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Membrane association and release of wild-type and pathological tau from organotypic brain slice cultures

Membrane association and release of wild-type and pathological tau from organotypic brain slice cultures
Membrane association and release of wild-type and pathological tau from organotypic brain slice cultures
The spatiotemporal transmission of pathological tau in the brain is characteristic of Alzheimer's disease. Release of both soluble and abnormal tau species from healthy neurons is increased upon stimulation of neuronal activity. It is not yet understood whether the mechanisms controlling soluble tau release from healthy neurons is the same as those involved in the spread of pathological tau species. To begin to understand these events, we have studied tau distribution and release using organotypic brain slice cultures. The slices were cultured from postnatal wild-type and 3xTg-AD mice for up to 1 month. Tau distribution in subcellular compartments was examined by western blotting, and tau release into culture medium was determined using a sensitive sandwich ELISA. We show here that 3xTg-AD cultures have an accelerated development of pathological tau abnormalities including the redistribution of tau to synaptic and membrane compartments. The 3xTg-AD slice cultures show elevated basal tau release relative to total tau when compared with wild-type cultures. However, tau release from 3xTg-AD slices cannot be further stimulated when neuronal activity is increased with potassium chloride. Moreover, we report that there is an increased pool of dephosphorylated membrane-associated tau in conditions where tau release is increased. These data suggest that there may be differential patterns of tau release when using integrated slice culture models of wild-type and transgenic mouse brain, although it will be important to determine the effect of tau overexpression for these findings. These results further increase our knowledge of the molecular mechanisms underlying tau release and propagation in neurodegenerative tauopathies.

2041-4889
Croft, Cara L.
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Wade, Matthew A.
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Kurbatskaya, Ksenia
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Mastrandreas, Pavlina
8268ddb8-ccaa-4699-ac5e-78e544b63e84
Hughes, Martina M.
6149ee60-694b-4c55-b8f2-349284c55d66
Phillips, Emma
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Pooler, Amy M.
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Perkinton, Michael S.
98ab55b9-4364-4c89-806b-5937b516e4e6
Hanger, Diane P.
7f1b5bc4-2410-4239-b6ac-8988f65d2973
Noble, Wendy
e53fafef-a7f4-4b9c-982f-65ef7f00c35f
Croft, Cara L.
c557d59a-042a-43a4-b0a5-cc501677ec4d
Wade, Matthew A.
d8bcdc55-ee9e-4dd2-a653-7645578302b1
Kurbatskaya, Ksenia
11d25414-e10d-413a-aaf3-fb6b6c2cf890
Mastrandreas, Pavlina
8268ddb8-ccaa-4699-ac5e-78e544b63e84
Hughes, Martina M.
6149ee60-694b-4c55-b8f2-349284c55d66
Phillips, Emma
92b2a79b-834f-4b32-817b-99d1c3b5714e
Pooler, Amy M.
63e37697-47b6-49d8-acdc-63edfda916bd
Perkinton, Michael S.
98ab55b9-4364-4c89-806b-5937b516e4e6
Hanger, Diane P.
7f1b5bc4-2410-4239-b6ac-8988f65d2973
Noble, Wendy
e53fafef-a7f4-4b9c-982f-65ef7f00c35f

Croft, Cara L., Wade, Matthew A., Kurbatskaya, Ksenia, Mastrandreas, Pavlina, Hughes, Martina M., Phillips, Emma, Pooler, Amy M., Perkinton, Michael S., Hanger, Diane P. and Noble, Wendy (2017) Membrane association and release of wild-type and pathological tau from organotypic brain slice cultures. Cell Death and Disease, 8. (doi:10.1038/cddis.2017.97).

Record type: Article

Abstract

The spatiotemporal transmission of pathological tau in the brain is characteristic of Alzheimer's disease. Release of both soluble and abnormal tau species from healthy neurons is increased upon stimulation of neuronal activity. It is not yet understood whether the mechanisms controlling soluble tau release from healthy neurons is the same as those involved in the spread of pathological tau species. To begin to understand these events, we have studied tau distribution and release using organotypic brain slice cultures. The slices were cultured from postnatal wild-type and 3xTg-AD mice for up to 1 month. Tau distribution in subcellular compartments was examined by western blotting, and tau release into culture medium was determined using a sensitive sandwich ELISA. We show here that 3xTg-AD cultures have an accelerated development of pathological tau abnormalities including the redistribution of tau to synaptic and membrane compartments. The 3xTg-AD slice cultures show elevated basal tau release relative to total tau when compared with wild-type cultures. However, tau release from 3xTg-AD slices cannot be further stimulated when neuronal activity is increased with potassium chloride. Moreover, we report that there is an increased pool of dephosphorylated membrane-associated tau in conditions where tau release is increased. These data suggest that there may be differential patterns of tau release when using integrated slice culture models of wild-type and transgenic mouse brain, although it will be important to determine the effect of tau overexpression for these findings. These results further increase our knowledge of the molecular mechanisms underlying tau release and propagation in neurodegenerative tauopathies.

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Accepted/In Press date: 13 February 2017
e-pub ahead of print date: 16 March 2017
Published date: 2017

Identifiers

Local EPrints ID: 420385
URI: http://eprints.soton.ac.uk/id/eprint/420385
ISSN: 2041-4889
PURE UUID: 9e45d68c-1b09-4501-9782-9bdd1c52a8d5
ORCID for Ksenia Kurbatskaya: ORCID iD orcid.org/0000-0002-8471-2165

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Date deposited: 04 May 2018 16:30
Last modified: 16 Mar 2024 04:29

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Contributors

Author: Cara L. Croft
Author: Matthew A. Wade
Author: Pavlina Mastrandreas
Author: Martina M. Hughes
Author: Emma Phillips
Author: Amy M. Pooler
Author: Michael S. Perkinton
Author: Diane P. Hanger
Author: Wendy Noble

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