Diabetes-induced alterations in the expression, functioning and phosphorylation state of the inhibitory guanine nucleotide regulatory protein Gi-2 in hepatocytes

Bushfield, Mark; Griffiths, Susanne L.; Murphy, Gregory; Pyne, Nigel J.; Knowler, John T.; Milligan, Graeme; Parker, Peter J.; Mollner, Stefan; Houslay, Miles D.

doi:10.1042/bj2710365

Cited by 94 publications

(56 citation statements)

References 42 publications

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“…In hepatocytes of streptozotocin-induced diabetic rats [25,26] there is a loss of Gi function which appears to result from both a reduction in the expression of Gi-2 and also its increased phosphorylation by protein kinase C. Treatment of a variety of different cell types with tumour promoting phorbol esters has been shown to lead to the loss of guanine nucleotide-elicited, G~-mediated inhibition of adenylate cyclase activity [13,37]. Similar observations of crippled G~ function have also been seen in cells challenged with ligands which stimulate phospholipid metabolism or with DAG [13], suggesting that it is the activation of protein kinase C which provides the molecular basis of this phenomenon.…”

Section: Resultsmentioning

confidence: 99%

“…As well as this, activation of protein kinase C also causes the loss of 'tonic' GTP-mediated inhibition of adenylyl cyclase through Gi [17]. This apparently physiological 'crosstalk' mechanism appears, however, to be inappropriately activated in streptozotocin-induced diabetes [25,26] where we have noted the loss of such 'tonic' GTP-elicited inhibition of adenylyl cyclase [25,26]. This appears to be due in part to the reduced expression of the inhibitory G-protein ~-Gi-2 but also to the increased phosphorylation, through the action of PKC, of ~-Gi-2 itself [18,26].…”

Section: Introductionmentioning

confidence: 99%

“…It is possible that abnormalities in PKC expression might occur in hepatocytes from streptozotocin-induced diabetes as reflecting the altered functioning of this enzyme activity deduced from analyses done on Gi function and phosphorylation [25,26]. We here describe the use of a panel of sub-type specific antisera to probe alterations in the expression and distribution, between membrane and cytosol compartments, of various protein kinase C isoforms.…”

Section: Introductionmentioning

confidence: 99%

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Diabetes induces selective alterations in the expression of protein kinase C isoforms in hepatocytes

et al. 1993

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Membrane and cytosol fractions from hepatocytes of both normal and streptozotocin-induced diabetic animals were probed with a panel of polyclonal anti-peptide antisera in order to identify protein kinase C (PKC) isoforms. Immunoreactive species were noted with antisera specific for ~ (-81 kDa), fl-ll (-82 kDA), E (--95 kDa) and ~" (~ 79 kDa). In addition, a species migrating with an apparent size of -94 kDa was also detected in cytosol fractions using an antiserum specific for PKC-c~. Each of these species was specifically displaced when the PKC-isoform specific peptide was included in the immunodetection system. No immunoreactive species consistent with the presence of the fl-I, 7, ~ and 1/isoforms of protein kinase C was observed. Induction of diabetes using streptozotocin invoked selective alterations in the expression of PKC isoforms which were reversed upon insulin therapy. In the cytosol fraction, marked increases of ~ 3-fold occurred in levels of the fl-I1 isoform and the ~ 90 kDa (upper) form of PKC-~, with no apparent/little change in the levels of the -81 kDa (lower) form of PKC-cc and those of PKC-~'. Diabetes induction also appeared to have elicited the translocation of PKC-fl-II and the -81 kDa (lower) form of PKC-c~ to the membrane fraction where immunoreactivity for these species was now apparent. The level of PKC-e, which was noted only in membrane fractions, was also increased upon induction of diabetes. It is suggested that the selective alterations in the expression of PKC isoforms occurring upon streptozotocin-induced diabetes may lead to altered cellular functioning and underly defects in inhibitory G-protein functioning and insulin action which characterise this animal model of diabetes.

