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The Journal of Neuroscience, January 1, 2003, 23(1):187-192
Genetic Modulation of Tau Phosphorylation in the Mouse
Jochen Brich1, Feng-Shiun Shie4, Brian W. Howell5, Renhua Li6, Katalin Tus2, Edward K. Wakeland2, Lee-Way Jin4, Marc Mumby3, Gary Churchill6, Joachim Herz1, and Jonathan A. Cooper5 Departments of 1 Molecular Genetics, 2 Immunology, and 3 Pharmacology, University of Texas Southwestern Medical Center, Dallas, Texas 75390, 4 Alzheimer Disease Research Center, University of Washington, Seattle, Washington 98195, 5 Fred Hutchinson Cancer Research Center, Seattle, Washington 98109, and 6 The Jackson Laboratory, Bar Harbor, Maine 04609
ABSTRACT
TOP
ABSTRACT
Introduction
The axonal microtubule stabilizing protein tau is hyperphosphorylated in several neurodegenerative conditions, including Alzheimer's disease, yet the genes that regulate tau phosphorylation are largely unknown. Disabled-1 (Dab1) is a cytoplasmic adapter protein that interacts with apolipoprotein E (ApoE) receptors and controls neuronal positioning during embryonic brain development. We have investigated the role of Dab1 in tau phosphorylation. We found that wild-type Dab1, but not a mutant lacking tyrosine phosphorylation sites, protects mice from the hyperphosphorylation of tau. However, the absence of Dab1 is not sufficient to cause tau hyperphosphorylation, because hyperphosphorylation is manifested only when Dab1 is mutated in specific mouse strain backgrounds. Tau hyperphosphorylation correlates with early death in susceptible mouse strains, and it occurs in the neurons of the hippocampus and dentate gyrus. By quantitative trait locus (QTL) analysis of Dab1-deficient mice on a hybrid strain background, we uncovered one significant and three suggestive chromosomal loci that modulate tau phosphorylation. Two of these QTL regions contain genes that are defective in early onset Alzheimer's disease. Our findings suggest that Dab1 gene disruption sensitizes mice to tau hyperphosphorylation contingent on specific haplotypes that are linked to Alzheimer's disease loci. Dab1 mutant mice provide an animal model for studying the relationships between ApoE receptors, tau hyperphosphorylation, and Alzheimer's disease.
Key words: Reeler; Disabled-1; tau hyperphosphorylation; quantitative trait locus analysis; Alzheimer's disease; genetic interactions
Introduction
The microtubule-associated protein tau regulates microtubule assembly and disassembly during neuronal differentiation (Mandelkow and Mandelkow, 1995
). Tau functions are regulated by phosphorylation at many different sites, and overall tau phosphorylation is high during brain development but declines after birth. Abnormally high levels of tau phosphorylation in adult brains are associated with various neurological pathologies (Lee, 1996
protein, and for the multiple membrane-spanning proteins presenilin-1 (PS-1) and PS-2, which process APP (Hardy, 1996
4 isoform of apolipoprotein E (ApoE) (Schmechel et al., 1993
There is great interest in developing mouse model systems to study tau hyperphosphorylation (Gotz, 2001
We reported previously that genetic deficiency of two ApoE receptors (ApoERs), known as very-low-density lipoprotein receptor (VLDLR) and ApoER2, causes tau hyperphosphorylation that is readily detectable at weaning (Hiesberger et al., 1999
We have now investigated the role of Disabled-1 (Dab1), another gene in the Reln-dependent developmental pathway (Rice and Curran, 1999
Materials and Methods
Western blotting. Postnatal day 18 (P18) to P20 brains were extracted, and heat-soluble proteins were purified as described previously (Matsuo et al., 1994
Immunohistochemistry. P18-P20 brains were fixed in 4% paraformaldehyde and cryoprotected in sucrose, and frozen sections were prepared. Sections were reacted with antibody TG-3 (Jicha et al., 1997
Quantitative trait locus analysis. Dab1
/
Data were analyzed by a whole genome scan for linkage as described previously (Lander and Kruglyak, 1995
Criteria for significant and suggestive QTLs. Criteria for significant and suggestive thresholds were determined by performing 1000 analyses on permuted data sets. The maximum likelihood log odds (LOD) score exceeds the threshold for significant linkage in 5% of the permuted data analyses, and it exceeds the suggestive threshold in 37%, in accordance with accepted standards for significance in genome-wide QTL scans (Lander and Kruglyak, 1995
Results
Effects of Dab1 mutation on tau phosphorylation
We tested whether Dab1 regulates tau phosphorylation, initially using mice of the 129Sv × C57BL/6 (SB) hybrid strain background that is commonly used for maintaining knock-out strains. As found previously (Hiesberger et al., 1999
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Figure 1. Tau phosphorylation at several sites is regulated by genes of the Reln-Dab1 pathway. Brain extracts were prepared at P18-P20, and equal quantities of heat-stable protein were analyzed by SDS PAGE and Western blotting. A, Samples from various mutant mice of different strain backgrounds were analyzed simultaneously with antibodies recognizing phosphorylated (top) and dephosphorylated (bottom) tau. B, Selected samples were reanalyzed with antibodies recognizing additional epitopes on tau. Antibody specificity was determined previously using human tau as the antigen: +P, Phosphorylation dependent; P, dephosphorylation dependent; Pi, phosphorylation independent (see Materials and Methods for references). Note the altered migration of tau from mutant brains (asterisks), which is indicative of increased phosphorylation.
