Genetic Analysis Reveals that Amyloid Precursor Protein and Death Receptor 6 Function in the Same Pathway to Control Axonal Pruning Independent of β-Secretase

Olsen, Olav; Kallop, Dara; McLaughlin, Todd; Huntwork‐Rodriguez, Sarah; Wu, Zhuhao; Duggan, Cynthia; Simon, David; Lu, Yanmei; Easley-Neal, Courtney; Takeda, Kentaro; Hass, Philip E.; Jaworski, Alexander; O’Leary, Dennis D.M.; Weimer, Robby M.; Tessier‐Lavigne, Marc

doi:10.1523/jneurosci.3522-13.2014

Cited by 50 publications

(70 citation statements)

References 17 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Previous studies have elucidated the structures of the unbound APP extracellular domains (Wang and Ha 2004;Dahms et al 2010Dahms et al , 2012Hoopes et al 2010;Lee et al 2011; Xue et al 2011a,b;Coburger et al 2013Coburger et al , 2014. High-affinity binding of APP to death receptor 6 (DR6, also known as TNFRSF21), a death domain-containing member of the extended TNF receptor superfamily (Pan et al 1998), was recently documented (Nikolaev et al 2009) and shown to be mediated by the E2 domain of APP (Olsen et al 2014). DR6 has four cysteine-rich domain (CRD) modules in its extracellular region, followed by a transmembrane domain and death domain in its cytoplasmic region.…”

mentioning

confidence: 99%

“…The structure of the unbound DR6 ectodomain (ECD) (Kuester et al 2011;Ru et al 2012) revealed an elongated architecture with a kink between CRD modules 2 and 3. Genetic analysis of DR6 and APP mutant mice showed that the animals share several coincident phenotypes, including behavioral deficits, altered synapse formation, and delayed axon pruning during development or following sensory deprivation Olsen et al 2014). These and other data Olsen et al 2014) indicate that APP and DR6 function cell-autonomously and in the same pathway to stimulate axon pruning and synapse elimination.…”

mentioning

confidence: 99%

“…Genetic analysis of DR6 and APP mutant mice showed that the animals share several coincident phenotypes, including behavioral deficits, altered synapse formation, and delayed axon pruning during development or following sensory deprivation Olsen et al 2014). These and other data Olsen et al 2014) indicate that APP and DR6 function cell-autonomously and in the same pathway to stimulate axon pruning and synapse elimination. However, how APP and DR6 interact to mediate their actions is poorly understood.…”

mentioning

confidence: 99%

See 2 more Smart Citations

The crystal structure of DR6 in complex with the amyloid precursor protein provides insight into death receptor activation

Olsen

Tzvetkova-Robev

et al. 2015

Genes Dev.

View full text Add to dashboard Cite

The amyloid precursor protein (APP) has garnered considerable attention due to its genetic links to Alzheimer's disease. Death receptor 6 (DR6) was recently shown to bind APP via the protein extracellular regions, stimulate axonal pruning, and inhibit synapse formation. Here, we report the crystal structure of the DR6 ectodomain in complex with the E2 domain of APP and show that it supports a model for APP-induced dimerization and activation of cell surface DR6. The amyloid precursor protein (APP) is a single-pass transmembrane protein best known for its genetic association with Alzheimer's disease (AD). APP serves as the proteolytic precursor to Aβ, the major peptide component of amyloid plaques in the brains of Alzheimer's patients (Selkoe 2011). Therapeutic strategies to modify APP processing or clear Aβ from plaques in Alzheimer's patients have not yet proven effective (Gandy and DeKosky 2013), encouraging the search for additional approaches for treating AD. This has stimulated interest in understanding the normal physiological role of APP in the developing and adult nervous system in the hope that this will provide new insights into how perturbed APP function may contribute to disease onset and/or progression. These studies have implicated APP in several physiological processes, including axon pruning, synapse formation, axonal transport, and cellular adhesion (Kamal et al. 2001;Priller et al. 2006;Bittner et al. 2009;Nikolaev et al. 2009;Wang et al. 2009). The extracellular domain of APP is comprised of an N-terminal domain termed E1 and a more C-terminal domain termed E2 that are linked via an acidic unstructured sequence and followed by a transmembrane helix and a cytoplasmic region. Previous studies have elucidated the structures of the unbound APP extracellular domains (Wang and Ha 2004;Dahms et al. 2010Dahms et al. , 2012Hoopes et al. 2010;Lee et al. 2011; Xue et al. 2011a,b;Coburger et al. 2013Coburger et al. , 2014. High-affinity binding of APP to death receptor 6 (DR6, also known as TNFRSF21), a death domain-containing member of the extended TNF receptor superfamily (Pan et al. 1998), was recently documented (Nikolaev et al. 2009) and shown to be mediated by the E2 domain of APP (Olsen et al. 2014). DR6 has four cysteine-rich domain (CRD) modules in its extracellular region, followed by a transmembrane domain and death domain in its cytoplasmic region. The structure of the unbound DR6 ectodomain (ECD) (Kuester et al. 2011;Ru et al. 2012) revealed an elongated architecture with a kink between CRD modules 2 and 3. Genetic analysis of DR6 and APP mutant mice showed that the animals share several coincident phenotypes, including behavioral deficits, altered synapse formation, and delayed axon pruning during development or following sensory deprivation Olsen et al. 2014). These and other data Olsen et al. 2014) indicate that APP and DR6 function cell-autonomously and in the same pathway to stimulate axon pruning and synapse elimination. However, how APP and DR6 interact to mediate their actions is poor...

show abstract

mentioning

confidence: 99%

mentioning

confidence: 99%

mentioning

confidence: 99%

See 1 more Smart Citation

The crystal structure of DR6 in complex with the amyloid precursor protein provides insight into death receptor activation

Olsen

Tzvetkova-Robev

et al. 2015

Genes Dev.

