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==Introduction==
Anthracimycin is an antibiotic that is able to kill gram-positive bacteria, namely anthrax (Bacillus Anthracis). In addition, a chlorinated variant has shown activity against certain gram-negative bacteria. It also may be able to kill the gram-positive methicillin-resistant staphylococcus aureus (MRSA), and therefore is an extremely relevant research topic. MRSA is a growing problem in the modern world because of its astonishing capacity to develop drug resistance, so a new antibiotic that defends again MRSA would be a revolutionary discovery.  Professor Wiliam Fenical, along with his team of researchers, discovered the compound in 2012 in an ocean microbe off the shores of Santa Barbara, California.


[[image:Image 1241 1-anthrax.jpg|thumb|300px|right| Electron microscopy view of anthracimycin, http://cdn4.sci-news.com/images/2013/07/image_1241_1-anthrax.jpg]]
[[image:Image 1241 1-anthrax.jpg|thumb|300px|right| Electron microscopy view of anthracimycin, http://cdn4.sci-news.com/images/2013/07/image_1241_1-anthrax.jpg]]
==Introduction==
Anthracimycin is an antibiotic that is able to kill gram-positive bacteria, namely anthrax (''Bacillus anthracis''). In addition, a chlorinated variant has shown activity against certain gram-negative bacteria. It also may be able to kill the gram-positive bacterium methicillin-resistant ''Staphylococcus aureus'' (MRSA), and therefore is an extremely relevant research topic. MRSA is a growing problem in the modern world, so a new antibiotic that defends again MRSA would be a revolutionary discovery.  Professor William Fenical, along with his team of researchers, discovered the compound in 2012 in an ocean microbe off the shores of Santa Barbara, California. Due to its recent discovery, there are still many unanswered questions about the structure and function of anthracimycin. It has not yet been approved for medical use or even tested on living subjects, but studies thus far suggest it may be in the future.


==Origin of Anthracimycin==
==Origin of Anthracimycin==
Anthracimycin is a metabolite derived from an ocean microbe called Streptomyces sp. Streptomyces belongs to the order Actinomycetales ("Actinomycetales Phylogeny"). This order is classified by Streptomyces is a very common bacterium; its compounds contribute to approximately 75% of commercially used antibiotics. However, the genus Streptomyces contains hundreds of different species, which can vary greatly in metabolite production and other basic characteristics (Shepherd et. al). The particular species from which anthracimycin was isolated
Anthracimycin is a metabolite derived from an ocean microbe called ''Streptomyces sp''. Streptomyces is a genus which belongs to the order Actinomycetales [http://patricbrc.org/portal/portal/patric/Phylogeny?cType=taxon&cId=2037<sup>(1)</sup]>]. This order is classified by gram-positive bacteria which are known for producing antibiotics, anticancer agents, and immunosuppressive agents [http://www.broadinstitute.org/annotation/genome/streptomyces_group/MultiHome.html<sup>(2)</sup]>]. Streptomyces is a very common and useful genus of bacteria; its compounds contribute to approximately 75% of commercially produced antibiotics and about 50% of naturally occurring antibiotics. The genus ''Streptomyces'' contains hundreds of different species, which can vary greatly in metabolite production and other basic characteristics [http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2950629/<sup>(3)</sup]>].  


==Chemical Structure of Anthracimycin==
==Chemical Structure of Anthracimycin==
Line 11: Line 14:
[[image:Image 1241 2-anthrax.jpg|thumb|300px|right| Chemical structure of anthracimycin, http://cdn4.sci-news.com/images/2013/07/image_1241_2-anthrax.jpg]]
[[image:Image 1241 2-anthrax.jpg|thumb|300px|right| Chemical structure of anthracimycin, http://cdn4.sci-news.com/images/2013/07/image_1241_2-anthrax.jpg]]


