Your search keyword '"Burmeister BT"' showing total 9 results

1. RARG variant predictive of doxorubicin-induced cardiotoxicity identifies a cardioprotective therapy.

Author

Magdy T, Jiang Z, Jouni M, Fonoudi H, Lyra-Leite D, Jung G, Romero-Tejeda M, Kuo HH, Fetterman KA, Gharib M, Burmeister BT, Zhao M, Sapkota Y, Ross CJ, Carleton BC, Bernstein D, and Burridge PW

Subjects

Animals, Antibiotics, Antineoplastic adverse effects, Doxorubicin adverse effects, Genome-Wide Association Study, Humans, Mice, Myocytes, Cardiac, Cardiotoxicity, Induced Pluripotent Stem Cells

Abstract

Doxorubicin is an anthracycline chemotherapy agent effective in treating a wide range of malignancies, but its use is limited by dose-dependent cardiotoxicity. A recent genome-wide association study identified a SNP (rs2229774) in retinoic acid receptor-γ (RARG) as statistically associated with increased risk of anthracycline-induced cardiotoxicity. Here, we show that human induced pluripotent stem cell-derived cardiomyocytes (hiPSC-CMs) from patients with rs2229774 and who suffered doxorubicin-induced cardiotoxicity (DIC) are more sensitive to doxorubicin. We determine that the mechanism of this RARG variant effect is mediated via suppression of topoisomerase 2β (TOP2B) expression and activation of the cardioprotective extracellular regulated kinase (ERK) pathway. We use patient-specific hiPSC-CMs as a drug discovery platform, determining that the RARG agonist CD1530 attenuates DIC, and we confirm this cardioprotective effect in an established in vivo mouse model of DIC. This study provides a rationale for clinical prechemotherapy genetic screening for rs2229774 and a foundation for the clinical use of RARG agonist treatment to protect cancer patients from DIC., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2021 Elsevier Inc. All rights reserved.)

Published

2021

2. Validating the pharmacogenomics of chemotherapy-induced cardiotoxicity: What is missing?

Author

Magdy T, Burmeister BT, and Burridge PW

Subjects

Animals, Antineoplastic Agents administration & dosage, Cardiotoxicity genetics, Cardiotoxicity physiopathology, Dose-Response Relationship, Drug, Genetic Predisposition to Disease, Genome-Wide Association Study, Humans, Induced Pluripotent Stem Cells cytology, Myocytes, Cardiac drug effects, Polymorphism, Single Nucleotide, Antineoplastic Agents adverse effects, Cardiotoxicity etiology, Pharmacogenetics

Abstract

The cardiotoxicity of certain chemotherapeutic agents is now well-established, and has led to the development of the field of cardio-oncology, increased cardiac screening of cancer patients, and limitation of patients' maximum cumulative chemotherapeutic dose. The effect of chemotherapeutic regimes on the heart largely involves cardiomyocyte death, leading to cardiomyopathy and heart failure, or the induction of arrhythmias. Of these cardiotoxic drugs, those resulting in clinical cardiotoxicity can range from 8 to 26% for doxorubicin, 7-28% for trastuzumab, or 5-30% for paclitaxel. For tyrosine kinase inhibitors, QT prolongation and arrhythmia, ischemia and hypertension have been reported in 2-35% of patients. Furthermore, newly introduced chemotherapeutic agents are commonly used as part of changed combinational regimens with significantly increased incidence of cardiotoxicity. It is widely believed that the mechanism of action of these drugs is often independent of their cardiotoxicity, and the basis for why these drugs specifically affect the heart has yet to be established. The genetic rationale for why certain patients experience cardiotoxicity whilst other patients can tolerate high chemotherapy doses has proven highly illusive. This has led to significant genomic efforts using targeted and genome-wide association studies (GWAS) to divine the pharmacogenomic cause of this predilection. With the advent of human induced pluripotent stem cell-derived cardiomyocytes (hiPSC-CMs), the putative risk and protective role of single nucleotide polymorphisms (SNPs) can now be validated in a human model. Here we review the state of the art knowledge of the genetic predilection to chemotherapy-induced cardiotoxicity and discuss the future for establishing and validating the role of the genome in this disease., Competing Interests: The authors declare that there are no conflicts of interest., (Copyright © 2016 Elsevier Inc. All rights reserved.)

