Systematic genetic study of Alzheimer disease in Latin America: Mutation frequencies of the amyloid β precursor protein and presenilin genes in Colombia* |
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Authors: | Diana Arango Marc Cruts Orlando Torres Hubert Backhovens Martha L. Serrano Elsa Villareal Patricia Montañes Diana Matallana Carlos Cano Martine Jacquier |
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Affiliation: | 1. Neuro‐Sciences Group, Instituto Nacional de Salud, Bogotá, Colombia;2. Molecular Genetics Department, Flanders Interuniversity Institute for Biotechnology (VIB), University of Antwerp (UIA), Antwerp, Belgium;3. Marc Cruts is a postdoctoral fellow of the FWO.;4. Memory Clinic, Universidad Javeriana, Santafé de Bogotá, Colombia |
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Abstract: | Nearly all mutations in the presenilin 1 (PSEN1), presenilin 2 (PSEN2), and amyloid β precursor protein (APP) genes lead to early‐onset Alzheimer disease (EOAD, onset age at or before 65 years). In order to assess the genetic contribution of these genes in a series of Colombian AD cases, we performed a systematic mutation analysis in 11 autosomal dominant, 23 familial, and 42 sporadic AD patients (34% with age of onset ≤ 65 years). No APP missense mutations were identified. In three autosomal dominant cases (27.2%), two different PSEN1 missense mutations were identified. Both PSEN1 mutations are missense mutations that occurred in early‐onset autosomal AD cases: an I143T mutation in one case (onset age 30 years) and an E280A mutation in two other cases (onset ages 35 and 42 years). In addition, a novel PSEN1 V94M mutation was present in one early‐onset AD case without known family history (onset age 53 years) and absent in 53 controls. The E318G polymorphism was present in five AD cases and absent in controls. In PSEN2, two different silent mutations were detected, including one not reported elsewhere (P129). The majority of the Colombian AD cases, predominantly late‐onset, were negative for PSEN and APP mutations. © 2001 Wiley‐Liss, Inc. |
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Keywords: | Alzheimer disease APP PSEN1 PSEN2 mutation analysis G708 V94M I143T E280A E318G P129 S236 |
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