regulation. These findings provide a basis for future work investigating B55α in cardiac stress settings.

Published

2024

2. Deletion of the muscle enriched lncRNA Oip5os1 induces atrial dysfunction in male mice with diabetes

Author

Aowen Zhuang, Yanie Tan, Yingying Liu, Christine Yang, Helen Kiriazis, Kyah Grigolon, Shannen Walker, Simon T. Bond, Julie R. McMullen, Anna C. Calkin, and Brian G. Drew

Subjects

atrial dysfunction, cardiomyopathy, diabetes, non‐coding RNA, Physiology, QP1-981

Abstract

Abstract Long ncRNAs (lncRNAs) have been shown to play a biological and physiological role in various tissues including the heart. We and others have previously established that the lncRNA Oip5os1 (1700020I14Rik, OIP5‐AS1, Cyrano) is enriched in striated muscles, and its deletion in mice leads to defects in both skeletal and cardiac muscle function. In the present study, we investigated the impact of global Oip5os1 deletion on cardiac function in the setting of streptozotocin (STZ)‐induced diabetes. Specifically, we studied male WT and KO mice with or without diabetes for 24 weeks, and phenotyped animals for metabolic and cardiac endpoints. Independent of genotype, diabetes was associated with left ventricular diastolic dysfunction based on a fall in E'/A' ratio. Deletion of Oip5os1 in a setting of diabetes had no significant impact on ventricular function or ventricular weight, but was associated with left atrial dysfunction (reduced fractional shortening) and myopathy which was associated with anesthesia intolerance and premature death in the majority of KO mice tested during cardiac functional assessment. This atrial phenotype was not observed in WT diabetic mice. The most striking molecular difference was a reduction in the metabolic regulator ERRalpha in the atria of KO mice compared with WT mice. There was also a trend for a reduction in Serca2a. These findings highlight Oip5os1 as a gene of interest in aspects of atrial function in the setting of diabetes, highlighting an additional functional role for this lncRNA in cardiac pathological settings.

Published

2023

3. IGF1–PI3K-induced physiological cardiac hypertrophy: Implications for new heart failure therapies, biomarkers, and predicting cardiotoxicity

Author

Sebastian Bass-Stringer, Celeste M.K. Tai, and Julie R. McMullen

Subjects

Cardiac protection, Cardiotoxicity, Exercise, Heart failure, IGF1, PI3K, Sports, GV557-1198.995, Sports medicine, RC1200-1245

Abstract

Heart failure represents the end point of a variety of cardiovascular diseases. It is a growing health burden and a leading cause of death worldwide. To date, limited treatment options exist for the treatment of heart failure, but exercise has been well-established as one of the few safe and effective interventions, leading to improved outcomes in patients. However, a lack of patient adherence remains a significant barrier in the implementation of exercise-based therapy for the treatment of heart failure. The insulin-like growth factor 1 (IGF1)–phosphoinositide 3-kinase (PI3K) pathway has been recognized as perhaps the most critical pathway for mediating exercised-induced heart growth and protection. Here, we discuss how modulating activity of the IGF1–PI3K pathway may be a valuable approach for the development of therapies that mimic the protective effects of exercise on the heart. We outline some of the promising approaches being investigated that utilize PI3K-based therapy for the treatment of heart failure. We discuss the implications for cardiac pathology and cardiotoxicity that arise in a setting of reduced PI3K activity. Finally, we discuss the use of animal models of cardiac health and disease, and genetic mice with increased or decreased cardiac PI3K activity for the discovery of novel drug targets and biomarkers of cardiovascular disease.

Published

2021

4. A protocol for rapid and parallel isolation of myocytes and non-myocytes from multiple mouse hearts

Author

Gabriella E. Farrugia, Micheal A. McLellan, Kate L. Weeks, Aya Matsumoto, Charles D. Cohen, Crisdion Krstevski, Taylah L. Gaynor, Adam C. Parslow, Julie R. McMullen, and Alexander R. Pinto

Subjects

Cell Biology, Cell isolation, Cell separation/fractionation, Science (General), Q1-390

Abstract

Summary: This protocol features parallel isolation of myocytes and non-myocytes from murine hearts. It was designed with considerations for (1) time required to extract cardiac cells, (2) cell viability, and (3) protocol scalability. Here, a peristaltic pump and 3D-printed elements are combined to perfuse the heart with enzymes to dissociate cells. Myocytes and non-myocytes extracted using this protocol are separated by centrifugation and/or fluorescence-activated cell sorting for use in downstream applications including single-cell omics or other bio-molecular analyses.For complete details on the use and execution of this protocol, please refer to McLellan et al. (2020).

Published

2021

5. Tissue-specific expression of Cas9 has no impact on whole-body metabolism in four transgenic mouse lines

Author

Simon T. Bond, Aowen Zhuang, Christine Yang, Eleanor A.M. Gould, Tim Sikora, Yingying Liu, Ying Fu, Kevin I. Watt, Yanie Tan, Helen Kiriazis, Graeme I. Lancaster, Paul Gregorevic, Darren C. Henstridge, Julie R. McMullen, Peter J. Meikle, Anna C. Calkin, and Brian G. Drew

Subjects

CRISPR, Cas9, Transgenic mice, Metabolism, Tissue specific, Phenotype, Internal medicine, RC31-1245

Abstract

Objective: CRISPR/Cas9 technology has revolutionized gene editing and fast tracked our capacity to manipulate genes of interest for the benefit of both research and therapeutic applications. Whilst many advances have, and continue to be made in this area, perhaps the most utilized technology to date has been the generation of knockout cells, tissues and animals. The advantages of this technology are many fold, however some questions still remain regarding the effects that long term expression of foreign proteins such as Cas9, have on mammalian cell function. Several studies have proposed that chronic overexpression of Cas9, with or without its accompanying guide RNAs, may have deleterious effects on cell function and health. This is of particular concern when applying this technology in vivo, where chronic expression of Cas9 in tissues of interest may promote disease-like phenotypes and thus confound the investigation of the effects of the gene of interest. Although these concerns remain valid, no study to our knowledge has yet to demonstrate this directly. Methods: In this study we used the lox-stop-lox (LSL) spCas9 ROSA26 transgenic (Tg) mouse line to generate four tissue-specific Cas9-Tg models that express Cas9 in the heart, liver, skeletal muscle or adipose tissue. We performed comprehensive phenotyping of these mice up to 20-weeks of age and subsequently performed molecular analysis of their organs. Results: We demonstrate that Cas9 expression in these tissues had no detrimental effect on whole body health of the animals, nor did it induce any tissue-specific effects on whole body energy metabolism, liver health, inflammation, fibrosis, heart function or muscle mass. Conclusions: Our data suggests that these models are suitable for studying the tissue specific effects of gene deletion using the LSL-Cas9-Tg model, and that phenotypes observed utilizing these models can be confidently interpreted as being gene specific, and not confounded by the chronic overexpression of Cas9.

Published

2021

6. In Vivo Inhibition of miR-34a Modestly Limits Cardiac Enlargement and Fibrosis in a Mouse Model with Established Type 1 Diabetes-Induced Cardiomyopathy, but Does Not Improve Diastolic Function

Author

Bianca C. Bernardo, Gunes S. Yildiz, Helen Kiriazis, Claudia A. Harmawan, Celeste M. K. Tai, Rebecca H. Ritchie, and Julie R. McMullen

Subjects

diabetes, microRNA, miR-34a, cardiomyopathy, fibrosis, Cytology, QH573-671

Abstract

MicroRNA 34a (miR-34a) is elevated in the heart in a setting of cardiac stress or pathology, and we previously reported that inhibition of miR-34a in vivo provided protection in a setting of pressure overload-induced pathological cardiac hypertrophy and dilated cardiomyopathy. Prior work had also shown that circulating or cardiac miR-34a was elevated in a setting of diabetes. However, the therapeutic potential of inhibiting miR-34a in vivo in the diabetic heart had not been assessed. In the current study, type 1 diabetes was induced in adult male mice with 5 daily injections of streptozotocin (STZ). At 8 weeks post-STZ, when mice had established type 1 diabetes and diastolic dysfunction, mice were administered locked nucleic acid (LNA)-antimiR-34a or saline-control with an eight-week follow-up. Cardiac function, cardiac morphology, cardiac fibrosis, capillary density and gene expression were assessed. Diabetic mice presented with high blood glucose, elevated liver and kidney weights, diastolic dysfunction, mild cardiac enlargement, cardiac fibrosis and reduced myocardial capillary density. miR-34a was elevated in the heart of diabetic mice in comparison to non-diabetic mice. Inhibition of miR-34a had no significant effect on diastolic function or atrial enlargement, but had a mild effect on preventing an elevation in cardiac enlargement, fibrosis and ventricular gene expression of B-type natriuretic peptide (BNP) and the anti-angiogenic miRNA (miR-92a). A miR-34a target, vinculin, was inversely correlated with miR-34a expression, but other miR-34a targets were unchanged. In summary, inhibition of miR-34a provided limited protection in a mouse model with established type 1 diabetes-induced cardiomyopathy and failed to improve diastolic function. Given diabetes represents a systemic disorder with numerous miRNAs dysregulated in the diabetic heart, as well as other organs, strategies targeting multiple miRNAs and/or earlier intervention is likely to be required.

Published

2022

7. Loss of the long non-coding RNA OIP5-AS1 exacerbates heart failure in a sex-specific manner

Author

Aowen Zhuang, Anna C. Calkin, Shannen Lau, Helen Kiriazis, Daniel G. Donner, Yingying Liu, Simon T. Bond, Sarah C. Moody, Eleanor A.M. Gould, Timothy D. Colgan, Sergio Ruiz Carmona, Michael Inouye, Thomas Q. de Aguiar Vallim, Elizabeth J. Tarling, Gregory A. Quaife-Ryan, James E. Hudson, Enzo R. Porrello, Paul Gregorevic, Xiao-Ming Gao, Xiao-Jun Du, Julie R. McMullen, and Brian G. Drew

Subjects

Cardiovascular medicine, Molecular physiology, Transcriptomics, Science

Abstract

Summary: Long non-coding RNAs (lncRNAs) have been demonstrated to influence numerous biological processes, being strongly implicated in the maintenance and physiological function of various tissues including the heart. The lncRNA OIP5-AS1 (1700020I14Rik/Cyrano) has been studied in several settings; however its role in cardiac pathologies remains mostly uncharacterized. Using a series of in vitro and ex vivo methods, we demonstrate that OIP5-AS1 is regulated during cardiac development in rodent and human models and in disease settings in mice. Using CRISPR, we engineered a global OIP5-AS1 knockout (KO) mouse and demonstrated that female KO mice develop exacerbated heart failure following cardiac pressure overload (transverse aortic constriction [TAC]) but male mice do not. RNA-sequencing of wild-type and KO hearts suggest that OIP5-AS1 regulates pathways that impact mitochondrial function. Thus, these findings highlight OIP5-AS1 as a gene of interest in sex-specific differences in mitochondrial function and development of heart failure.

Published

2021

8. Andersen–Tawil Syndrome Is Associated With Impaired PIP2 Regulation of the Potassium Channel Kir2.1

Author

Reem Handklo-Jamal, Eshcar Meisel, Daniel Yakubovich, Leonid Vysochek, Roy Beinart, Michael Glikson, Julie R. McMullen, Nathan Dascal, Eyal Nof, and Shimrit Oz

Subjects

Andersen–Tawil syndrome, cardiac arrhythmia, PIP2, inward-rectifier potassium channel, slide helix, G-loop, Therapeutics. Pharmacology, RM1-950

Abstract

Andersen–Tawil syndrome (ATS) type-1 is associated with loss-of-function mutations in KCNJ2 gene. KCNJ2 encodes the tetrameric inward-rectifier potassium channel Kir2.1, important to the resting phase of the cardiac action potential. Kir-channels’ activity requires interaction with the agonist phosphatidylinositol-4,5-bisphosphate (PIP2). Two mutations were identified in ATS patients, V77E in the cytosolic N-terminal “slide helix” and M307V in the C-terminal cytoplasmic gate structure “G-loop.” Current recordings in Kir2.1-expressing HEK cells showed that each of the two mutations caused Kir2.1 loss-of-function. Biotinylation and immunostaining showed that protein expression and trafficking of Kir2.1 to the plasma membrane were not affected by the mutations. To test the functional effect of the mutants in a heterozygote set, Kir2.1 dimers were prepared. Each dimer was composed of two Kir2.1 subunits joined with a flexible linker (i.e. WT-WT, WT dimer; WT-V77E and WT-M307V, mutant dimer). A tetrameric assembly of Kir2.1 is expected to include two dimers. The protein expression and the current density of WT dimer were equally reduced to ~25% of the WT monomer. Measurements from HEK cells and Xenopus oocytes showed that the expression of either WT-V77E or WT-M307V yielded currents of only about 20% compared to the WT dimer, supporting a dominant-negative effect of the mutants. Kir2.1 sensitivity to PIP2 was examined by activating the PIP2 specific voltage-sensitive phosphatase (VSP) that induced PIP2 depletion during current recordings, in HEK cells and Xenopus oocytes. PIP2 depletion induced a stronger and faster decay in Kir2.1 mutant dimers current compared to the WT dimer. BGP-15, a drug that has been demonstrated to have an anti-arrhythmic effect in mice, stabilized the Kir2.1 current amplitude following VSP-induced PIP2 depletion in cells expressing WT or mutant dimers. This study underlines the implication of mutations in cytoplasmic regions of Kir2.1. A newly developed calibrated VSP activation protocol enabled a quantitative assessment of changes in PIP2 regulation caused by the mutations. The results suggest an impaired function and a dominant-negative effect of the Kir2.1 variants that involve an impaired regulation by PIP2. This study also demonstrates that BGP-15 may be beneficial in restoring impaired Kir2.1 function and possibly in treating ATS symptoms.

