Your search keyword '"Christian Haass"' showing total 36 results

1. Proteolytic Processing of Neuregulin 1 Type III by Three Intramembrane-cleaving Proteases

Author

Daniel Fleck, Camilla Giudici, Matthias Voss, Michael Willem, Dieter Edbauer, Elisabeth Kremmer, Moritz J. Rossner, Martina Haug-Kröper, Akio Fukumori, Christian Haass, Harald Steiner, Ben Brankatschk, Benjamin M. Schwenk, Regina Fluhrer, and Heike Hampel

Subjects

0301 basic medicine, metabolism [Peptide Hydrolases], Biochemistry, Substrate Specificity, metabolism [Neuregulin-1], Amyloid precursor protein, Aspartic Acid Endopeptidases, genetics [Schizophrenia], Peptide sequence, metabolism [C-Peptide], Neurons, C-Peptide, biology, medicine.diagnostic_test, Molecular Bases of Disease, metabolism [Aspartic Acid Endopeptidases], Adam, Alzheimer Disease, Amyloid-beta (ab), Beta-secretase 1 (bace1), Gamma-secretase, Neurodegeneration, Transmembrane domain, metabolism [Neurons], ddc:540, genetics [Polymorphism, Single Nucleotide], Signal peptide, Proteases, Neuregulin-1, Proteolysis, Molecular Sequence Data, chemistry [Peptides], genetics [Mutation], Polymorphism, Single Nucleotide, Regulated Intramembrane Proteolysis, genetics [Amino Acid Substitution], 03 medical and health sciences, mental disorders, medicine, Animals, Humans, ddc:610, Amino Acid Sequence, Molecular Biology, enzymology [Cell Membrane], Cell Membrane, Cell Biology, Sheddase, Protein Structure, Tertiary, Rats, HEK293 Cells, 030104 developmental biology, Amino Acid Substitution, genetics [Aspartic Acid Endopeptidases], Mutation, Schizophrenia, biology.protein, Peptides, Peptide Hydrolases

Abstract

Numerous membrane-bound proteins undergo regulated intramembrane proteolysis. Regulated intramembrane proteolysis is initiated by shedding, and the remaining stubs are further processed by intramembrane-cleaving proteases (I-CLiPs). Neuregulin 1 type III (NRG1 type III) is a major physiological substrate of β-secretase (β-site amyloid precursor protein-cleaving enzyme 1 (BACE1)). BACE1-mediated cleavage is required to allow signaling of NRG1 type III. Because of the hairpin nature of NRG1 type III, two membrane-bound stubs with a type 1 and a type 2 orientation are generated by proteolytic processing. We demonstrate that these stubs are substrates for three I-CLiPs. The type 1-oriented stub is further cleaved by γ-secretase at an ϵ-like site five amino acids N-terminal to the C-terminal membrane anchor and at a γ-like site in the middle of the transmembrane domain. The ϵ-cleavage site is only one amino acid N-terminal to a Val/Leu substitution associated with schizophrenia. The mutation reduces generation of the NRG1 type III β-peptide as well as reverses signaling. Moreover, it affects the cleavage precision of γ-secretase at the γ-site similar to certain Alzheimer disease-associated mutations within the amyloid precursor protein. The type 2-oriented membrane-retained stub of NRG1 type III is further processed by signal peptide peptidase-like proteases SPPL2a and SPPL2b. Expression of catalytically inactive aspartate mutations as well as treatment with 2,2'-(2-oxo-1,3-propanediyl)bis[(phenylmethoxy)carbonyl]-l-leucyl-l-leucinamide ketone inhibits formation of N-terminal intracellular domains and the corresponding secreted C-peptide. Thus, NRG1 type III is the first protein substrate that is not only cleaved by multiple sheddases but is also processed by three different I-CLiPs.

Published

2016

2. Progranulin Transcripts with Short and Long 5′ Untranslated Regions (UTRs) Are Differentially Expressed via Posttranscriptional and Translational Repression

Author

Christian Haass, Anja Capell, and Katrin Fellerer

Subjects

Untranslated region, metabolism [Intercellular Signaling Peptides and Proteins], Five prime untranslated region, Biochemistry, genetics [Peptide Chain Termination, Translational], Progranulins, Neurobiology, Protein Isoforms, 3' Untranslated Regions, Genetics, genetics [Intercellular Signaling Peptides and Proteins], Translation (biology), respiratory system, DNA-Binding Proteins, genetics [Amyotrophic Lateral Sclerosis], ddc:540, genetics [3' Untranslated Regions], Intercellular Signaling Peptides and Proteins, genetics [Frontotemporal Lobar Degeneration], metabolism [DNA-Binding Proteins], genetics [Protein Isoforms], Translational efficiency, genetics [5' Untranslated Regions], genetics [DNA-Binding Proteins], Biology, behavioral disciplines and activities, genetics [RNA, Messenger], Open Reading Frames, mental disorders, Upstream open reading frame, Humans, RNA, Messenger, pathology [Amyotrophic Lateral Sclerosis], Molecular Biology, Psychological repression, pathology [Frontotemporal Lobar Degeneration], Three prime untranslated region, metabolism [Amyotrophic Lateral Sclerosis], Amyotrophic Lateral Sclerosis, Cell Biology, Peptide Chain Termination, Translational, metabolism [Frontotemporal Lobar Degeneration], nervous system diseases, Open reading frame, HEK293 Cells, nervous system, Gene Expression Regulation, Mutation, GRN protein, human, Frontotemporal Lobar Degeneration, 5' Untranslated Regions

Abstract

Frontotemporal lobar degeneration is associated with cytoplasmic or nuclear deposition of the TAR DNA-binding protein 43 (TDP-43). Haploinsufficiency of progranulin (GRN) is a major genetic risk factor for frontotemporal lobar degeneration associated with TDP-43 deposition. Therefore, understanding the mechanisms that control cellular expression of GRN is required not only to understand disease etiology but also for the development of potential therapeutic strategies. We identified different GRN transcripts with short (38-93 nucleotides) or long (219 nucleotides) 5' UTRs and demonstrate a cellular mechanism that represses translation of GRN mRNAs with long 5' UTRs. The long 5' UTR of GRN mRNA contains an upstream open reading frame (uORF) that is absent in all shorter transcripts. Because such UTRs can be involved in translational control as well as in mRNA stability, we compared the expression of GRN in cells expressing cDNAs with and without 5' UTRs. This revealed a selective repression of GRN translation and a reduction of mRNA levels by the 219-nucleotide-long 5' UTR. The specific ability of this GRN 5' UTR to repress protein expression was further confirmed by its transfer to an independent reporter. Deletion analysis identified a short stretch between nucleotides 76 and 125 containing two start codons within one uORF that is required and sufficient for repression of protein expression. Mutagenesis of the two AUG codons within the uORF is sufficient to reduce translational repression. Therefore initiating ribosomes at the AUGs of the uORF fail to efficiently initiate translation at the start codon of GRN. In parallel the 5' UTR also affects mRNA stability; thus two independent mechanisms determine GRN expression via mRNA stability and translational efficiency.

Published

2014

3. Loss of Parkin or PINK1 Function Increases Drp1-dependent Mitochondrial Fragmentation

Author

Karina Kloos, Christian Haass, Frank Vogel, Kerstin Lämmermann, Andreas S. Reichert, Lena Bouman, Julia S. Schlehe, Bettina Brunner, Wolfgang Wurst, Annerose Kurz-Drexler, A. Kathrin Lutz, Daniela Vogt-Weisenhorn, Mareike E. Fett, Nicole Exner, Konstanze F. Winklhofer, and Jörg Tatzelt

Subjects

OPA1 protein, Drosophila, MFN2, parkin protein, Apoptosis, genetics [RNA, Small Interfering], park protein, Drosophila, Mitochondrion, Biochemistry, Parkin, PINK1 protein, Drosophila, Mice, Adenosine Triphosphate, genetics [Drosophila Proteins], Drosophila Proteins, DRP1 protein, Drosophila, RNA, Small Interfering, Cells, Cultured, genetics [Ubiquitin-Protein Ligases], Gene knockdown, Reverse Transcriptase Polymerase Chain Reaction, genetics [Protein Kinases], physiology [Protein Serine-Threonine Kinases], Protein-Serine-Threonine Kinases, Phenotype, Mitochondria, genetics [Membrane Proteins], Drosophila melanogaster, mitochondrial fusion, ddc:540, physiology [Cytoskeletal Proteins], RNA Interference, Mitochondrial fission, PTEN-induced putative kinase, genetics [GTP-Binding Proteins], Ubiquitin-Protein Ligases, physiology [Protein Kinases], genetics [Protein Serine-Threonine Kinases], PINK1, Protein Serine-Threonine Kinases, Biology, genetics [Protein-Serine-Threonine Kinases], Cell Line, Molecular Basis of Cell and Developmental Biology, GTP-Binding Proteins, Animals, Molecular Biology, genetics [Cytoskeletal Proteins], physiology [Protein-Serine-Threonine Kinases], physiology [Membrane Proteins], Membrane Proteins, Cell Biology, physiology [Drosophila Proteins], physiology [RNA, Small Interfering], oxidative stress, neurodegenerative diseases, cell-death, dysfunction, drosophila, fission, morphology, protein, phosphorylation, pathology, metabolism [Mitochondria], Molecular biology, nervous system diseases, Mice, Inbred C57BL, Cytoskeletal Proteins, physiology [GTP-Binding Proteins], metabolism [Adenosine Triphosphate], physiology [Ubiquitin-Protein Ligases], Marf protein, Drosophila, genetics [Mitochondria], Protein Kinases

Abstract

Loss-of-function mutations in the parkin gene (PARK2) and PINK1 gene (PARK6) are associated with autosomal recessive parkinsonism. PINK1 deficiency was recently linked to mitochondrial pathology in human cells and Drosophila melanogaster, which can be rescued by parkin, suggesting that both genes play a role in maintaining mitochondrial integrity. Here we demonstrate that an acute down-regulation of parkin in human SH-SY5Y cells severely affects mitochondrial morphology and function, a phenotype comparable with that induced by PINK1 deficiency. Alterations in both mitochondrial morphology and ATP production caused by either parkin or PINK1 loss of function could be rescued by the mitochondrial fusion proteins Mfn2 and OPA1 or by a dominant negative mutant of the fission protein Drp1. Both parkin and PINK1 were able to suppress mitochondrial fragmentation induced by Drp1. Moreover, in Drp1- deficient cells the parkin/PINK1 knockdown phenotype did not occur, indicating that mitochondrial alterations observed in parkin- or PINK1-deficient cells are associated with an increase in mitochondrial fission. Notably, mitochondrial fragmentation is an early phenomenon upon PINK1/parkin silencing that also occurs in primary mouse neurons and Drosophila S2 cells. We propose that the discrepant findings in adult flies can be explained by the time of phenotype analysis and suggest that in mammals different strategies may have evolved to cope with dysfunctional mitochondria.

