|
Cloning of a gene bearing missense mutations in early-onset familial
Alzheimer's disease R. Sherrington*, E.
I. Rogaev*, Y. Liang*, E.
A. Rogaeva*, G. Levesque*, M. Ikeda*, H. Chi*, C. Lin*, G. Li*, K. Holman*, T. Tsuda*, L. Mar‡, J.-F. Foncin§, A.
C. Bruni , M.
P. Montesi , S. Sorbi¶, I. Rainero£, L. Pinessi£, L. Nee , I. Chumakov**, D. Pollen††, A. Brookes†, P. Sanseau¶¶, R.
J. Polinsky££, W. Wasco‡‡, H.
A. R. Da Silva§§, J.
L. Haines‡‡, M.
A. Pericak-Vance§§, R.
E. Tanzi‡‡, A.
D. Roses§§, P.
E. Fraser*, J.
M. Rommens‡ & P. H. St
George-Hyslop* 
* Centre
for Research into Neurodegenerative Diseases, Departments of Medicine
(Neurology) and Medical Biophysics, University of Toronto, Toronto, and
Department of Medicine, Division of Neurology, The Toronto Hospital, Toronto,
Ontario, M5S 1A8, Canada
‡ Research Institute,
The Hospital for Sick Children, and Department of Molecular and Medical
Genetics, University of Toronto, Toronto, Ontario, M5S 1A8,
Canada
§ Laboratoire de Neurohistologie, Ecole
Pratique des Hautes Etudes and U106, INSERM La Salpetriere, 75651 Paris Cedex
13, France
USL-6 and UO-CNR, 88046 Lamezia
Terme, Italy
¶ Department of Neurology and
Psychiatry, University of Florence, viale Morgagni 85, Florence,
Italy
£ Department of Neurology, University of
Turin, via Cherasco 15, 10126 Turin, Italy
Clinical Neuropharmaeology Section, NINDS, 9000 Rockville Pike, Bethesda,
Maryland 20892, USA
** Centre d'Etude
Polymorphisme Humaine, 27 Rue Juliette Dodu, 75010, Paris,
France
†† Department of Neurology,
University of Massachusetts Medical Center, 55 Lake Avenue, Worcester,
Massachusetts 01655, USA
‡‡ Molecular
Neurogenetics Laboratory and Laboratory of Genetics and Aging, Massachusetts
General Hospital, Departments of Neurology and Genetics, Harvard Medical
School, Boston, Massachusetts 02114, USA
§§
Bryan Alzheimer's Disease Research Center, Duke University Medical Center,
Durham, North Carolina 27710, USA
¶¶
Molecular Pathology, Glaxo Research and Development, Greenford Road, Greenford,
Middlesex UB6 OHE, UK
££ Sandoz Research
Institute, Sandoz Pharmaceuticals Corporation, 59 Route 10, East Hanover, New
Jersey 07936, USA
† MRC Human Genetics Unit,
Western General Hospital, Crewe Road, Edinburgh,
UK
 To whom correspondence should be
addressed.
Some cases of Alzheimer's disease are inherited as an autosomal dominant
trait. Genetic linkage studies have mapped a locus (AD3) associated with
susceptibility to a very aggressive form of Alzheimer's disease to chromosome
14q24.3. We have defined a minimal cosegregating region containing the AD3
gene, and isolated at least 19 different transcripts encoded within this
region. One of these transcripts (S182) corresponds to a novel gene whose
product is predicted to contain multiple transmembrane domains and resembles an
integral membrane protein. Five different missense mutations have been found
that cosegregate with early-onset familial Alzheimer's disease. Because these
changes occurred in conserved domains of this gene, and are not present in
normal controls, they are likely to be causative of AD3.
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