Anthracimycin, according to Professor Fenical, has a "new and unique chemical structure" (Aguilera). New antibiotics do not often have completely unique structures, which is what makes the discovery of anthracimycin particularly important. The chemical formula of anthracimycin is C25H32O4. It is composed of three rings: one has fourteen carbon atoms, and two have six carbon atoms each (Jang et. al. 2). These rings are of a polyketide origin, which simply means that they contain ketone groups. Ketones contain carbonyl groups connected to carbon atoms in the middle of a carbon chain. ("Organic Chemistry" 3).  
Anthracimycin, according to Professor Fenical, has a "new and unique chemical structure" [https://scripps.ucsd.edu/news/anthracimycin-compound-shows-promise-anthrax<sup>(4)</sup]>]. New antibiotics do not often have completely unique structures, which is what makes the discovery of anthracimycin particularly important. In its pure form, anthracimycin is a white solid with the chemical formula C<sub>25</sub>H<sub>32</sub>O<sub>4</sub>. It is composed of three rings: one has fourteen carbon atoms, and two have six carbon atoms each [http://0-onlinelibrary.wiley.com.dewey2.library.denison.edu/doi/10.1002/anie.201302749/abstract<sup>(5)</sup]>]. These rings are of a polyketide origin, which simply means that they contain multiple ketone groups. Ketones contain carbonyl groups connected to carbon atoms in the middle of a carbon chain. <sup>(6)</sup]>.  


Although anthracimycin has a unique structure, it is closely related to a compound called chlorotonil A.  Chlorotonil A is a metabolite derived from a terrestrial bacterium called Sorangium cellulosum ("Anthrax Killer From the Sea"). It differs in structure from anthracimycin in that it contains two chlorine atoms and it has a slightly different carbon skeleton (Jang et. al). The bioactivity of chlorotonil A has not yet been determined, but the most recent research suggests that it may have uses similar to anthracimycin (Gerth et al.)
Although anthracimycin has a unique structure, it is closely related to a compound called chlorotonil A.  Chlorotonil A is a rare metabolite derived from a terrestrial bacterium called ''Sorangium cellulosum'' [http://www.chemistryviews.org/details/ezine/4972631/Anthrax_Killer_from_the_Sea.html<sup>(7)</sup]>]. It differs in structure from anthracimycin in that it contains two chlorine atoms and it has a slightly different carbon skeleton [http://0-onlinelibrary.wiley.com.dewey2.library.denison.edu/doi/10.1002/anie.201302749/abstract<sup>(5)</sup]>]. The bioactivity of chlorotonil A has not yet been determined, but the most recent research suggests that it may have uses similar to anthracimycin [http://0-onlinelibrary.wiley.com.dewey2.library.denison.edu/doi/10.1002/anie.200703993/abstract<sup>(8)</sup]>].


The main techniques used to determine the chemical structure of anthracimycin were spectroscopy and x-ray crystallography. Spectroscopy is a process often used to study the structure of molecules. It involves determining the wavelength of different elements of a molecule, and using that information to determine its chemical structure (Kulesa). X-ray crystallography involves beaming x-rays at a crystallized compound and studying the diffraction pattern to determine the chemical structure of the compound. In the Jang, et al. study, spectroscopy provided a more general picture of anthracimycin's structure, while x-ray crystallography gave the specific locations of carbon atoms (2).  
The main techniques used to determine the chemical structure of anthracimycin were spectroscopy and x-ray crystallography. Spectroscopy is a process often used to study the structure of complex molecules. It involves determining the wavelength of different elements of a molecule, and using that information to determine its chemical structure [http://loke.as.arizona.edu/~ckulesa/camp/spectroscopy_intro.html<sup>(9)</sup]>]. X-ray crystallography involves beaming x-rays at a crystallized compound and studying the diffraction pattern to determine the chemical structure of the compound [http://www.stolaf.edu/people/hansonr/mo/x-ray.html<sup>(10)</sup]>]. In the Jang, et al. study, spectroscopy provided a more general picture of anthracimycin's structure, while x-ray crystallography gave the specific locations of carbon atoms [http://0-onlinelibrary.wiley.com.dewey2.library.denison.edu/doi/10.1002/anie.201302749/abstract<sup>(5)</sup]>].  


==Method of Action and Potential Uses==
==Method of Action and Potential Uses==
The method of action of anthracimycin is not yet determined. Scientists initially hypothesized that it inhibited DNA/RNA synthesis, but follow-up studies (Jang et. al) rejected this hypothesis.  
[[image:Jangtable.jpg|thumb|300px|right| Table from the Jang, et. al. paper displaying the effects of pure anthracimycin and the chlorinated variant on various bacteria. Lower MIC levels indicate higher antimicrobial activity.]]
The method of action of anthracimycin is not yet determined. Scientists initially hypothesized that it inhibited DNA/RNA synthesis, but follow-up studies concluded that this hypothesis was unlikely [http://0-onlinelibrary.wiley.com.dewey2.library.denison.edu/doi/10.1002/anie.201302749/abstract<sup>(5)</sup]>]. Another possible method of action has not been proposed.  