Published

2009

4. Intramembrane Proteolysis by Signal Peptide Peptidases: A Comparative Discussion of GXGD-type Aspartyl Proteases

Author

Harald Steiner, Christian Haass, and Regina Fluhrer

Subjects

Signal peptide, Proteases, Amino Acid Motifs, Molecular Sequence Data, Biology, Biochemistry, Deubiquitinating enzyme, Cell membrane, parasitic diseases, Retroviral aspartyl protease, medicine, Animals, Aspartic Acid Endopeptidases, Humans, ddc:610, Amino Acid Sequence, Molecular Biology, Peptide sequence, chemistry [Aspartic Acid Endopeptidases], enzymology [Cell Membrane], Cell Membrane, Minireviews, Cell Biology, metabolism [Aspartic Acid Endopeptidases], medicine.anatomical_structure, Membrane protein, ddc:540, signal peptide peptidase, biology.protein, Protein Processing, Post-Translational, Signal peptide peptidase

Abstract

Intramembrane-cleaving proteases are required for reverse signaling and membrane protein degradation. A major class of these proteases is represented by the GXGD-type aspartyl proteases. GXGD describes a novel signature sequence that distinguishes these proteases from conventional aspartyl proteases. Members of the family of the GXGD-type aspartyl proteases are the Alzheimer disease-related γ-secretase, the signal peptide peptidases and their homologs, and the bacterial type IV prepilin peptidases. We will describe the major biochemical and functional properties of the signal peptide peptidases and their relatives. We then compare these properties with those of γ-secretase and discuss common mechanisms but also point out a number of substantial differences.

Published

2009

5. Intramembrane Proteolysis of GXGD-type Aspartyl Proteases Is Slowed by a Familial Alzheimer Disease-like Mutation

Author

Harald Steiner, Elisabeth Kremmer, Regina Fluhrer, David B. Teplow, Edith Winkler, Gudula Grammer, Lucas Martin, Margaret M. Condron, Bärbel Klier, Christian Haass, Akio Fukumori, and Martina Haug-Kröper

Subjects

Signal peptide, Protein Structure, Biochemistry & Molecular Biology, Proteases, Amino Acid Motifs, Molecular Sequence Data, Mutant, Biology, Medical and Health Sciences, Models, Biological, Biochemistry, Catalysis, Presenilin, Cell Line, Models, Alzheimer Disease, mental disorders, Aspartic Acid Endopeptidases, Humans, Missense mutation, Amino Acid Sequence, ddc:610, Molecular Biology, Peptide sequence, Amyloid beta-Peptides, Enzyme Catalysis and Regulation, Tumor Necrosis Factor-alpha, Temperature, Cell Biology, Biological Sciences, Biological, Protein Structure, Tertiary, Chemical Sciences, Mutation, Peptides, Signal peptide peptidase, Tertiary, Intracellular

Abstract

More than 150 familial Alzheimer disease (FAD)-associated missense mutations in presenilins (PS1 and PS2), the catalytic subunit of the γ-secretase complex, cause aberrant amyloid β-peptide (Aβ) production, by increasing the relative production of the highly amyloidogenic 42-amino acid variant. The molecular mechanism behind this pathological activity is unclear, and different possibilities ranging from a gain of function to a loss of function have been discussed. γ-Secretase, signal peptide peptidase (SPP) and SPP-like proteases (SPPLs) belong to the same family of GXGD-type intramembrane cleaving aspartyl proteases and share several functional similarities. We have introduced the FAD-associated PS1 G384A mutation, which occurs within the highly conserved GXGD motif of PS1 right next to the catalytically critical aspartate residue, into the corresponding GXGD motif of the signal peptide peptidase-like 2b (SPPL2b). Compared with wild-type SPPL2b, mutant SPPL2b slowed intramembrane proteolysis of tumor necrosis factor α and caused a relative increase of longer intracellular cleavage products. Because the N termini of the secreted counterparts remain unchanged, the mutation selectively affects the liberation of the intracellular processing products. In vitro experiments demonstrate that the apparent accumulation of longer intracellular cleavage products is the result of slowed sequential intramembrane cleavage. The longer cleavage products are still converted to shorter peptides, however only after prolonged incubation time. This suggests that FAD-associated PS mutation may also result in reduced intramembrane cleavage of β-amyloid precursor protein (βAPP). Indeed, in vitro experiments demonstrate slowed intramembrane proteolysis by γ-secretase containing PS1 with the G384A mutation. As compared with wild-type PS1, the mutation selectively slowed Aβ40 production, whereas Aβ42 generation remained unaffected. Thus, the PS1 G384A mutation causes a selective loss of function by slowing the processing pathway leading to the benign Aβ40. © 2008 by The American Society for Biochemistry and Molecular Biology, Inc.

Published

2008

6. Generation of Aβ38 and Aβ42 Is Independently and Differentially Affected by Familial Alzheimer Disease-associated Presenilin Mutations and γ-Secretase Modulation

Author

Richard M. Page, Alexander Flohr, Karlheinz Baumann, Helmut Jacobsen, Blanca I. Pérez-Revuelta, Laurence Ozmen, Christian Haass, Harald Steiner, Masanori Tomioka, Thomas Luebbers, and Akio Fukumori

Subjects

Genetically modified mouse, Amyloid, Mutant, Mice, Transgenic, Kidney, Transfection, medicine.disease_cause, Biochemistry, Presenilin, Cell Line, Mice, Alzheimer Disease, Presenilin-2, mental disorders, Presenilin-1, medicine, Animals, Humans, Molecular Biology, Mutation, Amyloid beta-Peptides, biology, Wild type, Brain, Cell Biology, medicine.disease, Molecular biology, Peptide Fragments, nervous system diseases, biology.protein, Amyloid Precursor Protein Secretases, Alzheimer's disease, Amyloid precursor protein secretase

Abstract

Alzheimer disease amyloid beta-peptide (Abeta) is generated via proteolytic processing of the beta-amyloid precursor protein by beta- and gamma-secretase. Gamma-secretase can be blocked by selective inhibitors but can also be modulated by a subset of non-steroidal anti-inflammatory drugs, including sulindac sulfide. These drugs selectively reduce the generation of the aggregation-prone 42-amino acid Abeta(42) and concomitantly increase the levels of the rather benign Abeta(38). Here we show that Abeta(42) and Abeta(38) generation occur independently from each other. The amount of Abeta(42) produced by cells expressing 10 different familial Alzheimer disease (FAD)-associated mutations in presenilin (PS) 1, the catalytic subunit of gamma-secretase, appeared to correlate with the respective age of onset in patients. However, Abeta(38) levels did not show a negative correlation with the age of onset. Modulation of gamma-secretase activity by sulindac sulfide reduced Abeta(42) in the case of wild type PS1 and two FAD-associated PS1 mutations (M146L and A285V). The remaining eight PS1 FAD mutants showed either no reduction of Abeta(42) or only rather subtle effects. Strikingly, even the mutations that showed no effect on Abeta(42) levels allowed a robust increase of Abeta(38) upon treatment with sulindac sulfide. Similar observations were made for fenofibrate, a compound known to increase Abeta(42) and to decrease Abeta(38). For mutants that predominantly produce Abeta(42), the ability of fenofibrate to further increase Abeta(42) levels became diminished, whereas Abeta(38) levels were altered to varying extents for all mutants analyzed. Thus, we conclude that Abeta(38) and Abeta(42) production do not depend on each other. Using an independent non-steroidal anti-inflammatory drug derivative, we obtained similar results for PS1 as well as for PS2. These in vitro results were confirmed by in vivo experiments in transgenic mice expressing the PS2 N141I FAD mutant. Our findings therefore have strong implications on the selection of transgenic mouse models used for screening of the Abeta(42)-lowering capacity of gamma-secretase modulators. Furthermore, human patients with certain PS mutations may not respond to gamma-secretase modulators.

Published

2008

7. Regulated Intramembrane Proteolysis of the Interleukin-1 Receptor II by α-, β-, and γ-Secretase

Author

Bart De Strooper, Peer-Hendrik Kuhn, Christian Haass, Stefan F. Lichtenthaler, Axel Imhof, and Els Marjaux

Subjects

Proteases, biology, Cell Biology, Biochemistry, Regulated Intramembrane Proteolysis, Ectodomain, Membrane protein, Alpha secretase, biology.protein, Amyloid precursor protein, Molecular Biology, Amyloid precursor protein secretase, Gamma secretase

Abstract

Ectodomain shedding and intramembrane proteolysis of the amyloid precursor protein (APP) by alpha-, beta- and gamma-secretase are involved in the pathogenesis of Alzheimer disease (AD). Increased proteolytic processing and secretion of another membrane protein, the interleukin-1 receptor II (IL-1R2), have also been linked to the pathogenesis of AD. IL-1R2 is a decoy receptor that may limit detrimental effects of IL-1 in the brain. At present, the proteolytic processing of IL-1R2 remains little understood. Here we show that IL-1R2 can be proteolytically processed in a manner similar to APP. IL-1R2 expressed in human embryonic kidney 293 cells first undergoes ectodomain shedding in an alpha-secretase-like manner, resulting in secretion of the IL-1R2 ectodomain and the generation of an IL-1R2 C-terminal fragment. This fragment undergoes further intramembrane proteolysis by gamma-secretase, leading to the generation of the soluble intracellular domain of IL-1R2. Intramembrane cleavage of IL-1R2 was abolished by a highly specific inhibitor of gamma-secretase and was absent in mouse embryonic fibroblasts deficient in gamma-secretase activity. Surprisingly, the beta-secretase BACE1 and its homolog BACE2 increased IL-1R2 secretion resulting in C-terminal fragments nearly identical to the ones generated by the alpha-secretase-like cleavage. This suggests that both proteases may act as alternative alpha-secretase-like proteases. Importantly, BACE1 and BACE2 did not cleave several other membrane proteins, demonstrating that both proteases do not contribute to general membrane protein turnover but only cleave specific proteins. This study reveals a similar proteolytic processing of IL-1R2 and APP and may provide an explanation for the increased IL-1R2 secretion observed in AD.