Tau hyperphosphorylation in the hippocampus
To localize hyperphosphorylated tau, brain sections from wild-type and Dab1-deficient mice were stained with antibodies that recognize phosphorylated tau. Strong staining was detected in sections from Dab1 deletion and phenylalanine mutants in the SB strain background (Fig. 2A-D). Staining was restricted to cell bodies in the hippocampus proper and the dentate gyrus and to fiber tracts of the corpus callosum and fasciculus retroflexus. No staining was detected in the wild type (Fig. 2E). Cells in the hippocampus were misplaced, as would be expected when Reln-Dab1 signaling is disrupted (Rice and Curran, 1999
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Figure 2. Presence of phosphorylated tau in the hippocampus. All sections were stained for phosphorylated tau, and brown areas indicate immunoreactivity. A-D, Sections from a Dab1
Survival of Dab1 mutants depends on strain background: correlation with tau phosphorylation
We noticed that the viability of Dab1 mutant mice depends on the strain background. Dab1 mutations were originally made in the embryonic stem cells of 129Sv mice (SS), and maintained in pure SS or mixed SB backgrounds (Howell et al., 1997
We suspected that surviving mice may not have hyperphosphorylated tau. Indeed, we found that the Dab1 deletion in the CC strain background does not cause tau hyperphosphorylation, as detected by Western blotting (Fig. 1A, samples 12-15) or immunohistochemistry (Fig. 2F). When data from Dab1 mutations in various mouse strains were compared, there was a strong relationship between the lack of tau hyperphosphorylation and anticipated survival for >5 weeks (Table 1). This correlation suggests either that tau hyperphosphorylation causes death or that tau hyperphosphorylation and early death have a common cause.
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Table 1. Relationship between anticipated survival, tau phosphorylation, Dab1 genotype, and mouse strain background Mapping of genetic loci that modify tau hyperphosphorylation in Dab1
Because extensive, early onset tau hyperphosphorylation has not been observed previously in mutant mice, we initiated a search for QTLs that modify the phosphorylation of tau in the absence of Dab1. We bred Dab1
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Figure 3. Identification of genetic modifiers of tau phosphorylation. A, Dab1
Discussion
Combined with previous results from Reln, VLDLR, and ApoER2 mutants (Hiesberger et al., 1999
We also found that survival of Dab1 mutants for >5 weeks of age depended on the strain background and correlated strongly with the lack of high levels of phosphorylated tau (Table 1). A survey of published Reln and Dab1 mutants reveals variable survival of homozygotes, depending on strain background. Viable alleles and strains include Relned in the B6C3Fe strain (Falconer, 1951
The detection of hyperphosphorylated tau in the hippocampus and the dentate gyrus of Dab1
The map locations of QTLs that modify tau hyperphosphorylation in Dab1
In summary, our results do not distinguish whether the lack of postnatal Reln signals or abnormal brain architecture, secondary to defects in the Reln signaling pathway during development, is responsible for increased tau phosphorylation in Dab1
FOOTNOTES Received Aug. 15, 2002; revised Oct. 3, 2002; accepted Oct. 11, 2002.
This work was supported by grants from the National Institutes of Health (J.A.C., J.H., M.M., E.K.W.), from the Alzheimer Association, and from the Humboldt Foundation (J.H.). J.B. is a fellow of the Ernst and Hedda Wollheim Foundation and a recipient of a Boehringer Ingelheim scholarship. We thank P. K. O'Brien and T. Herrick for expert technical assistance, G. Schellenberg, V. Lee, and I. Vincent for antibodies, and E. Giniger, B. Ballif, and G. Schellenberg for valuable comments on this manuscript.
