Precipitation (chemistry): Difference between revisions
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==The Process== | ==The Process== | ||
===Introduction | |||
The process by which a dissolved chemical species comes out of solution as a solid is called precipitation. Precipitation is often employed in bioseparation applications for protein purification and concentration, although it may be used to extract other compounds, such as nucleic acids and other cell structures. Precipitation is achieved by altering the solubility of a target protein in a solution to cause it to become insoluble and thus precipitate, allowing for this concentrated solid to be more easily extracted from the liquid phase (supernatant). | |||
===Solubility of Macromolecules=== | |||
Solubility is the property of a substance (solute) – in either gas, liquid, or solid phases – to dissolve in a liquid (called the solvent) and form a homogenous (single-phase) solution. The extent of which a solute dissolves in a solvent is its solubility, and is based on factors such as temperature, the similarity between the solute’s net charge and the solvent’s polarity, the formation of hydration layers, and the concentration of solutes already dissolved in the solvent, as well as the solvent’s ionic strength. | |||
Macromolecules (such as proteins and nucleic acids) are typically present in aqueous solvents. They are able to dissolve as a result of assuming a stable conformation in the solvent and then being surrounded by hydration layer(s). When placed in an aqueous solution, the macromolecules adopt a structure in which most hydrophobic (nonpolar) portions of the molecules gather inwards, and most hydrophilic (charged/polar) portions surround the exterior, guided to a final conformation that has the lowest Gibbs free energy. The attraction between the hydrophilic surface of the macromolecule and the polar water molecules creates an interface in which similarly-oriented water molecules associate with, and surround, the solute’s surface to form a highly ordered layer, called the hydration layer (also called the interfacial double layer). The formation of hydration layers enhances the solubility of macromolecules by greatly reducing inter-macromolecular dipole-dipole attraction and thus preventing their association with other solutes. | |||
==History== | ==History== |
Revision as of 15:29, 12 December 2010
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A brief overview of your bioseparation topic (be sure to put its name in bold in the first sentence) and the scope of the article goes here.Also see CZ:How to start a new article
The following list of sections may serve as a loose guideline for developing the body of your article. Before deciding to follow it, take a look at some other articles on subjects like your own. You may like their structure better and if so, adopt it.
The works cited in references 2-5 are all fake (and are borrowed from another Eduzendium template); their purpose is to serve as a formatting model for your own citations.
The Process
===Introduction
The process by which a dissolved chemical species comes out of solution as a solid is called precipitation. Precipitation is often employed in bioseparation applications for protein purification and concentration, although it may be used to extract other compounds, such as nucleic acids and other cell structures. Precipitation is achieved by altering the solubility of a target protein in a solution to cause it to become insoluble and thus precipitate, allowing for this concentrated solid to be more easily extracted from the liquid phase (supernatant).
Solubility of Macromolecules
Solubility is the property of a substance (solute) – in either gas, liquid, or solid phases – to dissolve in a liquid (called the solvent) and form a homogenous (single-phase) solution. The extent of which a solute dissolves in a solvent is its solubility, and is based on factors such as temperature, the similarity between the solute’s net charge and the solvent’s polarity, the formation of hydration layers, and the concentration of solutes already dissolved in the solvent, as well as the solvent’s ionic strength.
Macromolecules (such as proteins and nucleic acids) are typically present in aqueous solvents. They are able to dissolve as a result of assuming a stable conformation in the solvent and then being surrounded by hydration layer(s). When placed in an aqueous solution, the macromolecules adopt a structure in which most hydrophobic (nonpolar) portions of the molecules gather inwards, and most hydrophilic (charged/polar) portions surround the exterior, guided to a final conformation that has the lowest Gibbs free energy. The attraction between the hydrophilic surface of the macromolecule and the polar water molecules creates an interface in which similarly-oriented water molecules associate with, and surround, the solute’s surface to form a highly ordered layer, called the hydration layer (also called the interfacial double layer). The formation of hydration layers enhances the solubility of macromolecules by greatly reducing inter-macromolecular dipole-dipole attraction and thus preventing their association with other solutes.
History
This section should describe the invention and development of the process. If the section runs long, divide it into chronological subsections, for example:
Invention and early development
This subsection should provide some historical context for the development of your process, describe its invention, and name some early developers and/or applications.[1]
Recent developments
This section should discuss new developments in the field. Don't hesitate to drop in brief mentions of processes or features you don't intend to discuss in depth. By so doing you are planting seeds of articles which will eventually be developed by others.[2]
Design and Operation
Use lots of subsections here as you describe various aspects of the process .[3]
Applications
This section should discuss how the process is used in practice.[4]
Examples
If you have used a lot of equations in your article, this may be a good place to show an example of how they are used. See the article on the Antoine Equation for an example.
References
- ↑ John Q. Sample, Chromatography, a new analytical tool. City: Publisher, 1885.
- ↑ "New Directions for Flocculation," American Flocculation Society. 2006. Retrieved July 21, 2009 from http://www.amflocsoc.org/future_devs.html
- ↑ First Author and Second Author, "Electro-absorpto-crossflow-sedimento-extractofractionation," Journal of Superspecialized Bioseparation Arcana 36:2 (2010) pp. 86-52.
- ↑ "Major Success for Bioprocess Fractionation," Anytown Daily News, January 1, 2015, p. A6.