Published

2007

8. SorLA Signaling by Regulated Intramembrane Proteolysis

Author

Harald Steiner, Christian Haass, Nicole M. Seibel, Birgit Henkel, Wolfgang Hampe, and Christopher Bohm

Subjects

Cytoplasm, Green Fluorescent Proteins, Molecular Sequence Data, Nuclear Localization Signals, Notch signaling pathway, Protein Sorting Signals, Biochemistry, Regulated Intramembrane Proteolysis, Presenilin, Endopeptidases, Presenilin-1, Aspartic Acid Endopeptidases, Humans, Amino Acid Sequence, Molecular Biology, LDL-Receptor Related Proteins, Cell Nucleus, biology, Activator (genetics), Membrane Proteins, Membrane Transport Proteins, Cell Biology, Cell biology, Transmembrane domain, Gene Expression Regulation, Receptors, LDL, Membrane protein, biology.protein, Amyloid Precursor Protein Secretases, Signal transduction, Peptides, Amyloid precursor protein secretase, Signal Transduction

Abstract

The single-transmembrane receptor SorLA/LR11 contains binding domains typical for lipoprotein receptors and a VPS10 domain, which binds the neuropeptide head-activator. This undecapeptide enhances proliferation of neuronal precursor cells in a SorLA-dependent manner. Using specific inhibitors we found previously that head activator activates shedding of SorLA by the metalloprotease TACE close to the transmembrane domain releasing the large extra-cellular part of the receptor. Here we show that the remaining COOH-terminal membrane fragment of SorLA is processed by gamma-secretase. Inhibition of gamma-secretase by specific inhibitors or overexpression of dominant negative presenilin mutants and knock out of the presenilin genes led to accumulation of the SorLA membrane fragment and also of full-length SorLA in the membrane. In an in vitro assay we observed the gamma-secretase-dependent release of the two soluble cleavage products, the SorLA cytoplasmic domain and the SorLA beta-peptide. These processing steps are reminiscent of a novel signaling pathway that has been described for the notch receptor. Here, the notch cytoplasmic domain is released into the cytoplasm by the gamma-secretase and migrates to the nucleus where it acts as a transcriptional regulator. In parallel we found that a fusion protein of the released cytoplasmic tail of SorLA with EGFP located to the nucleus only if the nuclear localization signal of SorLA was intact. In a reporter gene assay the cytoplasmic domain of SorLA acted as a transcriptional activator indicating that SorLA might directly regulate transcription after activation by gamma-secretase.

Published

2006

9. Amyloid Precursor-like Protein 1 Influences Endocytosis and Proteolytic Processing of the Amyloid Precursor Protein

Author

Christian Haass, Claus U. Pietrzik, Susanne Schöbel, Anna Trautwein, Stefan F. Lichtenthaler, Sebastian Jäger, and Stephanie Neumann

Subjects

Cytoplasm, Time Factors, Recombinant Fusion Proteins, Amino Acid Motifs, Blotting, Western, Genetic Vectors, Endocytic cycle, CHO Cells, Transfection, Endocytosis, Biochemistry, Cell Line, Amyloid beta-Protein Precursor, Genes, Reporter, Cricetinae, Chlorocebus aethiops, Endopeptidases, mental disorders, Amyloid precursor protein, Animals, Aspartic Acid Endopeptidases, Humans, Immunoprecipitation, APLP1, Molecular Biology, Models, Genetic, biology, Chemistry, HEK 293 cells, P3 peptide, Cell Biology, Protein Structure, Tertiary, Microscopy, Fluorescence, Alpha secretase, Ectodomain, COS Cells, biology.protein, Amyloid Precursor Protein Secretases, Peptides, Gene Deletion, Plasmids

Abstract

Ectodomain shedding of the amyloid precursor protein (APP) is a key regulatory step in the generation of the Alzheimer disease amyloid beta peptide (Abeta). The molecular mechanisms underlying the control of APP shedding remain little understood but are in part dependent on the low density lipoprotein receptor-related protein (LRP), which is involved in APP endocytosis. Here, we show that the APP homolog APLP1 (amyloid precursor-like protein 1) influences APP shedding. In human embryonic kidney 293 cells expression of APLP1 strongly activated APP shedding by alpha-secretase and slightly reduced beta-secretase cleavage. As revealed by domain deletion analysis, the increase in APP shedding required the NPTY amino acid motif within the cytoplasmic domain of APLP1. This motif is conserved in APP and is essential for the endocytosis of APP and APLP1. Unrelated membrane proteins containing similar endocytic motifs did not affect APP shedding, showing that the increase in APP shedding was specific to APLP1. In LRP-deficient cells APLP1 no longer induced APP shedding, suggesting that in wild-type cells APLP1 interferes with the LRP-dependent endocytosis of APP and there by increases APP alpha-cleavage. In fact, an antibody uptake assay revealed that expression of APLP1 reduced the rate of APP endocytosis. In summary, our study provides a novel mechanism for APP shedding, in which APLP1 affects the endocytosis of APP and makes more APP available for alpha-secretase cleavage.

Published

2006

10. Secretion of the Notch-1 Aβ-like Peptide during Notch Signaling

Author

Masatoshi Takeda, Jingwei Jiang, Naohiro Itoh, Harald Steiner, Christian Haass, Akio Fukumori, Ryo Kimura, Masayasu Okochi, and Shinji Tagami

Subjects

DNA, Complementary, Proteolysis, Immunoblotting, Molecular Sequence Data, Notch signaling pathway, Biology, Ligands, Models, Biological, Biochemistry, Regulated Intramembrane Proteolysis, Presenilin, Cell Line, Amyloid beta-Protein Precursor, Mice, Cytosol, Genes, Reporter, mental disorders, Presenilin-1, medicine, Animals, Humans, Immunoprecipitation, Amino Acid Sequence, Receptor, Notch1, Molecular Biology, Notch 1, Peptide sequence, medicine.diagnostic_test, Cell Membrane, Membrane Proteins, DNA, Cell Biology, Protein Structure, Tertiary, Cell biology, Transmembrane domain, Mutation, Signal transduction, Peptides, HeLa Cells, Protein Binding, Signal Transduction

Abstract

The canonical pathway of Notch signaling is mediated by regulated intramembrane proteolysis (RIP). In the pathway, ligand binding results in sequential proteolysis of the Notch receptor, and presenilin (PS)-dependent intramembrane proteolysis at the interface between the membrane and cytosol liberates the Notch-1 intracellular domain (NICD), a transcription modifier. Because the degradation of the Notch-1 transmembrane domain is thought to require an additional cleavage near the middle of the transmembrane domain, extracellular small peptides (Notch-1 Abeta-like peptide (Nbeta)) should be produced. Here we showed that Nbeta species are indeed secreted during the process of Notch signaling. We identified mainly two distinct molecular species of novel Nbeta, Nbeta21 and C-terminally elongated Nbeta25, which were produced in an approximately 5:1 ratio. This process is reminiscent of the production of Alzheimer disease-associated Abeta. PS pathogenic mutants increased the production of the longer species of Abeta (Abeta42) from beta-amyloid protein precursor. We revealed that several Alzheimer disease mutants also cause a parallel increase in the secretion of the longer form of Nbeta. Strikingly, chemicals that modify the Abeta42 level caused parallel changes in the Nbeta25 level. These results demonstrated that the characteristics of C-terminal elongation of Nbeta and Abeta are almost identical. In addition, because many other type 1 membrane-bound receptors release intracellular domains by PS-dependent intramembrane proteolysis, we suspect that the release of Abeta- or Nbeta-like peptides is a common feature of the proteolysis during RIP signaling. We anticipate that this study will open the door to searches for markers of RIP signaling and surrogate markers for Abeta42 production.

Published

2006

11. A Pathogenic PrP Mutation and Doppel Interfere with Polarized Sorting of the Prion Protein

Author

Adriano Aguzzi, Armgard Uelhoff, Christian Haass, Jörg Tatzelt, Konstanze F. Winklhofer, University of Zurich, and Winklhofer, K F

Subjects

1303 Biochemistry, Amyloid, Prions, Recombinant Fusion Proteins, animal diseases, Mutant, 10208 Institute of Neuropathology, 610 Medicine & health, Protein Sorting Signals, Biology, GPI-Linked Proteins, medicine.disease_cause, Biochemistry, Cell Line, Prion Diseases, 1307 Cell Biology, Mice, Dogs, Canine kidney, 1312 Molecular Biology, medicine, Animals, Missense mutation, Prion protein, Molecular Biology, Sequence Deletion, Epithelial polarity, chemistry.chemical_classification, Mutation, Cell Polarity, Cell Biology, Molecular biology, Protein Structure, Tertiary, nervous system diseases, Amino acid, Protein Transport, chemistry, 570 Life sciences, biology, Hydrophobic and Hydrophilic Interactions

Abstract

Several proteins linked to neurodegenerative diseases, such as the beta-amyloid precursor protein, amyloid beta-peptide, beta-secretase, and tau, undergo selective polarized sorting. We investigated polarized sorting of the mammalian prion protein (PrP(C)) and its homologue doppel (Dpl). In contrast to Dpl, which accumulates on the apical surface, PrP(C) is targeted selectively to the basolateral side in Madin-Darby canine kidney cells. An extensive deletion and domain swapping analysis revealed that the internal hydrophobic domain (HD) of PrP (amino acids 113-133) confers basolateral sorting in a dominant manner. PrP mutants lacking the HD are sorted apically, while Dpl chimeras containing the HD of PrP are directed to the basolateral membrane. Furthermore, a pathogenic PrP missense mutation within the HD leads to aberrant apical sorting of PrP as well.