Published

2020

9. Lipidomic Profiles of the Heart and Circulation in Response to Exercise versus Cardiac Pathology: A Resource of Potential Biomarkers and Drug Targets

Author

Yow Keat Tham, Bianca C. Bernardo, Kevin Huynh, Jenny Y.Y. Ooi, Xiao Ming Gao, Helen Kiriazis, Corey Giles, Peter J. Meikle, and Julie R. McMullen

Subjects

Biology (General), QH301-705.5

Abstract

Summary: Exercise-induced heart growth provides protection against cardiovascular disease, whereas disease-induced heart growth leads to heart failure. These distinct forms of growth are associated with different molecular profiles (e.g., mRNAs, non-coding RNAs, and proteins), and targeting differentially regulated genes has therapeutic potential for heart failure. The effects of exercise on the cardiac and circulating lipidomes in comparison to disease are unclear. Lipidomic profiling was performed on hearts and plasma of mice subjected to swim endurance training or a cardiac disease model (moderate or severe pressure overload). Several sphingolipid species and phospholipids containing omega-3/6 fatty acids were distinctly altered in heart and/or plasma with exercise versus pressure overload. A subset of lipids was validated in an independent mouse model with heart failure and atrial fibrillation. This study highlights the adaptations that occur to lipid profiles in response to endurance training versus pathology and provides a resource to investigate potential therapeutic targets and biomarkers. : Tham et al. utilized a HPLC-ESI/MS/MS targeted lipidomics approach to show distinct remodeling of the cardiac and plasma lipidomes in response to exercise in comparison to heart disease stimuli. Differentially altered lipids were validated in a model with heart failure and atrial fibrillation and represent potential biomarkers and drug targets. Keywords: lipids, heart, exercise, physiological hypertrophy, pathological hypertrophy, atrial fibrillation, phospholipids, sphingolipids, biomarkers, treatment

Published

2018

10. PP2A negatively regulates the hypertrophic response by dephosphorylating HDAC2 S394 in the heart

Author

Somy Yoon, Taewon Kook, Hyun-Ki Min, Duk-Hwa Kwon, Young Kuk Cho, Mira Kim, Sera Shin, Hosouk Joung, Seung Hoon Jeong, Sumin Lee, Gaeun Kang, Yunchul Park, Yong Sook Kim, Youngkeun Ahn, Julie R. McMullen, Ulrich Gergs, Joachim Neumann, Kyung Keun Kim, Jungchul Kim, Kwang-Il Nam, Young-Kook Kim, Hyun Kook, and Gwang Hyeon Eom

Subjects

Medicine, Biochemistry, QD415-436

Abstract

Cardiovascular disease: A brake for heart muscle growth A regulatory mechanism that controls how cardiac muscle responds to stress could inform development of new therapies for preventing heart failure. Physiological stimuli ranging from heavy exercise to heart attack can induce hypertrophy, an increase in cardiac muscle mass that is initially beneficial but can lead to organ failure. Researchers led by Gwang Hyeon Eom and Hyun Kook at the Chonnam National University Biomedical Research Center, Hwasungun, South Korea have found that an enzyme called protein phosphatase 2A (PP2A) keeps cardiac hypertrophy in check. PP2A binds to and inhibits a second protein known as HDAC2, which would otherwise stimulate the hypertrophic response to stress. The researchers have identified the biochemical mechanism by which PP2A inactivates HDAC2, and demonstrate that this inhibition effectively protects against hypertrophic cardiac damage in mice, revealing a possible avenue for clinical intervention.

Published

2018

11. Overexpression of Heat Shock Protein 70 Improves Cardiac Remodeling and Survival in Protein Phosphatase 2A-Expressing Transgenic Mice with Chronic Heart Failure

Author

Somy Yoon, Ulrich Gergs, Julie R. McMullen, and Gwang Hyeon Eom

Subjects

post-translational modification, phosphorylation, dilated cardiomyopathy, heart failure, HSP70, Cytology, QH573-671

Abstract

Heat shock protein (HSP) 70 is a molecular chaperone that regulates protein structure in response to thermal stress. In addition, HSP70 is involved in post-translational modification and is related to the severity of some diseases. Here, we tested the functional relevance of long-lasting HSP70 expression in a model of nonischemic heart failure using protein phosphatase 2 catalytic subunit A (PP2CA)-expressing transgenic mice. These transgenic mice, with cardiac-specific overexpression of PP2CA, abruptly died after 12 weeks of postnatal life. Serial echocardiograms to assess cardiac function revealed that the ejection fraction (EF) was gradually decreased in transgenic PP2CA (TgPP2CA) mice. In addition, PP2CA expression exacerbated systolic dysfunction and LV dilatation, with free wall thinning, which are indicators of fatal dilated cardiomyopathy. Interestingly, simultaneous expression of HSP70 in double transgenic mice (dTg) significantly improved the dilated cardiomyopathy phenotype of TgPP2CA mice. We observed better survival, preserved EF, reduced chamber enlargement, and suppression of free wall thinning. In the proposed molecular mechanism, HSP70 preferentially regulates the phosphorylation of AKT. Phosphorylation of AKT was significantly reduced in TgPP2CA mice but was not significantly lower in dTg mice. Signal crosstalk between AKT and its substrates, in association with HSP70, might be a useful intervention for patients with nonischemic heart failure to suppress cardiac remodeling and improve survival.

Published

2021

12. Old Drug, New Trick: Tilorone, a Broad-Spectrum Antiviral Drug as a Potential Anti-Fibrotic Therapeutic for the Diseased Heart

Author

Duncan Horlock, David M. Kaye, Catherine E. Winbanks, Xiao-Ming Gao, Helen Kiriazis, Daniel G. Donner, Paul Gregorevic, Julie R. McMullen, and Bianca C. Bernardo

Subjects

heart failure, fibrosis, tilorone, pressure overload, fibroblast, treatment, Medicine, Pharmacy and materia medica, RS1-441

Abstract

Cardiac fibrosis is associated with most forms of cardiovascular disease. No reliable therapies targeting cardiac fibrosis are available, thus identifying novel drugs that can resolve or prevent fibrosis is needed. Tilorone, an antiviral agent, can prevent fibrosis in a mouse model of lung disease. We investigated the anti-fibrotic effects of tilorone in human cardiac fibroblasts in vitro by performing a radioisotopic assay for [3H]-proline incorporation as a proxy for collagen synthesis. Exploratory studies in human cardiac fibroblasts treated with tilorone (10 µM) showed a significant reduction in transforming growth factor-β induced collagen synthesis compared to untreated fibroblasts. To determine if this finding could be recapitulated in vivo, mice with established pathological remodelling due to four weeks of transverse aortic constriction (TAC) were administered tilorone (50 mg/kg, i.p) or saline every third day for eight weeks. Treatment with tilorone was associated with attenuation of fibrosis (assessed by Masson’s trichrome stain), a favourable cardiac gene expression profile and no further deterioration of cardiac systolic function determined by echocardiography compared to saline treated TAC mice. These data demonstrate that tilorone has anti-fibrotic actions in human cardiac fibroblasts and the adult mouse heart, and represents a potential novel therapy to treat fibrosis associated with heart failure.

Published

2021

13. Generation of MicroRNA-34 Sponges and Tough Decoys for the Heart: Developments and Challenges

Author

Bianca C. Bernardo, Paul Gregorevic, Rebecca H. Ritchie, and Julie R. McMullen

Subjects

microRNAs, heart failure, tough decoy, microRNA sponge, antisense oligonucleotides, Therapeutics. Pharmacology, RM1-950

Abstract

Heart failure (HF) is a debilitating and deadly chronic disease, with almost 50% of patients with HF dying within 5 years of diagnosis. With limited effective therapies to treat or cure HF, new therapies are greatly needed. microRNAs (miRNAs) are small non-coding RNA molecules that are powerful regulators of gene expression and play a key role in almost every biological process. Disruptions in miRNA gene expression has been functionally linked to numerous diseases, including cardiovascular disease. Molecular tools for manipulating miRNA activity have been developed, and there is evidence from preclinical studies demonstrating the potential of miRNAs to be therapeutic targets for cardiovascular disease. For clinical application, miRNA sponges and tough decoys have been developed for more stable suppression and targeted delivery of the miRNA of choice. The aim of this study was to generate miRNA sponges and tough decoys to target miR-34 in the mouse heart. We present data to show that using both approaches we were unable to get significant knockdown of miR-34 or regulate miR-34 target genes in the heart in vivo. We also review recent applications of this method in the heart and discuss further considerations for optimisation in construct design and testing, and the obstacles to be overcome before they enter the clinic.

Published

2018

14. β‐Adrenergic Stimulation Induces Histone Deacetylase 5 (HDAC5) Nuclear Accumulation in Cardiomyocytes by B55α‐PP2A‐Mediated Dephosphorylation

Author

Kate L. Weeks, Antonella Ranieri, Agnieszka Karaś, Bianca C. Bernardo, Alexandra S. Ashcroft, Chris Molenaar, Julie R. McMullen, and Metin Avkiran

Subjects

adrenergic stimulation, B55α, confocal imaging, histone deacetylase 5, hypertrophy/remodeling, microscopy, Diseases of the circulatory (Cardiovascular) system, RC666-701

Abstract

BackgroundClass IIa histone deacetylase (HDAC) isoforms such as HDAC5 are critical signal‐responsive repressors of maladaptive cardiomyocyte hypertrophy, through nuclear interactions with transcription factors including myocyte enhancer factor‐2. β‐Adrenoceptor (β‐AR) stimulation, a signal of fundamental importance in regulating cardiac function, has been proposed to induce both phosphorylation‐independent nuclear export and phosphorylation‐dependent nuclear accumulation of cardiomyocyte HDAC5. The relative importance of phosphorylation at Ser259/Ser498 versus Ser279 in HDAC5 regulation is also controversial. We aimed to determine the impact of β‐AR stimulation on the phosphorylation, localization, and function of cardiomyocyte HDAC5 and delineate underlying molecular mechanisms. Methods and ResultsA novel 3‐dimensional confocal microscopy method that objectively quantifies the whole‐cell nuclear/cytoplasmic distribution of green fluorescent protein tagged HDAC5 revealed the β‐AR agonist isoproterenol to induce β1‐AR‐mediated and protein kinase A‐dependent HDAC5 nuclear accumulation in adult rat cardiomyocytes, which was accompanied by dephosphorylation at Ser259/279/498. Mutation of Ser259/Ser498 to Ala promoted HDAC5 nuclear accumulation and myocyte enhancer factor‐2 inhibition, whereas Ser279 ablation had no such effect and did not block isoproterenol‐induced nuclear accumulation. Inhibition of the Ser/Thr phosphatase PP2A blocked isoproterenol‐induced HDAC5 dephosphorylation. Co‐immunoprecipitation revealed a specific interaction of HDAC5 with the PP2A targeting subunit B55α, as well as catalytic and scaffolding subunits, which increased >3‐fold with isoproterenol. Knockdown of B55α in neonatal cardiomyocytes attenuated isoproterenol‐induced HDAC5 dephosphorylation. Conclusionsβ‐AR stimulation induces HDAC5 nuclear accumulation in cardiomyocytes by a mechanism that is protein kinase A‐dependent but requires B55α‐PP2A‐mediated dephosphorylation of Ser259/Ser498 rather than protein kinase A‐mediated phosphorylation of Ser279.