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Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Diabetes induces selective alterations in the expression of protein kinase C isoforms in hepatocytes

et al. 1993

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“…Another line of evidence comes from the altered function of Gi in diabetes, where abolished effects of insulin on Grlike proteins have been documented [33]. It has also been reported that the Gi function is impaired in liver membranes of animals with experimentally induced diabetes [34][35][36][37]. These suggest that some metabolic effects of insR may be mediated by Grlike proteins.…”

Section: Resultsmentioning

confidence: 94%

GTP‐binding protein‐activator sequences in the insulin receptor

Okamoto

Murayama

et al. 1993

FEBS Letters

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Some functions of the insulin receptor (insR) are assumed to be mediated by pertussis toxin‐sensitive Gi/Go. proteins. Here we have located G‐protein‐activator domains in the cytoplasmic region of the human insR. We searched the sequence of insR and found three candidate regions at residues 1039‐1061, 1147‐1168 and 1325‐1345, referred to as ISRP 1, ISRP2 and ISRP3, respectively. Among them, the Gi/Go‐activating function was observed only in peptide ISRP3. ISRP1 specifically activated G3, whereas ISRP2 had no effect on G proteins. ISRP2 and ISRP3 contained five of six autophosphorylated tyrosine residues in insR. After tyrosine phosphorylation, ISRP2 showed specific G1‐activating function, and ISRP3 potentiated its ability and became capable of activating G proteins generally. This is the first study that specifies G‐protein‐activator domains in insR and describes their modification by autophosphorylation.

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“…G i α2, but not G i α3 from hepatocytes, was found to be phosphorylated on serine residues by protein kinase C both in i o and in itro [37][38][39]. Elevated phosphorylation of G i α2 was correlated with decreased ability to inhibit adenylate cyclase [40,41]. Tyrosine phosphorylation of G q α [42], G s α [43] and functional consequences have also been reported.…”

Section: Discussionmentioning

confidence: 99%

Purification of A1 adenosine receptor–G-protein complexes: effects of receptor down-regulation and phosphorylation on coupling

Gao

Robeva

Linden

1999

Biochemical Journal

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We examined the effects of exposing A1 adenosine receptors (A1ARs) to an agonist on the stability and phosphorylation state of receptor–guanine nucleotide-binding regulatory protein (R–G-protein) complexes. Non-denatured recombinant human A1ARs extended on the N-terminus with hexahistidine (His6) and the FLAG (Asp-Tyr-Lys-Asp-Asp-Asp-Asp-Lys) epitope (H/F) were purified to near homogeneity from stably transfected Chinese-hamster ovary (CHO)-K1 cells. Purified receptors have pharmacological properties similar to receptors in membranes. G-proteins were co-purified with 15±2% of H/F-A1AR unless receptor–G-protein (R–G) complexes were uncoupled by pre-treating cell membranes with GTP. By silver staining, purified A1AR–G-protein complexes contain receptors, G-protein α and β subunits and an unidentified 97 kDa protein. Pretreating intact cells with N6-cyclopentyladenosine (CPA) for 24 h decreased both the total number of receptors measured in membranes and the number of purified A1ARs by about 50%. In contrast, pretreating cells with CPA decreased the number of R–G complexes measured in membranes (54±6%) significantly less than it decreased the number of purified R–G complexes (78±3%) as detected by 125I-N6-(4-aminobenzyl)adenosine binding or by Western blotting Giα2. The effect of CPA to decrease the fraction of receptors purified as R–G complexes was not associated with any change in low-level A1AR phosphorylation (found on serine), or low-level phosphorylation of G-protein α or β subunits or the 97 kDa protein. These experiments reveal a novel aspect of agonist-induced down-regulation, namely a diminished stability of receptor–G-protein complexes that is manifested as uncoupling during receptor purification.

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Diabetes-induced alterations in the expression, functioning and phosphorylation state of the inhibitory guanine nucleotide regulatory protein Gi-2 in hepatocytes

Cited by 94 publications

References 42 publications

Diabetes induces selective alterations in the expression of protein kinase C isoforms in hepatocytes

Diabetes induces selective alterations in the expression of protein kinase C isoforms in hepatocytes

GTP‐binding protein‐activator sequences in the insulin receptor

Purification of A1 adenosine receptor–G-protein complexes: effects of receptor down-regulation and phosphorylation on coupling

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