Literature DB >> 12773120

Insulin inhibition of the proteasome is dependent on degradation of insulin by insulin-degrading enzyme.

R G Bennett1, J Fawcett, M C Kruer, W C Duckworth, F G Hamel.   

Abstract

A consequence of insulin-dependent diabetes mellitus is the loss of lean muscle mass as a result of accelerated proteolysis by the proteasome. Insulin inhibition of proteasomal activity requires interaction with insulin-degrading enzyme (IDE), but it is unclear if proteasome inhibition is dependent merely on insulin-NIDE binding or if degradation of insulin by IDE is required. To test the hypothesis that degradation by IDE is required for proteasome inhibition, a panel of insulin analogues with variable susceptibility to degradation by IDE binding was used to assess effects on the proteasome. The analogues used were [Lys(B28), Pro(B29)]-insulin (lispro), [Asp(B10)]-insulin (Asp(B10)) and [Glu(B4), Gln(B16), Phe(B17)]-insulin (EQF). Lispro was as effective as insulin at inhibition of degradation of iodine-125 ((125)I)-labeled insulin, but Asp(B10) and EQF were somewhat more effective. All agents inhibited cross-linking of (125)I-insulin to IDE, suggesting that all were capable of IDE binding. In contrast, although insulin and lispro were readily degraded by IDE, Asp(B10) was degraded more slowly, and EQF degradation was undetectable. Both insulin and lispro inhibited the proteasome, but Asp(B10) was less effective, and EQF had little effect. In summary, despite effective IDE binding, EQF was poorly degraded by IDE, and was ineffective at proteasome inhibition. These data suggest that insulin inhibition of proteasome activity is dependent on degradation by IDE. The mechanism of proteasome inhibition may be the generation of inhibitory fragments of insulin, or by displacement of IDE from the proteasome.

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Year:  2003        PMID: 12773120     DOI: 10.1677/joe.0.1770399

Source DB:  PubMed          Journal:  J Endocrinol        ISSN: 0022-0795            Impact factor:   4.286


  19 in total

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4.  Differences in bioactivity between human insulin and insulin analogues approved for therapeutic use- compilation of reports from the past 20 years.

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6.  Structure-activity relationships of imidazole-derived 2-[N-carbamoylmethyl-alkylamino]acetic acids, dual binders of human insulin-degrading enzyme.

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Journal:  Eur J Med Chem       Date:  2014-12-04       Impact factor: 6.514

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8.  Insulin stimulates interleukin-6 expression and release in LS14 human adipocytes through multiple signaling pathways.

Authors:  Christopher R LaPensee; Eric R Hugo; Nira Ben-Jonathan
Journal:  Endocrinology       Date:  2008-07-10       Impact factor: 4.736

9.  Imidazole-derived 2-[N-carbamoylmethyl-alkylamino]acetic acids, substrate-dependent modulators of insulin-degrading enzyme in amyloid-β hydrolysis.

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Journal:  Eur J Med Chem       Date:  2014-04-04       Impact factor: 6.514

10.  Degradation of relaxin family peptides by insulin-degrading enzyme.

Authors:  Robert G Bennett; Dean G Heimann; Frederick G Hamel
Journal:  Ann N Y Acad Sci       Date:  2009-04       Impact factor: 5.691

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