Published

2017

15. The Interplay of Protein Coding and Non-Coding RNAs (circRNAs, lncRNAs) During Cardiac Differentiation

Author

Julie R. McMullen and Jenny Y.Y. Ooi

Subjects

Medicine, Medicine (General), R5-920

Published

2017

16. Estrogen receptor alpha deficiency in cardiomyocytes reprograms the heart-derived extracellular vesicle proteome and induces obesity in female mice

Author

Yow Keat Tham, Bianca C. Bernardo, Bethany Claridge, Gunes S. Yildiz, Liesel Min-Linn Woon, Simon Bond, Haoyun Fang, Jenny Y. Y. Ooi, Aya Matsumoto, Jieting Luo, Celeste M. K. Tai, Claudia A. Harmawan, Helen Kiriazis, Daniel G. Donner, Natalie A. Mellett, E. Dale Abel, Sohaib A. Khan, David P. De Souza, Sheik Nadeem Elahee Doomun, Kevin Liu, Ruidong Xiang, Manika Singh, Michael Inouye, Peter J. Meikle, Kate L. Weeks, Brian G. Drew, David W. Greening, and Julie R. McMullen

Published

2023

17. Inhibition of miR-154 protects against cardiac dysfunction and fibrosis in a mouse model of pressure overload

Author

Natalie L. Patterson, Xiao-Jun Du, Xiao-Ming Gao, Sally S. Nguyen, Julie R. McMullen, Jenny Y. Y. Ooi, Yow Keat Tham, Helen Kiriazis, Bianca C. Bernardo, Yidan Su, Colleen J. Thomas, and Ruby C.Y. Lin

Subjects

0301 basic medicine, Cardiac function curve, Male, Pathology, medicine.medical_specialty, Cardiac fibrosis, Pulmonary Fibrosis, Oligonucleotides, Left ventricular hypertrophy, Article, Muscle hypertrophy, 03 medical and health sciences, Mice, Fibrosis, Internal medicine, Pulmonary fibrosis, Natriuretic Peptide, Brain, medicine, Animals, Ventricular remodeling, Aorta, Cyclin-Dependent Kinase Inhibitor p15, Uncategorized, Pressure overload, Multidisciplinary, Ventricular Remodeling, business.industry, medicine.disease, 3. Good health, Mice, Inbred C57BL, Disease Models, Animal, MicroRNAs, 030104 developmental biology, Echocardiography, Hypertension, Cardiology, cardiovascular system, Hypertrophy, Left Ventricular, business, Atrial Natriuretic Factor

Abstract

Expression of miR-154 is upregulated in the diseased heart and was previously shown to be upregulated in the lungs of patients with pulmonary fibrosis. However, the role of miR-154 in a model of sustained pressure overload-induced cardiac hypertrophy and fibrosis had not been assessed. To examine the role of miR-154 in the diseased heart, adult male mice were subjected to transverse aortic constriction for four weeks and echocardiography was performed to confirm left ventricular hypertrophy and cardiac dysfunction. Mice were then subcutaneously administered a locked nucleic acid antimiR-154 or control over three consecutive days (25 mg/kg/day) and cardiac function was assessed 8 weeks later. Here, we demonstrate that therapeutic inhibition of miR-154 in mice with pathological hypertrophy was able to protect against cardiac dysfunction and attenuate adverse cardiac remodelling. The improved cardiac phenotype was associated with attenuation of heart and cardiomyocyte size, less cardiac fibrosis, lower expression of atrial and B-type natriuretic peptide genes, attenuation of profibrotic markers and increased expression of p15 (a miR-154 target and cell cycle inhibitor). In summary, this study suggests that miR-154 may represent a novel target for the treatment of cardiac pathologies associated with cardiac fibrosis, hypertrophy and dysfunction.

Published

2023

18. IGF1–PI3K-induced physiological cardiac hypertrophy: Implications for new heart failure therapies, biomarkers, and predicting cardiotoxicity

Author

Celeste M.K. Tai, Sebastian Bass-Stringer, and Julie R. McMullen

Subjects

Drug, medicine.medical_specialty, Heart growth, media_common.quotation_subject, Cardiomegaly, Mice, Transgenic, Physical Therapy, Sports Therapy and Rehabilitation, Review, Disease, PI3K, Mice, Phosphatidylinositol 3-Kinases, 03 medical and health sciences, 0302 clinical medicine, Animals, Humans, Medicine, Orthopedics and Sports Medicine, 030212 general & internal medicine, Insulin-Like Growth Factor I, Intensive care medicine, Exercise, PI3K/AKT/mTOR pathway, Cause of death, media_common, Heart Failure, Cardiotoxicity, business.industry, IGF1, 030229 sport sciences, medicine.disease, Cardiac protection, Therapies, Heart failure, Cardiac hypertrophy, GV557-1198.995, Sports medicine, Phosphatidylinositol 3-Kinase, business, RC1200-1245, Biomarkers, Sports, Signal Transduction

Abstract

Highlights • The IGF1–PI3K pathway mediates exercise induced heart growth and protection. • Strategies to mimic the benefits of exercise on the heart are of substantial interest. • Characterizing animal models of altered cardiac PI3K activity can identify new drug targets for heart disease, and biomarkers which distinguish the healthy and diseased heart. • Therapies that increase PI3K activity may provide a promising approach to improve function in the failing heart. • Systemic therapies that reduce PI3K activity, such as some cancer agents, may lead to cardiotoxicity., Heart failure represents the end point of a variety of cardiovascular diseases. It is a growing health burden and a leading cause of death worldwide. To date, limited treatment options exist for the treatment of heart failure, but exercise has been well-established as one of the few safe and effective interventions, leading to improved outcomes in patients. However, a lack of patient adherence remains a significant barrier in the implementation of exercise-based therapy for the treatment of heart failure. The insulin-like growth factor 1 (IGF1)–phosphoinositide 3-kinase (PI3K) pathway has been recognized as perhaps the most critical pathway for mediating exercised-induced heart growth and protection. Here, we discuss how modulating activity of the IGF1–PI3K pathway may be a valuable approach for the development of therapies that mimic the protective effects of exercise on the heart. We outline some of the promising approaches being investigated that utilize PI3K-based therapy for the treatment of heart failure. We discuss the implications for cardiac pathology and cardiotoxicity that arise in a setting of reduced PI3K activity. Finally, we discuss the use of animal models of cardiac health and disease, and genetic mice with increased or decreased cardiac PI3K activity for the discovery of novel drug targets and biomarkers of cardiovascular disease.

Published

2021

19. Fine-tuning cardiac insulin-like growth factor 1 receptor signaling to promote health and longevity

Author

Mahmoud Abdellatif, Viktoria Trummer-Herbst, Alexander Martin Heberle, Alina Humnig, Tobias Pendl, Sylvère Durand, Giulia Cerrato, Sebastian J. Hofer, Moydul Islam, Julia Voglhuber, José Miguel Ramos Pittol, Oliver Kepp, Gerald Hoefler, Albrecht Schmidt, Peter P. Rainer, Daniel Scherr, Dirk von Lewinski, Egbert Bisping, Julie R. McMullen, Abhinav Diwan, Tobias Eisenberg, Frank Madeo, Kathrin Thedieck, Guido Kroemer, and Simon Sedej

Subjects

Male, cardiomyopathies, autophagy, insulin-like growth factor 1, Longevity, aging, FACTOR-I, Health Promotion, Receptor, IGF Type 1, mitochondria, MICE, phosphatidylinositol 3-kinases, Physiology (medical), IGF-1, Animals, Humans, HEART-FAILURE, Myocytes, Cardiac, Insulin-Like Growth Factor I, Cardiology and Cardiovascular Medicine, General Economics, Econometrics and Finance, mouse, Aged, LIFE-SPAN

Abstract

Background: The insulin-like growth factor 1 (IGF1) pathway is a key regulator of cellular metabolism and aging. Although its inhibition promotes longevity across species, the effect of attenuated IGF1 signaling on cardiac aging remains controversial. Methods: We performed a lifelong study to assess cardiac health and lifespan in 2 cardiomyocyte-specific transgenic mouse models with enhanced versus reduced IGF1 receptor (IGF1R) signaling. Male mice with human IGF1R overexpression or dominant negative phosphoinositide 3-kinase mutation were examined at different life stages by echocardiography, invasive hemodynamics, and treadmill coupled to indirect calorimetry. In vitro assays included cardiac histology, mitochondrial respiration, ATP synthesis, autophagic flux, and targeted metabolome profiling, and immunoblots of key IGF1R downstream targets in mouse and human explanted failing and nonfailing hearts, as well. Results: Young mice with increased IGF1R signaling exhibited superior cardiac function that progressively declined with aging in an accelerated fashion compared with wild-type animals, resulting in heart failure and a reduced lifespan. In contrast, mice with low cardiac IGF1R signaling exhibited inferior cardiac function early in life, but superior cardiac performance during aging, and increased maximum lifespan, as well. Mechanistically, the late-life detrimental effects of IGF1R activation correlated with suppressed autophagic flux and impaired oxidative phosphorylation in the heart. Low IGF1R activity consistently improved myocardial bioenergetics and function of the aging heart in an autophagy-dependent manner. In humans, failing hearts, but not those with compensated hypertrophy, displayed exaggerated IGF1R expression and signaling activity. Conclusions: Our findings indicate that the relationship between IGF1R signaling and cardiac health is not linear, but rather biphasic. Hence, pharmacological inhibitors of the IGF1 pathway, albeit unsuitable for young individuals, might be worth considering in older adults.

Published

2022

20. Prevention of Pathological Atrial Remodeling and Atrial Fibrillation

Author

Thomas H. Marwick, Andre La Gerche, Yi Ching Chen, Julie R. McMullen, and Aleksandr Voskoboinik

Subjects

medicine.medical_specialty, Mitral regurgitation, Heart disease, Atrial enlargement, business.industry, Atrial fibrillation, 030204 cardiovascular system & hematology, medicine.disease, 03 medical and health sciences, 0302 clinical medicine, medicine.anatomical_structure, Internal medicine, Heart failure, Mitral valve, cardiovascular system, medicine, Cardiology, cardiovascular diseases, 030212 general & internal medicine, Animal studies, medicine.symptom, Cardiology and Cardiovascular Medicine, business, Pathological

Abstract

Atrial enlargement in response to pathological stimuli (e.g., hypertension, mitral valve disease) and physiological stimuli (exercise, pregnancy) can be comparable in magnitude, but the diseased enlarged atria is associated with complications such as atrial fibrillation (AF), whereas physiological atrial enlargement is not. Pathological atrial enlargement and AF is also observed in a small percentage of athletes undergoing extreme/intense endurance sport and pregnant women with preeclampsia. Differences between physiological and pathological atrial enlargement and underlying mechanisms are poorly understood. This review describes human and animal studies characterizing atrial enlargement under physiological and pathological conditions and highlights key knowledge gaps and clinical challenges, including: 1) the limited ability of atria to reverse remodel; and 2) distinguishing physiological and pathological enlargement via imaging/biomarkers. Finally, this review discusses how targeting distinct molecular mechanisms underlying physiological and pathological atrial enlargement could provide new therapeutic and diagnostic strategies for preventing or reversing atrial enlargement and AF.

Published

2021

21. Lipids regulated by exercise and phosphoinositide 3-kinase: potential role as biomarkers and therapeutic targets for cardiovascular disease

Author

Teleah G Belkin, Yow Keat Tham, and Julie R McMullen

Subjects

Physiology, Physiology (medical)

Published

2023

22. Exercise training reveals micro-RNAs associated with improved cardiac function and electrophysiology in rats with heart failure after myocardial infarction

Author

Anne Berit Johnsen, Karin Garten, Eirik Skogvoll, Nathan R. Scrimgeour, Godfrey L. Smith, Øyvind Ellingsen, Kari Jørgensen, Bjarne M. Nes, Tomas Stølen, Julie R. McMullen, José Bianco Nascimento Moreira, Muhammad Shakil Ahmed, Ulrik Wisløff, Maria P. Hortigon-Vinagre, Håvard Attramadal, Anne Marie Ormbostad Berre, Morten A. Høydal, and Victor Zamora

Subjects

0301 basic medicine, Cardiac function curve, medicine.medical_specialty, Myocardial Infarction, Infarction, Cardiomegaly, 030204 cardiovascular system & hematology, Rats, Sprague-Dawley, 03 medical and health sciences, 0302 clinical medicine, Endurance training, Physical Conditioning, Animal, Internal medicine, medicine, Animals, Aerobic exercise, Myocytes, Cardiac, Myocardial infarction, Molecular Biology, computer.programming_language, Heart Failure, sed, business.industry, Arrhythmias, Cardiac, medicine.disease, Myocardial Contraction, Aerobiosis, Electrophysiological Phenomena, MicroRNAs, Electrophysiology, 030104 developmental biology, Gene Expression Regulation, Heart failure, Ventricular Fibrillation, Cardiology, Female, Cardiology and Cardiovascular Medicine, business, computer, Biomarkers

Abstract

Aims Endurance training improves aerobic fitness and cardiac function in individuals with heart failure. However, the underlying mechanisms are not well characterized. Exercise training could therefore act as a tool to discover novel targets for heart failure treatment. We aimed to associate changes in Ca2+ handling and electrophysiology with micro-RNA (miRNA) profile in exercise trained heart failure rats to establish which miRNAs induce heart failure-like effects in Ca2+ handling and electrophysiology. Methods and results Post-myocardial infarction (MI) heart failure was induced in Sprague Dawley rats. Rats with MI were randomized to sedentary control (sed), moderate (mod)- or high-intensity (high) endurance training for 8 weeks. Exercise training improved cardiac function, Ca2+ handling and electrophysiology including reduced susceptibility to arrhythmia in an exercise intensity-dependent manner where high intensity gave a larger effect. Fifty-five miRNAs were significantly regulated (up or down) in MI-sed, of which 18 and 3 were changed towards Sham-sed in MI-high and MI-mod, respectively. Thereafter we experimentally altered expression of these “exercise-miRNAs” individually in human induced pluripotent stem cell-derived cardiomyocytes (hIPSC-CM) in the same direction as they were changed in MI. Of the “exercise-miRNAs”, miR-214-3p prolonged AP duration, whereas miR-140 and miR-208a shortened AP duration. miR-497-5p prolonged Ca2+ release whereas miR-214-3p and miR-31a-5p prolonged Ca2+ decay. Conclusion Using exercise training as a tool, we discovered that miR-214-3p, miR-497-5p, miR-31a-5p contribute to heart-failure like behaviour in Ca2+ handling and electrophysiology and could be potential treatment targets.

