Mycolic acids are long fatty acids found in the cell walls of the mycolata taxon, a group of bacteria that includes Mycobacterium tuberculosis, the causative agent of the disease tuberculosis. They form the major component of the cell wall of mycolata species. Despite their name, mycolic acids have no biological link to fungi; the name arises from the filamentous appearance their presence gives mycolata under high magnification. The presence of mycolic acids in the cell wall also gives mycolata a distinct gross morphological trait known as "cording." Mycolic acids were first isolated by Stodola et al. in 1938 from an extract of M. tuberculosis.
Mycolic acids are composed of a longer beta-hydroxy chain with a shorter alpha-alkyl side chain. Each molecule contains between 60 and 90 carbon atoms. The exact number of carbons varies by species and can be used as an identification aid. Most mycolic acids also contain various functional groups.
Contents
- 1 Mycolic acids of M. tuberculosis
- 2 Clinical relevance
- 3 Mycolic acids of Rhodococcus sp.
- 4 References
- 5 Further reading
- 6 External links
Mycolic acids of M. tuberculosis
Mycolic acids in
Mycobacterium tuberculosis.
M. tuberculosis produces three main types of mycolic acids: alpha-, methoxy-, and keto-. Alpha-mycolic acids comprise at least 70% of the mycolic acids present in the organism and contain several cyclopropane rings. Methoxy-mycolic acids, which contain several methoxy groups, comprise between 10% and 15% of the mycolic acids in the organism. The remaining 10% to 15% of the mycolic acids are keto-mycolic acids, which contain several ketone groups.
The presence of mycolic acids gives M. tuberculosis many characteristics that defy medical treatment. They lend the organism increased resistance to chemical damage and dehydration, and prevent the effective activity of hydrophobic antibiotics. In addition, the mycolic acids allow the bacterium to grow readily inside macrophages, effectively hiding it from the host's immune system. Mycolate biosynthesis is crucial for survival and pathogenesis of M. tuberculosis. The pathway and enzymes have been elucidated and reported in detail.[1][2] Five distinct stages are involved. These were summarised as follows:[3]
- Synthesis of the C26 saturated straight chain fatty acids by the enzyme fatty acid synthase-I (FAS-I) to provide the α-alkyl branch of the mycolic acids;
- Synthesis of the C56 fatty acids by FAS-II providing the meromycolate backbone;
- Introduction of functional groups to the meromycolate chain by numerous cyclopropane synthases;
- Condensation reaction catalysed by the polyketide synthase Pks13 between the α-branch and the meromycolate chain before a final reduction by the enzyme corynebacterineae mycolate reductase A (CmrA)[4] to generate the mycolic acid; and
- Transfer of mycolic acids to arabinogalactan and other acceptors such as trehalose via the antigen 85 complex
The fatty acid synthase-I and fatty acid synthase-II pathways producing mycolic acids are linked by the beta-ketoacyl-(acyl-carrier-protein) synthase III enzyme, often designated as mtFabH. Novel inhibitors of this enzyme could potentially be used as therapeutic agents.
The mycolic acids show interesting inflammation controlling properties. A clear tolerogenic response was promoted by natural mycolic acids in experimental asthma.[5] The natural extracts are however chemically heterogeneous and inflammatory. By organic synthesis, the different homologues from the natural mixture could be obtained in pure form and tested for biological activity. One subclass proved to be a very good suppressor of asthma, through a totally new mode of action. These compounds are now under further investigation. A second subclass triggered a cellular immune response (Th1 and Th17), so studies are ongoing to use this subclass as an adjuvant for vaccination.
The exact structure of mycolic acids appears to be closely linked to the virulence of the organism, as modification of the functional groups of the molecule can lead to an attenuation of growth in vivo. Further, individuals with mutations in genes responsible for mycolic acid synthesis exhibit altered cording.
Clinical relevance
An international multi-centre study has proved that delamanid (OPC-67683), a new agent derived from the nitro-dihydro-imidazooxazole class of compounds that inhibits mycolic acid synthesis, can increase the rate of sputum culture conversion in multi-drug resistant tuberculosis (MDRTB) at 2 months.[6]
Mycolic acids of Rhodococcus sp.
The mycolic acids of members of the genus Rhodococcus, another member of the mycolata taxon, differ in several ways from those of M. tuberculosis. They contain no functional groups, but instead may have several unsaturated bonds. Two different profiles of Rhodococcus mycolic acids exist. The first has between 28 and 46 carbon atoms with either 0 or 1 unsaturated bonds. The second has between 34 and 54 carbon atoms with between 0 and 4 unsaturated bonds. Sutcliffe (1998) has proposed that they are linked to the rest of the cell wall by arabinogalactan molecules.
References
- ^ Takayama, K.; Wang, C.; Besra, G. S. (2005). "Pathway to Synthesis and Processing of Mycolic Acids in Mycobacterium tuberculosis". Clinical Microbiology Reviews 18 (1): 81–101. doi:10.1128/CMR.18.1.81-101.2005. PMC 544180. PMID 15653820.
