The Transmembrane Domain Region of Nicastrin Mediates Direct Interactions with APH-1 and the γ-Secretase Complex

Morais, Vanessa A.; Crystal, Adam S.; Pijak, Donald S.; Carlin, Dan; Costa, Júlia; Lee, Virginia M.‐Y.; Doms, Robert W.

doi:10.1074/jbc.m305685200

Cited by 69 publications

(75 citation statements)

References 46 publications

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“…Interestingly, immature NCT and APH-1aL as well as the low levels of residual mature NCT (because of the incomplete PEN-2 knockdown) remained stable (Fig. 2B), consistent with the observation that these two proteins can independently stabilize each other (13,20,24,25). Taken together, these data demonstrate that PEN-2-⌬C is highly unstable.…”

Section: Resultssupporting

confidence: 75%

“…This is in contrast to correctly assembled ␥-secretase complex components, which have been shown to be very stable and have a long half-life time (9,17,44,48). The failure of PEN-2-⌬C to stably assemble with PS, NCT, and APH-1 was associated with a marked selective instability of the PS1 NTF and CTF, which also underwent proteasomal degradation, whereas NCT and APH-1 were stable, consistent with previous findings that these proteins can stabilize each other independently (20,24,25). These data suggest that PEN-2 has a dual function as follows: a function in the initiation of PS endoproteolysis as a first maturation step during ␥-secretase complex assembly, and a second function in the stabilization of the PS fragment heterodimer within the ␥-secretase complex that is required for further maturation of the ␥-secretase complex.…”

Section: Pen-2-dependent Stabilization Of Ps Ntf/ctf Heterodimersupporting

confidence: 78%

“…4). The anti-NCT antibody coimmunoprecipitated APH-1aL with immature NCT in the CHAPSO-solubilized membrane fractions from the PEN-2-⌬C-expressing cells, consistent with their independent stable interaction (13,20,24,25). Thus, these data demonstrate that PEN-2-⌬C does not undergo stable ␥-secretase complex formation.…”

Section: Pen-2-dependent Stabilization Of Ps Ntf/ctf Heterodimersupporting

confidence: 59%

“…Subsequent assembly of PEN-2 with this intermediate drives the conversion of the PS holoprotein into the active heterodimer (17). Furthermore, a potential NCT/APH-1 assembly intermediate has been observed recently (24), and NCT has been shown to stably interact with APH-1 in the absence of PS (20,25). Interestingly, ␥-secretase complex assembly is associated with a conformational change of the NCT ectodomain, which adopts a protease-resistant conformation (26).…”

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confidence: 99%

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Requirement of PEN-2 for Stabilization of the Presenilin N-/C-terminal Fragment Heterodimer within the γ-Secretase Complex

Prokop

Shirotani

Edbauer

et al. 2004

Journal of Biological Chemistry

111

128

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␥-Secretase is a protease complex composed of presenilin (PS), nicastrin (NCT), APH-1, and PEN-2, which catalyzes intramembrane cleavage of several type I transmembrane proteins including the Alzheimer's disease-associated ␤-amyloid precursor protein. We generated stable RNA interference-mediated PEN-2 knockdown cells to probe mutant PEN-2 variants for functional activity. Knockdown of PEN-2 was associated with impaired NCT maturation and deficient PS1 endoproteolysis, which was efficiently rescued by wild type or N-terminally tagged PEN-2 but not by C-terminally tagged PEN-2 or by the C-terminally truncated PEN-2-⌬C mutant. Although the latter mutants rescued the PS1 holoprotein accumulation associated with the PEN-2 knockdown, they failed to restore normal levels of the PS1 N-and C-terminal fragments and to maturate NCT. PEN-2-⌬C was highly unstable and rapidly turned over by proteasomal degradation consistent with its failure to become stably incorporated into the ␥-secretase complex. In addition, expression of PEN-2-⌬C caused a selective instability of the PS1 N-/C-terminal fragment heterodimer that underwent proteasomal degradation, whereas NCT and APH-1 were stable. Interestingly, when we knocked down PEN-2 in the background of the endoproteolysis-deficient PS1 ⌬exon9 mutant, immature NCT still accumulated, demonstrating that PEN-2 is also required for ␥-secretase complex maturation when PS endoproteolysis cannot occur. Taken together, our data suggest that PEN-2 is required for the stabilization of the PS fragment heterodimer within the ␥-secretase complex following PS endoproteolysis. This function critically depends on the PEN-2 C terminus. Moreover, our data show that PEN-2 is generally required for ␥-secretase complex maturation independent of its activity in PS1 endoproteolysis.The Alzheimer's disease (AD) 1 -associated ␥-secretase is a high molecular weight complex with an aspartyl protease activity that catalyzes the second of two subsequent proteolytic cleavages of the ␤-amyloid precursor protein (APP) implicated in AD (1). This unusual, intramembranous cleavage liberates the neurotoxic amyloid-␤ peptide from the membrane. Amyloid-␤ peptide aggregates and is deposited in the brain of AD patients in amyloid plaques, an invariant pathological hallmark of AD (2). The ␥-secretase complex is composed of either of the two presenilins (PS), PS1 and PS2, polytopic membrane proteins that are endoproteolytically cleaved into stable heterodimers consisting of an N-and C-terminal fragment (NTF and CTF) (3), the type I transmembrane glycoprotein nicastrin (NCT) (4, 5), and the polytopic membrane proteins PEN-2 (6), APH-1a, and/or APH-1b (6, 7). Expression of the ␥-secretase complex components is coordinately regulated. RNA interference (RNAi)-mediated knockdown studies in cultured Drosophila and mammalian cells as well as studies with cells derived from PS1, PS1/2, or NCT knockout mice have shown that ␥-secretase complex formation is coordinately regulated. Downregulation or genetic ablation of a given compone...

