Literature DB >> 18575773

Phosphoproteomic analysis of aged skeletal muscle.

Joan Gannon1, Lisa Staunton, Kathleen O'Connell, Philip Doran, Kay Ohlendieck.   

Abstract

One of the most important post-translational modifications is represented by phosphorylation on tyrosine, threonine and serine residues. Since abnormal phosphorylation is associated with various pathologies, it was of interest to perform a phosphoproteomic profiling of age-related skeletal muscle degeneration. We used the fluorescent phospho-specific Pro-Q Diamond dye to determine whether changes in the overall phosphorylation of the soluble skeletal muscle proteome differs significantly between young adult and senescent fibres. As an established model system of sarcopenia, we employed 30-month-old rat gastrocnemius fibres. Following the mass spectrometric identification of 59 major 2-D phosphoprotein landmark spots, the fluorescent dye staining survey revealed that 22 muscle proteins showed a differential expression pattern between 3-month- and 30-month-old muscle. Increased phosphorylation levels were shown for myosin light chain 2, tropomyosin alpha, lactate dehydrogenase, desmin, actin, albumin and aconitase. In contrast, decreased phospho-specific dye binding was observed for cytochrome c oxidase, creatine kinase and enolase. Thus, aging-induced alterations in phosphoproteins appear to involve the contractile machinery and the cytoskeleton, as well as the cytosolic and mitochondrial metabolism. This confirms that sarcopenia of old age is a complex neuromuscular pathology that is associated with drastic changes in the abundance and structure of key muscle proteins.

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Year:  2008        PMID: 18575773

Source DB:  PubMed          Journal:  Int J Mol Med        ISSN: 1107-3756            Impact factor:   4.101


  30 in total

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Review 4.  Proteomic responses of skeletal and cardiac muscle to exercise.

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5.  Label-free quantitative protein profiling of vastus lateralis muscle during human aging.

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Review 6.  Posttranslational modifications of desmin and their implication in biological processes and pathologies.

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7.  Muscle-specific inositide phosphatase (MIP/MTMR14) is reduced with age and its loss accelerates skeletal muscle aging process by altering calcium homeostasis.

Authors:  Sandra Romero-Suarez; Jinhua Shen; Leticia Brotto; Todd Hall; Chenglin Mo; Héctor H Valdivia; Jon Andresen; Michael Wacker; Thomas M Nosek; Cheng-Kui Qu; Marco Brotto
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Review 8.  Studies of complex biological systems with applications to molecular medicine: the need to integrate transcriptomic and proteomic approaches.

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9.  In vivo phosphoproteome of human skeletal muscle revealed by phosphopeptide enrichment and HPLC-ESI-MS/MS.

Authors:  Kurt Højlund; Benjamin P Bowen; Hyonson Hwang; Charles R Flynn; Lohith Madireddy; Thangiah Geetha; Paul Langlais; Christian Meyer; Lawrence J Mandarino; Zhengping Yi
Journal:  J Proteome Res       Date:  2009-11       Impact factor: 4.466

Review 10.  Aconitase post-translational modification as a key in linkage between Krebs cycle, iron homeostasis, redox signaling, and metabolism of reactive oxygen species.

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Journal:  Redox Rep       Date:  2013-11-22       Impact factor: 4.412

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