Yves‐Alain Barde scite author profile

Neurofibrillary tangles are composed of insoluble aggregates of the microtubule-associated protein tau. In Alzheimer's disease the accumulation of neurofibrillary tangles occurs in the absence of tau mutations. Here we present mice that develop pathology from non-mutant human tau, in the absence of other exogenous factors, including b-amyloid. The pathology in these mice is Alzheimer-like, with hyperphosphorylated tau accumulating as aggregated paired helical filaments. This pathologic tau accumulates in the cell bodies and dendrites of neurons in a spatiotemporally relevant distribution.

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Purification of a new neurotrophic factor from mammalian brain.

Barde¹,

Edgar²,

Thoenen³

1982

The EMBO Journal

1,626

724

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We report the purification from pig brain of a factor supporting the survival of, and fibre outgrowth from, cultured embryonic chick sensory neurons. The purified factor migrates as one single band, mol. wt. 12 300, on gel electrophoresis in the presence of sodium dodecylsulphate (SDS) and is a basic molecule (pI greater than or equal to 10.1). Approximately 1 microgram factor was isolated from 1.5 kg brain. The final degree of purification was estimated to be 1.4 X 10(6)‐fold, and the specific activity 0.4 ng/ml/unit, which is similar to that of nerve growth factor (NGF) using the same assay system. This factor is the first neurotrophic factor to be purified since NGF, from which it is clearly distinguished because it has different antigenic and functional properties.

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Neurotrophins: key regulators of cell fate and cell shape in the vertebrate nervous system

Bibel

Barde²

2000

Genes Dev.

967

702

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Trophic factors and neuronal survival

Barde¹

1989

Neuron

1,558

689

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Glial cells generate neurons: the role of the transcription factor Pax6

et al. 2002

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Radial glial cells, ubiquitous throughout the developing CNS, guide radially migrating neurons and are the precursors of astrocytes. Recent evidence indicates that radial glial cells also generate neurons in the developing cerebral cortex. Here we investigated the role of the transcription factor Pax6 expressed in cortical radial glia. We showed that radial glial cells isolated from the cortex of Pax6 mutant mice have a reduced neurogenic potential, whereas the neurogenic potential of non-radial glial precursors is not affected. Consistent with defects in only one neurogenic lineage, the number of neurons in the Pax6 mutant cortex in vivo is reduced by half. Conversely, retrovirally mediated Pax6 expression instructs neurogenesis even in astrocytes from postnatal cortex in vitro. These results demonstrated an important role of Pax6 as intrinsic fate determinant of the neurogenic potential of glial cells.

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Yves‐Alain Barde

Hyperphosphorylation and aggregation of tau in mice expressing normal human tau isoforms

Purification of a new neurotrophic factor from mammalian brain.

Neurotrophins: key regulators of cell fate and cell shape in the vertebrate nervous system

Trophic factors and neuronal survival

Glial cells generate neurons: the role of the transcription factor Pax6

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