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Literature DB >> 9190213

Functional interactions between the proline-rich and repeat regions of tau enhance microtubule binding and assembly.

B L Goode¹, P E Denis, D Panda, M J Radeke, H P Miller, L Wilson, S C Feinstein.

Abstract

Tau is a neuronal microtubule-associated protein that promotes microtubule assembly, stability, and bundling in axons. Two distinct regions of tau are important for the tau-microtubule interaction, a relatively well-characterized "repeat region" in the carboxyl terminus (containing either three or four imperfect 18-amino acid repeats separated by 13- or 14-amino acid long inter-repeats) and a more centrally located, relatively poorly characterized proline-rich region. By using amino-terminal truncation analyses of tau, we have localized the microtubule binding activity of the proline-rich region to Lys215-Asn246 and identified a small sequence within this region, 215KKVAVVR221, that exerts a strong influence on microtubule binding and assembly in both three- and four-repeat tau isoforms. Site-directed mutagenesis experiments indicate that these capabilities are derived largely from Lys215/Lys216 and Arg221. In marked contrast to synthetic peptides corresponding to the repeat region, peptides corresponding to Lys215-Asn246 and Lys215-Thr222 alone possess little or no ability to promote microtubule assembly, and the peptide Lys215-Thr222 does not effectively suppress in vitro microtubule dynamics. However, combining the proline-rich region sequences (Lys215-Asn246) with their adjacent repeat region sequences within a single peptide (Lys215-Lys272) enhances microtubule assembly by 10-fold, suggesting intramolecular interactions between the proline-rich and repeat regions. Structural complexity in this region of tau also is suggested by sequential amino-terminal deletions through the proline-rich and repeat regions, which reveal an unusual pattern of loss and gain of function. Thus, these data lead to a model in which efficient microtubule binding and assembly activities by tau require intramolecular interactions between its repeat and proline-rich regions. This model, invoking structural complexity for the microtubule-bound conformation of tau, is fundamentally different from previous models of tau structure and function, which viewed tau as a simple linear array of independently acting tubulin-binding sites.

Entities: Chemical Gene

Mesh：

Substances：

Year: 1997 PMID： 9190213 PMCID： PMC276085 DOI： 10.1091/mbc.8.2.353

Source DB: PubMed Journal: Mol Biol Cell ISSN： 1059-1524 Impact factor: 4.138

78 in total

Review 1. Non-motor microtubule-associated proteins.

Authors: G Lee
Journal: Curr Opin Cell Biol Date: 1993-02 Impact factor: 8.382

2. Abnormal tau phosphorylation at Ser396 in Alzheimer's disease recapitulates development and contributes to reduced microtubule binding.

Authors: G T Bramblett; M Goedert; R Jakes; S E Merrick; J Q Trojanowski; V M Lee
Journal: Neuron Date: 1993-06 Impact factor: 17.173

3. The balance between tau protein's microtubule growth and nucleation activities: implications for the formation of axonal microtubules.

Authors: R Brandt; G Lee
Journal: J Neurochem Date: 1993-09 Impact factor: 5.372

Review 4. Tau as a marker for Alzheimer's disease.

Authors: E M Mandelkow; E Mandelkow
Journal: Trends Biochem Sci Date: 1993-12 Impact factor: 13.807

5. Purification and biochemical characterization of tubulin from the budding yeast Saccharomyces cerevisiae.

Authors: A Davis; C R Sage; L Wilson; K W Farrell
Journal: Biochemistry Date: 1993-08-31 Impact factor: 3.162

6. Phosphorylation of Ser262 strongly reduces binding of tau to microtubules: distinction between PHF-like immunoreactivity and microtubule binding.

