Literature DB >> 7755564

Insulin increases mRNA levels of protein kinase C-alpha and -beta in rat adipocytes and protein kinase C-alpha, -beta and -theta in rat skeletal muscle.

A Avignon1, M L Standaert, K Yamada, H Mischak, B Spencer, R V Farese.   

Abstract

Effects of insulin of levels of mRNA encoding protein kinase C (PKC)-alpha, PKC-beta, PKC-epsilon and PKC-theta were examined by ribonuclease protection assay in primary cultures of rat adipocytes in vitro, and in rat adipose tissue and gastrocnemius muscle in vivo. In all cases, insulin increased the levels of PKC-alpha mRNA and PKC-beta mRNA, and, in muscle, insulin also increased the level of PKC-theta mRNA. PKC-epsilon mRNA levels, on the other hand, were not altered significantly. Insulin also stimulated the apparent translocation of PKC-alpha, -beta, -epsilon and -theta, to the membrane fractions of adipocytes, adipose tissue and gastrocnemius muscles, and, in some instances, total PKC levels were diminished, e.g. PKC-alpha and PKC-beta in cultured adipocytes in vitro and/or whole adipose tissue in vivo, and PKC-alpha and PKC-theta in the gastrocnemius muscle. Thus, insulin-induced increases in PKC mRNA may have been partly compensatory in nature to restore PKC levels following translocation and proteolytic losses. However, much more severe depletion of PKC-alpha and PKC-beta by phorbol ester treatment in cultured rat adipocytes in vitro resulted in, if anything, smaller increases in PKC-alpha mRNA and PKC-beta mRNA, and it therefore appears that insulin effects on PKC mRNA levels were not simply due to decreases in respective PKC levels. In addition, effects of insulin, particularly on PKC-beta mRNA, could not be attributed to increased glucose metabolism, which alone decreased PKC-beta mRNA in cultured adipocytes in vitro. We conclude that insulin-induced translocation and degradation of PKC-alpha, PKC-beta and PKC-theta are attended by selective increases in their mRNAs. This mechanism of increasing mRNA may be important in maintaining PKC levels during the continued action of insulin.

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Year:  1995        PMID: 7755564      PMCID: PMC1136861          DOI: 10.1042/bj3080181

Source DB:  PubMed          Journal:  Biochem J        ISSN: 0264-6021            Impact factor:   3.857


  25 in total

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Authors:  J E Chin; F Liu; R A Roth
Journal:  Mol Endocrinol       Date:  1994-01

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3.  Nucleotide sequences of cDNAs for alpha and gamma subspecies of rat brain protein kinase C.

Authors:  Y Ono; T Fujii; K Igarashi; U Kikkawa; K Ogita; Y Nishizuka
Journal:  Nucleic Acids Res       Date:  1988-06-10       Impact factor: 16.971

4.  Expression and properties of two types of protein kinase C: alternative splicing from a single gene.

Authors:  Y Ono; U Kikkawa; K Ogita; T Fujii; T Kurokawa; Y Asaoka; K Sekiguchi; K Ase; K Igarashi; Y Nishizuka
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Authors:  T Ishizuka; J Hoffman; D R Cooper; J E Watson; D B Pushkin; R V Farese
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7.  Insulin increases membrane protein kinase C activity in rat diaphragm.

Authors:  S I Walaas; R S Horn; A Adler; K A Albert; O Walaas
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8.  Tumor-promoting phorbol esters increase the Km of the ATP-binding site of the insulin receptor kinase from rat adipocytes.

Authors:  H Häring; D Kirsch; B Obermaier; B Ermel; F Machicao
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10.  Preferential activation of microsomal diacylglycerol/protein kinase C signaling during glucose treatment (De Novo phospholipid synthesis) of rat adipocytes.

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2.  PhosphoChain: a novel algorithm to predict kinase and phosphatase networks from high-throughput expression data.

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Review 3.  The emerging role of protein kinase Cθ in cytoskeletal signaling.

Authors:  Izabela Michalczyk; Aleksander F Sikorski; Leszek Kotula; Richard P Junghans; Patrycja M Dubielecka
Journal:  J Leukoc Biol       Date:  2012-11-27       Impact factor: 4.962

4.  Effects of insulin on the translocation of protein kinase C-theta and other protein kinase C isoforms in rat skeletal muscles.

Authors:  K Yamada; A Avignon; M L Standaert; D R Cooper; B Spencer; R V Farese
Journal:  Biochem J       Date:  1995-05-15       Impact factor: 3.857

5.  Expression of Protein Kinase C Isoforms in Pancreatic Islets and Liver of Male Goto-Kakizaki Rats, a Model of Type 2 Diabetes.

Authors:  Mohammed Seed Ahmed; Mohammed Seed Ahmed; Julien Pelletier; Hannes Leumann; Harvest F Gu; Claes-Göran Östenson
Journal:  PLoS One       Date:  2015-09-23       Impact factor: 3.240

6.  Molecular mechanisms of system responses to novel stimuli are predictable from public data.

Authors:  Samuel A Danziger; Alexander V Ratushny; Jennifer J Smith; Ramsey A Saleem; Yakun Wan; Christina E Arens; Abraham M Armstrong; Katherine Sitko; Wei-Ming Chen; Jung-Hsien Chiang; David J Reiss; Nitin S Baliga; John D Aitchison
Journal:  Nucleic Acids Res       Date:  2013-10-31       Impact factor: 16.971

  6 in total

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