Genetic determinants of white matter hyperintensities and amyloid angiopathy in familial Alzheimer's disease

Natalie S. Ryan; Geert Jan Biessels; Lois Kim; Jennifer M. Nicholas; Philip A. Barber; Phoebe Walsh; Priya Gami; Huw R. Morris; António J. Bastos-Leite; Jonathan M. Schott; Jon Beck; Simon Mead; Lucia Chavez-Gutierrez; Bart de Strooper; Martin N. Rossor; Tamas Revesz; Tammaryn Lashley; Nick C. Fox

doi:10.1016/j.neurobiolaging.2015.08.026

Genetic determinants of white matter hyperintensities and amyloid angiopathy in familial Alzheimer's disease

Natalie S. Ryan^*, Geert Jan Biessels, Lois Kim, Jennifer M. Nicholas, Philip A. Barber, Phoebe Walsh, Priya Gami, Huw R. Morris, António J. Bastos-Leite, Jonathan M. Schott, Jon Beck, Simon Mead, Lucia Chavez-Gutierrez, Bart de Strooper, Martin N. Rossor, Tamas Revesz, Tammaryn Lashley, Nick C. Fox

^*Corresponding author for this work

Brain

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

Familial Alzheimer's disease (FAD) treatment trials raise interest in the variable occurrence of cerebral amyloid angiopathy (CAA); an emerging important factor in amyloid-modifying therapy. Previous pathological studies reported particularly severe CAA with postcodon 200 PSEN1 mutations and amyloid beta coding domain APP mutations. As CAA may manifest as white matter hyperintensities (WMH) on magnetic resonance imaging, particularly posteriorly, we investigated WMH in 52 symptomatic FAD patients for associations with mutation position. WMH were visually rated in 39 PSEN1 (18 precodon 200); 13 APP mutation carriers and 25 healthy controls. Ten PSEN1 mutation carriers (5 precodon 200) had postmortem examination. Increased WMH were observed in the PSEN1 postcodon 200 group and in the single APP patient with an amyloid beta coding domain (p.Ala692Gly, Flemish) mutation. WMH burden on MRI correlated with severity of CAA and cotton wool plaques in several areas. The precodon 200 group had younger ages at onset, decreased axonal density and/or integrity, and a greater T-lymphocytic response in occipital deep white matter. Mutation site contributes to the phenotypic and pathological heterogeneity witnessed in FAD.

Original language	English
Pages (from-to)	3140-3151
Number of pages	12
Journal	Neurobiology of Aging
Volume	36
Issue number	12
DOIs	https://doi.org/10.1016/j.neurobiolaging.2015.08.026
Publication status	Published - 1 Dec 2015

Keywords

Amyloid precursor protein (APP)
Cerebral amyloid angiopathy
Familial Alzheimer's disease
Presenilin 1 (PSEN1, PS1)
White matter hyperintensities

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Ryan, N. S., Biessels, G. J., Kim, L., Nicholas, J. M., Barber, P. A., Walsh, P., Gami, P., Morris, H. R., Bastos-Leite, A. J., Schott, J. M., Beck, J., Mead, S., Chavez-Gutierrez, L., de Strooper, B., Rossor, M. N., Revesz, T., Lashley, T., & Fox, N. C. (2015). Genetic determinants of white matter hyperintensities and amyloid angiopathy in familial Alzheimer's disease. Neurobiology of Aging, 36(12), 3140-3151. https://doi.org/10.1016/j.neurobiolaging.2015.08.026

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title = "Genetic determinants of white matter hyperintensities and amyloid angiopathy in familial Alzheimer's disease",

abstract = "Familial Alzheimer's disease (FAD) treatment trials raise interest in the variable occurrence of cerebral amyloid angiopathy (CAA); an emerging important factor in amyloid-modifying therapy. Previous pathological studies reported particularly severe CAA with postcodon 200 PSEN1 mutations and amyloid beta coding domain APP mutations. As CAA may manifest as white matter hyperintensities (WMH) on magnetic resonance imaging, particularly posteriorly, we investigated WMH in 52 symptomatic FAD patients for associations with mutation position. WMH were visually rated in 39 PSEN1 (18 precodon 200); 13 APP mutation carriers and 25 healthy controls. Ten PSEN1 mutation carriers (5 precodon 200) had postmortem examination. Increased WMH were observed in the PSEN1 postcodon 200 group and in the single APP patient with an amyloid beta coding domain (p.Ala692Gly, Flemish) mutation. WMH burden on MRI correlated with severity of CAA and cotton wool plaques in several areas. The precodon 200 group had younger ages at onset, decreased axonal density and/or integrity, and a greater T-lymphocytic response in occipital deep white matter. Mutation site contributes to the phenotypic and pathological heterogeneity witnessed in FAD.",

keywords = "Amyloid precursor protein (APP), Cerebral amyloid angiopathy, Familial Alzheimer's disease, Presenilin 1 (PSEN1, PS1), White matter hyperintensities",

author = "Ryan, {Natalie S.} and Biessels, {Geert Jan} and Lois Kim and Nicholas, {Jennifer M.} and Barber, {Philip A.} and Phoebe Walsh and Priya Gami and Morris, {Huw R.} and Bastos-Leite, {Ant{\'o}nio J.} and Schott, {Jonathan M.} and Jon Beck and Simon Mead and Lucia Chavez-Gutierrez and {de Strooper}, Bart and Rossor, {Martin N.} and Tamas Revesz and Tammaryn Lashley and Fox, {Nick C.}",

year = "2015",

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doi = "10.1016/j.neurobiolaging.2015.08.026",