Anthracimycin has been shown to effectively kill gram positive-bacteria. In its pure form, it has shown limited to no antimicrobial activity against gram-negative bacteria (Jang et. al. 2). It has been proven effective against the spore-forming bacterium Bacillus anthracis, which causes an infectious disease called anthrax. This bacterium has been used most notably as a bioterrorism weapon, and is most common in people who handle farm animals (Jang et. al. 1). Anthrax is rare but potentially lethal, and can require months of treatment with multiple antibiotics ("Anthrax Killer from the Sea"). Therefore, discoveries of new antibiotics to treat anthrax are medically significant. Anthracimycin also showed antimicrobial activity against staphylococci, enterococci, and streptococci. Based on this action, scientists predict that it may be able to kill MRSA, another gram-positive bacterium.  
Anthracimycin has been shown to effectively kill gram positive-bacteria. In its pure form, it has shown limited to no antimicrobial activity against gram-negative bacteria [http://0-onlinelibrary.wiley.com.dewey2.library.denison.edu/doi/10.1002/anie.201302749/abstract<sup>(5)</sup]>]. It has proven effective against the spore-forming bacterium Bacillus anthracis, which causes an infectious disease called anthrax. This bacterium has been used most notably as a potent bioterrorism weapon, but it is most common in people who handle farm animals. Anthrax is rare but potentially lethal, and can require months of treatment with multiple antibiotics [http://0-onlinelibrary.wiley.com.dewey2.library.denison.edu/doi/10.1002/anie.201302749/abstract<sup>(5)</sup]>]. Therefore, discoveries of new antibiotics to treat anthrax are medically significant.  


In the Jang, et. al. study, two chlorine atoms were added to anthracimycin to determine whether the addition of chlorine changes the antibiotic's effects (3). Adding chlorine atoms altered the structure of anthracimycin to make it closer to the structure of chlorotonil. The addition of chlorine atoms reduced anthracimycin's effect on Bacillus anthracis by about half. However, adding chlorine atoms greatly increased its activity against certain gram-negative bacteria. These bacteria, such as E. coli and H. influenzae, have also been known to develop drug resistance. Therefore, the chlorinated derivative of anthracimycin may also prove to be medically useful.  
Anthracimycin also showed antimicrobial activity against multiple other species of staphylococci, enterococci, and streptococci. Based on this action, scientists predict that it may be able to kill MRSA, another gram-positive bacterium. MRSA is most commonly acquired in hospital settings, but outbreaks can also arise in communities. It is known for its astonishing capacity to develop drug resistance. Not only is MRSA resistant to methicillin, it is also resistant to an entire class of antibiotics called beta-lactams. Alarmingly, in recent years, cases were documented where strains of MRSA was resistant to the antibiotic vancomycin, which is considered one of the "drugs of last resort." Although vancomycin-resistant strains are extremely rare at this point, future evolution presents the frightening possibility of the development of an entirely drug-resistant bacterium. [http://www.niaid.nih.gov/topics/antimicrobialresistance/examples/mrsa/pages/default.aspx<sup>(11)</sup]>]
 
In the Jang, et. al. study, two chlorine atoms were added to anthracimycin to determine whether the addition of chlorine changes the antibiotic's effects [http://0-onlinelibrary.wiley.com.dewey2.library.denison.edu/doi/10.1002/anie.201302749/abstract<sup>(5)</sup]>]. Adding chlorine atoms altered the structure of anthracimycin to make it closer to the structure of chlorotonil. The addition of chlorine atoms reduced anthracimycin's effect on ''Bacillus anthracis'' by about half. However, adding chlorine atoms greatly increased its activity against certain gram-negative bacteria. These bacteria, such as ''E. coli'' and ''H. influenzae'', have also been known to develop drug resistance. Therefore, the chlorinated derivative of anthracimycin may also prove to be medically useful.  


==Conclusion==
==Conclusion==
Research on anthracimycin is still in the early stages. The antibiotic shows promising potential against gram-positive bacteria, and its chlorinated derivative shows potential against gram-negative bacteria. The marine origin of anthracimycin suggests that the oceans may be a new location to find medically important materials. The discovery of new antibiotics is key to staying ahead of bacterial evolution so that treatments against infections remain effective.  
Research on anthracimycin is still in the early stages. Further research will have to include animal testing [http://0-onlinelibrary.wiley.com.dewey2.library.denison.edu/doi/10.1002/anie.201302749/abstract<sup>(5)</sup]>]. If that is successful, anthracimycin may be effective and safe for human use. The antibiotic shows promising potential against gram-positive bacteria, and its chlorinated derivative shows potential against gram-negative bacteria. The marine origin of anthracimycin suggests that the oceans may be a new location to find medically important materials. There are likely a vast number of undiscovered marine microbes with new chemical structures. The discovery of new antibiotics is key to staying ahead of bacterial evolution so that treatments against infections remain effective.  