View full text Add to dashboard Cite

show abstract

“…Among different fragments of sAPP (Caille et al, 2004;Ohsawa et al, 1999;Olsen et al, 2014;Willem et al, 2015), the soluble Nterminal fragment (aa 18-286) and the 770 aa form sAPP(770) negatively regulate NSC growth but do not affect the number of neurospheres in the culture from acutely dissociated SVZ cells (Fig. S3).…”

Section: Resultsmentioning

confidence: 94%

Soluble APP functions as a vascular niche signal that controls adult neural stem cell number

Sato

Uchida

et al. 2017

Development

View full text Add to dashboard Cite

The molecular mechanism by which NSC number is controlled in the neurogenic regions of the adult brain is not fully understood but it has been shown that vascular niche signals regulate neural stem cell (NSC) quiescence and growth. Here, we have uncovered a role for soluble amyloid precursor protein (sAPP) as a vascular niche signal in the subventricular zone (SVZ) of the lateral ventricle of the adult mouse brain. sAPP suppresses NSC growth in culture. Further in vivo studies on the role of APP in regulating NSC number in the SVZ clearly demonstrate that endothelial deletion of App causes a significant increase in the number of BrdU label-retaining NSCs in the SVZ, whereas NSC/astrocyte deletion of App has no detectable effect on the NSC number. Taken together, these results suggest that endothelial APP functions as a vascular niche signal that negatively regulates NSC growth to control the NSC number in the SVZ.

show abstract

“…In 2009, Genentech discovered an interaction between DR6 and amyloid precursor protein (APP), 3 a neuronal surface protein that undergoes a series of proteolytic cleavages to yield the b-amyloid (Ab) fragment. Ab aggregates form the amyloid plaques that are the hallmarks of AD and are thought to be a main upstream trigger for neurodegeneration.…”

mentioning

confidence: 99%

The DR is out

Osherovich¹

2014

Science-Business eXchange

View full text Add to dashboard Cite

Five years after a Genentech Inc. team proposed that the receptor DR6 might be involved in Alzheimer's disease, the company and The Rockefeller University have concluded that the proapoptotic pathway is unlikely to affect the most overt feature of the disease-amyloid plaque formation.The Roche unit said that the new findings 1,2 mark the stopping point for its discovery efforts to target DR6 (tumor necrosis factor receptor superfamily member 21; TNFRSF21) in AD. Although the company is backing off DR6, the academics involved in the work think further studies with better disease models are warranted.DR6 is a member of a family of cell surface receptors that activates caspases-intracellular proapoptotic proteases-when neurons are deprived of trophic factors such as nerve growth factor (NGF) or brainderived neurotrophic factor (BDNF).In 2009, Genentech discovered an interaction between DR6 and amyloid precursor protein (APP), 3 a neuronal surface protein that undergoes a series of proteolytic cleavages to yield the b-amyloid (Ab) fragment. Ab aggregates form the amyloid plaques that are the hallmarks of AD and are thought to be a main upstream trigger for neurodegeneration. The group, led by then-CSO Marc Tessier-Lavigne, found that DR6 was activated by a fragment of APP left behind after the proteolytic processing formed Ab. 4 Tessier-Lavigne is now a professor and president at The Rockefeller University.Because activation of DR6 by the stray APP fragment led to neuronal apoptosis, the next question was whether DR6 activation played a role in Ab toxicity."We set out to test a specific hypothesis about the potential role of DR6 in an APP-driven model of AD, " said team leader and Genentech senior scientist Robby Weimer. "The conclusion from our results is that we didn't find a role for DR6 in amyloid formation, synapse loss or behavior consequence. Our take home is that DR6 doesn't represent a good target for APP-driven AD pathology. " Death receptor deadThe hope was that DR6 inhibition might enhance neuronal branching and thus counteract the neurotoxic effects of Ab. However, the new findings suggest that will not be the case.In two mouse models of AD in which overproduction of Ab leads to disease, DR6 deletion increased branching of mature neurons in some brain regions compared with no alteration. However, DR6 deletion did not reduce plaque formation or the behavioral and cognitive consequences of Ab toxicity. Results were reported in The Journal of Neuroscience.Weimer and Tessier-Lavigne said that the findings indicate that one of APP's normal functions outside of AD may be to interact with DR6 to control neuronal branching in the adult nervous system. However, this process likely occurs independently of the abnormal proteolytic processing of APP that leads to AD."It seems that APP has multiple functions, " said Weimer. "Its normal physiological function could be through DR6. We did find evidence for DR6 and APP acting together in the mature nervous system to regulate synapse sensitivity. "Tessier-Lavigne said t...

show abstract

Genetic Analysis Reveals that Amyloid Precursor Protein and Death Receptor 6 Function in the Same Pathway to Control Axonal Pruning Independent of β-Secretase

Cited by 50 publications

References 17 publications

The crystal structure of DR6 in complex with the amyloid precursor protein provides insight into death receptor activation

The crystal structure of DR6 in complex with the amyloid precursor protein provides insight into death receptor activation

Soluble APP functions as a vascular niche signal that controls adult neural stem cell number

The DR is out

Contact Info

Product

Resources

About