Published

2005

12. γ-Secretase Complex Assembly within the Early Secretory Pathway

Author

Christian Haass, Stefan Prokop, Mark S. Shearman, Harald Steiner, Anja Capell, Dirk Beher, and Christoph Kaether

Subjects

Conformational change, Protein Conformation, Nicastrin, Biology, Endoplasmic Reticulum, Transfection, Cleavage (embryo), Biochemistry, Presenilin, Cell Line, Amyloid beta-Protein Precursor, Endopeptidases, parasitic diseases, Presenilin-1, Aspartic Acid Endopeptidases, Humans, Molecular Biology, Secretory pathway, Amyloid beta-Peptides, Membrane Glycoproteins, Endoplasmic reticulum, Membrane Proteins, RNA, Cell Biology, Peptide Fragments, Cell biology, Biotinylation, biology.protein, Amyloid Precursor Protein Secretases, Peptide Hydrolases

Abstract

gamma-Secretase is an aspartyl protease complex composed of the four core components APH-1, nicastrin (NCT), presenilin (PS), and PEN-2. It catalyzes the final intramembranous cleavage of the beta-secretase-processed beta-amyloid precursor protein to liberate the neurotoxic amyloid beta-peptide. Whereas unassembled complex components appear to be unstable and/or to be retained within the endoplasmic reticulum (ER), the fully assembled complex is known to exert its biological function in late secretory compartments, including the plasma membrane. We thus hypothesized that the gamma-secretase complex undergoes a stepwise assembly within the ER. We demonstrate that gamma-secretase-associated NCT can be actively retained within the ER by the addition of a retention signal. Under these conditions, complex assembly occurred in the absence of maturation of NCT, and ER-retained immature NCT associated with APH-1, PEN-2, and PS fragments. Moreover, a biotinylated transition state gamma-secretase inhibitor allowed the preferential isolation of the fully assembled complex containing immature NCT. Furthermore, we observed a conformational change in immature NCT, which is known to be selectively associated with complete gamma-secretase complex assembly. This was also observed for a small amount of immature endogenous NCT. ER-retained NCT also rescued the biochemical phenotype observed upon RNA interference-mediated NCT knockdown, viz. reduced amyloid beta-peptide production; instability of PS, PEN-2, and APH-1; and accumulation of beta-amyloid precursor protein C-terminal fragments. Finally, we demonstrate that dimeric (NCT/APH-1) and trimeric (NCT/APH-1/PS) intermediates of gamma-secretase complex assembly containing endogenous NCT are retained within the ER and that the incorporation of the fourth and last binding partner (PEN-2) also occurs on immature NCT, suggesting a complete assembly of the gamma-secretase complex within the ER.

Published

2005

13. Human BACE Forms Dimers and Colocalizes with APP

Author

Gerd Multhaup, Andrea Schlicksupp, Markus Strauss, Ariane Schmechel, Rüdiger Pipkorn, Christian Haass, and Thomas A. Bayer

Subjects

medicine.medical_treatment, Mutant, Biochemistry, Catalysis, Chromatography, Affinity, Amyloid beta-Protein Precursor, Neuroblastoma, chemistry.chemical_compound, Cell Line, Tumor, Endopeptidases, medicine, Amyloid precursor protein, Animals, Aspartic Acid Endopeptidases, Humans, Molecular Biology, Brain Chemistry, chemistry.chemical_classification, Protease, biology, Active site, Cell Biology, Enzyme assay, Enzyme Activation, Enzyme, chemistry, Ectodomain, COS Cells, biology.protein, Amyloid Precursor Protein Secretases, Dimerization, Pepstatin

Abstract

Beta-site APP-cleaving enzyme (BACE) is a membrane-bound aspartyl protease with no strict primary preference for cleavage. The molecular mechanisms that link the gamma-secretase multicomponent amyloid precursor protein (APP) processing complex to biochemical properties of BACE generating the N terminus of the amyloid beta-peptide have not, as yet, been identified. We found that in human brain tissue, BACE occurred as a dimer. The overall stability of the BACE homodimer was based on intermolecular interactions that were not affected by high salt, nonionic detergents or reducing conditions. BACE homodimers could only partially be separated even under strong denaturing conditions and revealed dramatic differences in the surface charge distribution compared with the monomer. In contrast, the soluble ectodomain of truncated BACE revealed a seemingly lower avidity to the prototypic aspartate protease inhibitor pepstatin and exclusively occurred in the monomeric form. Immunocytochemical studies colocalized APP and BACE in the plasma membrane of cells expressing endogenous levels of BACE and overexpressing APP. In cells that were cotransfected with APP and a putative active site D289A mutant of BACE, colocalization persisted. Remaining enzyme activity was found to be attributable to the mutant protease. Accordingly, inactivation of the carboxyl-terminal active site motif of BACE without an impairment of overall enzyme activity suggests that the enzyme may act as a dimer. Thus, homodimerization of BACE may help the enzyme to acquire specific mechanisms to associate with its substrates to exert catalytic activity.

Published

2004

14. Co-expression of Nicastrin and Presenilin Rescues a Loss of Function Mutant of APH-1

Author

Dieter Edbauer, Harald Steiner, Christoph Kaether, and Christian Haass

Subjects

Membrane Glycoproteins, biology, HEK 293 cells, Mutant, Nicastrin, Membrane Proteins, Cell Biology, biology.organism_classification, Biochemistry, Presenilin, Cell Line, Transmembrane domain, Endopeptidases, Mutation, Aspartic acid, Presenilin-1, biology.protein, Humans, Amyloid Precursor Protein Secretases, APH-1, Molecular Biology, Alleles, Caenorhabditis elegans, Peptide Hydrolases

Abstract

gamma-Secretase is an intramembrane-cleaving aspartyl protease complex that mediates the final cleavage of beta-amyloid precursor protein to liberate the neurotoxic amyloid-beta peptide implicated in Alzheimer's disease. The four proteins presenilin (PS), nicastrin (NCT), APH-1, and PEN-2 are sufficient to reconstitute gamma-secretase activity in yeast. Although PS seems to contribute the catalytic core of the gamma-secretase complex, no distinct function could be attributed to the other components so far. In Caenorhabditis elegans, mutation of a glycine to an aspartic acid within a conserved GXXXG motif in the fourth transmembrane domain of APH-1 causes a loss of function phenotype. Surprisingly, we now found that the human homologue APH-1a carrying the equivalent mutation G122D is fully active in yeast co-expressing PS1, NCT, and PEN-2. To address this discrepancy, we expressed APH-1a G122D in HEK293 cells. As reported previously, overexpressed APH-1a G122D was not incorporated into the gamma-secretase complex. Separate overexpression of PS1, NCT, or PEN-2 together with APH-1a G122D allowed the formation of heterodimers lacking the other endogenous components. Only the combined overexpression of PS1 and NCT together with APH-1a G122D facilitated the formation of a fully active gamma-secretase complex. Under these conditions, APH-1a G122D supported the production of normal amounts of Abeta. We conclude that cooperative effects may stabilize a trim-eric complex of APH-1a G122D together with PS1 and NCT. Upon successful complex assembly, the GXXXG motif becomes dispensable for gamma-secretase activity.

Published

2004

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

Author

Harald Steiner, Keiro Shirotani, Stefan Prokop, Dieter Edbauer, and Christian Haass

Subjects

genetic structures, Mutant, Nicastrin, Biochemistry, Presenilin, Cell Line, Structure-Activity Relationship, PEN-2, Cricetinae, Endopeptidases, Presenilin-1, Animals, Aspartic Acid Endopeptidases, Humans, Molecular Biology, biology, Hydrolysis, C-terminus, Wild type, Membrane Proteins, Cell Biology, Molecular biology, Peptide Fragments, Transmembrane protein, biology.protein, Amyloid Precursor Protein Secretases, Dimerization, Amyloid precursor protein secretase

Abstract

Gamma-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 beta-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-DeltaC 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-DeltaC was highly unstable and rapidly turned over by proteasomal degradation consistent with its failure to become stably incorporated into the gamma-secretase complex. In addition, expression of PEN-2-DeltaC 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 Deltaexon9 mutant, immature NCT still accumulated, demonstrating that PEN-2 is also required for gamma-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 gamma-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 gamma-secretase complex maturation independent of its activity in PS1 endoproteolysis.

Published

2004

16. α-Synuclein Has a High Affinity for Packing Defects in a Bilayer Membrane

Author

Brigitte Nuscher, Christian Haass, Klaus Beyer, Sabine Odoy, Thomas Mehnert, Frits Kamp, and Philipp J. Kahle

Subjects

Folding (chemistry), Circular dichroism, Crystallography, Membrane, Differential scanning calorimetry, Chemistry, Vesicle, Bilayer, Helix, Cell Biology, Calorimetry, Molecular Biology, Biochemistry

Abstract

A number of neurodegenerative disorders, including Parkinson's disease, dementia with Lewy bodies, and multiple system atrophy, are characterized by the intracellular deposition of fibrillar aggregates that contain a high proportion of α-synuclein (αS). The interaction with the membrane-water interface strongly modulates folding and aggregation of the protein. The present study investigates the lipid binding and the coil-helix transition of αS, using titration calorimetry, differential scanning calorimetry, and circular dichroism spectroscopy. Titration of the protein with small unilamellar vesicles composed of zwitterionic phospholipids below the chain melting temperature of the lipids yielded exceptionally large exothermic heat values. The sigmoidal titration curves were evaluated in terms of a simple model that assumes saturable binding sites at the vesicle surface. The cumulative heat release and the ellipticity were linearly correlated as a result of simultaneous binding and helix folding. There was no heat release and folding of αS in the presence of large unilamellar vesicles, indicating that a small radius of curvature is necessary for the αS-membrane interaction. The heat release and the negative heat capacity of the protein-vesicle interaction could not be attributed to the coil-helix transition of the protein alone. We speculate that binding and helix folding of αS depends on the presence of defect structures in the membrane-water interface, which in turn results in lipid ordering in the highly curved vesicular membranes. This will be discussed with regard to a possible role of the protein for the stabilization of synaptic vesicle membranes.