Authors: J Biernat; N Gustke; G Drewes; E M Mandelkow; E Mandelkow
Journal: Neuron Date: 1993-07 Impact factor: 17.173

7. Microtubule-associated protein tau is required for axonal neurite elaboration by neuroblastoma cells.

Authors: T B Shea; M L Beermann; R A Nixon; I Fischer
Journal: J Neurosci Res Date: 1992-07 Impact factor: 4.164

8. The abnormal phosphorylation of tau protein at Ser-202 in Alzheimer disease recapitulates phosphorylation during development.

Authors: M Goedert; R Jakes; R A Crowther; J Six; U Lübke; M Vandermeeren; P Cras; J Q Trojanowski; V M Lee
Journal: Proc Natl Acad Sci U S A Date: 1993-06-01 Impact factor: 11.205

9. Increased microtubule stability and alpha tubulin acetylation in cells transfected with microtubule-associated proteins MAP1B, MAP2 or tau.

Authors: R Takemura; S Okabe; T Umeyama; Y Kanai; N J Cowan; N Hirokawa
Journal: J Cell Sci Date: 1992-12 Impact factor: 5.285

10. Brain microtubule-associated proteins modulate microtubule dynamic instability in vitro. Real-time observations using video microscopy.

Authors: N K Pryer; R A Walker; V P Skeen; B D Bourns; M F Soboeiro; E D Salmon
Journal: J Cell Sci Date: 1992-12 Impact factor: 5.285

96 in total

1. ZipA is a MAP-Tau homolog and is essential for structural integrity of the cytokinetic FtsZ ring during bacterial cell division.

Authors: D RayChaudhuri
Journal: EMBO J Date: 1999-05-04 Impact factor: 11.598

2. Mutations in tau gene exon 10 associated with FTDP-17 alter the activity of an exonic splicing enhancer to interact with Tra2 beta.

Authors: Zhihong Jiang; Hao Tang; Necat Havlioglu; Xiaochun Zhang; Stefan Stamm; Riqiang Yan; Jane Y Wu
Journal: J Biol Chem Date: 2003-03-20 Impact factor: 5.157

Functional interactions between the proline-rich and repeat regions of tau enhance microtubule binding and assembly.

Review 1. Non-motor microtubule-associated proteins.

2. Abnormal tau phosphorylation at Ser396 in Alzheimer's disease recapitulates development and contributes to reduced microtubule binding.

3. The balance between tau protein's microtubule growth and nucleation activities: implications for the formation of axonal microtubules.

Review 4. Tau as a marker for Alzheimer's disease.

5. Purification and biochemical characterization of tubulin from the budding yeast Saccharomyces cerevisiae.

6. Phosphorylation of Ser262 strongly reduces binding of tau to microtubules: distinction between PHF-like immunoreactivity and microtubule binding.

7. Microtubule-associated protein tau is required for axonal neurite elaboration by neuroblastoma cells.

8. The abnormal phosphorylation of tau protein at Ser-202 in Alzheimer disease recapitulates phosphorylation during development.

9. Increased microtubule stability and alpha tubulin acetylation in cells transfected with microtubule-associated proteins MAP1B, MAP2 or tau.

10. Brain microtubule-associated proteins modulate microtubule dynamic instability in vitro. Real-time observations using video microscopy.

1. ZipA is a MAP-Tau homolog and is essential for structural integrity of the cytokinetic FtsZ ring during bacterial cell division.

2. Mutations in tau gene exon 10 associated with FTDP-17 alter the activity of an exonic splicing enhancer to interact with Tra2 beta.

3. Concentration dependence of variability in growth rates of microtubules.

4. Tau induces cooperative Taxol binding to microtubules.

5. Evidence for two distinct binding sites for tau on microtubules.

6. Heterogeneous Tau-Tubulin Complexes Accelerate Microtubule Polymerization.

Review 7. Cellular factors modulating the mechanism of tau protein aggregation.

8. Visual arrestin binding to microtubules involves a distinct conformational change.

Review 9. The genetics of frontotemporal lobar degeneration.

10. Effect of Phosphorylation and O-GlcNAcylation on Proline-Rich Domains of Tau.