==References==
==References==
"Actinomycetales Phylogeny." PATRIC. Pathosystems Resource Integration Center. Web. 03 Dec. 2013.


Aguilera, Mario. "Compound Discovered at Sea Shows Potency against Anthrax." Scripps Institution of Oceanography. 17 July 2013. Web. 05 Nov. 2013.
1. "Actinomycetales Phylogeny." PATRIC. Pathosystems Resource Integration Center. Web. 03 Dec. 2013.
 
2. "Actinomycetales Group Database." Broad Institute. 17 Sep. 2013. Web. 04 Dec. 2013.
 
3. Shepherd, Micah D., et al. "Laboratory Maintenance of Streptomyces Species." National Center for Biotechnology Information. U.S. National Library of Medicine, 01 Nov. 2010. Web. 03 Dec. 2013.
 
4. Aguilera, Mario. "Compound Discovered at Sea Shows Potency against Anthrax." Scripps Institution of Oceanography. 17 July 2013. Web. 05 Nov. 2013.


"Anthracimycin: New Antibiotic Kills Anthrax, MRSA." Scinews.com. 19 July 2013. Web. 05 Nov. 2013.
5. Jang, Kyoung H, et. al. "Anthracimycin, a Potential Anthrax Antibiotic from a Marine-Derived Actinomycete." Angewandte Chemie International Edition 52.30 (2013): 7822-824. Wiley Online Library. Web. 7 Nov. 2013.


"Anthrax Killer from the Sea." Chemistry Views. 01 July 2013. Web. 7 Nov. 2013.
6. Organic Chemistry: Structure and Function. Ed. P. Vollhardt and N. Schore. 5th ed. New York: W. H. Freeman and, 2007. 3. Print.


Organic Chemistry: Structure and Function. Ed. P. Vollhardt and N. Schore. 5th ed. New York: W. H. Freeman and, 2007. 3. Print.
7. "Anthrax Killer from the Sea." Chemistry Views. 01 July 2013. Web. 07 Nov. 2013.


Gerth, K., et al. "Chlorotonil A, a Macrolide with a Unique gem-Dichloro-1,3-dione Functionality from Sorangium cellulosum, So ce1525." Angewandte Chemie International Edition 47.3 (2008): 600–602. Wiley Online Library. Web. 3 December 2013.  
8. Gerth, K., et al. "Chlorotonil A, a Macrolide with a Unique gem-Dichloro-1,3-dione Functionality from Sorangium cellulosum, So ce1525." Angewandte Chemie International Edition 47.3 (2008): 600–602. Wiley Online Library. Web. 03 Dec. 2013.  


Jang, Kyoung H, et. al. "Anthracimycin, a Potential Anthrax Antibiotic from a Marine-Derived Actinomycete." Angewandte Chemie International Edition 52.30 (2013): 7822-824. Wiley Online Library. Web. 7 Nov. 2013.
9. Kulesa, Craig. "What Is Spectroscopy?" What Is Spectroscopy? 4 Feb. 1997. Web. 02 Dec. 2013.


Kulesa, Craig. "What Is Spectroscopy?" What Is Spectroscopy? 4 Feb. 1997. Web. 02 Dec. 2013.
10. "X-ray Crystallography." X-RAY Crystallography. St. Olaf College. Web. 03 Dec. 2013.


Shepherd, Micah D., et al. "Laboratory Maintenance of Streptomyces Species." National Center for Biotechnology Information. U.S. National Library of Medicine, 1 Nov. 2010. Web. 03 Dec. 2013.
11. "Methicillin-Resistant Staphylococcus Aureus." National Institute of Allergy and Infectious Diseases. 03 April 2012. Web. 04 Dec 2013.


"X-ray Crystallography." X-RAY Crystallography. St. Olaf College. Web. 03 Dec. 2013.