- ^ Raman, K.; Rajagopalan, P.; Chandra, N. (2005). "Flux Balance Analysis of Mycolic Acid Pathway: Targets for Anti-Tubercular Drugs". PLoS Computational Biology 1 (5): e46. doi:10.1371/journal.pcbi.0010046. PMC 1246807. PMID 16261191.
- ^ Bhatt, A.; Molle, V.; Besra, G. S.; Jacobs, W. R.; Kremer, L. (2007). "The Mycobacterium tuberculosis FAS-II condensing enzymes: Their role in mycolic acid biosynthesis, acid-fastness, pathogenesis and in future drug development". Molecular Microbiology 64 (6): 1442–1454. doi:10.1111/j.1365-2958.2007.05761.x. PMID 17555433.
- ^ David J, Lea-Smith J; James S. Pyke; Dedreia Tull; Malcolm J. McConville; Ross L. Coppel; Paul K. Crellin (2007). "The Reductase That Catalyzes Mycolic Motif Synthesis Is Required for Efficient Attachment of Mycolic Acids to Arabinogalactan". Journal of Biological Chemistry 282 (15): 11000–11008. doi:10.1074/jbc.M608686200. PMID 17308303.
- ^ Korf, J. E.; Pynaert, G.; Tournoy, K.; Boonefaes, T.; Van Oosterhout, A.; Ginneberge, D.; Haegeman, A.; Verschoor, J. A.; De Baetselier, P.; Grooten, J. (2006). "Macrophage Reprogramming by Mycolic Acid Promotes a Tolerogenic Response in Experimental Asthma". American Journal of Respiratory and Critical Care Medicine 174 (2): 152–160. doi:10.1164/rccm.200507-1175OC. PMID 16675779.
- ^ Gler, M. T.; Skripconoka, V.; Sanchez-Garavito, E.; Xiao, H.; Cabrera-Rivero, J. L.; Vargas-Vasquez, D. E.; Gao, M.; Awad, M.; Park, S. K.; Shim, T. S.; Suh, G. Y.; Danilovits, M.; Ogata, H.; Kurve, A.; Chang, J.; Suzuki, K.; Tupasi, T.; Koh, W. J.; Seaworth, B.; Geiter, L. J.; Wells, C. D. (2012). "Delamanid for Multidrug-Resistant Pulmonary Tuberculosis". New England Journal of Medicine 366 (23): 2151–2160. doi:10.1056/NEJMoa1112433. PMID 22670901.
Further reading
- Barry Ce, 3.; Lee, R. E.; Mdluli, K.; Sampson, A. E.; Schroeder, B. G.; Slayden, R. A.; Yuan, Y. (1998). "Mycolic acids: Structure, biosynthesis and physiological functions". Progress in Lipid Research 37 (2–3): 143–179. doi:10.1016/S0163-7827(98)00008-3. PMID 9829124.
- Nishiuchi, Y.; Baba, T.; Yano, I. (2000). "Mycolic acids from Rhodococcus, Gordonia, and Dietzia". Journal of microbiological methods 40 (1): 1–9. doi:10.1016/S0167-7012(99)00116-5. PMID 10739337.
- Sutcliffe, I. C. (1998). "Cell envelope composition and organisation in the genus Rhodococcus". Antonie van Leeuwenhoek 74 (1–3): 49–58. doi:10.1023/A:1001747726820. PMID 10068788.
- Langford, K. W.; Penkov, B.; Derrington, I. M.; Gundlach, J. H. (2010). "Unsupported planar lipid membranes formed from mycolic acids of Mycobacterium tuberculosis". The Journal of Lipid Research 52 (2): 272–277. doi:10.1194/jlr.M012013. PMC 3023547. PMID 21076119.
External links
- Mycolic Acid at the US National Library of Medicine Medical Subject Headings (MeSH)
Microbiology: Bacteria
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Medical
microbiology |
- Bacterial disease
- Coley's toxins
- Exotoxin
- Lysogenic cycle
- Pathogenic bacteria
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Biochemistry
and ecology |
Oxygen
preference |
- Aerobic
- Anaerobic
- Microaerophile
- Nanaerobe
- Aerotolerant
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Other |
- Microbial metabolism
- Primary nutritional groups
- Nitrogen fixation
- Microbial ecology
- Human flora
- Gut flora
- Skin flora
- Vaginal flora
- Substrate preference
- Lipophilic
- Saccharophilic
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Morphology:
Shapes |
- Bacterial cellular morphologies
- L-form bacteria
- Coccus
- Bacillus
- Coccobacillus
- Spiral
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Morphology:
Structures |
Cell
envelope |
- Cell membrane
- Cell wall: Peptidoglycan
- Gram-positive bacteria only: Teichoic acid
- Lipoteichoic acid
- Endospore
- Gram-negative bacteria only: Bacterial outer membrane
- Periplasmic space
- Mycobacteria only: Arabinogalactan
- Mycolic acid
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Outside
envelope |
- Bacterial capsule
- Slime layer
- S-layer
- Glycocalyx
- Pilus
- Fimbria
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Composite |
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Bacterial
taxonomy |
- Bacteria (classifications)
- Bacterial phyla
- Former groupings: Schizomycetes
- Monera
- Prokaryota
- Gracilicutes
- Firmicutes
- Mollicutes
- Mendosicutes
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