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Ryan, NS, Biessels, GJ, Kim, L, Nicholas, JM, Barber, PA, Walsh, P, Gami, P, Morris, HR, Bastos-Leite, AJ, Schott, JM, Beck, J, Mead, S, Chavez-Gutierrez, L, de Strooper, B, Rossor, MN, Revesz, T, Lashley, T & Fox, NC 2015, 'Genetic determinants of white matter hyperintensities and amyloid angiopathy in familial Alzheimer's disease', Neurobiology of Aging, vol. 36, no. 12, pp. 3140-3151. https://doi.org/10.1016/j.neurobiolaging.2015.08.026

TY - JOUR

T1 - Genetic determinants of white matter hyperintensities and amyloid angiopathy in familial Alzheimer's disease

AU - Ryan, Natalie S.

AU - Biessels, Geert Jan

AU - Kim, Lois

AU - Nicholas, Jennifer M.

AU - Barber, Philip A.

AU - Walsh, Phoebe

AU - Gami, Priya

AU - Morris, Huw R.

AU - Bastos-Leite, António J.

AU - Schott, Jonathan M.

AU - Beck, Jon

AU - Mead, Simon

AU - Chavez-Gutierrez, Lucia

AU - de Strooper, Bart

AU - Rossor, Martin N.

AU - Revesz, Tamas

AU - Lashley, Tammaryn

AU - Fox, Nick C.

PY - 2015/12/1

Y1 - 2015/12/1

N2 - Familial Alzheimer's disease (FAD) treatment trials raise interest in the variable occurrence of cerebral amyloid angiopathy (CAA); an emerging important factor in amyloid-modifying therapy. Previous pathological studies reported particularly severe CAA with postcodon 200 PSEN1 mutations and amyloid beta coding domain APP mutations. As CAA may manifest as white matter hyperintensities (WMH) on magnetic resonance imaging, particularly posteriorly, we investigated WMH in 52 symptomatic FAD patients for associations with mutation position. WMH were visually rated in 39 PSEN1 (18 precodon 200); 13 APP mutation carriers and 25 healthy controls. Ten PSEN1 mutation carriers (5 precodon 200) had postmortem examination. Increased WMH were observed in the PSEN1 postcodon 200 group and in the single APP patient with an amyloid beta coding domain (p.Ala692Gly, Flemish) mutation. WMH burden on MRI correlated with severity of CAA and cotton wool plaques in several areas. The precodon 200 group had younger ages at onset, decreased axonal density and/or integrity, and a greater T-lymphocytic response in occipital deep white matter. Mutation site contributes to the phenotypic and pathological heterogeneity witnessed in FAD.

AB - Familial Alzheimer's disease (FAD) treatment trials raise interest in the variable occurrence of cerebral amyloid angiopathy (CAA); an emerging important factor in amyloid-modifying therapy. Previous pathological studies reported particularly severe CAA with postcodon 200 PSEN1 mutations and amyloid beta coding domain APP mutations. As CAA may manifest as white matter hyperintensities (WMH) on magnetic resonance imaging, particularly posteriorly, we investigated WMH in 52 symptomatic FAD patients for associations with mutation position. WMH were visually rated in 39 PSEN1 (18 precodon 200); 13 APP mutation carriers and 25 healthy controls. Ten PSEN1 mutation carriers (5 precodon 200) had postmortem examination. Increased WMH were observed in the PSEN1 postcodon 200 group and in the single APP patient with an amyloid beta coding domain (p.Ala692Gly, Flemish) mutation. WMH burden on MRI correlated with severity of CAA and cotton wool plaques in several areas. The precodon 200 group had younger ages at onset, decreased axonal density and/or integrity, and a greater T-lymphocytic response in occipital deep white matter. Mutation site contributes to the phenotypic and pathological heterogeneity witnessed in FAD.

KW - Amyloid precursor protein (APP)

KW - Cerebral amyloid angiopathy

KW - Familial Alzheimer's disease

KW - Presenilin 1 (PSEN1, PS1)

KW - White matter hyperintensities

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AN - SCOPUS:84947017996

SN - 0197-4580

VL - 36

SP - 3140

EP - 3151

JO - Neurobiology of Aging

JF - Neurobiology of Aging

IS - 12

ER -

Genetic determinants of white matter hyperintensities and amyloid angiopathy in familial Alzheimer's disease

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Keywords

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