Published

2004

17. Differential Effects of Parkinson's Disease-associated Mutations on Stability and Folding of DJ-1

Author

Karin Görner, Christian Haass, Klaus Beyer, Ayako Yamamoto, Sabine Odoy, Jörg T. Regula, Brigitte Nuscher, Eve Holtorf, and Philipp J. Kahle

Subjects

Proteasome Endopeptidase Complex, Protein Folding, Time Factors, Leupeptins, Protein Conformation, Protein Deglycase DJ-1, Mutant, Mutagenesis (molecular biology technique), Cysteine Proteinase Inhibitors, Cycloheximide, Biology, medicine.disease_cause, Biochemistry, Mass Spectrometry, Protein Structure, Secondary, Cell Line, chemistry.chemical_compound, Protein structure, Multienzyme Complexes, Escherichia coli, medicine, Humans, Point Mutation, Cysteine, Enzyme Inhibitors, Molecular Biology, Neurons, Oncogene Proteins, Protein Synthesis Inhibitors, Mutation, Reverse Transcriptase Polymerase Chain Reaction, Circular Dichroism, Point mutation, Intracellular Signaling Peptides and Proteins, Temperature, Protein turnover, PARK7, Parkinson Disease, Cell Biology, Molecular biology, Cysteine Endopeptidases, chemistry, Mutagenesis, Site-Directed, Gene Deletion

Abstract

Mutations in the PARK7/DJ-1 gene cause autosomal-recessive Parkinson's disease. In some patients the gene is deleted. The molecular basis of disease in patients with point mutations is less obvious. We have investigated the molecular properties of [L166P]DJ-1 and the novel variant [E64D]DJ-1. When transfected into non-neuronal and neuronal cell lines, steady-state expression levels of [L166P]DJ-1 were dramatically lower than wild-type [WT]DJ-1 and [E64D]DJ-1. Cycloheximide and pulse-chase experiments revealed that the decreased expression levels of [L166P]DJ-1 were because of accelerated protein turnover. Proteasomal degradation was not the major pathway of DJ-1 breakdown because treatment with the proteasome inhibitor MG-132 caused only minimal accumulation of DJ-1, even of the very unstable [L166P]DJ-1 mutant. Because of the structural resemblance of DJ-1 with bacterial cysteine proteases, we considered an autoproteolytic mechanism. However, neither pharmacological inhibition nor site-directed mutagenesis of the putative active site residue Cys-106 stabilized DJ-1. To gain further insight into the structural defects of DJ-1 mutants, human [WT]DJ-1 and both mutants were expressed in Escherichia coli. As in eukaryotic cells, expression levels of [L166P]DJ-1 were dramatically reduced compared with [WT]DJ-1 and [E64D]DJ-1. Circular dichroism spectrometry revealed that the solution structures of [WT]DJ-1 and [E64D]DJ-1 are rich in beta-strand and alpha-helix conformation. Alpha-helices were more susceptible to thermal denaturation than the beta-sheet, and [WT]DJ-1 was more flexible in this regard than [E64D]DJ-1. Thus, structural defects of [E64D]DJ-1 only become apparent upon denaturing conditions, whereas the L166P mutation causes a drastic defect that leads to excessive degradation.

Published

2004

18. The Cell Adhesion Protein P-selectin Glycoprotein Ligand-1 Is a Substrate for the Aspartyl Protease BACE1

Author

Stefan F. Lichtenthaler, Bart De Strooper, Diana Ines Dominguez, Brian Seed, Christian Haass, Paul Saftig, Karina Reiss, and Gil G. Westmeyer

Subjects

Sialyltransferase, Recombinant Fusion Proteins, Molecular Sequence Data, Biology, Cleavage (embryo), Biochemistry, Cell Line, Endopeptidases, mental disorders, Amyloid precursor protein, Aspartic Acid Endopeptidases, Humans, Amino Acid Sequence, Molecular Biology, Peptide sequence, DNA Primers, Membrane Glycoproteins, Base Sequence, integumentary system, Cell Differentiation, Exons, Cell Biology, Alkaline Phosphatase, Molecular biology, Transmembrane protein, Alternative Splicing, Ectodomain, biology.protein, P-selectin glycoprotein ligand-1, Amyloid Precursor Protein Secretases, Amyloid precursor protein secretase

Abstract

The aspartyl protease BACE1 cleaves the amyloid precursor protein and the sialyltransferase ST6Gal I and is important in the pathogenesis of Alzheimer's disease. The normal function of BACE1 and additional physiological substrates have not been identified. Here we show that BACE1 acts on the P-selectin glycoprotein ligand 1 (PSGL-1), which mediates leukocyte adhesion in inflammatory reactions. In human monocytic U937 and human embryonic kidney 293 cells expressing endogenous or transfected BACE1, PSGL-1 was cleaved by BACE1 to generate a soluble ectodomain and a C-terminal transmembrane fragment. No evidence of the cleavage fragment was seen in primary cells derived from mice deficient in BACE1. By using deletion constructs and enzymatic deglycosylation of the C-terminal PSGL-1 fragments, the cleavage site in PSGL-1 was mapped to the juxtamembrane region within the ectodomain. In an in vitro assay BACE1 catalyzed the formation of the PSGL-1 products seen in vivo. The cleavage occurred at a Leu-Ser peptide bond as identified by mass spectrometry using a synthetic peptide. We conclude that PSGL-1 is an additional substrate for BACE1.

Published

2003

19. Nicastrin Interacts with γ-Secretase Complex Components via the N-terminal Part of Its Transmembrane Domain

Author

Sabine Merkl, Christoph Kaether, Christian Haass, Anja Capell, Harald Steiner, Dieter Edbauer, and Keiro Shirotani

Subjects

Cytoplasm, DNA, Complementary, Amyloid, Protein Conformation, Recombinant Fusion Proteins, Blotting, Western, Molecular Sequence Data, Mutant, Nicastrin, Down-Regulation, Heterologous, Bioinformatics, Biochemistry, Cell Line, Endopeptidases, parasitic diseases, Aspartic Acid Endopeptidases, Humans, Amino Acid Sequence, Molecular Biology, Membrane Glycoproteins, Models, Genetic, Sequence Homology, Amino Acid, biology, Cell Biology, Protein Structure, Tertiary, Cell biology, Transmembrane domain, Phenotype, Mutation, biology.protein, Amyloid Precursor Protein Secretases, Amyloid precursor protein secretase, Function (biology), Protein Binding

Abstract

Two secretases are involved in the generation of amyloid beta-peptide, the principal component of amyloid plaques in the brains of Alzheimer's disease patients. While beta-secretase is a classical aspartyl protease, gamma-secretase activity is associated with a high molecular weight complex. One of the complex components, which is critically required for gamma-secretase activity is nicastrin (NCT). Here we investigate the assembly of NCT into the gamma-secretase complex. NCT mutants either lacking the entire cytoplasmic tail, the cytoplasmic tail, and the transmembrane domain (TMD), or containing a set of heterologous TMDs were expressed in cells with strongly reduced levels of endogenous NCT. Maturation of exogenous NCT, gamma-secretase complex formation and proteolytic function was then investigated. This revealed that the cytoplasmic tail of NCT is dispensable for gamma-secretase complex assembly and function. In contrast, the authentic TMD of NCT is critically required for the interaction with gamma-secretase complex components and for formation of an active gamma-secretase complex. Neither soluble NCT lacking any membrane anchor nor NCT containing a heterologous TMD were inserted into the gamma-secretase complex. We identified the N-terminal region of the NCT TMD as a functionally important entity of NCT. These data thus demonstrate that NCT interacts with other gamma-secretase complex components via its TMD.

Published

2003

20. Potential Link between Amyloid β-Protein 42 and C-terminal Fragment γ 49–99 of β-Amyloid Precursor Protein

Author

Hiroko Maruyama, Naoshi Dohmae, Hiroaki Misonou, Shoichi Ishiura, Edward H. Koo, Toru Sato, Yasuo Ihara, Koji Takio, Yue Qi, Christian Haass, Rie Mitsumori, Maho Morishima-Kawashima, and Nobuto Kakuda

Subjects

Amyloid beta, Mutant, CHO Cells, Plasma protein binding, Transfection, Cleavage (embryo), Biochemistry, Presenilin, Amyloid beta-Protein Precursor, Cricetinae, Animals, Molecular Biology, Amyloid beta-Peptides, Cell-Free System, biology, Chemistry, Chinese hamster ovary cell, P3 peptide, Cell Biology, Peptide Fragments, Cell biology, Gene Expression Regulation, Mutation, biology.protein, Protein Binding

Abstract

A novel cleavage of beta-amyloid precursor protein (APP), referred to as epsilon-cleavage, occurs downstream of the gamma-cleavage and generates predominantly a C-terminal fragment (CTFgamma) that begins at Val-50, according to amyloid beta-protein (Abeta) numbering. Whether this cleavage occurs independently of, or is coordinated with, gamma-cleavage is unknown. Using a cell-free system, we show here that, although Abeta40 and CTFgamma 50-99 were the predominant species produced by membranes prepared from cells overexpressing wild-type (wt) APP and wt presenilin (PS) 1 or 2, the production of CTFgamma 49-99, which begins at Leu-49, was remarkably enhanced in membranes from cells overexpressing mutant (mt) APP or mtPS1/2 that increases the production of Abeta42. Furthermore, a gamma-secretase inhibitor, which suppresses Abeta40 production and paradoxically enhances Abeta42 production at low concentrations, caused the proportion of CTFgamma 50-99 to decrease and that of CTFgamma 49-99 to increase significantly. These results strongly suggest a link between the production of Abeta42 and CTFgamma 49-99 and provide an important insight into the mechanisms of altered gamma-cleavage caused by mtAPP and mtPS1/2.

Published

2003

21. Neurotoxic Mechanisms Caused by the Alzheimer's Disease-linked Swedish Amyloid Precursor Protein Mutation

Author

Walter E. Müller, Christian Haass, Celio A. Marques, Astrid Bonert, Uta Keil, Barbara Steiner, and Anne Eckert

Subjects

Caspase-9, biology, Caspase 2, Neurodegeneration, Caspase 3, Cell Biology, medicine.disease, Caspase 8, Biochemistry, Molecular biology, Presenilin, Amyloid precursor protein, biology.protein, medicine, Molecular Biology, Caspase

Abstract

Autosomal dominant forms of familial Alzheimer's disease (FAD) are caused by mutations of the amyloid precursor protein (APP) gene and by mutations of the genes encoding for presenilin 1 or presenilin 2. Simultaneously, evidence is provided that increased oxidative stress might play a crucial role in the rapid progression of the Swedish FAD. Here we investigated the effect of the Swedish double mutation (K670M/N671L) in the beta-amyloid precursor protein on oxidative stress-induced cell death mechanisms in PC12 cells. Western blot analysis and cleavage studies of caspase substrates revealed an elevated activity of the executor caspase 3 after treatment with hydrogen peroxide in cells containing the Swedish APP mutation. This elevated activity is the result of the enhanced activation of both intrinsic and extrinsic apoptosis pathways, including activation of caspase 2 and caspase 8. Furthermore, we observed an enhanced activation of JNK pathway and an attenuation of apoptosis by SP600125, a JNK inhibitor, through protection of mitochondrial dysfunction and reduction of caspase 9 activity. Our findings provide evidence that the massive neurodegeneration in early age of FAD patients could be a result of an increased vulnerability of neurons through activation of different apoptotic pathways as a consequence of elevated levels of oxidative stress.