<br>Edited by [Emily Vachon], student of [mailto:slonczewski@kenyon.edu Joan Slonczewski] for [http://biology.kenyon.edu/courses/biol116/biol116_Fall_2013.html BIOL 116 Information in Living Systems], 2013, [http://www.kenyon.edu/index.xml Kenyon College].
<br>Edited by Emily Vachon, student of [mailto:slonczewski@kenyon.edu Joan Slonczewski] for [http://biology.kenyon.edu/courses/biol116/biol116_Fall_2013.html BIOL 116 Information in Living Systems], 2013, [http://www.kenyon.edu/index.xml Kenyon College].




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<!--Do not edit or remove this line-->[[Category:Pages edited by students of Joan Slonczewski at Kenyon College]]

Latest revision as of 00:32, 6 December 2013

Electron microscopy view of anthracimycin, http://cdn4.sci-news.com/images/2013/07/image_1241_1-anthrax.jpg


Introduction

Anthracimycin is an antibiotic that is able to kill gram-positive bacteria, namely anthrax (Bacillus anthracis). In addition, a chlorinated variant has shown activity against certain gram-negative bacteria. It also may be able to kill the gram-positive bacterium methicillin-resistant Staphylococcus aureus (MRSA), and therefore is an extremely relevant research topic. MRSA is a growing problem in the modern world, so a new antibiotic that defends again MRSA would be a revolutionary discovery. Professor William Fenical, along with his team of researchers, discovered the compound in 2012 in an ocean microbe off the shores of Santa Barbara, California. Due to its recent discovery, there are still many unanswered questions about the structure and function of anthracimycin. It has not yet been approved for medical use or even tested on living subjects, but studies thus far suggest it may be in the future.

Origin of Anthracimycin

Anthracimycin is a metabolite derived from an ocean microbe called Streptomyces sp. Streptomyces is a genus which belongs to the order Actinomycetales (1)</sup>]. This order is classified by gram-positive bacteria which are known for producing antibiotics, anticancer agents, and immunosuppressive agents (2)</sup>]. Streptomyces is a very common and useful genus of bacteria; its compounds contribute to approximately 75% of commercially produced antibiotics and about 50% of naturally occurring antibiotics. The genus Streptomyces contains hundreds of different species, which can vary greatly in metabolite production and other basic characteristics (3)</sup>].

Chemical Structure of Anthracimycin

Anthracimycin, according to Professor Fenical, has a "new and unique chemical structure" (4)</sup>]. New antibiotics do not often have completely unique structures, which is what makes the discovery of anthracimycin particularly important. In its pure form, anthracimycin is a white solid with the chemical formula C25H32O4. It is composed of three rings: one has fourteen carbon atoms, and two have six carbon atoms each (5)</sup>]. These rings are of a polyketide origin, which simply means that they contain multiple ketone groups. Ketones contain carbonyl groups connected to carbon atoms in the middle of a carbon chain. (6)</sup]>.

Although anthracimycin has a unique structure, it is closely related to a compound called chlorotonil A. Chlorotonil A is a rare metabolite derived from a terrestrial bacterium called Sorangium cellulosum (7)</sup>]. It differs in structure from anthracimycin in that it contains two chlorine atoms and it has a slightly different carbon skeleton (5)</sup>]. The bioactivity of chlorotonil A has not yet been determined, but the most recent research suggests that it may have uses similar to anthracimycin (8)</sup>].

The main techniques used to determine the chemical structure of anthracimycin were spectroscopy and x-ray crystallography. Spectroscopy is a process often used to study the structure of complex molecules. It involves determining the wavelength of different elements of a molecule, and using that information to determine its chemical structure (9)</sup>]. X-ray crystallography involves beaming x-rays at a crystallized compound and studying the diffraction pattern to determine the chemical structure of the compound (10)</sup>]. In the Jang, et al. study, spectroscopy provided a more general picture of anthracimycin's structure, while x-ray crystallography gave the specific locations of carbon atoms (5)</sup>].

Method of Action and Potential Uses

Table from the Jang, et. al. paper displaying the effects of pure anthracimycin and the chlorinated variant on various bacteria. Lower MIC levels indicate higher antimicrobial activity.

The method of action of anthracimycin is not yet determined. Scientists initially hypothesized that it inhibited DNA/RNA synthesis, but follow-up studies concluded that this hypothesis was unlikely (5)</sup>]. Another possible method of action has not been proposed.

