Difference between revisions of "Biotransformation"
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<p><strong>Biotransformation</strong> is the chemical modification (or modifications) made by an organism on a chemical compound. If this modification ends in mineral compounds like CO<sub>2</sub>, NH<sub>3</sub><sup>+</sup> or H<sub>2</sub>O, the biotransformation is called mineralisation. Biotransformation means chemical alteration of the drug</p> | <p><strong>Biotransformation</strong> is the chemical modification (or modifications) made by an organism on a chemical compound. If this modification ends in mineral compounds like CO<sub>2</sub>, NH<sub>3</sub><sup>+</sup> or H<sub>2</sub>O, the biotransformation is called mineralisation. Biotransformation means chemical alteration of the drug</p> | ||
<p>in the body . It is needed to render nonpolar compounds polar so that they are not reabsorbed in renal tubules and are excreted.</p> | <p>in the body . It is needed to render nonpolar compounds polar so that they are not reabsorbed in renal tubules and are excreted.</p> | ||
| − | + | ||
| − | |||
| − | |||
| − | |||
| − | |||
<p><font color="#000080"></font></p> | <p><font color="#000080"></font></p> | ||
<h2><span class="mw-headline">Drug metabolism</span></h2> | <h2><span class="mw-headline">Drug metabolism</span></h2> | ||
<p>The <font color="#000080">metabolism</font> of a <font color="#000080">drug</font> or <font color="#000080">toxin</font> in a body is an example of a biotransformation. Typically the body deals with a foreign compound by making it more soluble, to increase the rate of its excretion through the urine. There are a number of different process that can occur,The pathways of drug metabolism can divided in to:</p> | <p>The <font color="#000080">metabolism</font> of a <font color="#000080">drug</font> or <font color="#000080">toxin</font> in a body is an example of a biotransformation. Typically the body deals with a foreign compound by making it more soluble, to increase the rate of its excretion through the urine. There are a number of different process that can occur,The pathways of drug metabolism can divided in to:</p> | ||
<ul> | <ul> | ||
| − | <li>phase І</li> | + | <li>phase І </li> |
| − | <li>phase II</li> | + | <li>phase II </li> |
</ul> | </ul> | ||
<p><br /> | <p><br /> | ||
| Line 18: | Line 14: | ||
<h4><span class="mw-headline">Phase I reaction</span></h4> | <h4><span class="mw-headline">Phase I reaction</span></h4> | ||
<ul> | <ul> | ||
| − | <li>It includes oxidative, reductive and hydrolytic reactions.</li> | + | <li>It includes oxidative, reductive and hydrolytic reactions. </li> |
</ul> | </ul> | ||
<ul> | <ul> | ||
| − | <li>In case of these type of reactions, the polar group is either introduced or unmasked,so the drug molecule becomes solublised and excreted.</li> | + | <li>In case of these type of reactions, the polar group is either introduced or unmasked,so the drug molecule becomes solublised and excreted. </li> |
</ul> | </ul> | ||
<p> </p> | <p> </p> | ||
<h4><span class="mw-headline">Phase II reaction</span></h4> | <h4><span class="mw-headline">Phase II reaction</span></h4> | ||
<ul> | <ul> | ||
| − | <li>These reactions involve covalent attachment of small polar endogenous molecule like glucuronic acid, sulphate, glycine etc. to form highly water soluble substances.</li> | + | <li>These reactions involve covalent attachment of small polar endogenous molecule like glucuronic acid, sulphate, glycine etc. to form highly water soluble substances. </li> |
</ul> | </ul> | ||
<ul> | <ul> | ||
| − | <li>Thus, they are known as conjugation reaction</li> | + | <li>Thus, they are known as conjugation reaction </li> |
</ul> | </ul> | ||
<ul> | <ul> | ||
| − | <li>The formed products have more molecular size. So, termed as synthetic reaction.</li> | + | <li>The formed products have more molecular size. So, termed as synthetic reaction. </li> |
</ul> | </ul> | ||
<p> </p> | <p> </p> | ||
| Line 47: | Line 43: | ||
<h2><span class="mw-headline">See also</span></h2> | <h2><span class="mw-headline">See also</span></h2> | ||
<ul> | <ul> | ||