Published

2016

3. Protein Kinase A (PKA) Phosphorylation of Shp2 Protein Inhibits Its Phosphatase Activity and Modulates Ligand Specificity.

Author

Burmeister BT, Wang L, Gold MG, Skidgel RA, O'Bryan JP, and Carnegie GK

Subjects

Animals, Cells, Cultured, HEK293 Cells, Humans, Ligands, Mutation, Phosphorylation, Protein Binding, Rats, Receptors, Adrenergic, beta metabolism, Serine chemistry, Signal Transduction, Threonine chemistry, Tyrosine chemistry, src Homology Domains, Cardiomegaly genetics, Cyclic AMP-Dependent Protein Kinases metabolism, Protein Tyrosine Phosphatase, Non-Receptor Type 11 metabolism

Abstract

Pathological cardiac hypertrophy (an increase in cardiac mass resulting from stress-induced cardiac myocyte growth) is a major factor underlying heart failure. Src homology 2 domain-containing phosphatase (Shp2) is critical for cardiac function because mutations resulting in loss of Shp2 catalytic activity are associated with congenital cardiac defects and hypertrophy. We identified a novel mechanism of Shp2 inhibition that may promote cardiac hypertrophy. We demonstrate that Shp2 is a component of the protein kinase A anchoring protein (AKAP)-Lbc complex. AKAP-Lbc facilitates PKA phosphorylation of Shp2, which inhibits Shp2 phosphatase activity. We identified two key amino acids in Shp2 that are phosphorylated by PKA. Thr-73 contributes a helix cap to helix αB within the N-terminal SH2 domain of Shp2, whereas Ser-189 occupies an equivalent position within the C-terminal SH2 domain. Utilizing double mutant PKA phosphodeficient (T73A/S189A) and phosphomimetic (T73D/S189D) constructs, in vitro binding assays, and phosphatase activity assays, we demonstrate that phosphorylation of these residues disrupts Shp2 interaction with tyrosine-phosphorylated ligands and inhibits its protein-tyrosine phosphatase activity. Overall, our data indicate that AKAP-Lbc integrates PKA and Shp2 signaling in the heart and that AKAP-Lbc-associated Shp2 activity is reduced in hypertrophic hearts in response to chronic β-adrenergic stimulation and PKA activation. Therefore, although induction of cardiac hypertrophy is a multifaceted process, inhibition of Shp2 activity through AKAP-Lbc-anchored PKA is a previously unrecognized mechanism that may promote this compensatory response., (© 2015 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2015

4. UCR1C is a novel activator of phosphodiesterase 4 (PDE4) long isoforms and attenuates cardiomyocyte hypertrophy.

Author

Wang L, Burmeister BT, Johnson KR, Baillie GS, Karginov AV, Skidgel RA, O'Bryan JP, and Carnegie GK

Subjects

A Kinase Anchor Proteins metabolism, Amino Acid Sequence, Animals, Cardiomegaly metabolism, Cardiomegaly pathology, Cells, Cultured, Cyclic AMP metabolism, Cyclic AMP-Dependent Protein Kinases metabolism, Cyclic Nucleotide Phosphodiesterases, Type 4 chemistry, HEK293 Cells, Humans, Molecular Sequence Data, Myocytes, Cardiac metabolism, Phosphorylation drug effects, Protein Isoforms chemistry, Protein Isoforms metabolism, Rats, Signal Transduction drug effects, Cardiomegaly drug therapy, Cyclic Nucleotide Phosphodiesterases, Type 4 metabolism, Enzyme Activation drug effects, Myocytes, Cardiac drug effects, Myocytes, Cardiac pathology, Peptides chemistry, Peptides pharmacology

Abstract

Hypertrophy increases the risk of heart failure and arrhythmia. Prevention or reversal of the maladaptive hypertrophic phenotype has thus been proposed to treat heart failure. Chronic β-adrenergic receptor (β-AR) stimulation induces cardiomyocyte hypertrophy by elevating 3',5'-cyclic adenosine monophosphate (cAMP) levels and activating downstream effectors such protein kinase A (PKA). Conversely, hydrolysis of cAMP by phosphodiesterases (PDEs) spatiotemporally restricts cAMP signaling. Here, we demonstrate that PDE4, but not PDE3, is critical in regulating cardiomyocyte hypertrophy, and may represent a potential target for preventing maladaptive hypertrophy. We identify a sequence within the upstream conserved region 1 of PDE4D, termed UCR1C, as a novel activator of PDE4 long isoforms. UCR1C activates PDE4 in complex with A-kinase anchoring protein (AKAP)-Lbc resulting in decreased PKA signaling facilitated by AKAP-Lbc. Expression of UCR1C in cardiomyocytes inhibits hypertrophy in response to chronic β-AR stimulation. This effect is partially due to inhibition of nuclear PKA activity, which decreases phosphorylation of the transcription factor cAMP response element-binding protein (CREB). In conclusion, PDE4 activation by UCR1C attenuates cardiomyocyte hypertrophy by specifically inhibiting nuclear PKA activity., (Published by Elsevier Inc.)