Anthracimycin has been shown to effectively kill gram positive-bacteria. In its pure form, it has shown limited to no antimicrobial activity against gram-negative bacteria (5)</sup>]. It has proven effective against the spore-forming bacterium Bacillus anthracis, which causes an infectious disease called anthrax. This bacterium has been used most notably as a potent bioterrorism weapon, but it is most common in people who handle farm animals. Anthrax is rare but potentially lethal, and can require months of treatment with multiple antibiotics (5)</sup>]. Therefore, discoveries of new antibiotics to treat anthrax are medically significant.

Anthracimycin also showed antimicrobial activity against multiple other species of staphylococci, enterococci, and streptococci. Based on this action, scientists predict that it may be able to kill MRSA, another gram-positive bacterium. MRSA is most commonly acquired in hospital settings, but outbreaks can also arise in communities. It is known for its astonishing capacity to develop drug resistance. Not only is MRSA resistant to methicillin, it is also resistant to an entire class of antibiotics called beta-lactams. Alarmingly, in recent years, cases were documented where strains of MRSA was resistant to the antibiotic vancomycin, which is considered one of the "drugs of last resort." Although vancomycin-resistant strains are extremely rare at this point, future evolution presents the frightening possibility of the development of an entirely drug-resistant bacterium. (11)</sup>]

In the Jang, et. al. study, two chlorine atoms were added to anthracimycin to determine whether the addition of chlorine changes the antibiotic's effects (5)</sup>]. Adding chlorine atoms altered the structure of anthracimycin to make it closer to the structure of chlorotonil. The addition of chlorine atoms reduced anthracimycin's effect on Bacillus anthracis by about half. However, adding chlorine atoms greatly increased its activity against certain gram-negative bacteria. These bacteria, such as E. coli and H. influenzae, have also been known to develop drug resistance. Therefore, the chlorinated derivative of anthracimycin may also prove to be medically useful.

Conclusion

Research on anthracimycin is still in the early stages. Further research will have to include animal testing (5)</sup>]. If that is successful, anthracimycin may be effective and safe for human use. The antibiotic shows promising potential against gram-positive bacteria, and its chlorinated derivative shows potential against gram-negative bacteria. The marine origin of anthracimycin suggests that the oceans may be a new location to find medically important materials. There are likely a vast number of undiscovered marine microbes with new chemical structures. The discovery of new antibiotics is key to staying ahead of bacterial evolution so that treatments against infections remain effective.

References

1. "Actinomycetales Phylogeny." PATRIC. Pathosystems Resource Integration Center. Web. 03 Dec. 2013.

2. "Actinomycetales Group Database." Broad Institute. 17 Sep. 2013. Web. 04 Dec. 2013.

3. Shepherd, Micah D., et al. "Laboratory Maintenance of Streptomyces Species." National Center for Biotechnology Information. U.S. National Library of Medicine, 01 Nov. 2010. Web. 03 Dec. 2013.

4. Aguilera, Mario. "Compound Discovered at Sea Shows Potency against Anthrax." Scripps Institution of Oceanography. 17 July 2013. Web. 05 Nov. 2013.

5. Jang, Kyoung H, et. al. "Anthracimycin, a Potential Anthrax Antibiotic from a Marine-Derived Actinomycete." Angewandte Chemie International Edition 52.30 (2013): 7822-824. Wiley Online Library. Web. 7 Nov. 2013.

6. Organic Chemistry: Structure and Function. Ed. P. Vollhardt and N. Schore. 5th ed. New York: W. H. Freeman and, 2007. 3. Print.

7. "Anthrax Killer from the Sea." Chemistry Views. 01 July 2013. Web. 07 Nov. 2013.

8. Gerth, K., et al. "Chlorotonil A, a Macrolide with a Unique gem-Dichloro-1,3-dione Functionality from Sorangium cellulosum, So ce1525." Angewandte Chemie International Edition 47.3 (2008): 600–602. Wiley Online Library. Web. 03 Dec. 2013.

9. Kulesa, Craig. "What Is Spectroscopy?" What Is Spectroscopy? 4 Feb. 1997. Web. 02 Dec. 2013.

10. "X-ray Crystallography." X-RAY Crystallography. St. Olaf College. Web. 03 Dec. 2013.

11. "Methicillin-Resistant Staphylococcus Aureus." National Institute of Allergy and Infectious Diseases. 03 April 2012. Web. 04 Dec 2013.



Edited by Emily Vachon, student of Joan Slonczewski for BIOL 116 Information in Living Systems, 2013, Kenyon College.