Low-density lipoprotein receptor-related protein 8

Low-density lipoprotein receptor-related protein 8 (LRP8), also known as apolipoprotein E receptor 2 (ApoER2), is a is_associated_with::protein that in humans is encoded by the LRP8 is_associated_with::gene. ApoER2 is a is_associated_with::cell surface receptor that is part of the low-density lipoprotein receptor family. These receptors function in signal transduction and endocytosis of specific ligands. Through interactions with one of its ligands, is_associated_with::reelin, ApoER2 plays an important role in embryonic neuronal migration and postnatal is_associated_with::long-term potentiation. Another LDL family receptor, VLDLR, also interacts with reelin, and together these two receptors influence brain development and function. Decreased expression of ApoER2 is associated with certain neurological diseases.

Structure
ApoER2 is a protein made up of 870 amino acids. It is separated into a ligand binding domain of eight ligand binding regions, an is_associated_with::EGF-like domain containing three is_associated_with::cysteine-rich repeats, an O-linked is_associated_with::glycosylation domain of 89 amino acids, a transmembrane domain of 24 amino acids, and a cytoplasmic domain of 115 amino acids, including an NPXY motif. Each letter in the NPXY motif represents a certain amino acid where N is is_associated_with::arginine, P is is_associated_with::proline, X is any amino acid, and Y is is_associated_with::tyrosine.

Cytoplasmic tail
All LDL receptor family proteins contain a cytoplasmic tail with at least one NPXY motif. This motif is important for binding intracellular adapter proteins and is_associated_with::endocytosis. ApoER2 is distinct from most other members of the LDL family of receptors due to a unique insert on its cytoplasmic tail. In ApoER2, there is a proline-rich 59 amino acid insert encoded by the alternatively spliced exon 19. This insert allows for protein interactions that are unable to occur with other is_associated_with::LDL receptors. It binds the is_associated_with::PSD-95 adapter protein, cross-linking ApoER2 and the is_associated_with::NMDA receptors during the process of is_associated_with::long-term potentiation, and is also bound specifically by JIP-2, an important interaction in the is_associated_with::JNK signalling pathway. It is also speculated that this insert may diminish the function of ApoER2 in is_associated_with::lipoprotein endocytosis by somehow disrupting the NPXY motif.

Reelin/Dab1 signalling pathway
ApoER2 plays a critical role as a receptor in the reelin signalling pathway, which is important for brain development and postnatal function of the brain. This pathway specifically affects cortical migration and long-term potentiation.

Cortical migration
In development, reelin is secreted by is_associated_with::Cajal-Retzius cells. Reelin acts as an extracellular ligand binding to ApoER2 and VLDLR on migrating neurons. A specific lysine residue on reelin binds to the first repeat on the ligand binding domain of ApoER2. This interaction with the two receptors activates intracellular processes that begin with the phosphorylation of Dab1, a tyrosine kinase phosphorylated protein which is encoded by the is_associated_with::DAB1 gene. This protein associates with the NPXY motifs on the intracellular tails of ApoER2 and VLDLR. Upon reelin binding, Dab1 is phosphorylated by two is_associated_with::tyrosine kinases, Fyn and Src. The phosphorylated Dab1 then causes further activation of these two kinases and others, including a phosphatidylinositol-3-kinase (PI3K). PI3K activation leads to inhibitory phosphorylation of the tau kinase glycogen synthase kinase 3 beta (is_associated_with::GSK3B), which alters the activity of tau protein, a protein involved in stabilizing microtubules. This transduction is combined with the activation of other pathways that influence the cytoskeletal rearrangement necessary for proper cortical cell migration.

The result of proper neuronal migration through the is_associated_with::cortical plate (CP) is an inside-out arrangement of neurons, where the younger neurons migrate past the older neurons to their proper locations. Studies in is_associated_with::reeler mutant mice show that knocking out the reeler gene results in aberrant migration as well as outside-in layering, in which younger neurons are unable to travel past the older ones. Such abnormal layering is also seen in VLDLR−apoER2− and dab1- mutants, indicating the importance of this entire pathway in cortical migration of the developing embryo.