Published

2015

5. The C-terminus of the long AKAP13 isoform (AKAP-Lbc) is critical for development of compensatory cardiac hypertrophy.

Author

Taglieri DM, Johnson KR, Burmeister BT, Monasky MM, Spindler MJ, DeSantiago J, Banach K, Conklin BR, and Carnegie GK

Subjects

A Kinase Anchor Proteins chemistry, A Kinase Anchor Proteins genetics, Angiotensin II adverse effects, Animals, Aorta pathology, Apoptosis, Cardiomegaly chemically induced, Cardiomegaly genetics, Cardiomegaly pathology, Collagen genetics, Collagen metabolism, Female, Gene Expression Regulation, Guanine Nucleotide Exchange Factors chemistry, Guanine Nucleotide Exchange Factors genetics, Heart Failure chemically induced, Heart Failure genetics, Heart Failure pathology, Histone Deacetylases genetics, Histone Deacetylases metabolism, Male, Mice, Mice, Transgenic, Minor Histocompatibility Antigens, Myocardium pathology, Phenylephrine adverse effects, Protein Kinase C genetics, Protein Structure, Tertiary, Signal Transduction, A Kinase Anchor Proteins metabolism, Cardiomegaly metabolism, Guanine Nucleotide Exchange Factors metabolism, Heart Failure metabolism, Myocardium metabolism, Protein Kinase C metabolism

Abstract

The objective of this study was to determine the role of A-Kinase Anchoring Protein (AKAP)-Lbc in the development of heart failure, by investigating AKAP-Lbc-protein kinase D1 (PKD1) signaling in vivo in cardiac hypertrophy. Using a gene-trap mouse expressing a truncated version of AKAP-Lbc (due to disruption of the endogenous AKAP-Lbc gene), that abolishes PKD1 interaction with AKAP-Lbc (AKAP-Lbc-ΔPKD), we studied two mouse models of pathological hypertrophy: i) angiotensin (AT-II) and phenylephrine (PE) infusion and ii) transverse aortic constriction (TAC)-induced pressure overload. Our results indicate that AKAP-Lbc-ΔPKD mice exhibit an accelerated progression to cardiac dysfunction in response to AT-II/PE treatment and TAC. AKAP-Lbc-ΔPKD mice display attenuated compensatory cardiac hypertrophy, increased collagen deposition and apoptosis, compared to wild-type (WT) control littermates. Mechanistically, reduced levels of PKD1 activation are observed in AKAP-Lbc-ΔPKD mice compared to WT mice, resulting in diminished phosphorylation of histone deacetylase 5 (HDAC5) and decreased hypertrophic gene expression. This is consistent with a reduced compensatory hypertrophy phenotype leading to progression of heart failure in AKAP-Lbc-ΔPKD mice. Overall, our data demonstrates a critical in vivo role for AKAP-Lbc-PKD1 signaling in the development of compensatory hypertrophy to enhance cardiac performance in response to TAC-induced pressure overload and neurohumoral stimulation by AT-II/PE treatment., (© 2013.)

Published

2014

6. AKAP13 Rho-GEF and PKD-binding domain deficient mice develop normally but have an abnormal response to β-adrenergic-induced cardiac hypertrophy.

