8.4 Modeling cell assemblies (Page 3/9)

Page 3 / 9

\frac{d V}{d t} = \frac{(V_{l e a k} - V) G_{m} + \sum (V_{c o m p} - V) G_{c o r e} + I_{c h a n n e l s} + I_{s y n}}{C_{m}}

Variable	Description
V	Compartment Potential
$E_{l e a k}$	Outside Potential
$G_{m}$	Membrane conductance
$E_{c o m p}$	Neighbor compartment voltage
$G_{c o r e}$	Conductance between Compartments
$I_{c h a n n e l s}$	Ion channel current (only in soma compartment)
$C_{m}$	Membrane capacitance

Ion channels

The cell dynamics use a model that is derived from the Hodgkin-Huxley model. The ion currents take the general form of a driving force (which is due to the different concentrations of the ions on the inside and outside of the cell) being multiplied by a conductance term (the reciprocal of resistance) and a product of voltage dependant variables that indicate the fraction of the ion channels open. For example, the sodium current is:

I_{N a} = (V_{N a} - V_{s o m a}) G_{N a} m^{3} h .

Where $V_{N a}$ is the reversal potential (indicating the concentration of $N a^{+}$ in the surrounding fluid). $G_{N a}$ is the conductance of $N a^{+}$ . $m$ is called the activation variable of the $N a^{+}$ channels and $h$ is the inactivation variable. They are governed by the following differential equations:

\begin{matrix} \frac{d m}{d t} = α_{m} (1 - m) - β_{m} m \end{matrix}

Here $α_{m}$ is the opening rate and $β_{m}$ is the closing rate. These rates are dependent on the soma potential. A, B and C are fitting parameters that will later be prescribed.

\begin{matrix} α_{m} & = \frac{A (V_{s o m a} - B)}{1 - e^{(B - V_{s o m a}) / C}} & β_{m} & = \frac{A (B - V_{s o m a})}{1 - e^{(V_{s o m a} - B) / C}} \end{matrix}

The inactivation variable $h$ is slightly different, and has its own fitting parameters.

\begin{matrix} \frac{d h}{d t} & = α_{h} (1 - h) - β_{h} h \\ α_{h} & = \frac{A (B - V_{s o m a})}{1 - e^{(V_{s o m a} - B) / C}} & β_{h} & = \frac{A}{1 + e^{(B - V_{s o m a}) / C}} \end{matrix}

The $K^{+}$ channels are similar. There is only one gating variable $n$ .

\begin{matrix} I_{K} & = (V_{K} - V_{s o m a}) G_{K} n^{4} \\ \frac{d h}{d t} & = α_{h} (1 - h) - β_{h} h \\ α_{h} & = \frac{A (V_{s o m a} - B)}{1 - e^{(B - V_{s o m a}) / C}} & β_{h} & = \frac{A (B - V_{s o m a})}{1 - e^{(V_{s o m a} - B) / C}} \end{matrix}

For more details on the Hodgkin Huxley model visit (External Link) or look at the series of papers this module is designed after.

The change in net potential due the calcium flow is negligible. However, we still need to track it in order to control the Calcium dependent Potassium channels. As cell repeatedly fires calcium will build up leading to stronger repolarizations this will help allow for firing rate adaptation and provide the assembly a mechanism through which it will die out eventually.

\begin{matrix} I_{q} & = (V_{q} - V_{s o m a}) G_{q} n^{4} \\ \frac{d q}{d t} & = α_{q} (1 - h) - β_{q} q \\ α_{q} & = \frac{A (V_{s o m a} - B)}{1 - e^{(B - V_{s o m a}) / C}} & β_{q} & = \frac{A (B - V_{s o m a})}{1 - e^{(V_{s o m a} - B) / C}} \end{matrix}

The Calcium dependent Potassium channels:

\begin{matrix} I_{K (C a)} = (V_{K} - V_{S o m a}) G_{K (C a)} [C a_{A P}] \\ \frac{d [C a_{A P}]}{d t} = (V_{C a} - V_{s o m a}) ρ_{A P} q^{5} - δ_{A P} [C a_{A P}] \end{matrix}

$[C a_{A P}]$ is the intracellular calcium level. Constants $ρ_{A P}$ and $δ_{A P}$ are the rates of calcium ion influx and efflux (decay).