Published

2020

23. Clusterin is regulated by IGF1–PI3K signaling in the heart: implications for biomarker and drug target discovery, and cardiotoxicity

Author

Jenny Y Y Ooi, Sebastian Bass-Stringer, and Julie R. McMullen

Subjects

0301 basic medicine, Genetically modified mouse, Health, Toxicology and Mutagenesis, Heart growth, 010501 environmental sciences, Toxicology, 01 natural sciences, 03 medical and health sciences, medicine, PI3K/AKT/mTOR pathway, 0105 earth and related environmental sciences, Cardiotoxicity, Clusterin, biology, business.industry, Microarray analysis techniques, General Medicine, medicine.disease, eye diseases, 030104 developmental biology, Heart failure, biology.protein, Cancer research, Biomarker (medicine), sense organs, business

Abstract

Open-access gene expression data sets provide a useful resource for identifying novel drug targets and biomarkers. The IGF1-PI3K pathway is a critical mediator of physiological cardiac enlargement/hypertrophy and protection. This study arose after mining a gene microarray data set from a previous study that compared heart tissue from cardiac-specific PI3K transgenic mouse models. The top-ranked candidate identified from the microarray data was clusterin. Clusterin has been proposed as a biomarker for multiple diseases including heart failure, and as a cancer drug target. Here, we show that clusterin gene expression is increased in hearts of transgenic mice with increased PI3K and decreased in mice with depressed cardiac PI3K. In vitro, clusterin secretion was elevated in media from neonatal rat ventricular myocytes treated with IGF1. Furthermore, by mining gene expression data from hearts during normal mouse postnatal growth, we also report an increase in clusterin expression with postnatal heart growth. Given we show that clusterin is regulated by the IGF1-PI3K pathway in the heart, and this pathway mediates physiological cardiac hypertrophy and cardioprotection, caution is required when considering clusterin as a biomarker for heart failure and as a cancer target. Mining pre-existing cardiac profiling data sets may be a useful approach to assess whether regulating new drug targets is likely to lead to cardiac damage/toxicity.

Published

2020

24. A Step-By-Step Method to Detect Neutralizing Antibodies Against AAV using a Colorimetric Cell-Based Assay

Author

Julie R. McMullen, Kate L. Weeks, Paul Gregorevic, Clive N. May, Colleen J. Thomas, and Sebastian Bass-Stringer

Subjects

Sheep, General Immunology and Microbiology, General Chemical Engineering, General Neuroscience, Genetic Vectors, Animals, Colorimetry, Dependovirus, Antibodies, Viral, Antibodies, Neutralizing, General Biochemistry, Genetics and Molecular Biology

Abstract

Recombinant adeno-associated viruses (rAAV) have proven to be a safe and successful vector for transferring genetic material to treat various health conditions in both the laboratory and the clinic. However, pre-existing neutralizing antibodies (NAbs) against AAV capsids pose an ongoing challenge for the successful administration of gene therapies in both large animal experimental models and human populations. Preliminary screening for host immunity against AAV is necessary to ensure the efficacy of AAV-based gene therapies as both a research tool and as a clinically viable therapeutic agent. This protocol describes a colorimetric in vitro assay to detect neutralizing factors against AAV serotype 6 (AAV6). The assay utilizes the reaction between an AAV encoding an alkaline phosphatase (AP) reporter gene and its substrate NBT/BCIP, which generates an insoluble quantifiable purple stain upon combination. In this protocol, serum samples are combined with an AAV expressing AP and incubated to permit potential neutralizing activity to occur. Virus serum mixture is subsequently added to cells to allow for viral transduction of any AAVs that have not been neutralized. The NBT/BCIP substrate is added and undergoes a chromogenic reaction, corresponding to viral transduction and neutralizing activity. The proportion of area colored is quantitated using a free software tool to generate neutralizing titers. This assay displays a strong positive correlation between coloration and viral concentration. Assessment of serum samples from sheep before and after administration of a recombinant AAV6 led to a dramatic increase in neutralizing activity (125 to10,000-fold increase). The assay displayed adequate sensitivity to detect neutralizing activity in1:32,000 serum dilutions. This assay provides a simple, rapid, and cost-effective method to detect NAbs against AAVs.

Published

2021

25. Overexpression of Heat Shock Protein 70 Improves Cardiac Remodeling and Survival in Protein Phosphatase 2A-Expressing Transgenic Mice with Chronic Heart Failure

Author

Julie R. McMullen, Ulrich Gergs, Gwang Hyeon Eom, and Somy Yoon

Subjects

Cardiomyopathy, Dilated, medicine.medical_specialty, QH301-705.5, Transgene, heart failure, Mice, Transgenic, Article, Electrocardiography, Heat shock protein, Internal medicine, medicine, Animals, HSP70 Heat-Shock Proteins, Protein Phosphatase 2, Biology (General), Protein kinase B, HSP70, Ventricular Remodeling, business.industry, phosphorylation, Dilated cardiomyopathy, General Medicine, Protein phosphatase 2, medicine.disease, Survival Analysis, Hsp70, dilated cardiomyopathy, post-translational modification, Endocrinology, Phenotype, Gene Expression Regulation, Heart failure, Chronic Disease, Phosphorylation, business, Protein Processing, Post-Translational

Abstract

Heat shock protein (HSP) 70 is a molecular chaperone that regulates protein structure in response to thermal stress. In addition, HSP70 is involved in post-translational modification and is related to the severity of some diseases. Here, we tested the functional relevance of long-lasting HSP70 expression in a model of nonischemic heart failure using protein phosphatase 2 catalytic subunit A (PP2CA)-expressing transgenic mice. These transgenic mice, with cardiac-specific overexpression of PP2CA, abruptly died after 12 weeks of postnatal life. Serial echocardiograms to assess cardiac function revealed that the ejection fraction (EF) was gradually decreased in transgenic PP2CA (TgPP2CA) mice. In addition, PP2CA expression exacerbated systolic dysfunction and LV dilatation, with free wall thinning, which are indicators of fatal dilated cardiomyopathy. Interestingly, simultaneous expression of HSP70 in double transgenic mice (dTg) significantly improved the dilated cardiomyopathy phenotype of TgPP2CA mice. We observed better survival, preserved EF, reduced chamber enlargement, and suppression of free wall thinning. In the proposed molecular mechanism, HSP70 preferentially regulates the phosphorylation of AKT. Phosphorylation of AKT was significantly reduced in TgPP2CA mice but was not significantly lower in dTg mice. Signal crosstalk between AKT and its substrates, in association with HSP70, might be a useful intervention for patients with nonischemic heart failure to suppress cardiac remodeling and improve survival.

Published

2021

26. A protocol for rapid and parallel isolation of myocytes and non-myocytes from multiple mouse hearts

Author

Julie R. McMullen, Aya Matsumoto, Adam C. Parslow, Micheal A. McLellan, Alexander R. Pinto, Taylah L. Gaynor, Gabriella E. Farrugia, Kate L. Weeks, Charles D. Cohen, and Crisdion Krstevski

Subjects

Male, Science (General), Cell Culture Techniques, Peristaltic pump, Cell Separation, General Biochemistry, Genetics and Molecular Biology, Q1-390, Mice, Protocol, Myocyte, Animals, Myocytes, Cardiac, Viability assay, Cell isolation, Protocol (object-oriented programming), Cells, Cultured, General Immunology and Microbiology, Chemistry, General Neuroscience, Myocardium, Genomics, Cell Biology, Cell sorting, Cell biology, Mice, Inbred C57BL, Single-Cell Analysis, Cell separation/fractionation

Abstract

Summary This protocol features parallel isolation of myocytes and non-myocytes from murine hearts. It was designed with considerations for (1) time required to extract cardiac cells, (2) cell viability, and (3) protocol scalability. Here, a peristaltic pump and 3D-printed elements are combined to perfuse the heart with enzymes to dissociate cells. Myocytes and non-myocytes extracted using this protocol are separated by centrifugation and/or fluorescence-activated cell sorting for use in downstream applications including single-cell omics or other bio-molecular analyses. For complete details on the use and execution of this protocol, please refer to McLellan et al. (2020)., Graphical abstract, Highlights • Protocol for extracting myocytes and non-myocytes from multiple mouse hearts • Protocol is simple and scalable for processing one or many hearts • Significant time saving for rapid isolation of viable and high-quality cardiac cells • Isolated cells are suitable for cell culture, single-cell omics, and various assays, This protocol features parallel isolation of myocytes and non-myocytes from murine hearts. It was designed with considerations for (1) time required to extract cardiac cells, (2) cell viability, and (3) protocol scalability. Here, a peristaltic pump and 3D-printed elements are combined to perfuse the heart with enzymes to dissociate cells. Myocytes and non-myocytes extracted using this protocol are separated by centrifugation and/or fluorescence-activated cell sorting for use in downstream applications including single-cell omics or other bio-molecular analyses.

Published

2021

27. Tissue-specific expression of Cas9 has no impact on whole-body metabolism in four transgenic mouse lines

Author

Aowen Zhuang, Eleanor A.M. Gould, Julie R. McMullen, Anna C. Calkin, Simon T. Bond, Ying Fu, Yanie Tan, Paul Gregorevic, Tim Sikora, Yingying Liu, Christine Yang, Helen Kiriazis, Kevin I. Watt, Brian G. Drew, Darren C. Henstridge, Peter J. Meikle, and Graeme I. Lancaster

Subjects

Genetically modified mouse, Male, Transgene, Adipose tissue, Mice, Transgenic, Biology, Mice, Technical Report, Genome editing, Fibrosis, CRISPR-Associated Protein 9, medicine, CRISPR, Animals, Transgenic mice, Cas9, Internal medicine, Molecular Biology, Gene, Cell Biology, medicine.disease, RC31-1245, Phenotype, Cell biology, Mice, Inbred C57BL, Metabolism, Tissue specific, CRISPR-Cas Systems

Abstract

Objective CRISPR/Cas9 technology has revolutionized gene editing and fast tracked our capacity to manipulate genes of interest for the benefit of both research and therapeutic applications. Whilst many advances have, and continue to be made in this area, perhaps the most utilized technology to date has been the generation of knockout cells, tissues and animals. The advantages of this technology are many fold, however some questions still remain regarding the effects that long term expression of foreign proteins such as Cas9, have on mammalian cell function. Several studies have proposed that chronic overexpression of Cas9, with or without its accompanying guide RNAs, may have deleterious effects on cell function and health. This is of particular concern when applying this technology in vivo, where chronic expression of Cas9 in tissues of interest may promote disease-like phenotypes and thus confound the investigation of the effects of the gene of interest. Although these concerns remain valid, no study to our knowledge has yet to demonstrate this directly. Methods In this study we used the lox-stop-lox (LSL) spCas9 ROSA26 transgenic (Tg) mouse line to generate four tissue-specific Cas9-Tg models that express Cas9 in the heart, liver, skeletal muscle or adipose tissue. We performed comprehensive phenotyping of these mice up to 20-weeks of age and subsequently performed molecular analysis of their organs. Results We demonstrate that Cas9 expression in these tissues had no detrimental effect on whole body health of the animals, nor did it induce any tissue-specific effects on whole body energy metabolism, liver health, inflammation, fibrosis, heart function or muscle mass. Conclusions Our data suggests that these models are suitable for studying the tissue specific effects of gene deletion using the LSL-Cas9-Tg model, and that phenotypes observed utilizing these models can be confidently interpreted as being gene specific, and not confounded by the chronic overexpression of Cas9., Highlights • Detailed characterization of 4 tissue specific Cas9 TG mice in relevant metabolic tissues. • Demonstration that these models express robust Cas9 in a tissue specific manner. • Detailed phenotyping demonstrates that chronic Cas9 expression has no impact on tissue weight, body composition or body weight. • Metabolic phenotyping demonstrates that Cas9 expression does not impact whole body glucose tolerance, or heart function. • Tissue specific characterization confirms that there is no discernible effect on tissue health or function.

