Role of the extended MAPT haplotype in the worsening of psychotic symptoms and treatment response in Alzheimer disease

TY - JOUR

T1 - Role of the extended MAPT haplotype in the worsening of psychotic symptoms and treatment response in Alzheimer disease

AU - Creese, Byron

AU - Corbett, Anne

AU - Jones, Emma

AU - Fox, Chris

AU - Ballard, Clive

PY - 2014/12

Y1 - 2014/12

N2 - IntroductionThere is evidence that neurofibrillary tangle (NFT) burden is associated with psychotic symptoms in Alzheimer disease (AD). However, it is not clear whether this association is direct or mediated through the increased cognitive impairment associated with NFTs.MethodsWe sought to determine whether the extended MAPT haplotype was associated with the worsening of delusions and hallucinations in a combined cohort of 95 patients who participated in 2 clinical trials of treatment with memantine.ResultsAfter controlling for baseline dementia severity, exposure to memantine, and antipsychotics, analysis shows that carriers of at least one H2 allele had a 5.4-fold (P = .03) increased risk of worsening hallucinations. There was some evidence of association with worsening delusions but only in analysis by allele.ConclusionThese results are the first to indicate that the H2 allele of the extended MAPT haplotype negatively affects the course of psychotic symptoms in AD independently of disease severity. It will be important for future research to examine MAPT transcription in people with AD with and without psychotic symptoms to understand the exact mechanisms underlying these findings.

AB - IntroductionThere is evidence that neurofibrillary tangle (NFT) burden is associated with psychotic symptoms in Alzheimer disease (AD). However, it is not clear whether this association is direct or mediated through the increased cognitive impairment associated with NFTs.MethodsWe sought to determine whether the extended MAPT haplotype was associated with the worsening of delusions and hallucinations in a combined cohort of 95 patients who participated in 2 clinical trials of treatment with memantine.ResultsAfter controlling for baseline dementia severity, exposure to memantine, and antipsychotics, analysis shows that carriers of at least one H2 allele had a 5.4-fold (P = .03) increased risk of worsening hallucinations. There was some evidence of association with worsening delusions but only in analysis by allele.ConclusionThese results are the first to indicate that the H2 allele of the extended MAPT haplotype negatively affects the course of psychotic symptoms in AD independently of disease severity. It will be important for future research to examine MAPT transcription in people with AD with and without psychotic symptoms to understand the exact mechanisms underlying these findings.

U2 - 10.1016/j.jamda.2014.08.011

DO - 10.1016/j.jamda.2014.08.011

M3 - Article

SN - 1525-8610

VL - 15

SP - 934

EP - 937

JO - Journal Of The American Medical Directors Association

JF - Journal Of The American Medical Directors Association

IS - 12

ER -