There is some confusion as to the exact function of the reelin-signalling pathway in the process of cortical migration. Some studies have shown that reelin release is necessary for the initiation of cell movement to its proper location, whereas others have shown that it is part of the process of terminating migration. These conflicting results have led researchers to speculate that it plays a role in both processes through interactions with different molecules at different stages of is_associated_with::neuronal migration.

Long-term potentiation
After development, reelin is secreted in the cortex and is_associated_with::hippocampus by gamma-aminobutyric acid-ergic interneurons. Through binding of ApoER2 in the hippocampus, it plays a role in the is_associated_with::NMDA receptor activation that is required for long-term potentiation, a mechanism by which two neurons gain a stronger, longer-lasting transmission due to simultaneous firing. The increased is_associated_with::synaptic plasticity associated with this process is essential in development of memory and spatial learning. Studies with mice have shown less expression of ApoER2 leads to impaired spatial learning, fear conditioned learning, and a mild disruption to the hippocampus.

In the hippocampus, ApoER2 is complexed with NMDA receptors through the is_associated_with::PSD-95 adapter protein. When reelin binds ApoER2, it initiates tyrosine phosphorylation of NMDA receptors. This occurs through Dab-1 activation of is_associated_with::Src family kinases, which have been shown to play a role in regulating synaptic plasticity. VLDLR also acts as a receptor coupled to ApoER2 as it does during development, but its role is not well-understood. ApoER2 plays a more important role in this process, most likely due to its ability to bind the PSD-95 adapter protein through the 59 amino acid insert on its cytoplasmic tail. Studies with mice have shown that knocking out ApoER2 or just the alternatively spliced exon 19 causes a much greater impairment of LTP than knocking out VLDLR.

Apolipoprotein E
is_associated_with::Apolipoprotein E (ApoE) plays an important role in phospholipid and cholesterol homeostasis. After binding ApoER2, ApoE is taken up into the cell and may remain in the intracellular space, be shipped to the cell surface, or be degraded. ApoE binding leads to the cleavage of ApoER2 into secreted proteins by the actions of the plasma membrane protein is_associated_with::gamma secretase. ApoE may be the signalling ligand responsible for ApoER2's role in modulating the JNK signalling pathway.

FE65
FE65 is an intracellular protein that binds to the NPXY motif of ApoER2 and plays a role in linking other proteins, such as is_associated_with::amyloid precursor protein, to ApoER2. This protein aids in a cell's migrational functions. Knockout studies of FE65 have shown a link to is_associated_with::lissencephaly.

JIP1 and JIP2
JIP1 and JIP2 are involved in the JNK-signaling pathway and interact with exon 19 of ApoER2. For JIP2, interaction with exon 19 of ApoER2 is through the PID domain. This interaction has led researchers to believe that ApoER2 is involved in many interactions at the surface of cells.

Selenoprotein P
is_associated_with::Selenoprotein P transports the trace element is_associated_with::selenium from the liver to the testes and brain, and binds to ApoER2 in these areas. ApoER2 functions to internalize this complex to maintain normal levels of selenium in these cells. Selenium is necessary in the testes for proper spermatozoa development. Mice that have had their ApoER2 or Selenoprotein P expression knocked out show impaired spermatozoa development and decreased fertility. In the brain, deficiencies in selenium and selenium uptake mechanisms result in brain damage.

Thrombospondin and F-spondin
is_associated_with::Thrombospondin is a protein found in the is_associated_with::extracellular matrix that competes with reelin to bind ApoER2. It is involved with cell-to-cell communication and migration of neurons, and causes the activation of Dab1. F-spondin is a secreted protein that also binds ApoER2 and leads to phosphorylation of Dab1.

Alzheimer's disease
is_associated_with::Alzheimer's disease is the most common form of dementia, and studies have shown that manipulation of pathways involving LRP8/ApoER2 can lead to the disease. Certain is_associated_with::alleles, such as apoe, app, ps1 and ps2, may lead to being genetically predisposed to the disease. A decrease in LRP8 expression is observed in patients with Alzheimer’s disease. An example of a decrease in expression of LRP8 is when is_associated_with::gamma secretase cleaves LRP8 as well as the ligand is_associated_with::amyloid precursor protein (APP). The degradation products control transcription factors, which lead to the expression of a is_associated_with::tau protein. The cascade dysfunction caused by the altered gene expression may be implicated with Alzheimer’s disease.