Published

2021

28. Protein phosphatase 2A in the healthy and failing heart: New insights and therapeutic opportunities

Author

Nicola M. Sergienko, Daniel G. Donner, Lea M.D. Delbridge, Julie R. McMullen, and Kate L. Weeks

Subjects

Humans, Heart, Cell Biology, Protein Phosphatase 2, Phosphorylation, Phosphoproteins, Protein Processing, Post-Translational

Abstract

Protein phosphatases have emerged as critical regulators of phosphoprotein homeostasis in settings of health and disease. Protein phosphatase 2A (PP2A) encompasses a large subfamily of enzymes that remove phosphate groups from serine/threonine residues within phosphoproteins. The heterogeneity in PP2A structure, which arises from the grouping of different catalytic, scaffolding and regulatory subunit isoforms, creates distinct populations of catalytically active enzymes (i.e. holoenzymes) that localise to different parts of the cell. This structural complexity, combined with other regulatory mechanisms, such as interaction of PP2A heterotrimers with accessory proteins and post-translational modification of the catalytic and/or regulatory subunits, enables PP2A holoenzymes to target phosphoprotein substrates in a highly specific manner. In this review, we summarise the roles of PP2A in cardiac physiology and disease. PP2A modulates numerous processes that are vital for heart function including calcium handling, contractility, β-adrenergic signalling, metabolism and transcription. Dysregulation of PP2A has been observed in human cardiac disease settings, including heart failure and atrial fibrillation. Efforts are underway, particularly in the cancer field, to develop therapeutics targeting PP2A activity. The development of small molecule activators of PP2A (SMAPs) and other compounds that selectively target specific PP2A holoenzymes (e.g. PP2A/B56α and PP2A/B56ε) will improve understanding of the function of different PP2A species in the heart, and may lead to the development of therapeutics for normalising aberrant protein phosphorylation in settings of cardiac remodelling and dysfunction.

Published

2021

29. Prevention of Pathological Atrial Remodeling and Atrial Fibrillation: JACC State-of-the-Art Review

Author

Yi Ching, Chen, Aleksandr, Voskoboinik, Andre La, Gerche, Thomas H, Marwick, and Julie R, McMullen

Subjects

Sex Characteristics, Heart Diseases, Athletes, Pregnancy, Atrial Fibrillation, Animals, Humans, Female, Atrial Remodeling

Abstract

Atrial enlargement in response to pathological stimuli (e.g., hypertension, mitral valve disease) and physiological stimuli (exercise, pregnancy) can be comparable in magnitude, but the diseased enlarged atria is associated with complications such as atrial fibrillation (AF), whereas physiological atrial enlargement is not. Pathological atrial enlargement and AF is also observed in a small percentage of athletes undergoing extreme/intense endurance sport and pregnant women with preeclampsia. Differences between physiological and pathological atrial enlargement and underlying mechanisms are poorly understood. This review describes human and animal studies characterizing atrial enlargement under physiological and pathological conditions and highlights key knowledge gaps and clinical challenges, including: 1) the limited ability of atria to reverse remodel; and 2) distinguishing physiological and pathological enlargement via imaging/biomarkers. Finally, this review discusses how targeting distinct molecular mechanisms underlying physiological and pathological atrial enlargement could provide new therapeutic and diagnostic strategies for preventing or reversing atrial enlargement and AF.

Published

2021

30. FoxO1 is required for physiological cardiac hypertrophy induced by exercise but not by constitutively active PI3K

Author

Bianca C. Bernardo, Helen Kiriazis, Yonali Alexander, Ronald A. DePinho, D. Donner, Claudia A Harmawan, Amy Hsu, Julie R. McMullen, Kate L. Weeks, Aya Matsumoto, Yow Keat Tham, Elizabeth A. Woodcock, Suzan G Yildiz, and E. Dale Abel

Subjects

0301 basic medicine, Male, endocrine system, medicine.medical_specialty, Heart disease, Physiology, Class I Phosphatidylinositol 3-Kinases, Transgene, FOXO1, Cardiomegaly, 030204 cardiovascular system & hematology, Muscle hypertrophy, Receptor, IGF Type 1, 03 medical and health sciences, 0302 clinical medicine, Physiology (medical), Internal medicine, Medicine, Animals, HSP70 Heat-Shock Proteins, Myocytes, Cardiac, Cardiomegaly, Exercise-Induced, Phosphorylation, Protein kinase B, PI3K/AKT/mTOR pathway, Swimming, Insulin-like growth factor 1 receptor, Mice, Knockout, business.industry, Forkhead Box Protein O1, Forkhead Box Protein O3, medicine.disease, Fibrosis, Enzyme Activation, 030104 developmental biology, Endocrinology, Phenotype, Gene Expression Regulation, Heart failure, Female, Cardiology and Cardiovascular Medicine, business, Proto-Oncogene Proteins c-akt, Signal Transduction

Abstract

The insulin-like growth factor 1 receptor (IGF1R) and phosphoinositide 3-kinase p110α (PI3K) are critical regulators of exercise-induced physiological cardiac hypertrophy and provide protection in experimental models of pathological remodeling and heart failure. Forkhead box class O1 (FoxO1) is a transcription factor that regulates cardiomyocyte hypertrophy downstream of IGF1R/PI3K activation in vitro, but its role in physiological hypertrophy in vivo was unknown. We generated cardiomyocyte-specific FoxO1 knockout (cKO) mice and assessed the phenotype under basal conditions and settings of physiological hypertrophy induced by 1) swim training or 2) cardiac-specific transgenic expression of constitutively active PI3K (caPI3KTg+). Under basal conditions, male and female cKO mice displayed mild interstitial fibrosis compared with control (CON) littermates, but no other signs of cardiac pathology were present. In response to exercise training, female CON mice displayed an increase (∼21%) in heart weight normalized to tibia length vs. untrained mice. Exercise-induced hypertrophy was blunted in cKO mice. Exercise increased cardiac Akt phosphorylation and IGF1R expression but was comparable between genotypes. However, differences in Foxo3a, Hsp70, and autophagy markers were identified in hearts of exercised cKO mice. Deletion of FoxO1 did not reduce cardiac hypertrophy in male or female caPI3KTg+ mice. Cardiac Akt and FoxO1 protein expressions were significantly reduced in hearts of caPI3KTg+ mice, which may represent a negative feedback mechanism from chronic caPI3K, and negate any further effect of reducing FoxO1 in the cKO. In summary, FoxO1 contributes to exercise-induced hypertrophy. This has important implications when one is considering FoxO1 as a target for treating the diseased heart.NEW & NOTEWORTHY Regulators of exercise-induced physiological cardiac hypertrophy and protection are considered promising targets for the treatment of heart failure. Unlike pathological hypertrophy, the transcriptional regulation of physiological hypertrophy has remained largely elusive. To our knowledge, this is the first study to show that the transcription factor FoxO1 is a critical mediator of exercise-induced cardiac hypertrophy. Given that exercise-induced hypertrophy is protective, this finding has important implications when one is considering FoxO1 as a target for treating the diseased heart.

Published

2021

31. Correction for McMullen et al., 'Deletion of Ribosomal S6 Kinases Does Not Attenuate Pathological, Physiological, or Insulin-Like Growth Factor 1 Receptor–Phosphoinositide 3-Kinase-Induced Cardiac Hypertrophy'

Author

Julie R. McMullen, George Thomas, Sarah Longnus, Tetsuo Shioi, Seigo Izumo, Kathleen A. Martin, Oleg Tarnavski, John Blenis, Li Zhang, Mario Pende, Megan C. Sherwood, and Adam L. Dorfman

Subjects

medicine.medical_treatment, Cardiomegaly, Mice, Transgenic, Ribosomal Protein S6 Kinases, 90-kDa, Receptor, IGF Type 1, Mice, Phosphatidylinositol 3-Kinases, Insulin-like growth factor, Fetus, Physical Conditioning, Animal, medicine, Animals, Author Correction, Receptor, Molecular Biology, Pathological, Aorta, Swimming, Mice, Knockout, Sirolimus, Antibiotics, Antineoplastic, Phosphoinositide 3-kinase, biology, Kinase, Gene Expression Regulation, Developmental, Organ Size, Cell Biology, Ribosomal RNA, Cell biology, Cardiac hypertrophy, biology.protein, Female, Stress, Mechanical, Signal Transduction

Abstract

Ribosomal S6 kinases (S6Ks) have been depicted as critical effectors downstream of growth factor pathways, which play an important role in the regulation of protein synthesis by phosphorylating the ribosomal protein, S6. The goal of this study was to determine whether S6Ks regulate heart size, are critical for the induction of cardiac hypertrophy in response to a pathological or physiological stimulus, and whether S6Ks are critical downstream effectors of the insulin-like growth factor 1 (IGF1)-phosphoinositide 3-kinase (PI3K) pathway. For this purpose, we generated and characterized cardiac-specific S6K1 and S6K2 transgenic mice and subjected S6K1(-/-), S6K2(-/-), and S6K1(-/-) S6K2(-/-) mice to a pathological stress (aortic banding) or a physiological stress (exercise training). To determine the genetic relationship between S6Ks and the IGF1-PI3K pathway, S6K transgenic and knockout mice were crossed with cardiac-specific transgenic mice overexpressing the IGF1 receptor (IGF1R) or PI3K mutants. Here we show that overexpression of S6K1 induced a modest degree of hypertrophy, whereas overexpression of S6K2 resulted in no obvious cardiac phenotype. Unexpectedly, deletion of S6K1 and S6K2 had no impact on the development of pathological, physiological, or IGF1R-PI3K-induced cardiac hypertrophy. These studies suggest that S6Ks alone are not essential for the development of cardiac hypertrophy.

Published

2021

32. Loss of the Long Non-coding RNA OIP5-AS1 Exacerbates Heart Failure in a Sex-Specific Manner

Author

Julie R. McMullen, T. Q. de Aguiar Vallim, James E. Hudson, Aowen Zhuang, S. Lau, Elizabeth J. Tarling, Paul Gregorevic, Sarah C. Moody, Sergio Ruiz-Carmona, D. Donner, Xiao-Jun Du, Eleanor A.M. Gould, Yingying Liu, Xiao-Ming Gao, Helen Kiriazis, Brian G. Drew, Simon T. Bond, Gregory A. Quaife-Ryan, Michael Inouye, Enzo R. Porrello, Anna C. Calkin, and Timothy D. Colgan

Subjects

Pressure overload, Transcriptome, Heart failure, Cellular differentiation, medicine, Disease, Biology, medicine.disease, Bioinformatics, Gene, Phenotype, Long non-coding RNA

Abstract

BackgroundLong ncRNAs (lncRNAs) are known to influence numerous biological processes including cellular differentiation and tissue development. They are also implicated in the maintenance, health and physiological function of many tissues including the heart. Indeed, manipulating the expression of specific lncRNAs has been shown to improve pathological cardiac phenotypes such as heart failure. One lncRNA studied in various settings is OIP5-AS1 (also known as 1700020I14Rik and Cyrano), however its role in cardiac pathologies remains mostly uncharacterised.MethodsWe used data generated from FACS sorted murine cardiomyocytes, human iPSC derived cardiomyocytes, as well as heart tissue from various animal models to investigate OIP5-AS1 expression in health and disease. Using CRISPR we engineered a global OIP5-AS1 knock out (KO) mouse model and performed cardiac pressure overload experiments to study heart failure in these animals. RNA-sequencing of left ventricles provided mechanistic insight between WT and KO mice.ResultsWe demonstrate that OIP5-AS1 expression is regulated during cardiac development and cardiac specific pathologies in both rodent and human models. Moreover, we demonstrate that global female OIP5-AS1 KO mice develop exacerbated heart failure, but male mice do not. Transcriptomics and gene set enrichment analysis suggests that OIP5-AS1 may regulate pathways that impact mitochondrial function.ConclusionsOIP5-AS1 is regulated in cardiac tissue and its deletion leads to worsening heart function under pressure overload in female mice. This may be due to impairments in mitochondrial function, highlighting OIP5-AS1 as a gene of interest in sex-specific differences in heart failure.

Published

2021

33. Novel lipid species for detecting and predicting atrial fibrillation in patients with type 2 diabetes

Author

Julie R. McMullen, Peter J. Meikle, John Chalmers, Graham S. Hillis, Sophia Zoungas, Jenny Y. Y. Ooi, Adam Alexander T. Smith, Kevin Huynh, Corey Giles, Zahir H. Alshehry, Kaushala S. Jayawardana, Yow Keat Tham, and Ada Admin

Subjects

lipids (amino acids, peptides, and proteins)

Abstract

The incidence of atrial fibrillation (AF) is higher in patients with diabetes. The goal of this study was to assess if the addition of plasma lipids to traditional risk factors could improve the ability to detect and predict future AF in patients with type 2 diabetes. Logistic regression models were used to identify lipids associated with AF/future AF from plasma lipids (n=316) measured from participants from the ADVANCE trial (n=3,772). To gain mechanistic insight, follow-up lipid analysis was undertaken in a mouse model which has an insulin-resistant heart and is susceptible to AF. Sphingolipids, cholesteryl esters and phospholipids were associated with AF prevalence, whereas two GM3 ganglioside species were associated with future AF. For AF detection and prediction, addition of 6 and 3 lipids, respectively, to a base model (12 conventional risk factors) increased the C-statistics (detection:0.661 to 0.725; prediction:0.674 to 0.715), and categorical net reclassification indices. GM3(d18:1/24:1) was lower in patients who developed AF, improved the C-statistic for the prediction of future AF, and was lower in the plasma of the mouse model susceptible to AF. This study demonstrates that plasma lipids have the potential to improve both the detection and prediction of AF in patients with diabetes.

