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Transcript
Molecular Cell Biology
Intermediate Filaments
Cooper
Introduction

Filaments 10 nm wide => “intermediate”

Present in Metazoa / Animals
• i.e. not Plants or Unicellular Organisms

Complex Gene Superfamily
• 70 in Human Genome

Specific Expression at Different Times and Places
Intermediate Filament
Biochemical Properties In Vitro

Very stable. Little subunit exchange.

Very strong. Filaments do not break.
• MT’s strong but brittle
• Actin weak
Intermediate Filament
Potential Functions In Vivo

Mechanical Strength of Cytoplasm

Help a Layer of Epithelial Cells Resist Shear
Stress - Filaments Connect to Cell-cell
Junctions

Hold Nucleus in Center of Cell
Intermediate
Filament
Structure &
Assembly
Intermediate
Filaments
by EM:
Filament
Unraveling
Classes of Intermediate Filaments
Name
Acidic Keratin
Basic Keratin
Cells
Epithelia
Epithelia
Number of
Isoforms
~15
~15
Mesenchy ma l
Muscle
Gli a
1
1
1
53
52
51
III
Vim entin
Desmi n
Gli al Fibrill ary
Acidic Protein (GFAP)
Peripher in
Neurons
>1
58
IV
IV
IV
IV
Neurofila ment H
Neurofila ment M
Neurofila ment L
Nestin
Neurons
Neurons
Neurons
Gli al scars, Early
neu rons & muscle
1
1
1
1
V
V
Lami n A
Lami n B
All
All
1
1
Class
I
II
III
III
III
Size
(kD)
40-60
50-70
Polymers
Obli gate Heteropolymers
One acidic + one basic
Homopolymers (singl e
type of subun it) or
co-polymers w/ each
other at varied ratios
135-150
105-110 H & M each require
60-70 L for polymer
240
60-75
60-75
Homopolymers or
Heteropolymer
Regulation of IF Assembly

Notoriously Stable
• No Nucleotide

Filaments Move Little
• Precursors Move More

Disassemble Somewhat during Mitosis
• Phosphorylation by Cyclin-depen Kinase
Vimentin Filaments in a Cultured Cell
Vimentin

All Cells in Early Development

Cage Around Nucleus

Interacts with Mt’s

Vimentin Knockout Mouse
• Initially normal at gross inspection
• Cultured cells have altered properties of
uncertain significance
FRAP of Vimentin
vs. Keratin in One
Cell
Left: Vimentin (Green)
Right: Keratin (Red)
10 min time intervals
Dynamics of Keratin Particles in Periphery
Qui ckTime™ and a
Photo - JPEG decompr essor
are needed to see thi s pi cture.
11 micrometers
over 10 minutes
QuickTime™ and a
Photo - JPEG decompressor
are needed to see this pict ure.
18 micrometers
over 10 minutes
Desmin

Expressed in Muscle

Elastic Elements to Prevent Over-stretching

Connects / Aligns Z lines

Knockout Mouse - Deranged Myofibril
Architecture
Keratins

Expressed in Epithelia

Keratin Filaments Connect to Desmosome and
Hemidesmosomes

Differentiation of Epidermis includes Production of
Massive Amounts of Keratin

Provides Outer Protection of Skin

Composes Hair, Nails, Feathers, etc.
Density of Keratin Filaments in Outer
Epidermis Layers
Keratin Mutations are Basis for
Human Epidermal Diseases

Structure/Function Analysis of Keratin
Assembly

Point Mutation in Terminal Domain Fails to
Assemble

Mutant is Dominant, even in Low Amounts,
in Cultured Cells and Mice
Epidermolysis Bullosa Simplex
Wild-type
Mutant
Keratins and EBS
Neurons

Neurofilament H, M, L Copolymer

Prevent Axon Breakage

Diseases with Clumps of Neurofilaments
• Superoxide dismutase model for ALS
• Clumps are secondary, not causative
Neurofilament Transport in Axons
QuickTime™ and a
Sorenson Video 3 decompressor
are needed to see this picture.
Photobleached Zone in the Middle
Neurofilament Transport in Axons
QuickTime™ and a
Sorenson Video 3 decompressor
are needed to see this picture.
Photobleached Zone in the Middle
Lamins

Square Lattice on Inner Surface of Nuclear Membrane

Present in Metazoans (Animals, not Plants or
unicellular organisms)

Mitosis Breakdown
• Phosphorylation of A & C by Cyclin-depen Kinase
• B remains with Membrane

Mutations Cause Accelerated Aging Diseases
• Progerias - Dominant Mutations
EM of Nuclear Lamina
Nuclear Pores
End