The presence of amyloid beta (Aβ) protein deposits in neuronal extracellular space is one of the hallmarks of Alzheimer’s disease. The role of ApoER2 in Alzheimer’s disease is relevant, yet incompletely understood. New evidence suggests ApoER2 plays a major role in the regulation of amyloid-β formation in the brain. The amyloid-β peptide is derived from the cleavage of APP by gamma secretase. ApoER2 works to reduce APP trafficking by altering break down. This interaction decreases APP is_associated_with::endocytosis leading to an increase in amyloid-β production. In addition, the expression of ApoER2 within intracellular compartments leads to increased gamma secretase activity, a protease which works to cleave APP into Aβ.

ApoER2 splice variants can act as a receptor for is_associated_with::alpha-2-macroglobulin which can have a role in clearance of alpha-2-macroglobulin/proteinase complex. is_associated_with::Proteases may play a role in is_associated_with::synaptic plasticity balancing proteolytic activity and inhibition, which is controlled by proteolytic inhibitors such as alpha-2-macroglobulin. Studies have shown that a high presence of alpha-2-macroglobulin is present in the neuritic plaques in many Alzheimer patients. Isolation of cDNA encoding proteins associated with Aβ was used to discover alpha-2-macroglobulin. These discoveries may link alpha-2-macroglobulin and its receptors, one of them being ApoER2, to Alzheimer’s disease.

ApoER2 interaction with reelin and ApoE has implications with Alzheimer’s disease. Binding of reelin to ApoER2 leads to cascade of signals that modulate is_associated_with::NMDA receptor functions. ApoE competes with reelin in binding to ApoER2 resulting in weakened reelin signaling. Reduced reelin signaling leads to impaired plasticity in neurons and increases in the is_associated_with::phosphorylation of tau protein, which is a is_associated_with::microtubule stabilizing protein that is abundant in the is_associated_with::Central Nervous System (CNS), producing is_associated_with::neurofibrillary tangles which are implicated in Alzheimer’s disease.

Antiphospholipid syndrome
is_associated_with::Antiphospholipid syndrome is an is_associated_with::autoimmune disease characterized by is_associated_with::thrombosis and complications during pregnancy, often leading to fetal death. It is caused by the presence of antibodies against anionic is_associated_with::phospholipids and β2-glycoprotein I (β2GPI). The anti-β2GPI antibodies are most prevalent in causing the is_associated_with::symptoms of the disease. When bound by an antibody, β2GPI begins to interact with is_associated_with::monocytes, endothelial cells, and is_associated_with::platelets. ApoER2 is thought to play a key role in the process of platelet binding. β2GPI has the proper binding site for interaction with ApoER2 and other LDL family receptors, and it is speculated that the antibody/β2GPI complexes interact with ApoER2 on platelets. This causes the phosphorylation of a p38MAPkinase, resulting in the production of is_associated_with::thromboxane A2. Thromboxane A2 functions to activate more platelets, and this leads to a greater chance for blood clots to form. There is also speculation that the antibody/β2GPI complexes sensitize other cell types through various LDL family receptors to lead to less common symptoms other than thrombosis.

Major depressive disorder
Reduced expression of ApoER2 in is_associated_with::peripheral blood lymphocytes can contribute to is_associated_with::major depressive disorder (MDD) in some patients. Major depressive disorder is the most common psychiatric disorder, where people show symptoms of low self-esteem and a loss of interest in pleasure. By studying the levels of ApoER2 mRNA, low levels of ApoER2 were discovered. Results from experiments have shown that this could be because of transcriptional alterations in lymphocytes. However, low levels of ApoER2 do not appear to correlate with the severity or duration of the disease. It only aids as a trait marker in identification of the disease. The impact of the low levels of ApoER2 mRNA function relating to the disease remains unknown.