Correspondence should be addressed to either of the following: Jonathan A. Cooper, Fred Hutchinson Cancer Research Center A2-025, 1100 Fairview Avenue North, Seattle, WA 98109, E-mail: jcooper{at}fhcrc.org; or Joachim Herz, University of Texas Southwestern Medical Center, Dallas, TX 75390, E-mail: joachim.herz{at}utsouthwestern.edu.
J. Brich's present address: Department of Clinical Biochemistry and Pathobiochemistry, Julius-Maximilians-University, D-97078 Würzburg, Germany.
B. W. Howell's present address: National Institute of Neurological Disorders and Stroke, National Institutes of Health, Building 10, 3B04, 10 Center Drive, Bethesda, MD 20892
References
- Binder LI, Frankfurter A, Rebhun LI (1985) The distribution of tau in the mammalian central nervous system. J Cell Biol 101:1371-1378
[Abstract/Free Full Text] .- Blake JA, Eppig JT, Richardson JE, Bult CJ, Kadin JA (2001) The Mouse Genome Database (MGD): integration nexus for the laboratory mouse. Nucleic Acids Res 29:91-94
[Abstract/Free Full Text] .- Blake JA, Richardson JE, Bult CJ, Kadin JA, Eppig JT (2002) The Mouse Genome Database (MGD): the model organism database for the laboratory mouse. Nucleic Acids Res 30:113-115
[Abstract/Free Full Text] .- D'Arcangelo G, Miao GG, Chen SC, Soares HD, Morgan JI, Curran T (1995) A protein related to extracellular matrix proteins deleted in the mouse mutant reeler. Nature 374:719-723[Medline].
- D'Arcangelo G, Homayouni R, Keshvara L, Rice DS, Sheldon M, Curran T (1999) Reelin is a ligand for lipoprotein receptors. Neuron 24:471-479[ISI][Medline].
- Del Rio JA, Heimrich B, Borrell V, Forster E, Drakew A, Alcantara S, Nakajima K, Miyata T, Ogawa M, Mikoshiba K, Derer P, Frotscher M, Soriano E (1997) A role for Cajal-Retzius cells and reelin in the development of hippocampal connections. Nature 385:70-74[Medline].
- Deng HX, Hentati A, Tainer JA, Iqbal Z, Cayabyab A, Hung WY, Getzoff ED, Hu P, Herzfeldt B, Roos RP (1993) Amyotrophic lateral sclerosis and structural defects in Cu, Zn superoxide dismutase. Science 261:1047-1051
[Abstract/Free Full Text] .- Falconer DS (1951) Two new mutants, "trembler" and "reeler", with neurological actions in the house mouse. J Genet 50:192-201[ISI].
- Garretson JD, Neumann PE (1993) Further evidence that a mouse chromosome 4 locus influences cerebellar folial pattern. Brain Res 630:221-225[Medline].
- Goedert M, Jakes R, Crowther RA, Six J, Lubke U, Vandermeeren M, Cras P, Trojanowski JQ, Lee VM (1993) The abnormal phosphorylation of tau protein at Ser-202 in Alzheimer disease recapitulates phosphorylation during development. Proc Natl Acad Sci USA 90:5066-5070
[Abstract/Free Full Text] .- Goedert M, Jakes R, Crowther RA, Cohen P, Vanmechelen E, Vandermeeren M, Cras P (1994) Epitope mapping of monoclonal antibodies to the paired helical filaments of Alzheimer's disease: identification of phosphorylation sites in tau protein. Biochem J 301:871-877.
- Goffinet AM (1990) Cerebellar phenotype of two alleles of the "reeler" mutation on similar backgrounds. Brain Res 519:355-357[Medline].
- Gotz J (2001) Tau and transgenic animal models. Brain Res Brain Res Rev 35:266-286[Medline].
- Gotz J, Chen F, van Dorpe J, Nitsch RM (2001) Formation of neurofibrillary tangles in P301l tau transgenic mice induced by A
[Abstract/Free Full Text] .- Gupta A, Tsai LH, Wynshaw-Boris A (2002) Life is a journey: a genetic look at neocortical development. Nat Rev Genet 3:342-355[ISI][Medline].
- Hardy J (1996) New insights into the genetics of Alzheimer's disease. Ann Med 28:255-258[Medline].
