Inactivation of the mouse huntington's disease gene homolog Hdh

Mabel P. Duyao; Anna B. Auerbach; Angela Ryan; Francesca Persichetti; Glenn T. Barnes; Sandra M. McNeil; Pei Ge; Jean Paul Vonsattel; James F. Gusella; Alexandra L. Joyner; Marcy E. MacDonald

doi:10.1126/science.7618107

Inactivation of the mouse huntington's disease gene homolog Hdh

Mabel P. Duyao, Anna B. Auerbach, Angela Ryan, Francesca Persichetti, Glenn T. Barnes, Sandra M. McNeil, Pei Ge, Jean Paul Vonsattel, James F. Gusella, Alexandra L. Joyner, Marcy E. MacDonald

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

Abstract

Huntington's disease (HD) is a dominant neurodegenerative disorder caused by expansion of a CAG repeat in the gene encoding huntingtin, a protein of unknown function. To distinguish between "loss of function" and "gain of function" models of HD, the murine HD homolog Hdh was inactivated by gene targeting. Mice heterozygous for Hdh inactivation were phenotypically normal, whereas homozygosity resulted in embryonic death. Homozygotes displayed abnormal gastrulation at embryonic day 7.5 and were resorbing by day 8.5. Thus, huntingtin is critical early in embryonic development, before the emergence of the nervous system. That Hdh inactivation does not mimic adult HD neuropathology suggests that the human disease involves a gain of function.

Lingua originale	Inglese
pagine (da-a)	407-410
Numero di pagine	4
Rivista	Science
Volume	269
Numero di pubblicazione	5222
DOI	https://doi.org/10.1126/science.7618107
Stato di pubblicazione	Pubblicato - 1995
Pubblicato esternamente	Sì

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title = "Inactivation of the mouse huntington's disease gene homolog Hdh",

abstract = "Huntington's disease (HD) is a dominant neurodegenerative disorder caused by expansion of a CAG repeat in the gene encoding huntingtin, a protein of unknown function. To distinguish between {"}loss of function{"} and {"}gain of function{"} models of HD, the murine HD homolog Hdh was inactivated by gene targeting. Mice heterozygous for Hdh inactivation were phenotypically normal, whereas homozygosity resulted in embryonic death. Homozygotes displayed abnormal gastrulation at embryonic day 7.5 and were resorbing by day 8.5. Thus, huntingtin is critical early in embryonic development, before the emergence of the nervous system. That Hdh inactivation does not mimic adult HD neuropathology suggests that the human disease involves a gain of function.",

author = "Duyao, {Mabel P.} and Auerbach, {Anna B.} and Angela Ryan and Francesca Persichetti and Barnes, {Glenn T.} and McNeil, {Sandra M.} and Pei Ge and Vonsattel, {Jean Paul} and Gusella, {James F.} and Joyner, {Alexandra L.} and MacDonald, {Marcy E.}",

year = "1995",

doi = "10.1126/science.7618107",

language = "English",

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T1 - Inactivation of the mouse huntington's disease gene homolog Hdh

AU - Duyao, Mabel P.

AU - Auerbach, Anna B.

AU - Ryan, Angela

AU - Persichetti, Francesca

AU - Barnes, Glenn T.

AU - McNeil, Sandra M.

AU - Ge, Pei

AU - Vonsattel, Jean Paul

AU - Gusella, James F.

AU - Joyner, Alexandra L.

AU - MacDonald, Marcy E.

PY - 1995

Y1 - 1995

N2 - Huntington's disease (HD) is a dominant neurodegenerative disorder caused by expansion of a CAG repeat in the gene encoding huntingtin, a protein of unknown function. To distinguish between "loss of function" and "gain of function" models of HD, the murine HD homolog Hdh was inactivated by gene targeting. Mice heterozygous for Hdh inactivation were phenotypically normal, whereas homozygosity resulted in embryonic death. Homozygotes displayed abnormal gastrulation at embryonic day 7.5 and were resorbing by day 8.5. Thus, huntingtin is critical early in embryonic development, before the emergence of the nervous system. That Hdh inactivation does not mimic adult HD neuropathology suggests that the human disease involves a gain of function.

AB - Huntington's disease (HD) is a dominant neurodegenerative disorder caused by expansion of a CAG repeat in the gene encoding huntingtin, a protein of unknown function. To distinguish between "loss of function" and "gain of function" models of HD, the murine HD homolog Hdh was inactivated by gene targeting. Mice heterozygous for Hdh inactivation were phenotypically normal, whereas homozygosity resulted in embryonic death. Homozygotes displayed abnormal gastrulation at embryonic day 7.5 and were resorbing by day 8.5. Thus, huntingtin is critical early in embryonic development, before the emergence of the nervous system. That Hdh inactivation does not mimic adult HD neuropathology suggests that the human disease involves a gain of function.

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U2 - 10.1126/science.7618107

DO - 10.1126/science.7618107

M3 - Article

SN - 0036-8075

VL - 269

SP - 407

EP - 410

JO - Science

JF - Science

IS - 5222

ER -

Inactivation of the mouse huntington's disease gene homolog Hdh

Abstract

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