Your search keyword '"Aβ, Amyloid-β"' showing total 7 results

1. A novel nicotinic mechanism underlies β-amyloid-induced neurotoxicity.

Author

Liu, Qiang, Xie, Xitao, Emadi, Sharareh, Sierks, Michael R., and Wu, Jie

Subjects

*NEUROTOXICOLOGY, *ALZHEIMER'S disease treatment, *NICOTINIC antagonists, *COGNITION disorders research, *LACTATE dehydrogenase

Abstract

Loss of basal forebrain cholinergic neurons (BFCN) correlates with cognitive deficits in Alzheimer disease (AD). Our recent evidence suggests that chronic exposure to Aβ up-regulated neuronal α7-nAChRs and increased neuronal excitability in cultured hippocampal neurons. However, the impact of the up-regulated α7-nAChRs on Aβ-induced neurotoxicity remains unclear. In this study, we investigated the role of α7-nAChRs in the mediation of Aβ-induced neurotoxicity. The effects of Aβ exposure on α7-nAChRs and cytotoxicity were examined using whole-cell patch clamp recordings, atomic force microscope (AFM) imaging, immunoprecipitation, and lactate dehydrogenase (LDH) release assay in primary cultured hippocampal neurons as well as differentiated human neuroblastoma (SH-SY5Y) cells with cholinergic characteristics. We found that α7-nAChRs are necessary for Aβ-induced neurotoxicity in hippocampal neurons because chronic Aβ significantly increased LDH level in hippocampal cultures, which was prevented by either α7-nAChR antagonist methyllycaconitine (MLA) or by α7 subunit gene deletion (cultures prepared from nAChR α7 subunit KO mice), whereas β2-containing nAChR antagonist (dihydro-β-erythroidine, DhβE) or the genetic deletion of nAChR β2 subunit (cultures prepared from β2 KO mice) failed to prevent Aβ-induced toxicity. In SH-SY5Y cells, larger aggregates of Aβ preferentially up-regulated α7-nAChR expression and function accompanied by a significant decrease in cell viability. Co-treatment MLA, but not mecamylamine (MEC), prevented Aβ exposure-induced neurotoxicity. Our results suggest a detrimental role of upregulated α7-nAChRs in the mediation of Aβ-induced neurotoxicity. [ABSTRACT FROM AUTHOR]

Published

2015

2. SUMO1 promotes Aβ production via the modulation of autophagy.

Author

Cho, Sun-Jung, Yun, Sang-Moon, Jo, Chulman, Lee, Dae-hoon, Choi, Ki Ju, Song, Jae Chun, Park, Sang Ick, Kim, You-Jin, and Koh, Young Ho

Published

2015

3. Transglutaminase catalyzes differential crosslinking of small heat shock proteins and amyloid-β

Author

Boros, Sandor, Kamps, Bram, Wunderink, Lisa, de Bruijn, Willem, de Jong, Wilfried W., and Boelens, Wilbert C.

Subjects

*PROTEINS, *AMINO acids, *ORGANIC acids, *TRANSGLUTAMINASES

Abstract

Crosslinking of proteins by tissue transglutaminase (tTG) is enhanced in amyloid (Aβ) deposits characteristic of Alzheimer''s disease and sporadic inclusion body myositis. Small heat shock proteins (sHsps) also occur in amyloid deposits. We here report the substrate characteristics for tTG of six sHsps. Hsp27, Hsp20 and HspB8 are both lysine- and glutamine-donors, αB-crystallin only is a lysine-donor, HspB2 a glutamine-donor, and HspB3 no substrate at all. Close interaction of proteins stimulates crosslinking efficiency as crosslinking between different sHsps only takes place within the same heteromeric complex. We also observed that αB-crystallin, Hsp27 and Hsp20 associate with Aβ in vitro, and can be readily crosslinked by tTG. [Copyright &y& Elsevier]

Published

2004

4. Toward modeling hemorrhagic and encephalitic complications of Alzheimer amyloid-β vaccination in nonhuman primates

Author

Gandy, Sam and Walker, Lary

Subjects

*PRIMATES, *VACCINATION, *AMYLOID, *ALZHEIMER'S disease

Abstract

The potential of amyloid-β (Aβ) immunization as a disease-modifying therapy for Alzheimer’s disease is limited by the occurrence of encephalitic side effects in a subset of treated patients. The encephalitis was not predicted from immunization studies in transgenic, Aβ-depositing mice. More recently, studies in these same mice indicate that passive immunization with certain anti-Aβ antibodies can induce microhemorrhage. Cerebral amyloid angiopathy (CAA) may play a key role in determining the risk for these complications. Because aged nonhuman primates (NHPs) have a more human-like immune system than rodents, and because NHPs naturally develop senile plaques and CAA with age, NHPs appear to be important, adjunctive models for assessing the efficacy and safety of immunotherapeutics for Alzheimer’s disease. Conversely, the ability to model the complications of Aβ immunotherapy will be important for elucidating the bases of these complications, and for developing protocols that minimize or eliminate the risks of these serious adverse effects. [Copyright &y& Elsevier]

Published

2004

5. Diverse fibrillar peptides directly bind the Alzheimer’s amyloid precursor protein and amyloid precursor-like protein 2 resulting in cellular accumulation