- Hardy J, Duff K, Hardy KG, Perez-Tur J, Hutton M (1998) Genetic dissection of Alzheimer's disease and related dementias: amyloid and its relationship to tau. Nat Neurosci 1:355-358[ISI][Medline].
- Hiesberger T, Trommsdorff M, Howell BW, Goffinet A, Mumby MC, Cooper JA, Herz J (1999) Direct binding of Reelin to VLDL receptor and ApoE receptor 2 induces tyrosine phosphorylation of disabled-1 and modulates tau phosphorylation. Neuron 24:481-489[ISI][Medline].
- Holcomb L, Gordon MN, McGowan E, Yu X, Benkovic S, Jantzen P, Wright K, Saad I, Mueller R, Morgan D, Sanders S, Zehr C, O'Campo K, Hardy J, Prada CM, Eckman C, Younkin S, Hsiao K, Duff K (1998) Accelerated Alzheimer-type phenotype in transgenic mice carrying both mutant amyloid precursor protein and presenilin 1 transgenes. Nat Med 4:97-100[ISI][Medline].
- Homayouni R, Rice DS, Sheldon M, Curran T (1999) Disabled-1 binds to the cytoplasmic domain of amyloid precursor-like protein 1. J Neurosci 19:7507-7515
[Abstract/Free Full Text] .- Hong M, Zhukareva V, Vogelsberg-Ragaglia V, Wszolek Z, Reed L, Miller BI, Geschwind DH, Bird TD, McKeel D, Goate A, Morris JC, Wilhelmsen KC, Schellenberg GD, Trojanowski JQ, Lee VM (1998) Mutation-specific functional impairments in distinct tau isoforms of hereditary FTDP-17. Science 282:1914-1917
[Abstract/Free Full Text] .- Howell BW, Hawkes R, Soriano P, Cooper JA (1997) Neuronal position in the developing brain is regulated by mouse disabled-1. Nature 389:733-737[Medline].
- Howell BW, Herrick TM, Cooper JA (1999a) Reelin-induced tyrosine phosphorylation of disabled 1 during neuronal positioning. Genes Dev 13:643-648
[Abstract/Free Full Text] .- Howell BW, Lanier LM, Frank R, Gertler FB, Cooper JA (1999b) The disabled 1 phosphotyrosine-binding domain binds to the internalization signals of transmembrane glycoproteins and to phospholipids. Mol Cell Biol 19:5179-5188
[Abstract/Free Full Text] .- Howell BW, Herrick TM, Hildebrand JD, Zhang Y, Cooper JA (2000) Dab1 tyrosine phosphorylation sites relay positional signals during mouse brain development. Curr Biol 10:877-885[ISI][Medline].
- Hutton M, Lewis J, Dickson D, Yen SH, McGowan E (2001) Analysis of tauopathies with transgenic mice. Trends Mol Med 7:467-470[ISI][Medline].
- Jicha GA, Lane E, Vincent I, Otvos Jr L, Hoffmann R, Davies P (1997) A conformation- and phosphorylation-dependent antibody recognizing the paired helical filaments of Alzheimer's disease. J Neurochem 69:2087-2095[ISI][Medline].
- Kosik KS, Orecchio LD, Binder L, Trojanowski JQ, Lee VM, Lee G (1988) Epitopes that span the tau molecule are shared with paired helical filaments. Neuron 1:817-825[ISI][Medline].
- Lander E, Kruglyak L (1995) Genetic dissection of complex traits: guidelines for interpreting and reporting linkage results. Nat Genet 11:241-247[ISI][Medline].
- Lang E, Szendrei GI, Lee VM, Otvos Jr L (1992) Immunological and conformation characterization of a phosphorylated immunodominant epitope on the paired helical filaments found in Alzheimer's disease. Biochem Biophys Res Commun 187:783-790[ISI][Medline].
- Lee VM (1996) Regulation of tau phosphorylation in Alzheimer's disease. Ann NY Acad Sci 777:107-113[Abstract].
- Lee VM, Goedert M, Trojanowski JQ (2001) Neurodegenerative tauopathies. Annu Rev Neurosci 24:1121-1159[ISI][Medline].
- Lewis J, McGowan E, Rockwood J, Melrose H, Nacharaju P, Van Slegtenhorst M, Gwinn-Hardy K, Paul Murphy M, Baker M, Yu X, Duff K, Hardy J, Corral A, Lin WL, Yen SH, Dickson DW, Davies P, Hutton M (2000) Neurofibrillary tangles, amyotrophy and progressive motor disturbance in mice expressing mutant (P301L) tau protein. Nat Genet 25:402-405[ISI][Medline].
