@article { , title = {Common variants of ACE contribute to variable age-at-onset of Alzheimer's disease}, abstract = {Studies on the role that genetic variation may play in a complex human disease can be empowered by an assessment of both disease risk in case-control or family models and of quantitative traits that reflect elements of disease etiology. An excellent example of this can be found for the E4 allele of APOE in relation to Alzheimer's disease (AD) for which association with both risk and age-at-onset (AAO) is evident. Following a recent demonstration that variants of the gene encoding angiotensin I converting enzyme (ACE) contribute to AD risk, we have explored the potential influence of ACE upon AAO in AD. A total of 2861 individuals from three European populations, including six independent AD samples, have been examined in this study. Three single nucleotide polymorphisms (SNPs) previously demonstrated to have maximum effects upon ACE plasma levels and that span the ACE locus were genotyped in these materials. A strong effect upon AAO was observed for marker rs4343 in exon 17 (P}, doi = {10.1007/s00439-004-1093-y}, issn = {0340-6717}, issue = {5}, journal = {Human Genetics}, pages = {478-483}, publicationstatus = {Published}, publisher = {Springer (part of Springer Nature)}, url = {https://uwe-repository.worktribe.com/output/1061212}, volume = {114}, keyword = {Centre for Health and Clinical Research, ACE, variable age-at-onsetc Alzheimer's disease}, year = {2004}, author = {Wilcock, Gordon K. and Palmgren, Juni and de Faire, Ulf and Brookes, Anthony J. and Pedersen, Nancy L. and Blennow, Kaj and Prince, Jonathan A. and Katzov, Hagit and Gatz, Maragaret and Andreasen, Niels and Cairns, Nigel J. and Kehoe, Patrick G.} }