| Literature DB >> 20862336 |
Antonella Bobba1, Vito A Petragallo, Ersilia Marra, Anna Atlante.
Abstract
In this paper, we discuss the interplay between beta-amyloid (Aβ) peptide, Tau fragments, <span class="Disease">oxidative stress, and mitochondria in the neuronal model of cerebellar granule neurons (<span class="Gene">CGNs) in which the molecular events reminiscent of AD are activated. The identification of the death route and the cause/effect relationships between the events leading to death could be helpful to manage the progression of apoptosis in neurodegeneration and to define antiapoptotic treatments acting on precocious steps of the death process. Mitochondrial dysfunction is among the earliest events linked to AD and might play a causative role in disease onset and progression. Recent studies on CGNs have shown that adenine nucleotide translocator (ANT) impairment, due to interaction with toxic N-ter Tau fragment, contributes in a significant manner to bioenergetic failure and mitochondrial dysfunction. These findings open a window for new therapeutic strategies aimed at preserving and/or improving mitochondrial function.Entities:
Year: 2010 PMID: 20862336 PMCID: PMC2939402 DOI: 10.4061/2010/621870
Source DB: PubMed Journal: Int J Alzheimers Dis
Figure 1Schematic overview of Aβ peptide and Tau fragments production in CGNs. Aβ is produced intracellularly or taken up from extracellular sources and together with Tau fragments has various pathological effects on cell function.
Figure 2Proposed mechanism of Aβ peptide and N-ter Tau fragment interaction with mitochondria; for further details see text. mom, mitochondrial outer membrane; mim, mitochondrial inner membrane; TOM, translocase of the outer membrane; I–V, respiratory chain complexes; cyt c, cytochrome c; ANT, adenine nucleotide translocator; CyD, cyclophilin D; mPTP, mitochondrial permeability transition pore.
Figure 3Schematic representation of the time-dependent, dual role of nitric oxide in CGN apoptosis; see text for details. GC, guanylil cyclase; cGMP, cyclic GMP; nNOS, neuronal nitric oxide synthase; O 2 ∙ −, superoxide anion; O N O O −, peroxynitrite.
Figure 4Schematic overview of the interplay between Aβ, Tau, oxidative/nitrosative stress, and mitochondria; see text for details. GC, guanylil cyclase; cGMP, cyclic GMP; NOS, nitric oxide synthase; O 2 ∙ −, superoxide anion; O N O O −, peroxynitrite; ANT, adenine nucleotide translocator; GSK3beta, glycogen synthase kinase-3beta; GEN, Genistein.