- Lewis J, Dickson DW, Lin WL, Chisholm L, Corral A, Jones G, Yen SH, Sahara N, Skipper L, Yager D, Eckman C, Hardy J, Hutton M, McGowan E (2001) Enhanced neurofibrillary degeneration in transgenic mice expressing mutant tau and APP. Science 293:1487-1491
[Abstract/Free Full Text] .- Mandelkow E, Mandelkow EM (1995) Microtubules and microtubule-associated proteins. Curr Opin Cell Biol 7:72-81[ISI][Medline].
- Matsuo ES, Shin RW, Billingsley ML, Van deVoorde A, O'Connor M, Trojanowski JQ, Lee VM (1994) Biopsy-derived adult human brain tau is phosphorylated at many of the same sites as Alzheimer's disease paired helical filament tau. Neuron 13:989-1002[ISI][Medline].
- Neumann PE, Garretson JD, Skabardonis GP, Mueller GG (1993) Genetic analysis of cerebellar folial pattern in crosses of C57BL/6J and DBA/2J inbred mice. Brain Res 619:81-88[ISI][Medline].
- Poorkaj P, Tsuang D, Wijsman E, Steinbart E, Garruto RM, Craig UK, Chapman NH, Anderson L, Bird TD, Plato CC, Perl DP, Weiderholt W, Galasko D, Schellenberg GD (2001) TAU as a susceptibility gene for amyotrophic lateral sclerosis-parkinsonism dementia complex of Guam. Arch Neurol 58:1871-1878
[Abstract/Free Full Text] .- Price DL, Tanzi RE, Borchelt DR, Sisodia SS (1998) Alzheimer's disease: genetic studies and transgenic models. Annu Rev Genet 32:461-493[ISI][Medline].
- Rice DS, Curran T (1999) Mutant mice with scrambled brains: understanding the signaling pathways that control cell positioning in the CNS. Genes Dev 13:2758-2773
[Free Full Text] .- Rosen DR, Siddique T, Patterson D, Figlewicz DA, Sapp P, Hentati A, Donaldson D, Goto J, O'Regan JP, Deng HX (1993) Mutations in Cu/Zn superoxide dismutase gene are associated with familial amyotrophic lateral sclerosis. Nature 362:59-62[Medline].
- Schmechel DE, Saunders AM, Strittmatter WJ, Crain BJ, Hulette CM, Joo SH, Periack-Vance MA, Goldgaber D, Roses AD (1993) Increased amyloid
[Abstract/Free Full Text] .- Sen S, Churchill GA (2001) A statistical framework for quantitative trait mapping. Genetics 159:371-387
[Abstract/Free Full Text] .- Stockinger W, Brandes C, Fasching D, Hermann M, Gotthardt M, Herz J, Schneider WJ, Nimpf J (2000) The reelin receptor ApoER2 recruits JNK-interacting proteins-1 and -2. J Biol Chem 275:25625-25632
[Abstract/Free Full Text] .- Sweet HO, Bronson RT, Johnson KR, Cook SA, Davisson MT (1996) Scrambler, a new neurological mutation of the mouse with abnormalities of neuronal migration. Mamm Genome 7:798-802[ISI][Medline].
- Trommsdorff M, Borg JP, Margolis B, Herz J (1998) Interaction of cytosolic adaptor proteins with neuronal apolipoprotein E receptors and the amyloid precursor protein. J Biol Chem 273:33556-33560
[Abstract/Free Full Text] .- Wahlsten D, Andison M (1991) Patterns of cerebellar foliation in recombinant inbred mice. Brain Res 557:184-189[Medline].
- Weeber EJ, Beffert U, Jones C, Christian JM, Forster E, Sweatt JD, Herz J (2002) Reelin and ApoE receptors cooperate to enhance hippocampal synaptic plasticity and learning. J Biol Chem 277:39944-39952
[Abstract/Free Full Text] .- Yoneshima H, Nagata E, Matsumoto M, Yamada M, Nakajima K, Miyata T, Ogawa M, Mikoshiba K (1997) A novel neurological mutant mouse, yotari, which exhibits reeler-like phenotype but expresses CR-50 antigen/reelin. Neurosci Res 29:217-223[ISI][Medline].
Copyright © 2003 Society for Neuroscience 0270-6474/03/231187-06$05.00/0
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