Neurons Regulate Extracellular Levels of Amyloid β-Protein via Proteolysis by Insulin-Degrading Enzyme

Vekrellis, Konstantinos; Ye, Zhen; Qiu, Wei Qiao; Walsh, Dominic M.; Hartley, Dean M.; Chesneau, Valérie; Rosner, Marsha Rich; Selkoe, Dennis J.

doi:10.1523/jneurosci.20-05-01657.2000

Cited by 450 publications

(333 citation statements)

References 45 publications

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“…This enzyme, a metalloprotease enzyme responsible for insulin degradation, had been shown to have a key role in b-amyloid (Ab) peptide degradation both in vitro and in vivo, and was selective for Ab monomer. [9][10][11] Thus, substances which induce the upregulation of IDE enzyme are expected to be promising drugs for the treatment of Alzheimer's disease. Compound 1 induced reporter gene expression under the control of the IDE promoter more than three times at a concentration of 100 mM.…”

Section: Biological Activitymentioning

confidence: 99%

Isolation and structure elucidation of tumescenamides A and B, two peptides produced by Streptomyces tumescens YM23-260

et al. 2010

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Two peptides, tumescenamides A and B, were isolated from the fermentation broth of a marine bacterium, Streptomyces tumescens YM23-260. The structure of tumescenamide A was determined to be a cyclic depsipeptide consisting of a-amino-2-butenoic acid, tyrosine, valine, leucine and threonine, substituted with a 2,4-dimethylheptanoyl residue at the a-NH 2 position. INTRODUCTIONTerpenoids are the largest family of compounds found in nature with over 24 000 known examples and are mainly produced by fungi and plants. Production of these compounds by actinomycetes including Streptomyces, however, was rather rare, and only limited numbers of compounds were reported to date. 1 In view of the excellent ability of Streptomyces to produce many kinds of bioactive secondary metabolites with structural diversity, this phenomenon seemed to be interesting for us.Being stimulated in this phenomenon, we started screening for terpenoids produced by actinomycetes and succeeded in the isolation of oxaloterpins 2 and napyradiomycin analogs. 3 Our strategy for screening of terpenoids in these cases was as follows: (1) To carry out more efficient screening of terpenoids, we started using liquid chromatography NMR (LC-NMR) that enabled to detect

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Section: Biological Activitymentioning

confidence: 99%

Isolation and structure elucidation of tumescenamides A and B, two peptides produced by Streptomyces tumescens YM23-260

et al. 2010

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“…IDE (insulin-degrading enzyme) is a major endogenous Ab degrading enzyme that mediates Ab clearance, and its levels and enzymatic activity are negatively correlated with the size of the amyloid plaques and AD pathology. 3 In AD brains, IDE is mainly detected in astrocytes, 4 and located in the cytosol and intracellular compartments such as mitochondria and peroxisomes. 5 However, it is also known to play a role in the extracellular milieu via the secretory pathway.…”

Section: Introductionmentioning

confidence: 99%

Insulin-degrading enzyme secretion from astrocytes is mediated by an autophagy-based unconventional secretory pathway in Alzheimer disease

et al. 2016

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The secretion of proteins that lack a signal sequence to the extracellular milieu is regulated by their transition through the unconventional secretory pathway. IDE (insulin-degrading enzyme) is one of the major proteases of amyloid beta peptide (Ab), a presumed causative molecule in Alzheimer disease (AD) pathogenesis. IDE acts in the extracellular space despite having no signal sequence, but the underlying mechanism of IDE secretion extracellularly is still unknown. In this study, we found that IDE levels were reduced in the cerebrospinal fluid (CSF) of patients with AD and in pathology-bearing AD-model mice. Since astrocytes are the main cell types for IDE secretion, astrocytes were treated with Ab. Ab increased the IDE levels in a time-and concentration-dependent manner. Moreover, IDE secretion was associated with an autophagy-based unconventional secretory pathway, and depended on the activity of RAB8A and GORASP (Golgi reassembly stacking protein). Finally, mice with global haploinsufficiency of an essential autophagy gene, showed decreased IDE levels in the CSF in response to an intracerebroventricular (i.c.v.) injection of Ab. These results indicate that IDE is secreted from astrocytes through an autophagy-based unconventional secretory pathway in AD conditions, and that the regulation of autophagy is a potential therapeutic target in addressing Ab pathology.

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“…IDE is a 110 kDa zinc-requiring metalloproteinase located in the cytoplasm, cell membranes and some cell organelles (endosomes, peroxisomes and mitochondria) and is secreted into the extracellular space [6][7][8]. Insulin is the preferred substrate for IDE, but a large body of other substrates, including glucagon, atrial natriuretic peptide and β-amyloid peptide, were reported [6].…”

Section: Introductionmentioning

confidence: 99%

Glucose inhibits the insulin-induced activation of the insulin-degrading enzyme in HepG2 cells

et al. 2009

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Aims/hypothesis Hepatic insulin degradation decreases in type 2 diabetes. Insulin-degrading enzyme (IDE) plays a key role in insulin degradation and its gene is located in a diabetes-associated chromosomal region. We hypothesised that IDE may be regulated by insulin and/or glucose in a liver cell model. To validate the observed regulation of IDE in vivo, we analysed biopsies of human adipose tissue during different clamp experiments in men. Methods Human hepatoma HepG2 cells were incubated in normal (1 g/l) or high (4.5 g/l) glucose medium and treated with insulin for 24 h. Catalytic activity, mRNA and protein levels of IDE were assessed. IDE mRNA levels were measured in biopsies of human subcutaneous adipose tissue before and at 240 min of hyperinsulinaemic, euglycaemic and hyperglycaemic clamps. Results In HepG2 cells, insulin increased IDE activity under normal glucose conditions with no change in IDE mRNA or protein levels. Under conditions of high glucose, insulin increased mRNA levels of IDE without changes in IDE activity. Both in normal and high glucose medium, insulin increased levels of the catalytically more active 15a IDE isoform compared with the 15b isoform. In subcutaneous adipose tissue, IDE mRNA levels were not significantly upregulated after euglycaemic or hyperglycaemic clamps. Conclusions/interpretation Insulin increases IDE activity in HepG2 cells in normal but not in high glucose conditions. This disturbance cannot be explained by corresponding alterations in IDE protein levels or IDE splicing. The loss of insulin-induced regulation of IDE activity under hyperglycaemia may contribute to the reduced insulin extraction and peripheral hyperinsulinaemia in type 2 diabetes.

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Neurons Regulate Extracellular Levels of Amyloid β-Protein via Proteolysis by Insulin-Degrading Enzyme

Cited by 450 publications

References 45 publications

Isolation and structure elucidation of tumescenamides A and B, two peptides produced by Streptomyces tumescens YM23-260

Isolation and structure elucidation of tumescenamides A and B, two peptides produced by Streptomyces tumescens YM23-260

Insulin-degrading enzyme secretion from astrocytes is mediated by an autophagy-based unconventional secretory pathway in Alzheimer disease

Glucose inhibits the insulin-induced activation of the insulin-degrading enzyme in HepG2 cells

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