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Section: Resultssupporting

confidence: 75%

Section: Pen-2-dependent Stabilization Of Ps Ntf/ctf Heterodimersupporting

confidence: 78%

Section: Pen-2-dependent Stabilization Of Ps Ntf/ctf Heterodimersupporting

confidence: 59%

mentioning

confidence: 99%

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Requirement of PEN-2 for Stabilization of the Presenilin N-/C-terminal Fragment Heterodimer within the γ-Secretase Complex

Prokop

Shirotani

Edbauer

et al. 2004

Journal of Biological Chemistry

111

128

View full text Add to dashboard Cite

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“…Evidence for selfassociation of APH-1a with itself and with APH-1b was also reported previously [16]. Morais et al demonstrated that NCT and APH-1 were able to interact in vitro in the absence of PS [44]. Our results suggest that all four putative complex components could be detected in the PS complex for embryonic mouse brain after BN/PAGE, and that APH-1 association may be diminished by carbonate wash.…”

Section: Second Dimension Denaturing Electrophoretic Analysis Of Semisupporting

confidence: 69%

Characterization of presenilin complexes from mouse and human brain using Blue Native gel electrophoresis reveals high expression in embryonic brain and minimal change in complex mobility with pathogenic presenilin mutations

Culvenor

Ilaya

Ryan

et al. 2003

European Journal of Biochemistry

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The presenilin proteins are required for intramembrane cleavage of a subset of type 1 membrane proteins including the Alzheimer's disease amyloid precursor protein. Previous studies indicate presenilin proteins form enzymatically active high molecular mass complexes consisting of heterodimers of N‐ and C‐terminal fragments in association with nicastrin, presenilin enhancer‐2 and anterior pharynx defective‐1 proteins. Using Blue Native gel electrophoresis (BN/PAGE) we have studied endogenous presenilin 1 complex mass, stability and association with nicastrin, presenilin enhancer‐2 and anterior pharynx defective‐1. Solubilization of mouse or human brain membranes with dodecyl‐d‐maltoside produced a 360‐kDa species reactive with antibodies to presenilin 1. Presenilin 1 complex levels were high in embryonic brain. Complex integrity was sensitive to Triton X‐100 and SDS, but stable to reducing agent. Addition of 5 m urea caused complex dissolution and nicastrin to migrate as a subcomplex. Nicastrin and presenilin enhancer‐2 were detected in the presenilin 1 complex following BN/PAGE, electroelution and second‐dimension analysis. Anterior pharynx defective‐1 was detected as an 18‐kDa form and 9‐kDa C‐terminal fragment by standard SDS/PAGE of mouse tissues, and as a predominant 36‐kDa band after presenilin 1 complex second‐dimension analysis. Membranes from brain cortex of Alzheimer's disease patients, or from cases with presenilin 1 missense mutations, indicated no change in presenilin 1 complex mobility. Higher molecular mass presenilin 1‐reactive species were detected in brain containing presenilin 1 exon 9 deletion mutation. This abnormality was confirmed using cells transfected with the same presenilin deletion mutation.

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Molecular Models of the Interface between Anterior Pharynx‐Defective Protein 1 (APH‐1) and Presenilin Involving GxxxG Motifs

et al. 2008

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Gamma-secretase is an integral membrane protease, which is a complex of four membrane proteins. Improper functioning of gamma-secretase was found to be critical in the pathogenesis of Alzheimer's disease. Despite numerous efforts, the structure of the protease as well as its proteolytic mechanism remains poorly understood. In this work we constructed a model of interactions between two proteins forming gamma-secretase: APH-1 and presenilin. This interface is based on a highly conserved GxxxGxxxG motif in the APH-1 protein. It can form a tight contact with a small-residue AxxxAxxxG motif in presenilin. Here, four binding modes based on similar structures involving GxxxG motifs in glycophorin and aquaporin were proposed and verified. The resulting best model employs antiparallel orientations of interacting helices and is in agreement with the currently accepted topology of both proteins. This model can be used for further structural characterization of gamma-secretase and its components.

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The Transmembrane Domain Region of Nicastrin Mediates Direct Interactions with APH-1 and the γ-Secretase Complex

Cited by 69 publications

References 46 publications

Requirement of PEN-2 for Stabilization of the Presenilin N-/C-terminal Fragment Heterodimer within the γ-Secretase Complex

Requirement of PEN-2 for Stabilization of the Presenilin N-/C-terminal Fragment Heterodimer within the γ-Secretase Complex

Characterization of presenilin complexes from mouse and human brain using Blue Native gel electrophoresis reveals high expression in embryonic brain and minimal change in complex mobility with pathogenic presenilin mutations

Molecular Models of the Interface between Anterior Pharynx‐Defective Protein 1 (APH‐1) and Presenilin Involving GxxxG Motifs

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