Published

2003

22. Identification of a β-Secretase Activity, Which Truncates Amyloid β-Peptide after Its Presenilin-dependent Generation

Author

Regina Fluhrer, Christian Haass, Masayasu Okochi, Wolfram Bode, Gil G. Westmeyer, Gerd Multhaup, Andrea Schlicksupp, Jochen Walter, Masatoshi Takeda, Michael Willem, and Sven Lammich

Subjects

Amyloid beta, Molecular Sequence Data, Peptide, Kidney, Transfection, Cleavage (embryo), Biochemistry, Presenilin, Cell Line, Substrate Specificity, Amyloid beta-Protein Precursor, Alzheimer Disease, Endopeptidases, Presenilin-1, Aspartic Acid Endopeptidases, Humans, Secretion, Amino Acid Sequence, ddc:610, Molecular Biology, chemistry.chemical_classification, biology, Cell Membrane, Membrane Proteins, Cell Biology, Molecular biology, Recombinant Proteins, In vitro, Amino acid, chemistry, Mutation, biology.protein, Amyloid Precursor Protein Secretases, Amyloid precursor protein secretase

Abstract

The beta-amyloid precursor protein (beta APP) is proteolytically processed by two secretase activities to produce the pathogenic amyloid beta-peptide (A beta). N-terminal cleavage is mediated by beta-secretase (BACE) whereas C-terminal intramembraneous cleavage is exerted by the presenilin (PS) gamma-secretase complex. The A beta-generating gamma-secretase cleavage principally occurs after amino acid 40 or 42 and results in secretion of A beta-(1-40) or A beta-(1-42). Upon overexpression of BACE in cultured cells we unexpectedly noticed a reduction of secreted A beta-(1-40/42). However, mass spectrometry revealed a truncated A beta species, which terminates at amino acid 34 (A beta-(1-34)) suggesting an alternative gamma-secretase cut. Indeed, expression of a loss-of-function variant of PS1 inhibited not only the production of A beta-(1-40) and A beta-(1-42) but also that of A beta-(1-34). However, expression levels of BACE correlate with the amount of A beta-(1-34), and A beta-(1-34) is produced at the expense of A beta-(1-40) and A beta-(1-42). Since this suggested that BACE is involved in a C-terminal truncation of A beta, we incubated purified BACE with A beta-(1-40) in vitro. Under these conditions A beta-(1-34) was generated. Moreover, when conditioned media containing Abeta-(1-40) and A beta-(1-42) were incubated with cells expressing a loss-of-function PS1 variant together with BACE, A beta-(1-34) was efficiently produced in vivo. These data demonstrate that an apparently gamma-secretase-dependent A beta derivative is produced after the generation of the non-truncated A beta via an additional and unexpected activity of BACE.

Published

2003

23. Presenilin-dependent Intramembrane Proteolysis of CD44 Leads to the Liberation of Its Intracellular Domain and the Secretion of an Aβ-like Peptide

Author

Masayasu Okochi, Masatoshi Takeda, Christoph Kaether, Christian Haass, Anja Capell, Dieter Edbauer, Ann-Katrin Zimmer, Jochen Walter, Sven Lammich, and Harald Steiner

Subjects

Cleavage factor, Molecular Sequence Data, Cleavage (embryo), Biochemistry, Presenilin, Cell Line, Amyloid beta-Protein Precursor, Mice, Protein structure, Alzheimer Disease, Endopeptidases, Presenilin-2, Presenilin-1, Animals, Aspartic Acid Endopeptidases, Humans, Amino Acid Sequence, Enzyme Inhibitors, Molecular Biology, Triglycerides, gamma-Aminobutyric Acid, Mice, Knockout, Cleavage stimulation factor, Amyloid beta-Peptides, biology, Cell Membrane, Membrane Proteins, Dipeptides, Cell Biology, Fibroblasts, Protein Structure, Tertiary, Cell biology, Transmembrane domain, Hyaluronan Receptors, Membrane protein, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, biology.protein, Carbamates, Amyloid Precursor Protein Secretases, Peptides, Sequence Alignment, Amyloid precursor protein secretase

Abstract

Alzheimer's disease (AD)-associated gamma-secretase is a presenilin (PS)- dependent proteolytic activity involved in the intramembraneous cleavage of the beta-amyloid precursor protein, Notch, LDL receptor-related protein, E-cadherin, and ErbB-4. This cut produces the corresponding intracellular domains (ICD), which are required for nuclear signaling of Notch and probably ErbB-4, the beta-amyloid precursor protein, E-cadherin, and the LDL receptor-related protein as well. We have now investigated CD44, a cell surface adhesion molecule, which also undergoes an intramembraneous cleavage to liberate its ICD. We demonstrate that this cleavage requires a PS-dependent gamma-secretase activity. A loss-of-function PS1 mutation, a PS1/PS2 knockout, as well as two independent and highly specific gamma-secretase inhibitors, abolish this cleavage. Surprisingly, small peptides similar to the amyloid beta-peptide (Abeta) are generated by an additional cut in the middle of the transmembrane region of CD44. Like Abeta, these CD44 beta-peptides are generated in a PS-dependent manner. These findings therefore suggest a dual intramembraneous cleavage mechanism mediated by PS proteins. The dual cleavage mechanism is required for nuclear signaling as well as removal of remaining transmembrane domains, a general function of PS in membrane protein metabolism.

Published

2002

24. PEN-2 Is an Integral Component of the γ-Secretase Complex Required for Coordinated Expression of Presenilin and Nicastrin

Author

Marcus Kostka, Gabriele Basset, Edith Winkler, Christian Haass, Stefan Prokop, Aya Yamasaki, Dieter Edbauer, and Harald Steiner

Subjects

DNA, Complementary, Nicastrin, Down-Regulation, Biochemistry, Presenilin, Cell Line, Epitopes, Mice, RNA interference, PEN-2, Endopeptidases, Presenilin-2, Presenilin-1, Animals, Aspartic Acid Endopeptidases, Humans, APH-1, Molecular Biology, Mice, Knockout, Membrane Glycoproteins, biology, Membrane Proteins, Active site, RNA, Cell Biology, Precipitin Tests, Protein Structure, Tertiary, Cell biology, Gamma-secretase complex, biology.protein, Electrophoresis, Polyacrylamide Gel, Amyloid Precursor Protein Secretases, Protein Binding

Abstract

The Alzheimer disease-associated presenilin (PS) proteins apparently provide the active site of gamma-secretase, an unusual intramembrane-cleaving aspartyl protease. PSs principally occur as high molecular weight protein complexes that contain nicastrin (Nct) and additional so far unidentified components. Recently, PEN-2 has been implicated in gamma-secretase function. Here we identify PEN-2 as a critical component of PS1/gamma-secretase and PS2/gamma-secretase complexes. Strikingly, in the absence of PS1 and PS1/PS2, PEN-2 levels are strongly reduced. Similarly, PEN-2 levels are reduced upon RNA interference-mediated down-regulation of Nct. On the other side, down-regulation of PEN-2 by RNA interference is associated with reduced PS levels, impaired Nct maturation, and deficient gamma-secretase complex formation. We conclude that PEN-2 is an integral gamma-secretase complex component and that gamma-secretase complex components are expressed in a coordinated manner.

Published

2002

25. The Role of Presenilins in γ-Secretase Activity

Author

Christian Haass and Michael S. Wolfe

Subjects

Receptors, Notch, biology, Chemistry, Membrane Proteins, Receptors, Cell Surface, Cell Biology, Biochemistry, Presenilin, Amyloid beta-Protein Precursor, Post translational, Alzheimer Disease, Endopeptidases, Protein processing, biology.protein, Aspartic Acid Endopeptidases, Humans, Amyloid Precursor Protein Secretases, Receptor, Protein Processing, Post-Translational, Molecular Biology, Amyloid precursor protein secretase, Gamma secretase

Published

2001

26. A Loss of Function Mutant of the Presenilin Homologue SEL-12 Undergoes Aberrant Endoproteolysis in Caenorhabditis elegans and Increases Aβ42 Generation in Human Cells

Author

Ralf Baumeister, Anja Capell, Andreas Böttcher, Masayasu Okochi, Helmut Romig, Jochen Walter, Christian Haass, Harald Steiner, and Stefan Eimer

Subjects

Amyloid beta-Peptides, Receptors, Notch, Mutant, Membrane Proteins, Helminth Proteins, Cell Biology, Biology, Cleavage (embryo), biology.organism_classification, Biochemistry, Molecular biology, Presenilin, Cell Line, Cell culture, Caspases, Mutation, Animals, Humans, Allele, Caenorhabditis elegans, Caenorhabditis elegans Proteins, Molecular Biology, Gene, Loss function

Abstract

The familial Alzheimer's disease-associated presenilins (PSs) occur as a dimeric complex of proteolytically generated fragments, which functionally supports endoproteolysis of Notch and the beta-amyloid precursor protein (betaAPP). A homologous gene, sel-12, has been identified in Caenorhabditis elegans. We now demonstrate that wild-type (wt) SEL-12 undergoes endoproteolytic cleavage in C. elegans similar to the PSs in human tissue. In contrast, SEL-12 C60S protein expressed from the sel-12(ar131) allele is miscleaved in C. elegans, resulting in a larger mutant N-terminal fragment. Neither SEL-12 wt nor C60S undergo endoproteolytic processing upon expression in human cells, suggesting that SEL-12 is cleaved by a C. elegans-specific endoproteolytic activity. The loss of function of sel-12 in C. elegans is not associated with a dominant negative activity in human cells, because SEL-12 C60S and the corresponding PS1 C92S mutation do not interfere with Notch1 cleavage. Moreover, both mutant variants increase the aberrant production of the highly amyloidogenic 42-amino acid version of amyloid beta-peptide similar to familial Alzheimer's disease-associated human PS mutants. Our data therefore demonstrate that the C60S mutation in SEL-12 is associated with aberrant endoproteolysis and a loss of function in C. elegans, whereas a gain of misfunction is observed upon expression in human cells.