Published

2020

34. Novel Lipid Species for Detecting and Predicting Atrial Fibrillation in Patients With Type 2 Diabetes

Author

Sophia Zoungas, Adam Alexander T. Smith, Kaushala S. Jayawardana, Corey Giles, Peter J. Meikle, Yow Keat Tham, Kevin Huynh, Julie R. McMullen, Zahir H Alshehry, Graham S Hillis, John Chalmers, and Jenny Y Y Ooi

Subjects

0301 basic medicine, Male, medicine.medical_specialty, Heart disease, Endocrinology, Diabetes and Metabolism, 030209 endocrinology & metabolism, Type 2 diabetes, Logistic regression, Risk Assessment, 03 medical and health sciences, Mice, 0302 clinical medicine, Risk Factors, Internal medicine, Diabetes mellitus, Atrial Fibrillation, Internal Medicine, medicine, Animals, Humans, Aged, business.industry, Incidence (epidemiology), Atrial fibrillation, Middle Aged, medicine.disease, Sphingolipid, Lipids, 030104 developmental biology, Diabetes Mellitus, Type 2, Cardiology, lipids (amino acids, peptides, and proteins), Female, business, Risk assessment

Abstract

The incidence of atrial fibrillation (AF) is higher in patients with diabetes. The goal of this study was to assess if the addition of plasma lipids to traditional risk factors could improve the ability to detect and predict future AF in patients with type 2 diabetes. Logistic regression models were used to identify lipids associated with AF or future AF from plasma lipids (n = 316) measured from participants in the ADVANCE trial (n = 3,772). To gain mechanistic insight, follow-up lipid analysis was undertaken in a mouse model that has an insulin-resistant heart and is susceptible to AF. Sphingolipids, cholesteryl esters, and phospholipids were associated with AF prevalence, whereas two monosialodihexosylganglioside (GM3) ganglioside species were associated with future AF. For AF detection and prediction, addition of six and three lipids, respectively, to a base model (n = 12 conventional risk factors) increased the C-statistics (detection: from 0.661 to 0.725; prediction: from 0.674 to 0.715) and categorical net reclassification indices. The GM3(d18:1/24:1) level was lower in patients in whom AF developed, improved the C-statistic for the prediction of future AF, and was lower in the plasma of the mouse model susceptible to AF. This study demonstrates that plasma lipids have the potential to improve the detection and prediction of AF in patients with diabetes.

Published

2020

35. Gene therapy targeting cardiac phosphoinositide 3-kinase (p110α) attenuates cardiac remodeling in type 2 diabetes

Author

Hongwei Qian, Paul Gregorevic, Minh Deo, D. Donner, Julie R. McMullen, Rebecca H. Ritchie, Miles J. De Blasio, David M Nash, Kate L. Weeks, Darnel Prakoso, Helen Kiriazis, Mitchel Tate, and Laura J. Parry

Subjects

0301 basic medicine, Male, medicine.medical_specialty, Physiology, Cardiac fibrosis, Class I Phosphatidylinositol 3-Kinases, Diabetic Cardiomyopathies, Genetic Vectors, Cardiomyopathy, Type 2 diabetes, 030204 cardiovascular system & hematology, Diet, High-Fat, Diabetes Mellitus, Experimental, Impaired glucose tolerance, 03 medical and health sciences, Mice, 0302 clinical medicine, Physiology (medical), Internal medicine, Diabetes mellitus, Diabetic cardiomyopathy, medicine, Animals, Ventricular remodeling, Ventricular Remodeling, business.industry, Myocardium, Genetic Therapy, Dependovirus, medicine.disease, Endoplasmic Reticulum Stress, Fibrosis, 030104 developmental biology, Diabetes Mellitus, Type 2, Heart failure, Cardiology, Cardiology and Cardiovascular Medicine, business, Reactive Oxygen Species

Abstract

Diabetic cardiomyopathy is a distinct form of heart disease that represents a major cause of death and disability in diabetic patients, particularly, the more prevalent type 2 diabetes patient population. In the current study, we investigated whether administration of recombinant adeno-associated viral vectors carrying a constitutively active phosphoinositide 3-kinase (PI3K)(p110α) construct (rAAV6-caPI3K) at a clinically relevant time point attenuates diabetic cardiomyopathy in a preclinical type 2 diabetes (T2D) model. T2D was induced by a combination of a high-fat diet (42% energy intake from lipid) and low-dose streptozotocin (three consecutive intraperitoneal injections of 55 mg/kg body wt), and confirmed by increased body weight, mild hyperglycemia, and impaired glucose tolerance (all P < 0.05 vs. nondiabetic mice). After 18 wk of untreated diabetes, impaired left ventricular (LV) systolic dysfunction was evident, as confirmed by reduced fractional shortening and velocity of circumferential fiber shortening (Vcfc, all P < 0.01 vs. baseline measurement). A single tail vein injection of rAAV6-caPI3K gene therapy (2×1011vector genomes) was then administered. Mice were followed for an additional 8 wk before end point. A single injection of cardiac targeted rAAV6-caPI3K attenuated diabetes-induced cardiac remodeling by limiting cardiac fibrosis (reduced interstitial and perivascular collagen deposition, P < 0.01 vs. T2D mice) and cardiomyocyte hypertrophy (reduced cardiomyocyte size and Nppa gene expression, P < 0.001 and P < 0.05 vs. T2D mice, respectively). The diabetes-induced LV systolic dysfunction was reversed with rAAV6-caPI3K, as demonstrated by improved fractional shortening and velocity of circumferential fiber shortening (all P < 0.05 vs pre-AAV measurement). This cardioprotection occurred in combination with reduced LV reactive oxygen species ( P < 0.05 vs. T2D mice) and an associated decrease in markers of endoplasmic reticulum stress (reduced Grp94 and Chop, all P < 0.05 vs. T2D mice). Together, our findings demonstrate that a cardiac-selective increase in PI3K(p110α), via rAAV6-caPI3K, attenuates T2D-induced diabetic cardiomyopathy, providing proof of concept for potential translation to the clinic. NEW & NOTEWORTHY Diabetes remains a major cause of death and disability worldwide (and its resultant heart failure burden), despite current care. The lack of existing management of heart failure in the context of the poorer prognosis of concomitant diabetes represents an unmet clinical need. In the present study, we now demonstrate that delayed intervention with PI3K gene therapy (rAAV6-caPI3K), administered as a single dose in mice with preexisting type 2 diabetes, attenuates several characteristics of diabetic cardiomyopathy, including diabetes-induced impairments in cardiac remodeling, oxidative stress, and function. Our discovery here contributes to the previous body of work, suggesting the cardioprotective effects of PI3K(p110α) could be a novel therapeutic approach to reduce the progression to heart failure and death in diabetes-affected patients.

Published

2020

36. Standing up to the cardiometabolic consequences of hematological cancers

Author

David W. Dunstan, Julie R. McMullen, Erin J. Howden, Neville Owen, Andre La Gerche, Sharon Avery, Bronwyn A. Kingwell, Garry L. Jennings, and Jane F Arthur

Subjects

Oncology, medicine.medical_specialty, Heart Diseases, Context (language use), Disease, 030204 cardiovascular system & hematology, 03 medical and health sciences, 0302 clinical medicine, Metabolic Diseases, Deconditioning, Internal medicine, Diabetes mellitus, medicine, Animals, Humans, Obesity, Cardiotoxicity, Leukemia, Physical activity, business.industry, Diabetes, Hematological cancer, Cardiac function, Disease Management, Cancer, Hematology, Cardiovascular disease, medicine.disease, Combined Modality Therapy, Sedentary behavior, Hematologic Neoplasms, 030220 oncology & carcinogenesis, Heart Function Tests, Physical deconditioning, Metabolic syndrome, Energy Metabolism, business

Abstract

Hematological cancer survivors are highly vulnerable to cardiometabolic complications impacting long-term health status, quality of life and survival. Elevated risk of diabetes and cardiovascular disease arises not only from the effects of the cancers themselves, but also from the toxic effects of cancer therapies, and deconditioning arising from reduced physical activity levels. Regular physical activity can circumvent or reverse adverse effects on the heart, skeletal muscle, vasculature and blood cells, through a combination of systemic and molecular mechanisms. We review the link between hematological cancers and cardiometabolic risk with a focus on adult survivors, including the contributing mechanisms and discuss the potential for physical activity interventions, which may act to oppose the negative effects of both physical deconditioning and therapies (conventional and targeted) on metabolic and growth signaling (kinase) pathways in the heart and beyond. In this context, we focus particularly on strategies targeting reducing and breaking up sedentary time and provide recommendations for future research.

Published

2018

37. Lipidomic Profiles of the Heart and Circulation in Response to Exercise versus Cardiac Pathology: A Resource of Potential Biomarkers and Drug Targets

Author

Kevin Huynh, Julie R. McMullen, Corey Giles, Jenny Y. Y. Ooi, Xiao-Ming Gao, Helen Kiriazis, Yow Keat Tham, Bianca C. Bernardo, and Peter J. Meikle

Subjects

0301 basic medicine, Heart growth, Cardiomegaly, Disease, 030204 cardiovascular system & hematology, Bioinformatics, General Biochemistry, Genetics and Molecular Biology, Mice, 03 medical and health sciences, 0302 clinical medicine, Endurance training, Physical Conditioning, Animal, Atrial Fibrillation, medicine, Animals, Humans, lcsh:QH301-705.5, Phospholipids, Heart Failure, Pressure overload, Sphingolipids, business.industry, Myocardium, Hypertrophic cardiomyopathy, Atrial fibrillation, medicine.disease, Sphingolipid, Disease Models, Animal, 030104 developmental biology, lcsh:Biology (General), Heart failure, business, Biomarkers

Abstract

Summary: Exercise-induced heart growth provides protection against cardiovascular disease, whereas disease-induced heart growth leads to heart failure. These distinct forms of growth are associated with different molecular profiles (e.g., mRNAs, non-coding RNAs, and proteins), and targeting differentially regulated genes has therapeutic potential for heart failure. The effects of exercise on the cardiac and circulating lipidomes in comparison to disease are unclear. Lipidomic profiling was performed on hearts and plasma of mice subjected to swim endurance training or a cardiac disease model (moderate or severe pressure overload). Several sphingolipid species and phospholipids containing omega-3/6 fatty acids were distinctly altered in heart and/or plasma with exercise versus pressure overload. A subset of lipids was validated in an independent mouse model with heart failure and atrial fibrillation. This study highlights the adaptations that occur to lipid profiles in response to endurance training versus pathology and provides a resource to investigate potential therapeutic targets and biomarkers. : Tham et al. utilized a HPLC-ESI/MS/MS targeted lipidomics approach to show distinct remodeling of the cardiac and plasma lipidomes in response to exercise in comparison to heart disease stimuli. Differentially altered lipids were validated in a model with heart failure and atrial fibrillation and represent potential biomarkers and drug targets. Keywords: lipids, heart, exercise, physiological hypertrophy, pathological hypertrophy, atrial fibrillation, phospholipids, sphingolipids, biomarkers, treatment

Published

2018

38. Upregulated galectin-3 is not a critical disease mediator of cardiomyopathy induced by β2-adrenoceptor overexpression

Author

Anthony M. Dart, Julie R. McMullen, Yan Yang, Yidan Su, My-Nhan Nguyen, Helen Kiriazis, Xiao-Jun Du, and Xiao-Ming Gao

Subjects

0301 basic medicine, Physiology, Cardiac fibrosis, business.industry, Cardiomyopathy, 030204 cardiovascular system & hematology, medicine.disease, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Downregulation and upregulation, Fibrosis, Galectin-3, Physiology (medical), Knockout mouse, medicine, Cancer research, Myocardial fibrosis, Cardiology and Cardiovascular Medicine, Ventricular remodeling, business

Abstract

Preclinical studies have demonstrated that anti-galectin-3 (Gal-3) interventions are effective in attenuating cardiac remodeling, fibrosis, and dysfunction. We determined, in a transgenic (TG) mouse model of fibrotic cardiomyopathy, whether Gal-3 expression was elevated and whether Gal-3 played a critical role in disease development. We studied mice with fibrotic cardiomyopathy attributable to cardiac overexpression of human β2-adrenoceptors (β2-TG). Cardiac expression levels of Gal-3 and fibrotic or inflammatory genes were determined. The effect of Gal-3 inhibition in β2-TG mice was studied by treatment with Gal-3 inhibitors ( N-acetyllactosamine and modified citrus pectin) or by deletion of Gal-3 through crossing β2-TG and Gal-3 knockout mice. Changes in cardiomyopathy phenotypes were assessed by echocardiography and biochemical assays. In β2-TG mice at 3, 6, and 9 mo of age, upregulation of Gal-3 expression was observed at mRNA (~6- to 15-fold) and protein (~4- to 8-fold) levels. Treatment of β2-TG mice with N-acetyllactosamine (3 wk) or modified citrus pectin (3 mo) did not reverse cardiac fibrosis, inflammation, and cardiomyopathy. Similarly, Gal-3 gene deletion in β2-TG mice aged 3 and 9 mo did not rescue the cardiomyopathy phenotype. In conclusion, the β2-TG model of cardiomyopathy showed a robust upregulation of Gal-3 that correlated with disease severity, but Gal-3 inhibitors or Gal-3 gene deletion had no effect in halting myocardial fibrosis, remodeling, and dysfunction. Gal-3 may not be critical for cardiac fibrogenesis and remodeling in this cardiomyopathy model. NEW & NOTEWORTHY We showed a robust upregulation of cardiac galectin-3 (Gal-3) expression in a mouse model of cardiomyopathy attributable to cardiomyocyte-restricted transgenic activation of β2-adrenoceptors. However, pharmacological and genetic inhibition of Gal-3 did not confer benefit in this model, implying that Gal-3 may not be a critical disease mediator of cardiac remodeling in this model.