The second form of Calcium comes through NMDA channels that are located on the post-synapse. It is important to separate this Calcium source since it enters and leaves the cell with different time constants due to the different method it enters the cell. This contribution will be discussed in more details in the next section. The Calcium pool $[C a_{N M D A}]$ will be added to the total $C a^{2 +}$ count changing the total current from Calcium dependent Potassium channels to:

I_{K (C a)} = (V_{K} - V_{S o m a}) G_{K (C a)} ([C a_{A P}] + [C a_{N M D A}])

Synaptic connections

Cells communicate with synaptic connections where the bouton and post-synapse meet. The firing cell releases neurotransmitter into the synaptic cleft. These chemical open up ion channels in the postsynaptic receptor cell. This allows either a gain in postsynaptic potential (if the presynaptic cell is excitatory) or a depression in potential (for a inhibitory cell). The model for the synaptic current is show below:

Questions & Answers

what is microbiology

Agebe Reply

What is a cell

Odelana Reply

what is cell

Mohammed

how does Neisseria cause meningitis

Nyibol Reply

what is microbiologist

Muhammad Reply

what is errata

Muhammad

is the branch of biology that deals with the study of microorganisms.

Ntefuni Reply

What is microbiology

Mercy Reply

studies of microbes

Louisiaste

when we takee the specimen which lumbar,spin,

Ziyad Reply

How bacteria create energy to survive?

Muhamad Reply

Bacteria doesn't produce energy they are dependent upon their substrate in case of lack of nutrients they are able to make spores which helps them to sustain in harsh environments

_Adnan

But not all bacteria make spores, l mean Eukaryotic cells have Mitochondria which acts as powerhouse for them, since bacteria don't have it, what is the substitution for it?

Muhamad

they make spores

Louisiaste

what is sporadic nd endemic, epidemic

Aminu Reply

the significance of food webs for disease transmission

Abreham

food webs brings about an infection as an individual depends on number of diseased foods or carriers dully.

Mark

explain assimilatory nitrate reduction

Esinniobiwa Reply

Assimilatory nitrate reduction is a process that occurs in some microorganisms, such as bacteria and archaea, in which nitrate (NO3-) is reduced to nitrite (NO2-), and then further reduced to ammonia (NH3).

Elkana

This process is called assimilatory nitrate reduction because the nitrogen that is produced is incorporated in the cells of microorganisms where it can be used in the synthesis of amino acids and other nitrogen products

Elkana

Examples of thermophilic organisms

Shu Reply

Give Examples of thermophilic organisms

Shu

advantages of normal Flora to the host

Micheal Reply

Prevent foreign microbes to the host

Abubakar

they provide healthier benefits to their hosts

ayesha

They are friends to host only when Host immune system is strong and become enemies when the host immune system is weakened . very bad relationship!

Mark

what is cell

faisal Reply

cell is the smallest unit of life

Fauziya

cell is the smallest unit of life

Akanni

Innocent

cell is the structural and functional unit of life

Hasan

is the fundamental units of Life

Musa

what are emergency diseases

Micheal Reply

There are nothing like emergency disease but there are some common medical emergency which can occur simultaneously like Bleeding,heart attack,Breathing difficulties,severe pain heart stock.Hope you will get my point .Have a nice day ❣️

_Adnan

define infection ,prevention and control

Innocent

I think infection prevention and control is the avoidance of all things we do that gives out break of infections and promotion of health practices that promote life

Lubega

Heyy Lubega hussein where are u from?

_Adnan

en français

Adama

which site have a normal flora

ESTHER Reply

Many sites of the body have it Skin Nasal cavity Oral cavity Gastro intestinal tract

Safaa

skin

Asiina

skin,Oral,Nasal,GIt

Sadik

How can Commensal can Bacteria change into pathogen?

Sadik

How can Commensal Bacteria change into pathogen?

Sadik

all

Tesfaye

by fussion

Asiina

what are the advantages of normal Flora to the host

Micheal

what are the ways of control and prevention of nosocomial infection in the hospital

Micheal

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Source: OpenStax, The art of the pfug. OpenStax CNX. Jun 05, 2013 Download for free at http://cnx.org/content/col10523/1.34

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