DAPK1 variants are associated with Alzheimer's disease and allele-specific expression

Li, Yonghong; Grupe, Andrew; Rowland, Charles M.; Nowotny, Petra; Kauwe, John; Smemo, Scott; Hinrichs, Anthony L.; Tacey, Kristina; Toombs, T.; Kwok, Shirley; Catanese, Joseph J.; White, Thomas J.; Maxwell, Taylor J.; Hollingworth, Paul; Abraham, Richard; Rubinsztein, David C.; Brayne, Carol; Vrièze, Fabienne Wavrant‐De; Hardy, John; O'Donovan, Michael Conlon; Lovestone, Simon; Morris, John C.; Thal, Leon J.; Williams, Julie; Goate, Alison M.

doi:10.1093/hmg/ddl178

Cited by 118 publications

(87 citation statements)

References 46 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Linkage disequilibrium at 1q44 was reported in a study of 100 AD cases and 100 controls (Zubenko et al 1998), linkage at 2q22 and 2q24 was detected in a linkage study of 88 LOAD families (Lee et al 2004), and linkage at 9q34 was detected in a study of 466 families (Pericak-Vance et al 2000), close to the 9q33 syntenic region reported here. This 9q33 syntenic region is also close to a major region of interest in human AD on chromosome 9q, but lies slightly outside the 9q21-31 region typically identified with the strongest support, and does not contain the DAPK1 gene recently implicated in an association study (Li et al 2006). Unlike the more extensively reported areas of linkage on human chromosomes 9, 10, and 12, these syntenic human linkage findings have not been replicated by multiple studies, suggesting that they are unlikely to explain a major part of the observed heritability of AD risk.…”

Section: Discussionmentioning

confidence: 76%

Genetic loci modulating amyloid-beta levels in a mouse model of Alzheimer's disease

Ryman

Gao

Lamb

2008

Neurobiology of Aging

View full text Add to dashboard Cite

Genetic studies have demonstrated very high heritability for Alzheimer's disease (AD) risk in humans; however, these genetic contributions have proven extremely challenging to map in large studies of AD patients. Processing of the amyloid precursor protein (APP) to produce amyloidbeta (Aβ) peptide is increasingly believed to be of central importance in AD pathogenesis. Intriguingly, mice from the C57BL/6J and DBA2/J inbred strains carrying the R1.40 APP transgene produce identical levels of unprocessed APP, but demonstrate significant, heritable differences in Aβ levels. To identify specific loci responsible for the observed genetic control of Aβ metabolism in this model system, we have performed a whole-genome quantitative trait locus (QTL) mapping experiment on a total of 516 animals from a C57BL/6JxDBA/2J intercross using a dense set of SNP genetic markers. Our studies have identified three loci on mouse chromosomes 1, 2, and 7 showing significant or suggestive associations with brain Aβ levels, several of which contain regions syntenic to previous reports of linkage in human AD.

show abstract

Section: Discussionmentioning

confidence: 76%

Genetic loci modulating amyloid-beta levels in a mouse model of Alzheimer's disease

Ryman

Gao

Lamb

2008

Neurobiology of Aging

View full text Add to dashboard Cite

show abstract

“…With relevance to neurobiological mechanisms such as neuronal apoptosis and APP trafficking, early genetic studies of LOAD have identified several candidate genes (e.g. DAPK1 [11] and SORL1 [12,13]), but they are still insufficient to completely reveal the genetic factors for AD. A more thorough and efficient approach is required to study the genetic factors of complex diseases like AD.…”

Section: Introductionmentioning

confidence: 99%

An Overview of Genome-Wide Association Studies in Alzheimer’s Disease

Shen

Jia

2016

Neurosci. Bull.

View full text Add to dashboard Cite

Genome-wide association studies (GWASs) have revealed a plethora of putative susceptibility genes for Alzheimer's disease (AD). With the sole exception of the APOE gene, these AD susceptibility genes have not been unequivocally validated in independent studies. No single novel functional risk genetic variant has been identified. In this review, we evaluate recent GWASs of AD, and discuss their significance, limitations, and challenges in the investigation of the genetic spectrum of AD.

show abstract

“…29 A genome-wide SNP study reveals the association of DAPK with LOAD. 9 Furthermore, mice with a deletion in DAPK kinase domain exhibit an enhanced spatial memory. 30 Although these studies implicate a potential impact of DAPK on AD, our finding that DAPK enhances MARK-induced tau phosphorylation and tau toxicity provides a molecular linkage of DAPK to tauopathy-related neurodegenerative disorders, such as AD.…”

Section: Discussionmentioning

confidence: 99%

“…1,7,8 A further connection of DAPK to neuronal diseases comes from a largescale genetic study, which identifies the association of two single nucleotide polymorphisms (SNPs) in DAPK with lateonset Alzheimer's disease (LOAD). 9 However, the causal relationship between DAPK and LOAD has not been established.…”

mentioning

confidence: 99%

DAPK activates MARK1/2 to regulate microtubule assembly, neuronal differentiation, and tau toxicity

Tsai

Chen

et al. 2011

Cell Death Differ

View full text Add to dashboard Cite

Death-associated protein kinase (DAPK) is a key player in several modes of neuronal death/injury and has been implicated in the late-onset Alzheimer's disease (AD). DAPK promotes cell death partly through its effect on regulating actin cytoskeletons. In this study, we report that DAPK inhibits microtubule (MT) assembly by activating MARK/PAR-1 family kinases MARK1/2, which destabilize MT by phosphorylating tau and related MAP2/4. DAPK death domain, but not catalytic activity, is responsible for this activation by binding to MARK1/2 spacer region, thereby disrupting an intramolecular interaction that inhibits MARK1/2. Accordingly, DAPK À/À mice brain displays a reduction of tau phosphorylation and DAPK enhances the effect of MARK2 on regulating polarized neurite outgrowth. Using a well-characterized Drosophila model of tauopathy, we show that DAPK exerts an effect in part through MARK Drosophila ortholog PAR-1 to induce rough eye and loss of photoreceptor neurons. Furthermore, DAPK enhances tau toxicity through a PAR-1 phosphorylation-dependent mechanism. Together, our study reveals a novel mechanism of MARK activation, uncovers DAPK functions in modulating MT assembly and neuronal differentiation, and provides a molecular link of DAPK to tau phosphorylation, an event associated with AD pathology.

show abstract

DAPK1 variants are associated with Alzheimer's disease and allele-specific expression

Cited by 118 publications

References 46 publications

Genetic loci modulating amyloid-beta levels in a mouse model of Alzheimer's disease

Genetic loci modulating amyloid-beta levels in a mouse model of Alzheimer's disease

An Overview of Genome-Wide Association Studies in Alzheimer’s Disease

DAPK activates MARK1/2 to regulate microtubule assembly, neuronal differentiation, and tau toxicity

Contact Info

Product

Resources

About