Huntington’s disease cag trinucleotide repeats in pathologically confirmed post-mortem brains

Francesca Persichetti; Jayalakshmi Srinidhi; Lisa Kanaley; Pei Ge; Richard H. Myers; Kenneth D’Arrigo; Glenn T. Barnes; Marcy E. MacDonald; Jean Paul Vonsattel; James F. Gusella; Edward D. Bird

doi:10.1006/nbdi.1994.0019

Huntington’s disease cag trinucleotide repeats in pathologically confirmed post-mortem brains

Francesca Persichetti
, Jayalakshmi Srinidhi
, Lisa Kanaley
, Pei Ge
, Richard H. Myers
, Kenneth D’Arrigo
, Glenn T. Barnes
, Marcy E. MacDonald
, Jean Paul Vonsattel
, James F. Gusella
, Edward D. Bird

Risultato della ricerca: Contributo su rivista › Articolo in rivista › peer review

Abstract

CAG repeat expansion in the Huntington’s disease gene (HD) was examined in post-mortem brains from 310 clinically diagnosed and 15 ‗at risk‘ individuals. Presence of an expanded CAG allele (=37 units) was the cause of the disorder in almost all cases (307 of 310). Despite a diversity of reporting clinicians, neurological and psychiatric onset and age at death all displayed significant inverse correlations with CAG number indicating that diagnosis of onset is reasonably accurate, and that most patients die from the disease and its complications. Neuronal changes before clinical onset are not detected by conventional microscopic examination as three out of 15 ‗at risk‘ brains had an expanded CAG allele but no neuropathology. The cause of HD-like neuropathology in three exceptional brains from clinically diagnosed individuals is unclear. The disorder in these cases could be an HD phenocopy or result from alternative mutational mechanisms at the HD locus.

Lingua originale	Inglese
pagine (da-a)	159-166
Numero di pagine	8
Rivista	Neurobiology of Disease
Volume	1
Numero di pubblicazione	3
DOI	https://doi.org/10.1006/nbdi.1994.0019
Stato di pubblicazione	Pubblicato - 1994
Pubblicato esternamente	Sì

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10.1006/nbdi.1994.0019

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@article{3fa3e57c94b14a608e5330f15c9242bf,

title = "Huntington{\textquoteright}s disease cag trinucleotide repeats in pathologically confirmed post-mortem brains",

abstract = "CAG repeat expansion in the Huntington{\textquoteright}s disease gene (HD) was examined in post-mortem brains from 310 clinically diagnosed and 15 ‗at risk{\textquoteleft} individuals. Presence of an expanded CAG allele (=37 units) was the cause of the disorder in almost all cases (307 of 310). Despite a diversity of reporting clinicians, neurological and psychiatric onset and age at death all displayed significant inverse correlations with CAG number indicating that diagnosis of onset is reasonably accurate, and that most patients die from the disease and its complications. Neuronal changes before clinical onset are not detected by conventional microscopic examination as three out of 15 ‗at risk{\textquoteleft} brains had an expanded CAG allele but no neuropathology. The cause of HD-like neuropathology in three exceptional brains from clinically diagnosed individuals is unclear. The disorder in these cases could be an HD phenocopy or result from alternative mutational mechanisms at the HD locus.",

keywords = "Glycollate, Mutation, Neuropathology, Phenocopy, Post-mortem brain, Sodium pentosan polysulphate",

author = "Francesca Persichetti and Jayalakshmi Srinidhi and Lisa Kanaley and Pei Ge and Myers, \{Richard H.\} and Kenneth D{\textquoteright}Arrigo and Barnes, \{Glenn T.\} and MacDonald, \{Marcy E.\} and Vonsattel, \{Jean Paul\} and Gusella, \{James F.\} and Bird, \{Edward D.\}",

note = "Funding Information: This work was supported by NIH grants NS16367 (Huntington{\textquoteright}s Disease Center Without Walls), MH/NS31862 (Brain Bank), and by grants from the Hereditary Disease Foundation, and the Huntington{\textquoteright}s Disease Society of America.",

year = "1994",

doi = "10.1006/nbdi.1994.0019",

language = "English",

volume = "1",

pages = "159--166",

journal = "Neurobiology of Disease",

issn = "0969-9961",

publisher = "Academic Press Inc.",

number = "3",

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TY - JOUR

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AU - Persichetti, Francesca

AU - Srinidhi, Jayalakshmi

AU - Kanaley, Lisa

AU - Ge, Pei

AU - Myers, Richard H.

AU - D’Arrigo, Kenneth

AU - Barnes, Glenn T.

AU - MacDonald, Marcy E.

AU - Vonsattel, Jean Paul

AU - Gusella, James F.

AU - Bird, Edward D.

N1 - Funding Information: This work was supported by NIH grants NS16367 (Huntington’s Disease Center Without Walls), MH/NS31862 (Brain Bank), and by grants from the Hereditary Disease Foundation, and the Huntington’s Disease Society of America.

PY - 1994

Y1 - 1994

N2 - CAG repeat expansion in the Huntington’s disease gene (HD) was examined in post-mortem brains from 310 clinically diagnosed and 15 ‗at risk‘ individuals. Presence of an expanded CAG allele (=37 units) was the cause of the disorder in almost all cases (307 of 310). Despite a diversity of reporting clinicians, neurological and psychiatric onset and age at death all displayed significant inverse correlations with CAG number indicating that diagnosis of onset is reasonably accurate, and that most patients die from the disease and its complications. Neuronal changes before clinical onset are not detected by conventional microscopic examination as three out of 15 ‗at risk‘ brains had an expanded CAG allele but no neuropathology. The cause of HD-like neuropathology in three exceptional brains from clinically diagnosed individuals is unclear. The disorder in these cases could be an HD phenocopy or result from alternative mutational mechanisms at the HD locus.

AB - CAG repeat expansion in the Huntington’s disease gene (HD) was examined in post-mortem brains from 310 clinically diagnosed and 15 ‗at risk‘ individuals. Presence of an expanded CAG allele (=37 units) was the cause of the disorder in almost all cases (307 of 310). Despite a diversity of reporting clinicians, neurological and psychiatric onset and age at death all displayed significant inverse correlations with CAG number indicating that diagnosis of onset is reasonably accurate, and that most patients die from the disease and its complications. Neuronal changes before clinical onset are not detected by conventional microscopic examination as three out of 15 ‗at risk‘ brains had an expanded CAG allele but no neuropathology. The cause of HD-like neuropathology in three exceptional brains from clinically diagnosed individuals is unclear. The disorder in these cases could be an HD phenocopy or result from alternative mutational mechanisms at the HD locus.

KW - Glycollate

KW - Mutation

KW - Neuropathology

KW - Phenocopy

KW - Post-mortem brain

KW - Sodium pentosan polysulphate

UR - https://www.scopus.com/pages/publications/0028677475

U2 - 10.1006/nbdi.1994.0019

DO - 10.1006/nbdi.1994.0019

M3 - Article

SN - 0969-9961

VL - 1

SP - 159

EP - 166

JO - Neurobiology of Disease

JF - Neurobiology of Disease

IS - 3

ER -

Huntington’s disease cag trinucleotide repeats in pathologically confirmed post-mortem brains

Abstract

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