| − | <li><font color="#000080">Microbial biodegradation</font></li> | + | <li><font color="#000080">Microbial biodegradation</font> </li> |
| − | <li><font color="#000080">Xenobiotic metabolism</font></li> | + | <li><font color="#000080">Xenobiotic metabolism</font> </li> |
| − | <li><font color="#000080">Biodegradation</font></li> | + | <li><font color="#000080">Biodegradation</font> </li> |
| − | <li><font color="#000080">Bioremediation</font></li> | + | <li><font color="#000080">Bioremediation</font> </li> |
| − | <li><font color="#000080">Mineralisation</font></li> | + | <li><font color="#000080">Mineralisation</font> </li> |
</ul> | </ul> | ||
<p><font color="#000080"></font></p> | <p><font color="#000080"></font></p> | ||
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<div class="references-small"> | <div class="references-small"> | ||
<ol class="references"> | <ol class="references"> | ||
| − | <li id="cite_note-Diaz-0">^ <sup><em><strong><font color="#000080">a</font></strong></em></sup> <sup><em><strong><font color="#000080">b</font></strong></em></sup> <cite class="book" style="FONT-STYLE: normal">Diaz E (editor). (2008). <em><font color="#000080">Microbial Biodegradation: Genomics and Molecular Biology</font></em>, 1st ed., Caister Academic Press. <font color="#000080">ISBN 978-1-904455-17-2</font>.</cite><span class="Z3988" title="ctx_ver=Z39.88-2004&rft_val_fmt=info%3Aofi%2Ffmt%3Akev%3Amtx%3Abook&rft.genre=book&rft.btitle=Microbial+Biodegradation%3A+Genomics+and+Molecular+Biology&rft.au=Diaz+E+%28editor%29.&rft.date=2008&rft.edition=1st+ed.&rft.pub=Caister+Academic+Press&rft_id=http%3A%2F%2Fwww.horizonpress.com%2Fbiod"><span style="DISPLAY: none"> </span></span></li> | + | <li id="cite_note-Diaz-0">^ <sup><em><strong><font color="#000080">a</font></strong></em></sup> <sup><em><strong><font color="#000080">b</font></strong></em></sup> <cite class="book" style="FONT-STYLE: normal">Diaz E (editor). (2008). <em><font color="#000080">Microbial Biodegradation: Genomics and Molecular Biology</font></em>, 1st ed., Caister Academic Press. <font color="#000080">ISBN 978-1-904455-17-2</font>.</cite><span class="Z3988" title="ctx_ver=Z39.88-2004&rft_val_fmt=info%3Aofi%2Ffmt%3Akev%3Amtx%3Abook&rft.genre=book&rft.btitle=Microbial+Biodegradation%3A+Genomics+and+Molecular+Biology&rft.au=Diaz+E+%28editor%29.&rft.date=2008&rft.edition=1st+ed.&rft.pub=Caister+Academic+Press&rft_id=http%3A%2F%2Fwww.horizonpress.com%2Fbiod"><span style="DISPLAY: none"> </span></span> </li> |
| − | <li id="cite_note-chapter9-1"><strong><font color="#000080">^</font></strong> <cite class="book" style="FONT-STYLE: normal">Martins VAP et al (2008). "<font color="#000080">Genomic Insights into Oil Biodegradation in Marine Systems</font>", <em>Microbial Biodegradation: Genomics and Molecular Biology</em>. Caister Academic Press. <font color="#000080">ISBN 978-1-904455-17-2</font>.</cite><span class="Z3988" title="ctx_ver=Z39.88-2004&rft_val_fmt=info%3Aofi%2Ffmt%3Akev%3Amtx%3Abook&rft.genre=book&rft.btitle=Microbial+Biodegradation%3A+Genomics+and+Molecular+Biology&rft.atitle=Genomic+Insights+into+Oil+Biodegradation+in+Marine+Systems&rft.au=Martins+VAP+et+al&rft.date=2008&rft.pub=Caister+Academic+Press"><span style="DISPLAY: none"> </span></span></li> | + | <li id="cite_note-chapter9-1"><strong><font color="#000080">^</font></strong> <cite class="book" style="FONT-STYLE: normal">Martins VAP et al (2008). "<font color="#000080">Genomic Insights into Oil Biodegradation in Marine Systems</font>", <em>Microbial Biodegradation: Genomics and Molecular Biology</em>. Caister Academic Press. <font color="#000080">ISBN 978-1-904455-17-2</font>.</cite><span class="Z3988" title="ctx_ver=Z39.88-2004&rft_val_fmt=info%3Aofi%2Ffmt%3Akev%3Amtx%3Abook&rft.genre=book&rft.btitle=Microbial+Biodegradation%3A+Genomics+and+Molecular+Biology&rft.atitle=Genomic+Insights+into+Oil+Biodegradation+in+Marine+Systems&rft.au=Martins+VAP+et+al&rft.date=2008&rft.pub=Caister+Academic+Press"><span style="DISPLAY: none"> </span></span> </li> |