Author

White, Anthony R., Maher, Fran, Brazier, Marcus W., Jobling, Michael F., Thyer, James, Stewart, Leanne R., Thompson, Andrew, Gibson, Riki, Masters, Colin L., Multhaup, Gerd, Beyreuther, Konrad, Barrow, Colin J., Collins, Steven J., and Cappai, Roberto

Subjects

*ALZHEIMER'S disease, *AMYLOID beta-protein

Abstract

The Alzheimer’s disease Aβ peptide can increase the levels of cell-associated amyloid precursor protein (APP) in vitro. To determine the specificity of this response for Aβ and whether it is related to cytotoxicity, we tested a diverse range of fibrillar peptides including amyloid-β (Aβ), the fibrillar prion peptides PrP106–126 and PrP178–193 and human islet-cell amylin. All these peptides increased the levels of APP and amyloid precursor-like protein 2 (APLP2) in primary cultures of astrocytes and neurons. Specificity was shown by a lack of change to amyloid precursor-like protein 1, τ-1 and cellular prion protein (PrPc) levels. APP and APLP2 levels were elevated only in cultures exposed to fibrillar peptides as assessed by electron microscopy and not in cultures treated with non-fibrillogenic peptide variants or aggregated lipoprotein. We found that PrP106–126 and the non-toxic but fibril-forming PrP178–193 increased APP levels in cultures derived from both wild-type and PrPc-deficient mice indicating that fibrillar peptides up-regulate APP through a non-cytotoxic mechanism and irrespective of parental protein expression. Fibrillar PrP106–126 and Aβ peptides bound recombinant APP and APLP2 suggesting the accumulation of these proteins was mediated by direct binding to the fibrillated peptide. This was supported by decreased APP accumulation following extensive washing of the cultures to remove fibrillar aggregates. Pre-incubation of fibrillar peptide with recombinant APP18–146, the putative fibril binding site, also abrogated the accumulation of APP. These findings show that diverse fibrillogenic peptides can induce accumulation of APP and APLP2 and this mechanism could contribute to pathogenesis in neurodegenerative disorders. [Copyright &y& Elsevier]

Published

2003

6. Anterograde axonal transport of endopeptidase 24.15 in rat sciatic nerves

Author

Yamamoto, Masaru, Chikuma, Toshiyuki, Yamashita, Atsue, Yamaguchi, Mitsune, Hojo, Hiroshi, Ozeki, Yasuhiro, Ahmed, Mahiuddin, and Kato, Takeshi

Subjects

*ENDOPEPTIDASES, *AXONAL transport

Abstract

Axonal transport of endopeptidase 24.15 (EP24.15), a putative neuropeptide degrading-enzyme, was examined in the proximal, middle, and distal segments of rat sciatic nerves using a double ligation technique. At 48 h after ligation, a significant amount of the axonal transport of EP24.15 activity was found in the proximal segment, while axonal transport of deamidase activity, a lysosomal enzyme, increased in both proximal and distal segments. Western blot analysis of EP24.15 showed that EP24.15 immunoreactivity in the proximal segment was 1.8-fold higher than that in the middle segment. The immunohistochemical analysis of the segments also showed an increase in the immunoreactive EP24.15 in the proximal segment in comparison with that in the middle segment. In the distal segment, no axonal transport of EP24.15 was found in all methods examined, indicating that EP24.15 is mainly transported by an anterograde axonal flow. These observations suggest that EP24.15 may be involved in the metabolism of neuropeptides in nerve terminals or synaptic clefts. [Copyright &y& Elsevier]

Published

2003

7. Design of Peptide-based Inhibitors of Human Islet Amyloid Polypeptide Fibrillogenesis

Author

Scrocchi, Louise A., Chen, Yan, Waschuk, Stefko, Wang, Feng, Cheung, Sindy, Darabie, Audrey A., McLaurin, JoAnne, and Fraser, Paul E.

Subjects

*ENZYME inhibitors, *AMYLOID, *PANCREAS

Abstract

Human islet amyloid polypeptide (IAPP) is the major component of amyloid deposits found in the pancreas of over 90% of all cases of type-2 diabetes. We have generated a series of overlapping hexapeptides to target an amyloidogenic region of IAPP (residues 20–29) and examined their effects on fibril assembly. Peptide fragments corresponding to SNNFGA (residues 20–25) and GAILSST (residues 24–29) were strong inhibitors of the β-sheet transition and amyloid aggregation. Circular dichroism indicated that even at 1:1 molar ratios, these peptides maintained full-length IAPP (1–37) in a largely random coil conformation. Negative stain electron microscopy revealed that co-incubation of these peptides with IAPP resulted in the formation of only semi-fibrous aggregates and loss of the typical high density and morphology of IAPP fibrils. This inhibitory activity, particularly for the SNNFGA sequence, also correlated with a reduction in IAPP-induced cytotoxicity as determined by cell culture studies. In contrast, the peptide NFGAIL (residues 22–27) enhanced IAPP fibril formation. Conversion to the amyloidogenic β-sheet was immediate and the accompanying fibrils were more dense and complex than IAPP alone. The remaining peptide fragments either had no detectable effects or were only weakly inhibitory. Specificity of peptide activity was illustrated by the fragments, SSNNFG and AILSST. These differed from the most active inhibitors by only a single amino acid residue but delayed the random-to-β conformational change only when used at higher molar ratios. This study has identified internal IAPP peptide fragments which can regulate fibrillogenesis and may be of therapeutic use for the treatment of type-2 diabetes. [Copyright &y& Elsevier]

Published

2002