Published

2018

39. Understanding Key Mechanisms of Exercise-Induced Cardiac Protection to Mitigate Disease: Current Knowledge and Emerging Concepts

Author

Julie R. McMullen, Bianca C. Bernardo, Kate L. Weeks, Jenny Y. Y. Ooi, and Natalie L. Patterson

Subjects

0301 basic medicine, Cardiac function curve, Heart Diseases, Heart disease, Physiology, Disease, 030204 cardiovascular system & hematology, Cardiovascular Physiological Phenomena, Transcriptome, 03 medical and health sciences, 0302 clinical medicine, Physiology (medical), medicine, Metabolome, Animals, Humans, Myocytes, Cardiac, Endoplasmic reticulum unfolded protein response, Exercise, Molecular Biology, Genome, business.industry, Cardiac myocyte, Heart, General Medicine, medicine.disease, 030104 developmental biology, Heart failure, business, Neuroscience

Abstract

The benefits of exercise on the heart are well recognized, and clinical studies have demonstrated that exercise is an intervention that can improve cardiac function in heart failure patients. This has led to significant research into understanding the key mechanisms responsible for exercise-induced cardiac protection. Here, we summarize molecular mechanisms that regulate exercise-induced cardiac myocyte growth and proliferation. We discuss in detail the effects of exercise on other cardiac cells, organelles, and systems that have received less or little attention and require further investigation. This includes cardiac excitation and contraction, mitochondrial adaptations, cellular stress responses to promote survival (heat shock response, ubiquitin-proteasome system, autophagy-lysosomal system, endoplasmic reticulum unfolded protein response, DNA damage response), extracellular matrix, inflammatory response, and organ-to-organ crosstalk. We summarize therapeutic strategies targeting known regulators of exercise-induced protection and the challenges translating findings from bench to bedside. We conclude that technological advancements that allow for in-depth profiling of the genome, transcriptome, proteome and metabolome, combined with animal and human studies, provide new opportunities for comprehensively defining the signaling and regulatory aspects of cell/organelle functions that underpin the protective properties of exercise. This is likely to lead to the identification of novel biomarkers and therapeutic targets for heart disease.

Published

2018

40. Phosphoinositide 3-kinase (p110α) gene delivery limits diabetes-induced cardiac NADPH oxidase and cardiomyopathy in a mouse model with established diastolic dysfunction

Author

Miles J. De Blasio, Xiao-Jun Du, Chengxue Qin, Kate L. Weeks, Sarah Rosli, Julie R. McMullen, Helen Kiriazis, Paul Gregorevic, Darnel Prakoso, Rebecca H. Ritchie, and Hongwei Qian

Subjects

Male, 0301 basic medicine, medicine.medical_specialty, Time Factors, Diabetic Cardiomyopathies, Cardiac fibrosis, Genetic Vectors, Cardiomyopathy, Diastole, 030204 cardiovascular system & hematology, Ventricular Function, Left, Diabetes Mellitus, Experimental, Mice, Ventricular Dysfunction, Left, 03 medical and health sciences, 0302 clinical medicine, Transduction, Genetic, Diabetic cardiomyopathy, Diabetes mellitus, Internal medicine, Animals, Medicine, Ventricular remodeling, NADPH oxidase, Ventricular Remodeling, biology, business.industry, Myocardium, NADPH Oxidases, Genetic Therapy, General Medicine, Dependovirus, medicine.disease, 030104 developmental biology, Endocrinology, Heart failure, biology.protein, Cardiology, Phosphatidylinositol 3-Kinase, business, Signal Transduction

Abstract

Phosphoinositide 3-kinase [PI3K (p110α)] is able to negatively regulate the diabetes-induced increase in NADPH oxidase in the heart. Patients affected by diabetes exhibit significant cardiovascular morbidity and mortality, at least in part due to a cardiomyopathy characterized by oxidative stress and left ventricular (LV) dysfunction. Thus, PI3K (p110α) may represent a novel approach to protect the heart from diabetes-induced cardiac oxidative stress and dysfunction. In the present study, we investigated the therapeutic potential of a delayed intervention with cardiac-targeted PI3K gene therapy, administered to mice with established diabetes-induced LV diastolic dysfunction. Diabetes was induced in 6-week-old male mice by streptozotocin (STZ). After 8 weeks of untreated diabetes, LV diastolic dysfunction was confirmed by a reduction in echocardiography-derived transmitral E/A ratio. Diabetic and non-diabetic mice were randomly allocated to receive either recombinant adeno-associated viral vector-6 carrying a constitutively-active PI3K construct (recombinant adeno-associated-virus 6-constitutively active PI3K (p110α) (caPI3K) (rAAV6-caPI3K), single i.v. injection, 2 × 1011 vector genomes) or null vector, and were followed for a further 6 or 8 weeks. At study endpoint, diabetes-induced LV dysfunction was significantly attenuated by a single administration of rAAV6-caPI3K, administered 8 weeks after the induction of diabetes. Diabetes-induced impairments in each of LV NADPH oxidase, endoplasmic reticulum (ER) stress, apoptosis, cardiac fibrosis and cardiomyocyte hypertrophy, in addition to LV systolic dysfunction, were attenuated by delayed intervention with rAAV6-caPI3K. Hence, our demonstration that cardiac-targeted PI3K (p110α) gene therapy limits diabetes-induced up-regulation of NADPH oxidase and cardiac remodelling suggests new insights into promising approaches for the treatment of diabetic cardiomyopathy, at a clinically relevant time point (after diastolic dysfunction is manifested).

Published

2017

41. Proteome characterisation of extracellular vesicles isolated from heart

Author

Aya Matsumoto, Haoyun Fang, Bethany Claridge, Alin Rai, Jieting Luo, David W. Greening, and Julie R. McMullen

Subjects

Proteomics, Differential centrifugation, 0303 health sciences, Proteome, TNNT2, Chemistry, 030302 biochemistry & molecular biology, Endothelial Cells, Biochemistry, Cell biology, Extracellular Vesicles, Mice, 03 medical and health sciences, Proteostasis, Animals, TSG101, Glycolysis, Molecular Biology, Biomarkers, Intracellular, 030304 developmental biology

Abstract

Cardiac intercellular communication is critical for heart function and often dysregulated in cardiovascular diseases. While cardiac extracellular vesicles (cEVs) are emerging mediators of signalling, their isolation remains a technical challenge hindering our understanding of cEV protein composition. Here, we utilised Langendorff-collagenase-based enzymatic perfusion and differential centrifugation to isolate cEVs from mouse heart (yield 3-6 μg/heart). cEVs are ∼200 nm, express classical EV markers (Cd63/81/9+ , Tsg101+ , Pdcd6ip/Alix+ ), and are depleted of blood (Alb/Fga/Hba) and cardiac damage markers (Mb, Tnnt2, Ldhb). Comparison with mechanically-derived EVs revealed greater detection of EV markers and decreased cardiac damage contaminants. Mass spectrometry-based proteomic profiling revealed 1721 proteins in cEVs, implicated in proteasomal and autophagic proteostasis, glycolysis, and fatty acid metabolism; essential functions often disrupted in cardiac pathologies. There was striking enrichment of 942 proteins in cEVs compared to mouse heart tissue - implicated in EV biogenesis, antioxidant activity, and lipid transport, suggesting active cargo selection and specialised function. Interestingly, cEVs contain marker proteins for cardiomyocytes, cardiac progenitors, B-cells, T-cells, macrophages, smooth muscle cells, endothelial cells, and cardiac fibroblasts, suggesting diverse cellular origin. We present a method of cEV isolation and provide insight into potential functions, enabling future studies into EV roles in cardiac physiology and disease.

Published

2021

42. Old Drug, New Trick: Tilorone, a Broad-Spectrum Antiviral Drug as a Potential Anti-Fibrotic Therapeutic for the Diseased Heart

Author

Julie R. McMullen, David M. Kaye, D. Donner, Helen Kiriazis, Catherine E. Winbanks, Duncan Horlock, Xiao-Ming Gao, Bianca C. Bernardo, and Paul Gregorevic

Subjects

0301 basic medicine, Cardiac fibrosis, heart failure, lcsh:Medicine, lcsh:RS1-441, Pharmaceutical Science, 030204 cardiovascular system & hematology, Pharmacology, fibroblast, lcsh:Pharmacy and materia medica, 03 medical and health sciences, 0302 clinical medicine, In vivo, Fibrosis, Drug Discovery, Medicine, Trichrome stain, Pressure overload, therapy, treatment, business.industry, Communication, fibrosis, lcsh:R, Tilorone, pressure overload, medicine.disease, tilorone, 030104 developmental biology, Heart failure, Molecular Medicine, business, Transforming growth factor, medicine.drug

Abstract

Cardiac fibrosis is associated with most forms of cardiovascular disease. No reliable therapies targeting cardiac fibrosis are available, thus identifying novel drugs that can resolve or prevent fibrosis is needed. Tilorone, an antiviral agent, can prevent fibrosis in a mouse model of lung disease. We investigated the anti-fibrotic effects of tilorone in human cardiac fibroblasts in vitro by performing a radioisotopic assay for [3H]-proline incorporation as a proxy for collagen synthesis. Exploratory studies in human cardiac fibroblasts treated with tilorone (10 µM) showed a significant reduction in transforming growth factor-β induced collagen synthesis compared to untreated fibroblasts. To determine if this finding could be recapitulated in vivo, mice with established pathological remodelling due to four weeks of transverse aortic constriction (TAC) were administered tilorone (50 mg/kg, i.p) or saline every third day for eight weeks. Treatment with tilorone was associated with attenuation of fibrosis (assessed by Masson’s trichrome stain), a favourable cardiac gene expression profile and no further deterioration of cardiac systolic function determined by echocardiography compared to saline treated TAC mice. These data demonstrate that tilorone has anti-fibrotic actions in human cardiac fibroblasts and the adult mouse heart, and represents a potential novel therapy to treat fibrosis associated with heart failure.