| − | <li id="cite_note-chapter12-2"><strong><font color="#000080">^</font></strong> <cite class="book" style="FONT-STYLE: normal">Meyer A and Panke S (2008). "<font color="#000080">Genomics in Metabolic Engineering and Biocatalytic Applications of the Pollutant Degradation Machinery</font>", <em>Microbial Biodegradation: Genomics and Molecular Biology</em>. Caister Academic Press. <font color="#000080">ISBN 978-1-904455-17-2</font>.</cite><span class="Z3988" title="ctx_ver=Z39.88-2004&rft_val_fmt=info%3Aofi%2Ffmt%3Akev%3Amtx%3Abook&rft.genre=book&rft.btitle=Microbial+Biodegradation%3A+Genomics+and+Molecular+Biology&rft.atitle=Genomics+in+Metabolic+Engineering+and+Biocatalytic+Applications+of+the+Pollutant+Degradation+Machinery&rft.au=Meyer+A+and+Panke+S&rft.date=2008&rft.pub=Caister+Academic+Press"><span style="DISPLAY: none"> </span></span></li> | + | <li id="cite_note-chapter12-2"><strong><font color="#000080">^</font></strong> <cite class="book" style="FONT-STYLE: normal">Meyer A and Panke S (2008). "<font color="#000080">Genomics in Metabolic Engineering and Biocatalytic Applications of the Pollutant Degradation Machinery</font>", <em>Microbial Biodegradation: Genomics and Molecular Biology</em>. Caister Academic Press. <font color="#000080">ISBN 978-1-904455-17-2</font>.</cite><span class="Z3988" title="ctx_ver=Z39.88-2004&rft_val_fmt=info%3Aofi%2Ffmt%3Akev%3Amtx%3Abook&rft.genre=book&rft.btitle=Microbial+Biodegradation%3A+Genomics+and+Molecular+Biology&rft.atitle=Genomics+in+Metabolic+Engineering+and+Biocatalytic+Applications+of+the+Pollutant+Degradation+Machinery&rft.au=Meyer+A+and+Panke+S&rft.date=2008&rft.pub=Caister+Academic+Press"><span style="DISPLAY: none"> </span></span> </li> |
</ol> | </ol> | ||
</div> | </div> | ||
| Line 65: | Line 61: | ||
<h2><span class="mw-headline">External links</span></h2> | <h2><span class="mw-headline">External links</span></h2> | ||
<ul> | <ul> | ||
| − | <li><a class="external text" title="http://www.pharmacology.googlepages.com/metabolism.html" href="http://www.pharmacology.googlepages.com/metabolism.html | + | <li><a class="external text" title="http://www.pharmacology.googlepages.com/metabolism.html" rel="nofollow" href="http://www.pharmacology.googlepages.com/metabolism.html"><font color="#000080">Biotransformation of Drugs</font></a> </li> |
| − | <li><a class="external text" title="http://www.horizonpress.com/gateway/biodegradation.html" href="http://www.horizonpress.com/gateway/biodegradation.html | + | <li><a class="external text" title="http://www.horizonpress.com/gateway/biodegradation.html" rel="nofollow" href="http://www.horizonpress.com/gateway/biodegradation.html"><font color="#000080">Biodegradation, Bioremediation and Biotransformation</font></a> </li> |
| − | <li><a class="external text" title="http://www.horizonpress.com/blogger/2007/09/microbial-biodegradation-bioremediation.html" href="http://www.horizonpress.com/blogger/2007/09/microbial-biodegradation-bioremediation.html | + | <li><a class="external text" title="http://www.horizonpress.com/blogger/2007/09/microbial-biodegradation-bioremediation.html" rel="nofollow" href="http://www.horizonpress.com/blogger/2007/09/microbial-biodegradation-bioremediation.html"><font color="#000080">Microbial Biodegradation</font></a> </li> |
</ul> | </ul> | ||
Latest revision as of 11:12, 7 October 2008
Biotransformation is the chemical modification (or modifications) made by an organism on a chemical compound. If this modification ends in mineral compounds like CO2, NH3+ or H2O, the biotransformation is called mineralisation. Biotransformation means chemical alteration of the drug
in the body . It is needed to render nonpolar compounds polar so that they are not reabsorbed in renal tubules and are excreted.
Contents
Drug metabolism
The metabolism of a drug or toxin in a body is an example of a biotransformation. Typically the body deals with a foreign compound by making it more soluble, to increase the rate of its excretion through the urine. There are a number of different process that can occur,The pathways of drug metabolism can divided in to:
- phase І
- phase II
Phase I reaction
- It includes oxidative, reductive and hydrolytic reactions.
- In case of these type of reactions, the polar group is either introduced or unmasked,so the drug molecule becomes solublised and excreted.
