Toxin Tx7335

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== Relevance ==
== Relevance ==
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This change in configuration causes the activation of pH-gated potassium channels [[Image:1218_Voltage-gated_Channels.jpg]] that no other 3FTx has been shown to cause. Activation of this potassium channel is caused by increasing the mean open time of the channel and the open probability of the channel. These changes are dose-dependent. The addition of 2 micromolar Tx7335 caused a roughly 8-fold increase in open-gate time for the wild-type KcsA and roughly 13-fold increase in the pmut3 KcsA. The open probability increased about 40-fold for the wild-type and about 90-fold for the pmut3 channels. The toxin added to the intracellular side of the cells did not cause any change in the channel (4).
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This change in configuration causes the activation of pH-gated potassium channels [[Media:Example.ogg]] that no other 3FTx has been shown to cause. Activation of this potassium channel is caused by increasing the mean open time of the channel and the open probability of the channel. These changes are dose-dependent. The addition of 2 micromolar Tx7335 caused a roughly 8-fold increase in open-gate time for the wild-type KcsA and roughly 13-fold increase in the pmut3 KcsA. The open probability increased about 40-fold for the wild-type and about 90-fold for the pmut3 channels. The toxin added to the intracellular side of the cells did not cause any change in the channel (4).
The Potassium-ion channel in Streptomyces lividans (KcsA) are a good model for K+-selective ion channel pores found in humans. These pores are necessary in the cardiac and neuronal electronic signaling pathways. Failure in these pores has been linked to cardiac and neuronal diseases as well as various cancers (4). Ion flow through these channels are generally regulated by the activation due to a stimulus like voltage increase or ligand bonding and inactivation that is not dependent on a stimulus. Tx7335 is a ligand binding activator, and only activated the KcsA single channel system when it was introduced outside of the cell. This means that it does not directly affect the internal pH gate, but rather shifts the equilibrium towards the conductive state of the inactivation gate. Since this protein has a unique pathway to affect KcsA, it will be useful in studying the allosteric regulation of the KcsA, and other potassium channel inactivation by extension.
The Potassium-ion channel in Streptomyces lividans (KcsA) are a good model for K+-selective ion channel pores found in humans. These pores are necessary in the cardiac and neuronal electronic signaling pathways. Failure in these pores has been linked to cardiac and neuronal diseases as well as various cancers (4). Ion flow through these channels are generally regulated by the activation due to a stimulus like voltage increase or ligand bonding and inactivation that is not dependent on a stimulus. Tx7335 is a ligand binding activator, and only activated the KcsA single channel system when it was introduced outside of the cell. This means that it does not directly affect the internal pH gate, but rather shifts the equilibrium towards the conductive state of the inactivation gate. Since this protein has a unique pathway to affect KcsA, it will be useful in studying the allosteric regulation of the KcsA, and other potassium channel inactivation by extension.

Revision as of 15:27, 29 April 2019

Toxin Tx7335: A Three Finger Protein

1F94, resolution 1.55Å

Drag the structure with the mouse to rotate

References

1) Shin, F.C., et al. “Crystal Structure of a Three Finger Toxin from M Fulvius.” Cell, 18 May 2016, www.rcsb.org/structure/4RUD.

2) Sarika, Chaitra, and Priyanka Purkayastha. “Differential Structural Interactions of Three-Finger Family Proteins from Snake Venoms on Acetylcholine Receptors.” Maryville Library Off-Campus Access, scifinder-cas-org.proxy.library.maryville.edu/scifinder/view/scifinder/scifinderExplore.jsf.

3) Mark J Margres, Karalyn Aronow, Jacob Loyacano and Darin R Rokyta. “The venom-gland transcriptome of the eastern coral snake (Micrurus fulvius) reveals high venom complexity in the intragenomic evolution of venoms” BMC Genomics, 2 August 2013, https://bmcgenomics.biomedcentral.com/articles/10.1186/1471-2164-14-531.


4) Yuri N Utkin. “Last decade update for three-finger toxins: Newly emerging structures and biological activities” Baishideng Publishing Group Inc., Jan 7, 2019, http://resolver.ebscohost.com.proxy.library.maryville.edu/openurl?sid=EBSCO%3acmedm&genre=article&issn=19498454&ISBN=&volume=10&issue=1&date=20190107&spage=17&pages=17-27&title=World+Journal+Of+Biological+Chemistry&atitle=Last+decade+update+for+three-finger+toxins%3a+Newly+emerging+structures+and+biological+activities.&aulast=Utkin+YN&id=DOI%3a10.4331%2fwjbc.v10.i1.17&site=ftf-live

5) Iván O. Rivera-Torres, Tony B. Jin, Martine Cadene, Brian T. Chait, & Sébastien F. Poget. “Discovery and characterisation of a novel toxin from Dendroaspis angusticeps, named Tx7335, that activates the potassium channel KcsAz” Scientific Reports, 5 April 2016, https://www-nature-com.proxy.library.maryville.edu/articles/srep23904

6) OpenStax. “The Action Potential.” Anatomy and Physiology, OpenStax, 6 Mar. 2013, opentextbc.ca/anatomyandphysiology/chapter/12-4-the-action-potential/.

  1. Hanson, R. M., Prilusky, J., Renjian, Z., Nakane, T. and Sussman, J. L. (2013), JSmol and the Next-Generation Web-Based Representation of 3D Molecular Structure as Applied to Proteopedia. Isr. J. Chem., 53:207-216. doi:http://dx.doi.org/10.1002/ijch.201300024
  2. Herraez A. Biomolecules in the computer: Jmol to the rescue. Biochem Mol Biol Educ. 2006 Jul;34(4):255-61. doi: 10.1002/bmb.2006.494034042644. PMID:21638687 doi:10.1002/bmb.2006.494034042644

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Ben Difani, Michal Harel

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