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This course is a short series of lectures on Statistical Bioinformatics. Topics covered are listed in the Table of Contents. The notes were preparedby Ewa Paszek, Lukasz Wita and Marek Kimmel. The development of this course has been supported by NSF 0203396 grant.

Gene networks.

A gene regulatory network (also called a GRN or genetic regulatory network, ) is a collection of DNA segments in a cell which interact with each other and with other substances in the cell, thereby governing the rates at which genes are transcribed into mRNA. Genes can be viewed as nodes in such a network, with input being proteins such as transcription factors , and outputs being the level of gene expression. The node itself can also be viewed as a function which can be obtained by combining basic functions upon the inputs (in the Boolean network these are boolean functions or gates computed using the basic AND OR and NOT gates in electronics). These functions have been interpreted as performing a kind information processing within cell which determine cellular behaviour. The basic drivers within cells are levels of some proteins, which determine both spatial (tissue related) and temporal (developmental stage) co-ordinates of the cell, as a kind of "cellular memory". The gene networks are only beginning to be understood, and it is a next step for biology to attempt to deduce the functions for each gene "node", to assist in modeling behaviour of a cell. Mathematical models of GRNs have been developed to allow predictions of the models to be tested. Various modeling techniques have been used, including boolean networks, Petri nets, Bayesian networks, and sets of differential equations. Conversely, techniques have been proposed for generating models of GRNs that best explain a set of time series observations.

One gene can affect the expression of another gene by binding of the gene product of one gene to the promoter region of another gene. Looking at more than two genes, we refer to the regulatory network as the regulatory interactions between the genes. If we have a large number of measurements of the expression level of a number of genes, we should be able to model or reverse engineer the regulatory network that controls their expression level. The problem can be attacked in two fundamentally different ways: using time-series data and using steady-state data of gene knockout.

GRNs act as analog biochemical computers to specify the identity and level of expression of groups of target genes. Central to this computation are DNA recognition sequences with which transcription factors associate. When active transcription factors associate with the promontory region of target genes, they can function to specifically repress (down-regulate) or induce (up-regulate) synthesis of the corresponding RNA. The immediate molecular output of a gene regulatory network is the constellation of RNAs and proteins encoded by network target genes. The resulting cellular outputs are changes in the structure, metabolic capacity, or behavior of the cell mediated by new expression of up-regulated proteins and elimination of down-regulated proteins.

GRNs are remarkably diverse in their structure, but several basic properties are illustrated in the figure below (Figure1.) . In this example, two different signals converge on a single target gene where the cis-regulatory elements provide for an integrated output in response to the two inputs. Signal molecule A triggers the conversion of inactive transcription factor A (green oval) into an active form that binds directly to the target gene's cis-regulatory sequence. The process for signal B is more complex. Signal B triggers the separation of inactive B (red oval) from an inhibitory factor (yellow rectangle). B is then free to form an active complex that binds to the active A transcription factor on the cis-regulatory sequence. The net output is expression of the target gene at a level determined by the action of factors A and B. In this way, cis-regulatory DNA sequences, together with the proteins that assemble on them, integrate information from multiple signaling inputs to produce an appropriately regulated readout. A more realistic network might contain multiple target genes regulated by signal A alone, others by signal B alone, and still others by the pair of A and B. Co-regulated target genes often code for proteins that act together to build a specific cell structure or to effect a concerted change in cell function. For example, genes encoding components of the multiprotein proteasome machine (see The Machines of Life) are co-regulated at the RNA level. This was shown by microarray gene chip analyses in yeast cells, and each gene was found to possess a similar cis-regulatory DNA sequence that mediates binding of a particular transcription factor. Similarly, a bacterium may respond to a shortage of its preferred energy source by activating expression of genes whose protein products function in a biochemical pathway that allows it to use a different, more abundant source of energy.

The gene regulatory network.

Boolean Networks
Probabilistic Boolean Networks
Bayesian Networks

Questions & Answers

it is the relatively stable flow of income
Chidubem Reply
what is circular flow of income
Divine Reply
branches of macroeconomics
SHEDRACK Reply
what is Flexible exchang rate?
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is gdp a reliable measurement of wealth
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introduction to econometrics
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Tom
Why is unemployment rate never zero at full employment?
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bcoz of existence of frictional unemployment in our economy.
Umashankar
what is flexible exchang rate?
poudel
due to existence of the pple with disabilities
Abdulraufu
the demand of a good rises, causing the demand for another good to fall
Rushawn Reply
is it possible to leave every good at the same level
Joseph
I don't think so. because check it, if the demand for chicken increases, people will no longer consume fish like they used to causing a fall in the demand for fish
Anuolu
is not really possible to let the value of a goods to be same at the same time.....
Salome
Suppose the inflation rate is 6%, does it mean that all the goods you purchase will cost 6% more than previous year? Provide with reasoning.
Geetha Reply
Not necessarily. To measure the inflation rate economists normally use an averaged price index of a basket of certain goods. So if you purchase goods included in the basket, you will notice that you pay 6% more, otherwise not necessarily.
Waeth
discus major problems of macroeconomics
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what is the problem of macroeconomics
Yoal
Economic growth Stable prices and low unemployment
Ephraim
explain inflationcause and itis degre
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what is inflation
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increase in general price levels
WEETO
Good day How do I calculate this question: C= 100+5yd G= 2000 T= 2000 I(planned)=200. Suppose the actual output is 3000. What is the level of planned expenditures at this level of output?
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how to calculate actual output?
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Beshir
Criteria for determining money supply
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Muhammad
Aggregate demand
Mohammed
C=k100 +9y and i=k50.calculate the equilibrium level of output
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money as unit of account means what?
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A unit of account is something that can be used to value goods and services and make calculations
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Muhammad
I want to know how can we define macroeconomics in one line
Muhammad
it must be .9 or 0.9 no Mpc is greater than 1 Y=100+.9Y+50 Y-.9Y=150 0.1Y/0.1=150/0.1 Y=1500
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hi can someone help me on this question If a negative shocks shifts the IS curve to the left, what type of policy do you suggest so as to stabilize the level of output? discuss your answer using appropriate graph.
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if interest rate is increased this will will reduce the level of income shifting the curve to the left ◀️
Kalombe
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Source:  OpenStax, Introduction to bioinformatics. OpenStax CNX. Oct 09, 2007 Download for free at http://cnx.org/content/col10240/1.3
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