Phase II reaction
- These reactions involve covalent attachment of small polar endogenous molecule like glucuronic acid, sulphate, glycine etc. to form highly water soluble substances.
- Thus, they are known as conjugation reaction
- The formed products have more molecular size. So, termed as synthetic reaction.
Microbial biotransformation
Biotransformation of various pollutants is a sustainable way to clean up contaminated environments.[1] These bioremediation and biotransformation methods harness the naturally occurring, microbial catabolic diversity to degrade, transform or accumulate a huge range of compounds including hydrocarbons (e.g. oil), polychlorinated biphenyls (PCBs), polyaromatic hydrocarbons (PAHs), pharmaceutical substances, radionuclides and metals. Major methodological breakthroughs in recent years have enabled detailed genomic, metagenomic, proteomic, bioinformatic and other high-throughput analyses of environmentally relevant microorganisms providing unprecedented insights into biotransformation and biodegradative pathways and the ability of organisms to adapt to changing environmental conditions.
Biological processes play a major role in the removal of contaminants and pollutants from the environment. Some microorganisms possess an astonishing catabolic versatility to degrade or transform such compounds. New methodological breakthroughs in sequencing, genomics, proteomics, bioinformatics and imaging are producing vast amounts of information. In the field of Environmental Microbiology, genome-based global studies open a new era providing unprecedented in silico views of metabolic and regulatory networks, as well as clues to the evolution of biochemical pathways relevant to biotransformation and to the molecular adaptation strategies to changing environmental conditions. Functional genomic and metagenomic approaches are increasing our understanding of the relative importance of different pathways and regulatory networks to carbon flux in particular environments and for particular compounds and they are accelerating the development of bioremediation technologies and biotransformation processes.[1] Also there is other approach of biotransformation called enzymatic biotransformation.
Oil Biodegradation
Petroleum oil is toxic for most life forms and episodic and chronic pollution of the environment by oil causes major ecological perturbations. Marine environments are especially vulnerable since oil spills of coastal regions and the open sea are poorly containable and mitigation is difficult. In addition to pollution through human activities, millions of tons of petroleum enter the marine environment every year from natural seepages. Despite its toxicity, a considerable fraction of petroleum oil entering marine systems is eliminated by the hydrocarbon-degrading activities of microbial communities, in particular by a remarkable recently discovered group of specialists, the so-called hydrocarbonoclastic bacteria (HCB). Alcanivorax borkumensis, a paradigm of HCB and probably the most important global oil degrader, was the first to be subjected to a functional genomic analysis. This analysis has yielded important new insights into its capacity for (i) n-alkane degradation including metabolism, biosurfactant production and biofilm formation, (ii) scavenging of nutrients and cofactors in the oligotrophic marine environment, as well as (iii) coping with various habitat-specific stresses. The understanding thereby gained constitutes a significant advance in efforts towards the design of new knowledge-based strategies for the mitigation of ecological damage caused by oil pollution of marine habitats. HCB also have potential biotechnological applications in the areas of bioplastics and biocatalysis.[2]
Metabolic Engineering and Biocatalytic Applications
The study of the fate of persistent organic chemicals in the environment has revealed a large reservoir of enzymatic reactions with a large potential in preparative organic synthesis, which has already been exploited for a number of oxygenases on pilot and even on industrial scale. Novel catalysts can be obtained from metagenomic libraries and DNA sequence based approaches. Our increasing capabilities in adapting the catalysts to specific reactions and process requirements by rational and random mutagenesis broadens the scope for application in the fine chemical industry, but also in the field of biodegradation. In many cases, these catalysts need to be exploited in whole cell bioconversions or in fermentations, calling for system-wide approaches to understanding strain physiology and metabolism and rational approaches to the engineering of whole cells as they are increasingly put forward in the area of systems biotechnology and synthetic biology.[3]
See also
- Microbial biodegradation
- Xenobiotic metabolism
- Biodegradation
- Bioremediation
- Mineralisation
References
- ^ a b Diaz E (editor). (2008). Microbial Biodegradation: Genomics and Molecular Biology, 1st ed., Caister Academic Press. ISBN 978-1-904455-17-2.
- ^ Martins VAP et al (2008). "Genomic Insights into Oil Biodegradation in Marine Systems", Microbial Biodegradation: Genomics and Molecular Biology. Caister Academic Press. ISBN 978-1-904455-17-2.
- ^ Meyer A and Panke S (2008). "Genomics in Metabolic Engineering and Biocatalytic Applications of the Pollutant Degradation Machinery", Microbial Biodegradation: Genomics and Molecular Biology. Caister Academic Press. ISBN 978-1-904455-17-2.