Author

Spindler MJ, Burmeister BT, Huang Y, Hsiao EC, Salomonis N, Scott MJ, Srivastava D, Carnegie GK, and Conklin BR

Subjects

A Kinase Anchor Proteins metabolism, Animals, Breeding, Cardiomegaly chemically induced, Cardiomegaly metabolism, Electrocardiography, Embryo, Mammalian, Female, Gene Expression Regulation, Developmental, Guanine Nucleotide Exchange Factors metabolism, Heart drug effects, Heart embryology, Male, Mice, Mice, Transgenic, Minor Histocompatibility Antigens, Organ Size, Protein Structure, Tertiary, Signal Transduction, A Kinase Anchor Proteins genetics, Cardiomegaly physiopathology, Guanine Nucleotide Exchange Factors genetics, Heart physiopathology, Isoproterenol adverse effects, Myocardial Contraction drug effects, Stroke Volume drug effects

Abstract

Background: A-kinase anchoring proteins (AKAPs) are scaffolding molecules that coordinate and integrate G-protein signaling events to regulate development, physiology, and disease. One family member, AKAP13, encodes for multiple protein isoforms that contain binding sites for protein kinase A (PKA) and D (PKD) and an active Rho-guanine nucleotide exchange factor (Rho-GEF) domain. In mice, AKAP13 is required for development as null embryos die by embryonic day 10.5 with cardiovascular phenotypes. Additionally, the AKAP13 Rho-GEF and PKD-binding domains mediate cardiomyocyte hypertrophy in cell culture. However, the requirements for the Rho-GEF and PKD-binding domains during development and cardiac hypertrophy are unknown., Methodology/principal Findings: To determine if these AKAP13 protein domains are required for development, we used gene-trap events to create mutant mice that lacked the Rho-GEF and/or the protein kinase D-binding domains. Surprisingly, heterozygous matings produced mutant mice at Mendelian ratios that had normal viability and fertility. The adult mutant mice also had normal cardiac structure and electrocardiograms. To determine the role of these domains during β-adrenergic-induced cardiac hypertrophy, we stressed the mice with isoproterenol. We found that heart size was increased similarly in mice lacking the Rho-GEF and PKD-binding domains and wild-type controls. However, the mutant hearts had abnormal cardiac contractility as measured by fractional shortening and ejection fraction., Conclusions: These results indicate that the Rho-GEF and PKD-binding domains of AKAP13 are not required for mouse development, normal cardiac architecture, or β-adrenergic-induced cardiac hypertrophic remodeling. However, these domains regulate aspects of β-adrenergic-induced cardiac hypertrophy.

Published

2013

7. Src homology 2 domain-containing phosphatase 2 (Shp2) is a component of the A-kinase-anchoring protein (AKAP)-Lbc complex and is inhibited by protein kinase A (PKA) under pathological hypertrophic conditions in the heart.

Author

Burmeister BT, Taglieri DM, Wang L, and Carnegie GK

Subjects

A Kinase Anchor Proteins genetics, Animals, Cardiomegaly genetics, Cardiomegaly pathology, Cyclic AMP-Dependent Protein Kinases genetics, Humans, Male, Mice, Minor Histocompatibility Antigens, Protein Binding, Protein Tyrosine Phosphatase, Non-Receptor Type 11 genetics, Proto-Oncogene Proteins genetics, A Kinase Anchor Proteins metabolism, Cardiomegaly enzymology, Cyclic AMP-Dependent Protein Kinases metabolism, Protein Tyrosine Phosphatase, Non-Receptor Type 11 metabolism, Proto-Oncogene Proteins metabolism

Abstract

Background: AKAP-Lbc is a scaffold protein that coordinates cardiac hypertrophic signaling., Results: AKAP-Lbc interacts with Shp2, facilitating its regulation by PKA., Conclusion: AKAP-Lbc integrates PKA and Shp2 signaling in the heart. Under pathological hypertrophic conditions Shp2 is phosphorylated by PKA, and phosphatase activity is inhibited., Significance: Inhibition of Shp2 activity through AKAP-Lbc-anchored PKA is a previously unrecognized mechanism that may promote pathological cardiac hypertrophy. Pathological cardiac hypertrophy (an increase in cardiac mass resulting from stress-induced cardiac myocyte growth) is a major factor underlying heart failure. Our results identify a novel mechanism of Shp2 inhibition that may promote cardiac hypertrophy. We demonstrate that the tyrosine phosphatase, Shp2, is a component of the A-kinase-anchoring protein (AKAP)-Lbc complex. AKAP-Lbc facilitates PKA phosphorylation of Shp2, which inhibits its protein-tyrosine phosphatase activity. Given the important cardiac roles of both AKAP-Lbc and Shp2, we investigated the AKAP-Lbc-Shp2 interaction in the heart. AKAP-Lbc-tethered PKA is implicated in cardiac hypertrophic signaling; however, mechanism of PKA action is unknown. Mutations resulting in loss of Shp2 catalytic activity are also associated with cardiac hypertrophy and congenital heart defects. Our data indicate that AKAP-Lbc integrates PKA and Shp2 signaling in the heart and that AKAP-Lbc-associated Shp2 activity is reduced in hypertrophic hearts in response to chronic β-adrenergic stimulation and PKA activation. Thus, while induction of cardiac hypertrophy is a multifaceted process, inhibition of Shp2 activity through AKAP-Lbc-anchored PKA is a previously unrecognized mechanism that may promote compensatory cardiac hypertrophy.