Published

2000

27. Phosphorylation of the β-Amyloid Precursor Protein at the Cell Surface by Ectocasein Kinases 1 and 2

Author

Alice Schindzielorz, Bianka Hartung, Christian Haass, and Jochen Walter

Subjects

inorganic chemicals, GTP', Cell, Extracellular matrix component, Protein Serine-Threonine Kinases, Biology, Models, Biological, Biochemistry, Amyloid beta-Protein Precursor, medicine, Humans, Phosphorylation, Casein Kinase II, Protein kinase A, Molecular Biology, Heparin, Kinase, Cell Membrane, fungi, Cell Biology, Protein Structure, Tertiary, Cell biology, medicine.anatomical_structure, Ectodomain, Casein kinase 1, Casein Kinases, Protein Kinases

Abstract

The beta-amyloid precursor protein (betaAPP) is one of the rare proteins known to be phosphorylated within its ectodomain. We have shown previously that betaAPP can be phosphorylated within secretory vesicles and at the cell surface (Walter, J., Capell, A., Hung, A. Y. , Langen, H., Schnölzer, M., Thinakaran, G., Sisodia, S. S., Selkoe, D. J., and Haass, C. (1997) J. Biol. Chem. 272, 1896-1903). We have now specifically characterized the phosphorylation of cell surface-located betaAPP and identified two ectoprotein kinases that phosphorylate betaAPP at the outer face of the plasma membrane. By using selective protein kinase inhibitors and by investigating the usage of ATP and GTP as cosubstrates, we demonstrate that membrane-bound betaAPP as well as secreted forms of betaAPP can be phosphorylated by casein kinase (CK) 1- and CK2-like ectoprotein kinases. The ectodomain of betaAPP was also phosphorylated by purified CK1 and CK2 in vitro, but not by protein kinases A and C. Phosphorylation of betaAPP by ectoprotein kinases and by purified CK1 and CK2 occurred within an acidic domain in the N-terminal half of the protein. Heparin strongly inhibited the phosphorylation of cell-surface betaAPP by ecto-CK1 and ecto-CK2, indicating a regulatory role of this extracellular matrix component in betaAPP phosphorylation.

Published

2000

28. Expression of Alzheimer’s Disease-associated Presenilin-1 Is Controlled by Proteolytic Degradation and Complex Formation

Author

Christian Haass, Harald Steiner, Martin Citron, Dennis J. Selkoe, Helmut Romig, Anja Capell, Peter M. Kloetzel, Klaus Mendla, and Brigitte Pesold

Subjects

Models, Molecular, Proteasome Endopeptidase Complex, Amyloid, Mutant, Transfection, Biochemistry, Protein Structure, Secondary, Presenilin, Cell Line, Amyloid beta-Protein Precursor, Alzheimer Disease, Multienzyme Complexes, mental disorders, Presenilin-1, Humans, Molecular Biology, Gene, Caspase, biology, Membrane Proteins, Cell Biology, Metabolism, Peptide Fragments, Cysteine Endopeptidases, Gene Expression Regulation, Proteasome, biology.protein, Dimerization, Protein Processing, Post-Translational, Cysteine

Abstract

Numerous mutations causing early onset Alzheimer's disease have been identified in the presenilin (PS) genes, particularly the PS1 gene. Like the mutations identified within the beta-amyloid precursor protein gene, PS mutations cause the increased generation of a highly neurotoxic variant of amyloid beta-peptide. PS proteins are proteolytically processed to an N-terminal approximately 30-kDa (NTF) and a C-terminal approximately 20-kDa fragment (CTF20) that form a heterodimeric complex. We demonstrate that this complex is resistant to proteolytic degradation, whereas the full-length precursor is rapidly degraded. Degradation of the PS1 holoprotein is sensitive to inhibitors of the proteasome. Formation of a heterodimeric complex is required for the stability of both PS1 fragments, since fragments that do not co-immunoprecipitate with the PS complex are rapidly degraded by the proteasome. Mutant PS fragments not incorporated into the heterodimeric complex lose their pathological activity in abnormal amyloid beta-peptide generation even after inhibition of their proteolytic degradation. The PS1 heterodimeric complex can be attacked by proteinases of the caspase superfamily that generate an approximately 10-kDa proteolytic fragment (CTF10) from CTF20. CTF10 is rapidly degraded most likely by a calpain-like cysteine proteinase. From these data we conclude that PS1 metabolism is highly controlled by multiple proteolytic activities indicating that subtle changes in fragment generation/degradation might be important for Alzheimer's disease-associated pathology.

Published

1998

29. Intracellular Generation and Accumulation of Amyloid β-Peptide Terminating at Amino Acid 42

Author

Anja Capell, Yasuo Ihara, Harald Steiner, Uwe Leimer, Christian Haass, Tsuneo Yamazaki, and Christine Wild-Bode

Subjects

chemistry.chemical_classification, Amyloid beta-Peptides, Brefeldin A, Endoplasmic reticulum, Kidney metabolism, Cyclopentanes, Cell Biology, Biology, Golgi apparatus, Endoplasmic Reticulum, Kidney, Biochemistry, Cell Line, Amino acid, chemistry.chemical_compound, symbols.namesake, chemistry, symbols, Humans, Senile plaques, Molecular Biology, Intracellular, Secretory pathway

Abstract

Amyloid beta-peptide (Abeta) is known to accumulate in senile plaques of Alzheimer's disease (AD) patients and is now widely believed to play a major role in the disease. Two populations of peptides occur terminating either at amino acid 40 or at amino acid 42 (Abeta1-40 and Abeta1-42). Alternative N-terminal cleavages produce additional heterogeneity (Abetax-40 and Abetax-42). Peptides terminating at amino acid 42 are believed to be the major player in sporadic AD as well as familial AD (FAD). Whereas the cellular mechanism for the generation of Abeta terminating at amino acid 40 is well understood, very little is known about the cleavage of Abeta after amino acid 42. By using two independent methods we demonstrate intracellular Abeta1-42 as well as Abetax-42 but less Abetax-40 and Abeta1-40 in kidney 293 cells stably transfected with wild type beta-amyloid precursor protein (betaAPP) or the FAD-associated Val/Gly mutation. Moreover, retention of betaAPP within the endoplasmic reticulum (ER) by treatment with brefeldin A does not block the cleavage at amino acid 42 but results in an increased production of all species of Abeta terminating at amino acid 42. This indicates that the cleavage after amino acid 42 can occur within the ER. Treatment of cells with monensin, which blocks transport of (betaAPP) within the Golgi causes a marked accumulation of intracellular Abetax-42 and Abetax-40. Therefore these experiments indicate that the gamma-secretase cleavage of Abeta after amino acid 42 can occur within the ER and later within the secretory pathway within the Golgi. Moreover inhibition of reinternalization by cytoplasmic deletions of betaAPP as well as inhibition of intracellular acidification by NH4Cl does not block intracellular Abeta1-42 or Abetax-42 production.

Published

1997

30. Enhanced Production and Oligomerization of the 42-residue Amyloid β-Protein by Chinese Hamster Ovary Cells Stably Expressing Mutant Presenilins

Author

Weiming Xia, Dennis J. Selkoe, Marcia B. Podlisny, Martin Citron, Edward H. Koo, Peter Seubert, Dora Kholodenko, Jimin Zhang, Christian Haass, and David B. Teplow

Subjects

Cell, Mutant, CHO Cells, Biology, Transfection, Biochemistry, Presenilin, Residue (chemistry), Biopolymers, Cricetulus, Cricetinae, Presenilin-2, mental disorders, Presenilin-1, medicine, Animals, Molecular Biology, Gene, Amyloid beta-Peptides, Hydrolysis, Chinese hamster ovary cell, Endoplasmic reticulum, Membrane Proteins, Cell Biology, Molecular biology, nervous system diseases, medicine.anatomical_structure, nervous system

Abstract

Mutations in the presenilin 1 (PS1) and presenilin 2 (PS2) genes cause the most common and aggressive form of early onset familial Alzheimer's disease. To elucidate their pathogenic mechanism, wild-type (wt) or mutant (M146L, C410Y) PS1 and wt or mutant (M239V) PS2 genes were stably transfected into Chinese hamster ovary cells that overexpress the beta-amyloid precursor protein (APP). The identity of the 43-45-kDa PS1 holoproteins was confirmed by N-terminal radiosequencing. PS1 was rapidly processed (t1/2 = 40 min) in the endoplasmic reticulum into stable fragments. Wild-type and mutant PS2 holoproteins exhibited similar half lives (1.5 h); however, their endoproteolytic fragments showed both mutation-specific and cell type-specific differences. Mutant PS1 or PS2 consistently induced a 1.4-2.5-fold increase (p0.001) in the relative production of the highly amyloidogenic 42-residue form of amyloid beta-protein (Abeta42) as determined by quantitative immunoprecipitation and by enzyme-linked immunosorbent assay. In mutant PS1 and PS2 cell lines with high increases in Abeta42/Abetatotal ratios, spontaneous formation of low molecular weight oligomers of Abeta42 was observed in media, suggesting enhanced Abeta aggregation from the elevation of Abeta42. We conclude that mutant PS1 and PS2 proteins enhance the proteolysis of beta-amyloid precursor protein by the gamma-secretase cleaving at Abeta residue 42, thereby promoting amyloidogenesis.

Published

1997

31. Ectodomain Phosphorylation of β-Amyloid Precursor Protein at Two Distinct Cellular Locations

Author

Gopal Thinakaran, Dennis J. Selkoe, Albert Y. Hung, Anja Capell, Hanno Langen, Jochen Walter, Christian Haass, Martina Schnölzer, and Sangram S. Sisodia

Subjects

inorganic chemicals, Golgi Apparatus, Biology, environment and public health, Biochemistry, Cell Line, Serine, Amyloid beta-Protein Precursor, chemistry.chemical_compound, Humans, Phosphorylation, Molecular Biology, Endoplasmic reticulum, C-terminus, Cell Membrane, Wild type, Cell Biology, Brefeldin A, Molecular biology, Transmembrane protein, enzymes and coenzymes (carbohydrates), Ectodomain, chemistry, Mutation, Protein Kinases, Subcellular Fractions

Abstract

The beta-amyloid precursor protein (betaAPP) is a transmembrane protein that is exclusively phosphorylated on serine residues within its ectodomain. To identify the cellular site of betaAPP phosphorylation, we took advantage of an antibody that specifically detects the free C terminus of beta-secretase-cleaved betaAPP containing the Swedish missense mutation (APPssw-beta). This antibody previously established the cellular location of the beta-secretase cleavage of Swedish betaAPP as a post-Golgi secretory compartment (Haass, C., Lemere, C., Capell, A., Citron, M., Seubert, P., Schenk, D., Lannfelt, L., and Selkoe, D. J. (1995) Nature Med. 1, 1291-1296). We have now localized the selective ectodomain phosphorylation of betaAPP to the same compartment. Moreover, the phosphorylation sites of betaAPP were identified at Ser198 and Ser206 of betaAPP695 by tryptic peptide mapping, mass spectrometry, and site-directed mutagenesis. Intracellular phosphorylation of betaAPP was inhibited by Brefeldin A and by incubating cells at 20 degrees C, thus excluding phosphorylation in the endoplasmic reticulum or trans-Golgi network. Ectodomain phosphorylation within a post-Golgi compartment occurred not only with mutant Swedish betaAPP, but also with wild type betaAPP. In addition to phosphorylation within a post-Golgi compartment, betaAPP was also found to undergo phosphorylation at the cell surface by an ectoprotein kinase. Therefore, this study revealed two distinct cellular locations for betaAPP phosphorylation.

