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Diversity of Form and

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Diversity of Form and Function of Voltage-Gated Potassium Channels 80 Family Members 5 Architectures 3 Gene SubFamilies Classes to highlight function: – PowerPoint PPT presentation

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Title: Diversity of Form and


1
Diversity of Form and Function of Voltage- Gated
Potassium Channels
80 Family Members 5 Architectures 3 Gene
SubFamilies
Classes to highlight function 1. Shaker
2. KCa 3. KIR
2
3 Gene SubFamilies 6TM 2 TM 4TM Evolutionary
tree does not cluster by architecture and
architectures do not align to specific function.
3
Frequency-modulated code The stronger the
injected current, the higher the rate of AP
frequency
4
IK vs. IA Function can be separated not only
pharmacologically, but physiologically by Vh.
The former drives repolarization while the later
spaces successive AP more widely. Each act to
dampen excitability.
5
3 types of KCa BK, Maxi K IK, fast AHP SK, slow
AHP
Why are state kinetic diagrams so complex for
this type of calcium-activated channel?
6
Spike Frequency Adaptation Membranes may
hyperpolarize twice and different KCa channels
drive the slow and fast component. Called
Phasic Firing Patterns
7
Bursting Pacemaker Electrical Activity
8
KIR The anomalous rectifiers
9
Ih can increase cardiac pacemaker activity
10
Cl Channels are currently classified according to
the activating stimulus to gate the channel,
rather than by molecular structure
11
Fatt and Collaborators First discovery of
the Calcium Action Potential What is a
Calcium Spike? Calcium Shapes the Regenerative
A.P. And is in EVERY excitable cell.
12
  • Internal Calcium Three Best Studied Roles
  • Contraction of Muscle
  • Secretion
  • Gating

Why is calcium said to be The Ion? How does it
act to be A Second Messenger?
13
Calcium-dependent Exocytosis -
Neurotransmitters and Digestive Enzymes
  • Probability of NT
  • release is proportional
  • to Ca3.9
  • 2 Sources of Calcium
  • PM Ca Channels
  • Intracellular
  • Storing Organelles
  • 100s of Docking
  • Associated Proteins!

14
Resting Calcium Concentration In most cells 30
200 nM Increases in calcium measured with
fluorescent Ca indicators small rise and slow
fall.. Is this what physiologically occurs?
15
  1. 1970s Llinas HVA and LVA
  2. 1988 Tsien T and L type
  3. 1990s Pharmacology P/Q, N, and R type
  4. 2000 Molecular Structural Architecture

16
Therefore the nominclature following molecular
era is still a mix of phenomenological and
cloning classification!
17
Physiological time course of Inactivation of
calcium channels is likely much shorter
than biophysical experiments.. Due to high
use of barium to visualize the small currents.
2 Pulse To allow the internal Ca entry and then
measure fraction of Ca channels that are
inactivated.
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