Literature DB >> 22103917

Proteomic remodeling of mitochondria in heart failure.

John M Hollander1, Walter A Baseler, Erinne R Dabkowski.   

Abstract

Heart failure (HF) is a common disease that has been attributed, in part, to deprivation of cardiac energy. As a result, the interplay between metabolism and adenosine triphosphate production is fundamental in determining the mechanisms driving the disease progression. Due to its central role in energy production, metabolism, calcium homeostasis, and oxidative stress, the mitochondrion has been suggested to play a pivotal role in the progression of the heart to failure. Nevertheless, the mitochondrion's specific role(s) and the proteins contributing to the development and progression of HF are not entirely clear. Thus, changes in mitochondrial proteomic make-up during HF have garnered great interest. With the continued development of advanced tools for assessing proteomic make-up, characterization of mitochondrial proteomic changes during disease states such as HF are being realized. These studies have begun to identify potential biomarkers of disease progression as well as protein targets that may provide an avenue for therapeutic intervention. The goal of this review is to highlight some of the changes in mitochondrial proteomic make-up that are associated with the development of HF in an effort to identify target axes and candidate proteins contributing to disease development. Results from a number of different HF models will be evaluated to gain insight into some of the similarities and differences in mitochondrial proteomic alterations associated with morphological and functional changes that result from the disease. Congest Heart Fail.
© 2011 Wiley Periodicals, Inc.

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Year:  2011        PMID: 22103917      PMCID: PMC3229269          DOI: 10.1111/j.1751-7133.2011.00254.x

Source DB:  PubMed          Journal:  Congest Heart Fail        ISSN: 1527-5299


  40 in total

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2.  Proteomic alterations of distinct mitochondrial subpopulations in the type 1 diabetic heart: contribution of protein import dysfunction.

Authors:  Walter A Baseler; Erinne R Dabkowski; Courtney L Williamson; Tara L Croston; Dharendra Thapa; Matthew J Powell; Trust T Razunguzwa; John M Hollander
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3.  The nitrated proteome in heart mitochondria of the db/db mouse model: characterization of nitrated tyrosine residues in SCOT.

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4.  Sequence and organization of the human mitochondrial genome.

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5.  Modulation of mitochondrial proteome and improved mitochondrial function by biventricular pacing of dyssynchronous failing hearts.

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6.  Proteomic remodelling of mitochondrial oxidative pathways in pressure overload-induced heart failure.

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7.  Cardiac mitochondrial damage and biogenesis in a chronic model of type 1 diabetes.

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Review 9.  Animal models of human cardiovascular disease, heart failure and hypertrophy.

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10.  Mitochondrial dysfunction in the type 2 diabetic heart is associated with alterations in spatially distinct mitochondrial proteomes.

Authors:  Erinne R Dabkowski; Walter A Baseler; Courtney L Williamson; Matthew Powell; Trust T Razunguzwa; Jefferson C Frisbee; John M Hollander
Journal:  Am J Physiol Heart Circ Physiol       Date:  2010-06-11       Impact factor: 4.733

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  14 in total

1.  Differential regulation of EHD3 in human and mammalian heart failure.

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Review 2.  Calcineurin signaling in the heart: The importance of time and place.

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Review 3.  Physiological and structural differences in spatially distinct subpopulations of cardiac mitochondria: influence of cardiac pathologies.

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4.  Characterization, design, and function of the mitochondrial proteome: from organs to organisms.

Authors:  Christopher Lotz; Amanda J Lin; Caitlin M Black; Jun Zhang; Edward Lau; Ning Deng; Yueju Wang; Nobel C Zong; Jeong H Choi; Tao Xu; David A Liem; Paavo Korge; James N Weiss; Henning Hermjakob; John R Yates; Rolf Apweiler; Peipei Ping
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5.  Evidence of Altered Mitochondrial Protein Expression After Chronic Ethanol Consumption in the Aged Estrogen-Deficient Female Rat Heart.

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6.  Mitochondrial proteome remodeling in ischemic heart failure.

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7.  αB-crystallin regulates oxidative stress-induced apoptosis in cardiac H9c2 cells via the PI3K/AKT pathway.

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8.  Protection from oxidative and electrophilic stress in the Gsta4-null mouse heart.

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Review 9.  Mitochondrial oxidative metabolism and uncoupling proteins in the failing heart.

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Review 10.  Role of microRNA in metabolic shift during heart failure.

Authors:  Mark V Pinti; Quincy A Hathaway; John M Hollander
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