β-Amyloid-Induced Neurodegeneration and Protection by Structurally Diverse Microtubule-Stabilizing Agents

Michaelis, Mary L.; Ansar, Sabah; Chen, Yingxue; E, Reiff; Seyb, Kathleen; Himes, Richard H.; Audus, Kenneth L.; Georg, Gunda I.

doi:10.1124/jpet.104.074450

Cited by 90 publications

(87 citation statements)

References 40 publications

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“…We note that our finding that short exposures to Ab can induce MT stability in neurons challenges the current interpretation that a primary activity of Ab is to cause MT destabilization through tau hyperphosphorylation (Michaelis et al, 1998) Michaelis et al, 2005;Zempel et al, 2010;Zhang et al, 2012). We believe that our data, although surprising, are not in contradiction with the current model but rather suggest an original interpretation that deserves further testing, that is that progressive MT destabilization upon exposure to Ab might be a consequence of the cellular response to counteract a chronic induction in the levels of stable Glu MTs.…”

Section: Discussioncontrasting

confidence: 78%

Amyloid beta1-42 peptide regulates microtubule stability independently of tau

Pianu

Lefort

Thuiliere

et al. 2014

Journal of Cell Science

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Interference with microtubule stability by beta-amyloid peptide (Ab) has been shown to disrupt dendritic function and axonal trafficking, both early events in Alzheimer's disease. However, it is unclear whether Ab regulation of microtubule dynamics can occur independently of its action on tau. RhoA has been implicated in neurotoxicity by Ab but the mechanism by which this activation generates cytoskeletal changes is also unclear. We found that oligomeric Ab 1-42 induced the formation of stable detyrosinated microtubules in NIH3T3 cells and this function resulted from the activation of a RhoA-dependent microtubule stabilization pathway regulated by integrin signaling and the formin mDia1. Induction of microtubule stability by Ab was also initiated by dimerization of APP and required caspase activity, two previously characterized regulators of neurotoxicity downstream of Ab. Finally, we found that this function was conserved in primary neurons and abolished by Rho inactivation, reinforcing a link between induction of stable detyrosinated microtubules and neuropathogenesis by Ab. Our study reveals a novel activity of Ab on the microtubule cytoskeleton that is independent of tau and associated with pathways linked to microtubule stabilization and Ab-mediated neurotoxicity.

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Section: Discussioncontrasting

confidence: 78%

Amyloid beta1-42 peptide regulates microtubule stability independently of tau

Pianu

Lefort

Thuiliere

et al. 2014

Journal of Cell Science

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“…Paclitaxel also blocks Aβ-induced phosphorylation of tau by preventing the cleavage of p35 by calpain (Li et al 2003). Nanomolar concentrations of paclitaxel can protect neurons against various toxic insults and enhance survival by maintaining Ca 2+ homeostasis (Burke et al 1994;Furukawa and Mattson 1995;Furukawa et al 2003;Sponne et al 2003;Michaelis et al 2005) without evidence of toxicity (Trushina et al 2003). Our study demonstrates that tau is not phosphorylated by MTstabilizing/destabilizing drugs at lower doses, but it is phosphorylated at higher doses.…”

Section: Discussionmentioning

confidence: 61%

Effects of Cell Cycle Inhibitors on Tau Phosphorylation in N2aTau3R Cells

2008

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Neurofibrillary tangles are one of the pathologic hallmarks of Alzheimer's disease (AD). They are composed of paired helical filaments (PHF) containing hyperphosphorylated forms of tau. Hyperphosphorylation of certain tau sites favors its dissociation from the microtubules (MT), interfering with axonal transport and compromising the function and viability of neurons. Reappearance of cell cycle proteins have been reported in neurons exhibiting tau aggregation, suggesting that an aberrant cell cycle occurs before neurons die. Cell cycle suppression in neurons is crucial to survival, thus prevention of progression through the cell cycle may offer a therapeutic approach. Using a neuroblastoma cell line overexpressing 3-repeat (3R) tau, we investigated the effects of cell cycle inhibitors on tau phosphorylation. G2/M phase inhibitors did not alter phosphorylation of tau at Ser-202 and Ser-396/404 at the lower doses, but did at higher doses. Ser-202 and Ser-396/404 are phosphorylation sites of early and late neurofibrillary tangles, respectively, in AD. Cisplatin, a G1 phase inhibitor, did not phosphorylate tau. Cyclophosphamide and phosphoramide mustard, DNA cross-linking agents, decreased tau phosphorylation at Ser-396/404 site, but increased phosphorylation at Ser-202. These studies demonstrate that the G2/M blockers have a dose-dependent effect on tau phosphorylation. This seems to be a consequence of both the disruption of MT-organization and MT-dynamics when doses are higher, but only a disruption of MT-dynamics with lower doses. These results are also in agreement with the lack of phosphorylation seen for cisplatin, another inhibitor that produces disruption of the MT-dynamics.

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“…We used Aβ [25][26][27][28][29][30][31][32][33][34][35] at a concentration of 10 μM in the present studies based on earlier results. In previous studies we have shown that at this concentration we see Aβ induced loss of cortical cells by approximately 50% [20]. This level thus enables us to test drug effects that would not be possible if high Aβ concentration were used to destroy all cells.…”

Section: Measurement Of Cell Viabilitymentioning

confidence: 75%

TCP-FA4: A derivative of tranylcypromine showing improved blood–brain permeability

Desino

Pignatello

Guccione

et al. 2009

Biochemical Pharmacology

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(S. Guccione). ¥ This work is part of K.E. D. PhD thesis. A variety of approaches have been taken to improve the brain penetration of pharmaceutical agents. The amphipathic character of a compound can improve its interaction with the lipid bilayer within cell membranes, and as a result improve permeability. Fatty acid chains or lipoamino acids of various lengths were attached to tranylcypromine (TCP), in an attempt to improve the blood-brain barrier (BBB) permeability by increasing the lipophilicity as well as the amphiphatic character of the drug. TCP-FA4, one of the derivatives containing a four carbon alkyl acid chain, showed the greatest improvement in permeability. This molecule was slightly neuroprotective in a β-amyloid induced neurodegeneration assay and may also be capable of upregulating brain derived neurotrophic factor (BDNF), as indicated by cell culture assays using human umbilical vein endothelial cells. Since decreased levels of BDNF are observed in many CNS disorders, and direct injection of BDNF is not a viable option due to its poor permeability across the BBB, small molecules capable of regulating BDNF that also cross the BBB may be an interesting treatment option.

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β-Amyloid-Induced Neurodegeneration and Protection by Structurally Diverse Microtubule-Stabilizing Agents

Cited by 90 publications

References 40 publications

Amyloid beta1-42 peptide regulates microtubule stability independently of tau

Amyloid beta1-42 peptide regulates microtubule stability independently of tau

Effects of Cell Cycle Inhibitors on Tau Phosphorylation in N2aTau3R Cells

TCP-FA4: A derivative of tranylcypromine showing improved blood–brain permeability

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