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Literature DB >> 8449987

The transport properties of axonal microtubules establish their polarity orientation.

Abstract

It is well established that axonal microtubules (MTs) are uniformly oriented with their plus ends distal to the neuronal cell body (Heidemann, S. R., J. M. Landers, and M. A. Hamborg. 1981. J. Cell Biol. 91:661-665). However, the mechanisms by which these MTs achieve their uniform polarity orientation are unknown. Current models for axon growth differ with regard to the contributions of MT assembly and transport to the organization and elaboration of the axonal MT array. Do the transport properties or assembly properties of axonal MTs determine their polarity orientation? To distinguish between these possibilities, we wished to study the initiation and outgrowth of axons under conditions that would arrest MT assembly while maintaining substantial levels of preexisting polymer in the cell body that could still be transported into the axon. We found that we could accomplish this by culturing rat sympathetic neurons in the presence of nanomolar levels of vinblastine. In concentrations of the drug up to and including 100 nM, the neurons actively extend axons. The vinblastine-axons are shorter than control axons, but clearly contain MTs. To quantify the effects of the drug on MT mass, we compared the levels of polymer throughout the cell bodies and axons of neurons cultured overnight in the presence of 0, 16, and 50 nM vinblastine with the levels of MT polymer in freshly plated neurons before axon outgrowth. Without drug, the total levels of polymer increase by roughly twofold. At 16 nM vinblastine, the levels of polymer are roughly equal to the levels in freshly plated neurons, while at 50 nM, the levels of polymer are reduced by about half this amount. Thus, 16 nM vinblastine acts as a "kinetic stabilizer" of MTs, while 50 nM results in some net MT disassembly. At both drug concentrations, there is a progressive increase in the levels of MT polymer in the axons as they grow, and a corresponding depletion of polymer from the cell body. These results indicate that highly efficient mechanisms exist in the neuron to transport preassembled MTs from the cell body into the axon. These mechanisms are active even at the expense of the cell body, and even under conditions that promote some MT disassembly in the neuron. MT polarity analyses indicate that the MTs within the vinblastine-axons, like those in control axons, are uniformly plus-end-distal.(ABSTRACT TRUNCATED AT 400 WORDS)

Entities: Chemical Species

Mesh：

Substances：
Vinblastine

Year: 1993 PMID： 8449987 PMCID： PMC2119746 DOI： 10.1083/jcb.120.6.1427

Source DB: PubMed Journal: J Cell Biol ISSN： 0021-9525 Impact factor: 10.539

45 in total

1. Improved methods for using glass coverslips in cell culture and electron microscopy.

Authors: D S Whitlon; P W Baas
Journal: J Histochem Cytochem Date: 1992-06 Impact factor: 2.479

2. Microtubule polarity reversal accompanies regrowth of amputated neurites.

Authors: P W Baas; L A White; S R Heidemann
Journal: Proc Natl Acad Sci U S A Date: 1987-08 Impact factor: 11.205

3. Regional differences in microtubule dynamics in the axon.

Authors: F J Ahmad; T P Pienkowski; P W Baas
Journal: J Neurosci Date: 1993-02 Impact factor: 6.167

4. Microtubule dynamics in axons and dendrites.

Authors: P W Baas; T Slaughter; A Brown; M M Black
Journal: J Neurosci Res Date: 1991-09 Impact factor: 4.164

5. Gamma-tubulin is a centrosomal protein required for cell cycle-dependent microtubule nucleation.

Authors: H C Joshi; M J Palacios; L McNamara; D W Cleveland
Journal: Nature Date: 1992-03-05 Impact factor: 49.962

6. Effects of vinblastine, podophyllotoxin and nocodazole on mitotic spindles. Implications for the role of microtubule dynamics in mitosis.

Authors: M A Jordan; D Thrower; L Wilson
Journal: J Cell Sci Date: 1992-07 Impact factor: 5.285

7. Gamma-tubulin distribution in the neuron: implications for the origins of neuritic microtubules.

Authors: P W Baas; H C Joshi
Journal: J Cell Biol Date: 1992-10 Impact factor: 10.539

8. Differential behavior of photoactivated microtubules in growing axons of mouse and frog neurons.

Authors: S Okabe; N Hirokawa
Journal: J Cell Biol Date: 1992-04 Impact factor: 10.539

9. Processes induced by tau expression in Sf9 cells have an axon-like microtubule organization.

Authors: P W Baas; T P Pienkowski; K S Kosik
Journal: J Cell Biol Date: 1991-12 Impact factor: 10.539

10. Slow axonal transport mechanisms move neurofilaments relentlessly in mouse optic axons.

Authors: R J Lasek; P Paggi; M J Katz
Journal: J Cell Biol Date: 1992-05 Impact factor: 10.539

46 in total

1. Transport of Neuronal BC1 RNA in Mauthner Axons.

Authors: Ilham A Muslimov; Margaret Titmus; Edward Koenig; Henri Tiedge
Journal: J Neurosci Date: 2002-06-01 Impact factor: 6.167

2. Neurofilaments are transported rapidly but intermittently in axons: implications for slow axonal transport.

Authors: S Roy; P Coffee; G Smith; R K Liem; S T Brady; M M Black
Journal: J Neurosci Date: 2000-09-15 Impact factor: 6.167

3. The role of the cytoskeleton in the life cycle of viruses and intracellular bacteria: tracks, motors, and polymerization machines.

Authors: E L Bearer; P Satpute-Krishnan
Journal: Curr Drug Targets Infect Disord Date: 2002-09

The transport properties of axonal microtubules establish their polarity orientation.

1. Improved methods for using glass coverslips in cell culture and electron microscopy.

2. Microtubule polarity reversal accompanies regrowth of amputated neurites.

3. Regional differences in microtubule dynamics in the axon.

4. Microtubule dynamics in axons and dendrites.

5. Gamma-tubulin is a centrosomal protein required for cell cycle-dependent microtubule nucleation.

6. Effects of vinblastine, podophyllotoxin and nocodazole on mitotic spindles. Implications for the role of microtubule dynamics in mitosis.

7. Gamma-tubulin distribution in the neuron: implications for the origins of neuritic microtubules.

8. Differential behavior of photoactivated microtubules in growing axons of mouse and frog neurons.

9. Processes induced by tau expression in Sf9 cells have an axon-like microtubule organization.

10. Slow axonal transport mechanisms move neurofilaments relentlessly in mouse optic axons.

1. Transport of Neuronal BC1 RNA in Mauthner Axons.

2. Neurofilaments are transported rapidly but intermittently in axons: implications for slow axonal transport.

3. The role of the cytoskeleton in the life cycle of viruses and intracellular bacteria: tracks, motors, and polymerization machines.

4. Differential roles of microtubule assembly and sliding in proplatelet formation by megakaryocytes.

5. Functional analysis of dynactin and cytoplasmic dynein in slow axonal transport.

Review 6. A composite model for establishing the microtubule arrays of the neuron.

Review 7. Hooks and comets: The story of microtubule polarity orientation in the neuron.

8. Mitotic motors coregulate microtubule patterns in axons and dendrites.

9. Microtubule assembly in growing dendrites.

10. CNP/cGMP signaling regulates axon branching and growth by modulating microtubule polymerization.