Published

1997

32. Degradation of Amyloid β-Protein by a Serine Protease-α2-Macroglobulin Complex

Author

Wei Qiao Qiu, Wolfgang Borth, Christian Haass, David B. Teplow, Zhen Ye, and Dennis J. Selkoe

Subjects

Macromolecular Substances, medicine.medical_treatment, Proteolysis, Molecular Sequence Data, CHO Cells, Biochemistry, Multienzyme Complexes, Cricetinae, Zymogen, Chlorocebus aethiops, medicine, Animals, Protease Inhibitors, alpha-Macroglobulins, Amino Acid Sequence, Molecular Biology, Cells, Cultured, Serine protease, Amyloid beta-Peptides, Protease, Chymotrypsin, medicine.diagnostic_test, biology, Kunitz STI protease inhibitor, Serine Endopeptidases, P3 peptide, Cell Biology, Trypsin, Molecular biology, Culture Media, Molecular Weight, biology.protein, medicine.drug

Abstract

Progressive cerebral deposition of the amyloid beta-peptide (Abeta) is an early and constant feature of Alzheimer's disease. Abeta is derived by proteolysis from the beta-amyloid precursor protein. beta-Amyloid precursor protein processing and the generation of Abeta have been extensively characterized, but little is known about the mechanisms of degradation of this potentially neurotoxic peptide. We identified and purified a proteolytic activity in culture medium that can degrade secreted Abeta but not larger proteins in the medium. Detection of the activity in conditioned medium required the presence of fetal bovine serum and the passage of the cells with a pancreatic trypsin preparation. Its inhibitor profile showed that the activity was a serine protease other than trypsin or chymotrypsin. The protease occurs as a stable approximately 700-kDa complex with the inhibitor, alpha2-macroglobulin (alpha2M), that retains activity against small substrates such as Abeta. Its NH2-terminal sequence suggests that the protease is previously unidentified. Our results indicate that the Abeta-degrading protease we have detected is a non-trypsin component of a pancreatic trypsin preparation or else derives from a zymogen in serum that is activated by a protease in the latter preparation. Because Abeta-bearing plaques in Alzheimer's disease brain contain both alpha2M and receptors of alpha2M-protease complexes, the same or a similar alpha2M-protease complex could arise in vivo and play a role in Abeta clearance.

Published

1996

33. Metabolism of the 'Swedish' amyloid precursor protein variant in Madin-Darby canine kidney cells

Author

D. B. Teplow, Sangram S. Sisodia, Christian Haass, Amy C. Y. Lo, and S. L. Wagner

Subjects

chemistry.chemical_classification, biology, Kidney metabolism, Peptide, Cell Biology, Transfection, Biochemistry, Molecular biology, chemistry, Biotinylation, mental disorders, biology.protein, Amyloid precursor protein, Molecular Biology, Amyloid precursor protein secretase, Peptide sequence, Intracellular

Abstract

The 4-kDa beta-amyloid peptide (A beta), a major constituent of parenchymal amyloid deposits in Alzheimer's disease, is derived from larger amyloid precursor proteins (APP). We have examined the metabolism of APP in Madin-Darby canine kidney cells stably transfected with cDNA encoding either wild-type human APP-695 or human APP-695 that harbors the Swedish double mutation associated with familial early-onset Alzheimer's disease. Although approximately 90% of total soluble APP secreted from wild-type cells is secreted basolaterally following cleavage at the alpha-secretase site, soluble derivatives cleaved near or at the amino terminus of A beta (presumably the "beta-secretase" site) are preferentially secreted into the apical compartment of SWE cells. Concomitantly, levels of a specific A beta-containing carboxyl-terminal fragment are elevated in SWE cell lysates. Using domain-specific biotinylation and release assays, we failed to detect a beta-secretase-generated soluble derivative (APPs beta) released from the surface of SWE cells. However, APPs beta can be detected in SWE cell lysates, consistent with "beta-secretase" cleavage occurring in an intracellular compartment. Finally, we demonstrate that A beta is secreted into the basolateral compartment of SWE cells and that the majority of these A beta-related species contains an amino-terminal aspartate residue (+1).

Published

1994

34. Mutations associated with a locus for familial Alzheimer's disease result in alternative processing of amyloid beta-protein precursor

Author

Christian Haass, David B. Teplow, Dennis J. Selkoe, and Albert Y. Hung

Subjects

Genetics, biology, Amyloid beta, P3 peptide, Cell Biology, medicine.disease, Biochemistry, Phenotype, Molecular biology, medicine, Amyloid precursor protein, biology.protein, Alzheimer's disease, Site-directed mutagenesis, Protein precursor, Molecular Biology, Gene

Abstract

Alzheimer's disease (AD) is a progressive neurodegenerative disorder characterized by the extracellular deposition of amyloid beta-protein (A beta), a molecule produced by post-translational processing of the beta-amyloid precursor protein (beta APP). Mutations within the gene encoding beta APP have been linked to early onset forms of AD, but the pathogenetic mechanism(s) producing the phenotype are unknown. We analyzed the effects on beta APP processing in vitro of a naturally occurring Ala-->Gly mutation at position 692 of beta APP770 (A692G) (Hendriks, L., Duijin, C., Cras, P., Cruts, M., van Hul, W., van Harskamp, F., Warren, A., McInnis, M., Antonarakis, S., Martin, J.-J., Hofman, A., and van Broeckhoven, C. (1992) Nature Genet. 1, 218-221), as well as the effects of five genetically engineered mutations at or near this site. Substitution of glycine or proline for Ala692, or for Phe690, produced relative increases in secretion of A beta and relative decreases in secretion of the p3 peptide(s) arising after alpha-secretase generation of soluble APP (APPs). The Phe690-->Pro substitution also resulted in the synthesis of truncated APPs molecules. The structurally conservative substitutions Ala692-->Val and Phe690-->Tyr did not exhibit these effects. Certain of the substitutions also resulted in the production of a minor peptides, previously undescribed in vitro, beginning at Ala2, Lys16, and Phe19 of A beta. These data show that beta APP mutations carboxyl-terminal to alpha-secretase and beta-secretase cleavage sites can exert strong control over beta APP processing. Increased secretion of A beta may accelerate amyloidogenesis by providing more precursors for aggregation. It is also possible that truncated A beta peptides resulting from several of these mutations may accelerate amyloidogenesis through self-aggregation and/or seeding the fibrillogenesis of longer, more abundant A beta species.

Published

1994

35. Activation of protein kinase C inhibits cellular production of the amyloid beta-protein

Author

Roger Nitsch, Wei Qiao Qiu, Dennis J. Selkoe, Christian Haass, Martin Citron, Albert Y. Hung, Richard J. Wurtman, and John H. Growdon

Subjects

PTK2B, biology, Amyloid beta, Cell Biology, Biochemistry, Biochemistry of Alzheimer's disease, Cell biology, biology.protein, Protein phosphorylation, ASK1, PRKCB1, Signal transduction, Molecular Biology, Protein kinase C

Abstract

The 39-43-amino acid amyloid beta-protein (A beta), which is progressively deposited in cerebral plaques and blood vessels in Alzheimer's disease (AD), is released by cultured human cells during normal metabolism. Here we show that agents which activate protein kinase C or otherwise enhance protein phosphorylation caused a substantial decrease in A beta production in vitro. Protein kinase C activation also markedly decreased A beta release from cells that express mutant forms of the beta-amyloid precursor protein genetically linked to familial AD. Inhibition of A beta secretion could also be effected by direct stimulation of m1 muscarinic acetylcholine receptors with carbachol. These results demonstrate that activation of the protein kinase C signal transduction pathways down-regulates the generation of the amyloidogenic A beta peptide. Pharmacologic agents that activate this system, including a variety of first messengers, could potentially slow the development or growth of some A beta plaques during the early stages of AD.

Published

1993

36. beta-Amyloid peptide and a 3-kDa fragment are derived by distinct cellular mechanisms

Author

Michael G. Schlossmacher, David B. Teplow, Dennis J. Selkoe, Albert Y. Hung, and Christian Haass

Subjects

chemistry.chemical_classification, Endoplasmic reticulum, Leupeptin, Peptide, Cell Biology, Brefeldin A, Golgi apparatus, Biochemistry, chemistry.chemical_compound, symbols.namesake, medicine.anatomical_structure, chemistry, Lysosome, mental disorders, medicine, symbols, Secretion, Beta (finance), Molecular Biology

Abstract

We have analyzed the cellular processing pathways which produce the 4-kDa amyloid beta-peptide (A beta) and a 3-kDa derivative (p3) of the beta-amyloid precursor protein (beta APP) found in conditioned media of tissue culture cells and in cerebrospinal fluid. Pulse-chase experiments reveal that both peptides are secreted in parallel with soluble beta APP (APPs); no precursor-product relation between A beta and p3 was found. The protease inhibitor leupeptin did not influence the production of either peptide. In contrast, the weak base ammonium chloride (NH4Cl) showed a dose-dependent inhibition of A beta production with less decrease in p3. A similar effect was observed using the monovalent ionophore monensin. Brefeldin A completely inhibited the generation of both peptides, indicating that proteases located in the endoplasmic reticulum or early Golgi are not sufficient for the production of the small peptides. Deletion of the beta APP cytoplasmic domain, which removes a consensus sequence that probably mediates reinternalization, caused an increase in secretion of both APPs and p3 and did not abolish A beta production. These observations suggest that completely mature beta APP within the late Golgi and/or at the cell surface is a prerequisite for A beta production but processing within the lysosome might not be directly required. p3 appears to derive from the 10-kDa C-terminal stub of beta APP following secretion of APPs.

Published

1993