Novel presenilin 1 mutation with profound neurofibrillary pathology in an indigenous Southern African family with early-onset Alzheimer's disease

doi:10.1093/brain/awh009

Brain Advance Access originally published online on October 21, 2003

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Brain, Vol. 127, No. 1, 133-142, 2004
© 2004 Guarantors of Brain
doi: 10.1093/brain/awh009

Novel presenilin 1 mutation with profound neurofibrillary pathology in an indigenous Southern African family with early-onset Alzheimer’s disease

Jeannine M. Heckmann¹, Wee-Chuang Low⁴, Cora de Villiers¹, Stuart Rutherfoord^,3, Alvera Vorster², Harpal Rao⁴, Christopher M. Morris⁴, Raj S. Ramesar² and Raj N. Kalaria⁴

¹ Division of Neurology and ² MRC Human Genetics Research Unit, Division of Human Genetics, Groote Schuur Hospital and University of Cape Town, Cape Town, ³ Neuropathology Unit, Department of Anatomical Pathology, University of Stellenbosch, Tygerberg, South Africa and ⁴ Institute for Ageing and Health, Newcastle General Hospital, Newcastle upon Tyne, UK ${dagger}$ Deceased

Correspondence to: Professor R. N. Kalaria, Institute for Ageing and Health, Wolfson Unit, Newcastle General Hospital, Westgate Road, Newcastle upon Tyne NE4 6BE, UK E-mail: r.n.kalaria{at}ncl.ac.uk

Genetically determined Alzheimer’s disease (AD) is virtuallyunknown in Africa. We report clinicopathological findings anda presenilin 1 (PS1) mutation associated with early-onsetAD in a large Xhosa family from Southern Africa. Twelve individualsspanning four generations were affected, four of whom underwentclinical and psychometric evaluation. Their phenotype was characterizedby memory impairment beginning in the early part of the fifthdecade, with progressive dementing illness lasting 6–7years that did not appear to be modified by the presence ofan apolipoprotein E (APOE)- ${epsilon}$ 4 allele. Initial linkage-based analysisusing known DNA markers suggested allele cosegregation witha locus on chromosome 14. Direct sequencing of the PS1 genedisclosed a novel I143M (ATT to ATG at nucleotide 677) mutationthat lies in a cluster in the second transmembrane domain ofthe protein. Examination of the proband’s brain at autopsyrevealed severe AD pathology characterized by neuronal loss,abundant ß amyloid (Aß) neuritic plaques(Aß42) and neurofibrillary degeneration extendinginto the brainstem. The phenotype of the I143M mutation wasclearly associated with a high degree of neurofibrillary changecompared with early-onset sporadic AD cases. Although sporadiccases of AD do exist in African populations, our study confirmsthe existence of early-onset familial AD among indigenous SouthernAfricans.

Key Words: Africa; Alzheimer’s disease; apolipoprotein E; neurofibrillary tangles; presenilin

Abbreviations: Aß = ß amyloid peptide; AD = Alzheimer’s disease; APOE = apolipoprotein E; APP = ß amyloid precursor protein; DECO = détérioration cognitive observée; MMSE = Mini-Mental State Examination; PS1 = presenilin1 gene

Received February 27, 2003. Revised July 22, 2003. Accepted July 30, 2003.

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