Your search keyword '"Dimou, Eleni"' showing total 5 results

1. Unconventional Secretion Mediates the Trans-cellular Spreading of Tau.

Author

Katsinelos, Taxiarchis, Zeitler, Marcel, Dimou, Eleni, Karakatsani, Andromachi, Müller, Hans-Michael, Nachman, Eliana, Steringer, Julia P., Ruiz de Almodovar, Carmen, Nickel, Walter, and Jahn, Thomas R.

Abstract

Summary The progressive deposition of misfolded hyperphosphorylated tau is a pathological hallmark of tauopathies, including Alzheimer’s disease. However, the underlying molecular mechanisms governing the intercellular spreading of tau species remain elusive. Here, we show that full-length soluble tau is unconventionally secreted by direct translocation across the plasma membrane. Increased secretion is favored by tau hyperphosphorylation, which provokes microtubule detachment and increases the availability of free protein inside cells. Using a series of binding assays, we show that free tau interacts with components enriched at the inner leaflet of the plasma membrane, finally leading to its translocation across the plasma membrane mediated by sulfated proteoglycans. We provide further evidence that secreted soluble tau species spread trans-cellularly and are sufficient for the induction of intracellular tau aggregation in adjacent cells. Our study demonstrates the mechanistic details of tau secretion and provides insights into the initiation and progression of tau pathology. [ABSTRACT FROM AUTHOR]

Published

2018

2. Super-resolution imaging unveils the self-replication of tau aggregates upon seeding.

Author

Dimou, Eleni, Katsinelos, Taxiarchis, Meisl, Georg, Tuck, Benjamin J., Keeling, Sophie, Smith, Annabel E., Hidari, Eric, Lam, Jeff Y.L., Burke, Melanie, Lövestam, Sofia, Ranasinghe, Rohan T., McEwan, William A., and Klenerman, David

Abstract

Tau is a soluble protein interacting with tubulin to stabilize microtubules. However, under pathological conditions, it becomes hyperphosphorylated and aggregates, a process that can be induced by treating cells with exogenously added tau fibrils. Here, we employ single-molecule localization microscopy to resolve the aggregate species formed in early stages of seeded tau aggregation. We report that entry of sufficient tau assemblies into the cytosol induces the self-replication of small tau aggregates, with a doubling time of 5 h inside HEK cells and 1 day in murine primary neurons, which then grow into fibrils. Seeding occurs in the vicinity of the microtubule cytoskeleton, is accelerated by the proteasome, and results in release of small assemblies into the media. In the absence of seeding, cells still spontaneously form small aggregates at lower levels. Overall, our work provides a quantitative picture of the early stages of templated seeded tau aggregation in cells. [Display omitted] • Treatment with tau fibrils induces the formation of intracellular tau aggregates • Tau seeded aggregation takes place in the vicinity of the microtubule cytoskeleton • Spontaneous tau aggregation occurs in cells • The proteasome accelerates the tau seeded aggregation Dimou et al. employ super-resolution microscopy to resolve the species formed at the early stages of seeded aggregation. They identify that seeding occurs close to the microtubules and that it is accelerated by the proteasome. These results provide a quantitative picture of the initial steps in templated seeded tau aggregation. [ABSTRACT FROM AUTHOR]

Published

2023

3. Small Molecule Inhibitors Targeting Tec Kinase Block Unconventional Secretion of Fibroblast Growth Factor 2.

Author

La Venuta, Giuseppe, Wegehingel, Sabine, Sehr, Peter, Müller, Hans-Michael, Dimou, Eleni, Steringer, Julia P., Grotwinkel, Mareike, Hentze, Nikolai, Mayer, Matthias P., Will, David W., Uhrig, Ulrike, Lewis, Joe D., and Nickel, Walter

Subjects

*FIBROBLAST growth factor 2, *PROTEIN-tyrosine kinases, *MITOGENS, *NEOVASCULARIZATION, *CELL membranes

Abstract

Fibroblast growth factor 2 (FGF2) is a potent mitogen promoting both tumor cell survival and tumor-induced angiogenesis. It is secreted by an unconventional secretory mechanism that is based upon direct translocation across the plasma membrane. Key steps of this process are (i) phosphoinositide-dependent membrane recruitment, (ii) FGF2 oligomerization and membrane pore formation, and (iii) extracellular trapping mediated by membrane-proximal heparan sulfate proteoglycans. Efficient secretion of FGF2 is supported by Tec kinase that stimulatesmembranepore formation based upon tyrosine phosphorylation of FGF2. Here, we report the biochemical characterization of the direct interaction between FGF2 and Tec kinase as well as the identification of small molecules that inhibit (i) the interaction of FGF2 with Tec, (ii) tyrosine phosphorylation of FGF2 mediated by Tec in vitro and in a cellular context, and (iii) unconventional secretion of FGF2 from cells. We further demonstrate the specificity of these inhibitors for FGF2 because tyrosine phosphorylation of a different substrate of Tec is unaffected in their presence. Building on previous evidence using RNA interference, the identified compounds corroborate the role of Tec kinase in unconventional secretion of FGF2. In addition, they are valuable lead compounds with great potential for drug development aiming at the inhibition of FGF2-dependent tumor growth and metastasis. [ABSTRACT FROM AUTHOR]