Published

2012

8. Collagen XVII (BP180) modulates keratinocyte expression of the proinflammatory chemokine, IL-8.

Author

Van den Bergh F, Eliason SL, Burmeister BT, and Giudice GJ

Subjects

Autoantigens genetics, Cell Line, Epidermolysis Bullosa pathology, Gene Expression Regulation drug effects, Humans, Inflammation pathology, Integrin alpha6beta4 metabolism, Keratinocytes drug effects, Keratinocytes radiation effects, Lipopolysaccharides pharmacology, NF-kappa B metabolism, Non-Fibrillar Collagens deficiency, Non-Fibrillar Collagens genetics, RNA, Small Interfering pharmacology, Tetradecanoylphorbol Acetate pharmacology, Tumor Necrosis Factor-alpha pharmacology, Ultraviolet Rays, Collagen Type XVII, Autoantigens metabolism, Epidermolysis Bullosa metabolism, Inflammation metabolism, Interleukin-18 metabolism, Keratinocytes metabolism, Non-Fibrillar Collagens metabolism

Abstract

Collagen XVII (COL17), a transmembrane protein expressed in epidermal keratinocytes (EK), is targeted by pathogenic autoantibodies in bullous pemphigoid. Treatment of EK with anti-COL17 autoantibodies triggers the production of proinflammatory cytokines. In this study, we test the hypothesis that COL17 is involved in the regulation of the EK proinflammatory response, using IL-8 expression as the primary readout. The absence of COL17 in EK derived from a junctional epidermolysis bullosa patient or shRNA-mediated knockdown of COL17 in normal EK resulted in a dysregulation of IL-8 responses under various conditions. The COL17-deficient cells showed an abnormally high IL-8 response after treatment with lipopolysaccharide (LPS), ultraviolet-B radiation or tumor necrosis factor, but exhibited a blunted IL-8 response to phorbol 12-myristate 13-acetate exposure. Induction of COL17 expression in COL17-negative EK led to a normalization of the LPS-induced proinflammatory response. Although α6β4 integrin was found to be up-regulated in COL17-deficient EK, siRNA-mediated knockdown of the α6 and β4 subunits revealed that COL17's effects on the LPS IL-8 response are not dependent on this integrin. In LPS-treated cells, inhibition of NF-kappa B activity in COL17-negative EK resulted in a normalization of their IL-8 response, and expression of an NF-kappa B-driven reporter was shown to be higher in COL17-deficient, compared with normal EK. These findings support the hypothesis that COL17 plays an important regulatory role in the EK proinflammatory response, acting largely via NF-kappa B. Future investigations will focus on further defining the molecular basis of this novel control network., (© 2012 John Wiley & Sons A/S.)

Published

2012

9. A-kinase anchoring proteins that regulate cardiac remodeling.

Author

Carnegie GK and Burmeister BT

Subjects

Animals, Cardiomegaly metabolism, Excitation Contraction Coupling physiology, Humans, Sarcomeres metabolism, A Kinase Anchor Proteins physiology, Ventricular Remodeling physiology

Abstract

In response to injury or stress, the adult heart undergoes maladaptive changes, collectively defined as pathological cardiac remodeling. Here, we focus on the role of A-kinase anchoring proteins (AKAPs) in 3 main areas associated with cardiac remodeling and the progression of heart failure: excitation-contraction coupling, sarcomeric regulation, and induction of pathological hypertrophy. AKAPs are a diverse family of scaffold proteins that form multiprotein complexes, integrating cAMP signaling with protein kinases, phosphatases, and other effector proteins. Many AKAPs have been characterized in the heart, where they play a critical role in modulating cardiac function.

Published

2011