Published

2021

43. Oestrogen Receptor α in the Heart is Critical for Protection Against Systemic Obesity in Female Mice

Author

L. Woon, Bianca C. Bernardo, P. Chen, Kate L. Weeks, E. Abel, S. Khan, Julie R. McMullen, Yow Keat Tham, Natalie A. Mellett, S. Yildiz, Peter J. Meikle, and C. Tai

Subjects

Pulmonary and Respiratory Medicine, medicine.medical_specialty, Endocrinology, business.industry, Internal medicine, medicine, Cardiology and Cardiovascular Medicine, medicine.disease, business, Obesity, Oestrogen receptor α

Published

2021

44. Generation and Characterisation of Novel PI3K-Based Gene Therapies for the Treatment of Heart Failure

Author

Kate L. Weeks, Colleen J. Thomas, D. Donner, Sebastian Bass-Stringer, Julie R. McMullen, Bianca C. Bernardo, Paul Gregorevic, A. Brown, Clive N. May, and Helen Kiriazis

Subjects

Pulmonary and Respiratory Medicine, business.industry, Heart failure, medicine, Cardiology and Cardiovascular Medicine, Bioinformatics, medicine.disease, business, Gene, PI3K/AKT/mTOR pathway

Published

2021

45. Long non-coding RNAs (lncRNAs) in skeletal and cardiac muscle: potential therapeutic and diagnostic targets?

Author

Brian G. Drew and Julie R. McMullen

Subjects

0301 basic medicine, Duchenne muscular dystrophy, Therapeutics, Computational biology, Biology, Bioinformatics, 03 medical and health sciences, Diagnosis, medicine, Animals, Humans, Facioscapulohumeral muscular dystrophy, Disease, Muscle, Skeletal, Messenger RNA, Myocardium, Cardiac muscle, Skeletal muscle, RNA, General Medicine, medicine.disease, Non-coding RNA, 030104 developmental biology, medicine.anatomical_structure, RNA, Long Noncoding, Human genome

Abstract

The recent discovery that thousands of RNAs are transcribed by the cell but are never translated into protein, highlights a significant void in our current understanding of how transcriptional networks regulate cellular function. This is particularly astounding when we consider that over 75% of the human genome is transcribed into RNA, but only approximately 2% of RNA is translated into known proteins. This raises the question as to what function the other so-called ‘non-coding RNAs’ (ncRNAs) are performing in the cell. Over the last decade, an enormous amount of research has identified several classes of ncRNAs, predominantly short ncRNAs ( 200 nt). Several studies have recently shown that long non-coding RNAs (lncRNAs) are associated with tissue development and disease, particularly in cell types that undergo differentiation such as stem cells, cancer cells and striated muscle (skeletal/cardiac). Therefore, understanding the function of these lncRNAs and designing strategies to detect and manipulate them, may present novel therapeutic and diagnostic opportunities. This review will explore the current literature on lncRNAs in skeletal and cardiac muscle and discuss their recent implication in development and disease. Lastly, we will also explore the possibility of using lncRNAs as therapeutic and diagnostic tools and discuss the opportunities and potential shortcomings to these applications. * AAV, : adeno-associated virus; APF, : autophagy promoting factor; ASO, : antisense oligonucleotide; CARL, : cardiac apoptosis regulated lncRNA; CHAST, : cardiac hypertrophy-associated transcript; CHRF, : cardiac hypertrophy related factor; DRR, : distal regulatory region; DRR-eRNA, : DRR-enhancer RNA; DMD, : Duchenne muscular dystrophy; Dppa2 , : developmental pluripotency-associated 2 ; DUM , : Dppa2 upstream binding muscle lncRNA ; FSHD, : facioscapulohumeral muscular dystrophy; IMP2, : IGF2-mRNA-binding protein 2; lncRNA, : long non-coding RNA; LV, : left ventricular; MDRL, : mitochondrial dynamic related lncRNA; mRNA, : messenger RNA; nt, : nucleotides

Published

2016

46. Molecular Aspects of Exercise-induced Cardiac Remodeling

Author

Julie R. McMullen and Bianca C. Bernardo

Subjects

0301 basic medicine, medicine.medical_specialty, Angiogenesis, Strenuous exercise, Hemodynamics, 030204 cardiovascular system & hematology, Muscle hypertrophy, Contractility, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Humans, Myocytes, Cardiac, Cardiomegaly, Exercise-Induced, Molecular Biology, Ventricular Remodeling, business.industry, Cardiac myocyte, General Medicine, Cardiomyopathy, Hypertrophic, medicine.disease, 030104 developmental biology, Heart failure, cardiovascular system, Cardiology, Cardiology and Cardiovascular Medicine, business, Hormone

Abstract

Exercise-induced cardiac remodeling is typically an adaptive response associated with cardiac myocyte hypertrophy and renewal, increased cardiac myocyte contractility, sarcomeric remodeling, cell survival, metabolic and mitochondrial adaptations, electrical remodeling, and angiogenesis. Initiating stimuli/triggers of cardiac remodeling include increased hemodynamic load, increased sympathetic activity, and the release of hormones and growth factors. Prolonged and strenuous exercise may lead to maladaptive exercise-induced cardiac remodeling including cardiac dysfunction and arrhythmia. In addition, this article describes novel therapeutic approaches for the treatment of heart failure that target mechanisms responsible for adaptive exercise-induced cardiac remodeling, which are being developed and tested in preclinical models.

Published

2016

47. Sex differences in response to miRNA‐34a therapy in mouse models of cardiac disease: identification of sex‐, disease‐ and treatment‐regulated miRNAs

Author

Junichi Sadoshima, Natalie L. Patterson, Jenny Y. Y. Ooi, Aya Matsumoto, Julie R. McMullen, Saloni Singla, Bianca C. Bernardo, Ruby C.Y. Lin, Yow Keat Tham, Susanna Obad, and Helen Kiriazis

Subjects

Cardiomyopathy, Dilated, Male, 0301 basic medicine, Cardiac function curve, medicine.medical_specialty, Heart disease, Physiology, Cardiac fibrosis, Cardiomyopathy, Cardiomegaly, 030204 cardiovascular system & hematology, Cardiovascular, Bioinformatics, Mice, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Humans, Animals, Medicine, Gene silencing, Natriuretic Peptides, Heart Failure, Sex Characteristics, Ventricular Remodeling, business.industry, Heart, Dilated cardiomyopathy, medicine.disease, Disease Models, Animal, MicroRNAs, 030104 developmental biology, Cardiovascular Diseases, Heart failure, Cardiology, Female, Heart enlargement, business, Perspectives

Abstract

Key points MicroRNA (miRNA)-based therapies are in development for numerous diseases, including heart disease. Currently, very limited basic information is available on the regulation of specific miRNAs in male and female hearts in settings of disease. The identification of sex-specific miRNA signatures has implications for translation into the clinic and suggests the need for customised therapy. In the present study, we found that a miRNA-based treatment inhibiting miRNA-34a (miR-34a) was more effective in females in a setting of moderate dilated cardiomyopathy than in males. Furthermore, the treatment showed little benefit for either sex in a setting of more severe dilated cardiomyopathy associated with atrial fibrillation. The results highlight the importance of understanding the effect of miRNA-based therapies in cardiac disease settings in males and females. Abstract MicroRNA (miRNA)-34a (miR-34a) is elevated in the diseased heart in mice and humans. Previous studies have shown that inhibiting miR-34a in male mice in settings of pathological cardiac hypertrophy or ischaemia protects the heart against progression to heart failure. Whether inhibition of miR-34a protects the female heart is unknown. Furthermore, the therapeutic potential of silencing miR-34a in settings of dilated cardiomyopathy (DCM) and atrial fibrillation (AF) has not been assessed previously. In the present study, we examined the effect of silencing miR-34a in males and females in (1) a model of moderate DCM and (2) a model of severe DCM with AF. The cardiac disease models were administered with a locked nucleic acid-modified oligonucleotide (LNA-antimiR-34a) at 6-7 weeks of age when the models display cardiac dysfunction and conduction abnormalities. Cardiac function and morphology were measured 6 weeks after treatment. In the present study, we show that inhibition of miR-34a provides more protection in the DCM model in females than males. Disease prevention in LNA-antimiR-34a treated DCM female mice was characterized by attenuated heart enlargement and lung congestion, lower expression of cardiac stress genes (B-type natriuretic peptide, collagen gene expression), less cardiac fibrosis and better cardiac function. There was no evidence of significant protection in the severe DCM and AF model in either sex. Sex- and treatment-dependent regulation of miRNAs was also identified in the diseased heart, and may explain the differential response of males and females. These studies highlight the importance of examining the impact of miRNA-based drugs in both sexes and under different disease conditions.

Published

2016

48. 094 Characterisation of Novel Knockout Mouse Models to Investigate the Role of B55α in the Heart

Author

N. Sergienko, D. Donner, Kate L. Weeks, Helen Kiriazis, and Julie R. McMullen

Subjects

Pulmonary and Respiratory Medicine, business.industry, Knockout mouse, Medicine, Cardiology and Cardiovascular Medicine, business, Cell biology

Published

2020

49. Galectin-3 deficiency ameliorates fibrosis and remodeling in dilated cardiomyopathy mice with enhanced Mst1 signaling

Author

Qun Lu, Zara Thomas, Mark Ziemann, Haloom Rafehi, Assam El-Osta, D. Donner, Junichi Sadoshima, Xiao-Jun Du, Julie R. McMullen, My-Nhan Nguyen, Yidan Su, Wei-Bo Zhao, and Helen Kiriazis

Subjects

0301 basic medicine, Genetically modified mouse, Cardiomyopathy, Dilated, Physiology, Cardiac fibrosis, Galectin 3, Cardiomyopathy, 030204 cardiovascular system & hematology, 03 medical and health sciences, Mice, 0302 clinical medicine, Downregulation and upregulation, Fibrosis, Physiology (medical), Proto-Oncogene Proteins, medicine, Animals, Myocytes, Cardiac, Ventricular remodeling, Ventricular Remodeling, business.industry, Hepatocyte Growth Factor, Dilated cardiomyopathy, medicine.disease, Extracellular Matrix, 030104 developmental biology, Galectin-3, Cancer research, Collagen, Cardiology and Cardiovascular Medicine, business, Signal Transduction

Abstract

Dilated cardiomyopathy (DCM) is a major cause of heart failure without effective therapy. Fibrogenesis plays a key role in the development of DCM, but little is known of the expression of the profibrotic factor galectin-3 (Gal-3) and its role in DCM pathophysiology. In a mouse DCM model with transgenic (TG) overexpression of mammalian sterile 20-like kinase 1 (Mst1), we studied Gal-3 expression and effects of the Gal-3 inhibitor modified citrus pectin (MCP) or Gal-3 gene knockout (KO). Gal-3 deletion in TG mice (TG/KO) was achieved by crossbreeding Mst1-TG mice with Gal-3 KO mice. The DCM phenotype was assessed by echocardiography and micromanometry. Cardiac expression of Gal-3 and fibrosis were determined. The cardiac transcriptome was profiled by RNA sequencing. Mst1-TG mice at 3−8 mo of age exhibited upregulated expression of Gal-3 by ~40-fold. TG mice had dilatation of cardiac chambers, suppressed left ventricular (LV) ejection fraction, poor LV contractility and relaxation, a threefold increase in LV collagen content, and upregulated fibrotic genes. Four-month treatment with MCP showed no beneficial effects. Gal-3 deletion in Mst1-TG mice attenuated chamber dilatation, organ congestion, and fibrogenesis. RNA sequencing identified profound disturbances by Mst1 overexpression in the cardiac transcriptome, which largely remained in TG/KO hearts. Gal-3 deletion in Mst1-TG mice, however, partially reversed the dysregulated transcriptional signaling involving extracellular matrix remodeling and collagen formation. We conclude that cardiac Mst1 activation leads to marked Gal-3 upregulation and transcriptome disturbances in the heart. Gal-3 deficiency attenuated cardiac remodeling and fibrotic signaling.NEW & NOTEWORTHY We found in a transgenic mouse dilated cardiomyopathy (DCM) model a pronounced upregulation of galectin-3 in cardiomyocytes. Galectin-3 gene deletion reduced cardiac fibrosis and fibrotic gene profiles and ameliorated cardiac remodeling and dysfunction. These benefits of galectin-3 deletion were in contrast to the lack of effect of treatment with the galectin-3 inhibitor modified citrus pectin. Our study suggests that suppression of galectin-3 mRNA expression could be used to treat DCM with high cardiac galectin-3 content.

Published

2018

50. Multiple receptors converge on H2-Q10 to regulate NK and γδT-cell development

Author

Lucy C. Sullivan, Julie R. McMullen, Katharine J. Goodall, Sidonia B G Eckle, Angela Nguyen, Patrick Bertolino, Daniel M. Andrews, and Aya Matsumoto

Subjects

0301 basic medicine, T cell, Immunology, Antigen presentation, CD8-Positive T-Lymphocytes, Major histocompatibility complex, Ligands, Natural killer cell, Immunophenotyping, Immunomodulation, 03 medical and health sciences, Mice, 0302 clinical medicine, Immune system, Antigen, HLA-E, T-Lymphocyte Subsets, medicine, Immunology and Allergy, Animals, Receptors, Immunologic, Receptor, biology, H-2 Antigens, Cell Differentiation, Receptors, Antigen, T-Cell, gamma-delta, Cell Biology, Cell biology, Killer Cells, Natural, 030104 developmental biology, medicine.anatomical_structure, Liver, biology.protein, Biomarkers, 030215 immunology, Protein Binding

Abstract

Class Ib major histocompatibility complex (MHC) is an extended family of molecules, which demonstrate tissue-specific expression and presentation of monomorphic antigens. These characteristics tend to imbue class Ib MHC with unique functions. H2-Q10 is potentially one such molecule that is overexpressed in the liver but its immunological function is not known. We have previously shown that H2-Q10 is a ligand for the natural killer cell receptor Ly49C and now, using H2-Q10-deficient mice, we demonstrate that H2-Q10 can also stabilize the expression of Qa-1b. In the absence of H2-Q10, the development and maturation of conventional hepatic natural killer cells is disrupted. We also provide evidence that H2-Q10 is a new high affinity ligand for CD8αα and controls the development of liver-resident CD8αα γδT cells. These data demonstrate that H2-Q10 has multiple roles in the development of immune subsets and identify an overlap of recognition within the class Ib MHC that is likely to be relevant to the regulation of immunity.

Published

2018