Published

2016

4. Formation of Disulfide Bridges Drives Oligomerization, Membrane Pore Formation, and Translocation of Fibroblast Growth Factor 2 to Cell Surfaces.

Author

Müller, Hans-Michael, Steringer, Julia P., Wegehingel, Sabine, Bleicken, Stephanie, Münster, Maximilian, Dimou, Eleni, Unger, Sebastian, Weidmann, Georg, Andreas, Helena, García-Sáez, Ana J., Wild, Klemens, Sinning, Irmgard, and Nickel, Walter

Subjects

*DISULFIDES, *OLIGOMERIZATION, *BIOLOGICAL membranes, *FIBROBLAST growth factor 2, *PHOSPHOINOSITIDES, *NEOVASCULARIZATION

Abstract

Fibroblast growth factor 2 (FGF2) is a key signaling molecule in tumor-induced angiogenesis. FGF2 is secreted by an unconventional secretory mechanism that involves phosphatidylinositol 4,5-bisphosphate-dependent insertion of FGF2 oligomers into the plasma membrane. This process is regulated by Tec kinase-mediated tyrosine phosphorylation of FGF2. Molecular interactions driving FGF2 monomers into membrane-inserted FGF2 oligomers are unknown. Here we identify two surface cysteines that are critical for efficient unconventional secretion of FGF2. They represent unique features of FGF2 as they are absent from all signal-peptide-containing members of the FGF protein family. We show that phosphatidylinositol 4,5-bisphosphate-dependent FGF2 oligomerization concomitant with the generation of membrane pores depends on FGF2 surface cysteines as either chemical alkylation or substitution with alanines impairs these processes. We further demonstrate that the FGF2 variant forms lacking the two surface cysteines are not secreted from cells. These findings were corroborated by experiments redirecting a signal-peptide-containing FGF family member from the endoplasmic reticulum/Golgi-dependent secretory pathway into the unconventional secretory pathway of FGF2. Cis elements known to be required for unconventional secretion of FGF2, including the two surface cysteines, were transplanted into a variant form of FGF4 without signal peptide. The resulting FGF4/2 hybrid protein was secreted by unconventional means. We propose that the formation of disulfide bridges drives membrane insertion of FGF2 oligomers as intermediates in unconventional secretion of FGF2. [ABSTRACT FROM AUTHOR]

Published

2015

5. A Direct Role for ATP1A1 in Unconventional Secretion of Fibroblast Growth Factor 2.

Author

Zacherl, Sonja, La Venuta, Giuseppe, Müller, Hans-Michael, Wegehingel, Sabine, Dimou, Eleni, Sehr, Peter, Lewis, Joe D., Erfle, Holger, Pepperkok, Rainer, and Nickel, Walter

Subjects

*FIBROBLASTS, *GROWTH factors, *CELL membranes, *BIOLOGICAL membranes, *BIOLOGICAL interfaces

Abstract

Previous studies proposed a role for the Na/K-ATPase in unconventional secretion of fibroblast growth factor 2 (FGF2). This conclusion was based upon pharmacological inhibition of FGF2 secretion in the presence of ouabain. However, neither independent experimental evidence nor a potential mechanism was provided. Based upon an unbiased RNAi screen, we now report the identification of ATP1A1, the α1-chain of the Na/K-ATPase, as a factor required for efficient secretion of FGF2. As opposed to ATP1A1, down-regulation of the β1- and β3-chains (ATP1B1 and ATP1B3) of the Na/K-ATPase did not affect FGF2 secretion, suggesting that they are dispensable for this process. These findings indicate that it is not the membrane potential-generating function of the Na/K-ATPase complex but rather a so far unidentified role of potentially unassembled α1-chains that is critical for unconventional secretion of FGF2. Consistently, in the absence of β-chains, we found a direct interaction between the cytoplasmic domain of ATP1A1 and FGF2 with submicromolar affinity. Based upon these observations, we propose that ATP1A1 is a recruitment factor for FGF2 at the inner leaflet of plasma membranes that may control phosphatidylinositol 4,5-bisphosphate-dependent membrane translocation as part of the unconventional secretory pathway of FGF2. [ABSTRACT FROM AUTHOR]

Published

2015