BaseSpace
Correlation Engine 2.0
Import Your Data
Literature

FAQ

More FAQs

Back to top
Clear Search sequence regions
(e.g. GATA1, Angiogenesis, Obesity, Prostate, Autoimmunity, Cisplatin, rs2300478)
Bookmark Forward

C1q-induced LRP1B and GPR6 proteins expressed early in Alzheimer disease mouse models, are essential for the C1q-mediated protection against amyloid-β neurotoxicity.

Marie E Benoit, Michael X Hernandez, Minhan L Dinh, Francisca Benavente, Osvaldo Vasquez, Andrea J Tenner

The Journal of biological chemistry 2013 Jan 04


filter terms:
  • amyloid (12)
  • AP 1 (1)
  • brain (1)
  • C1q (10)
  • C1r (1)
  • C1s (1)
  • complement c1q (3)
  • complement c3 (1)
  • complement protein (1)
  • essential (1)
  • factors (1)
  • g protein (2)
  • gene (4)
  • GPR6 (6)
  • gpr6 protein, rat (1)
  • humans (1)
  • LRP1B (7)
  • mice (2)
  • neurons (3)
  • peptides (2)
  • proteases (1)
  • protein rat (2)
  • rats (1)
  • receptor (3)
  • receptors ldl (2)
  • tumor suppressor proteins (2)
    • Sizes of these terms reflect their relevance to your search.

    Complement protein C1q is induced in the brain in response to a variety of neuronal injuries, including Alzheimer disease (AD), and blocks fibrillar amyloid-β (fAβ) neurotoxicity in vitro. Here, we show that C1q protects immature and mature primary neurons against fAβ toxicity, and we report for the first time that C1q prevents toxicity induced by oligomeric forms of amyloid-β (Aβ). Gene expression analysis reveals C1q-activated phosphorylated cAMP-response element-binding protein and AP-1, two transcription factors associated with neuronal survival and neurite outgrowth, and increased LRP1B and G protein-coupled receptor 6(GPR6) expression in fAβ-injured neurons. Silencing of cAMP-response element-binding protein, LRP1B or GPR6 expression inhibited C1q-mediated neuroprotection from fAβ-induced injury. In addition, C1q altered the association of oligomeric and fAβ with neurons. In vivo, increased hippocampal expression of C1q, LRP1B, and GPR6 is observed as early as 2 months of age in the 3 × Tg mouse model of AD, whereas no such induction of LRP1B and GPR6 was seen in C1q-deficient AD mice. In contrast, expression of C1r and C1s, proteases required to activate the classical complement pathway, and C3 showed a significant age-dependent increase only after 10-13 months of age when plaques start to accumulate in this AD model. Thus, our results identify pathways by which C1q, up-regulated in vivo early in response to injury without the coordinate induction of other complement components, can induce a program of gene expression that promotes neuroprotection and thus may provide protection against in preclinical stages of AD and other neurodegenerative processes.

    Citation

    Marie E Benoit, Michael X Hernandez, Minhan L Dinh, Francisca Benavente, Osvaldo Vasquez, Andrea J Tenner. C1q-induced LRP1B and GPR6 proteins expressed early in Alzheimer disease mouse models, are essential for the C1q-mediated protection against amyloid-β neurotoxicity. The Journal of biological chemistry. 2013 Jan 04;288(1):654-65

    Expand section icon Mesh Tags

    Expand section icon Substances


    PMID: 23150673

    View Full Text
    • Copyright © 2024 Illumina Inc. All rights reserved.