mycolactone
{{chembox
| verifiedrevid = 421043852
| ImageFile=mycolactone 2.png
| ImageSize=
| PIN= (6S,7S,9E,12R)-12-[(2S,4E,6R,7R,9R)-7,9-Dihydroxy-4,6-dimethyldec-4-en-2-yl]-7,9-dimethyl-2-oxo-1-oxacyclododec-9-en-6-yl (2E,4E,6E,8E,10E,12S,13S,15S)-12,13,15-trihydroxy-4,6,10-trimethylhexadeca-2,4,6,8,10-pentaenoate
|Section1={{Chembox Identifiers
| ChemSpiderID_Ref = {{chemspidercite|correct|chemspider}}
| ChemSpiderID = 4445303
| InChI = 1/C44H70O9/c1-28(13-11-14-29(2)25-39(48)40(49)27-37(10)46)21-30(3)18-20-44(51)52-41-15-12-16-43(50)53-42(19-17-31(4)22-34(41)7)35(8)24-32(5)23-33(6)38(47)26-36(9)45/h11,13-14,17-18,20-21,23,25,33-42,45-49H,12,15-16,19,22,24,26-27H2,1-10H3/b14-11+,20-18+,28-13+,29-25+,30-21+,31-17+,32-23+/t33-,34+,35+,36-,37+,38-,39+,40+,41+,42-/m1/s1
| InChIKey = WKTLNJXZVDLRTJ-QRRXZRELBE
| StdInChI_Ref = {{stdinchicite|correct|chemspider}}
| StdInChI = 1S/C44H70O9/c1-28(13-11-14-29(2)25-39(48)40(49)27-37(10)46)21-30(3)18-20-44(51)52-41-15-12-16-43(50)53-42(19-17-31(4)22-34(41)7)35(8)24-32(5)23-33(6)38(47)26-36(9)45/h11,13-14,17-18,20-21,23,25,33-42,45-49H,12,15-16,19,22,24,26-27H2,1-10H3/b14-11+,20-18+,28-13+,29-25+,30-21+,31-17+,32-23+/t33-,34+,35+,36-,37+,38-,39+,40+,41+,42-/m1/s1
| StdInChIKey_Ref = {{stdinchicite|correct|chemspider}}
| StdInChIKey = WKTLNJXZVDLRTJ-QRRXZRELSA-N
| CASNo_Ref = {{cascite|correct|??}}
| CASNo=222050-77-3
| PubChem=5282079
| SMILES = O=C1O[C@H](C/C=C(/C[C@@H]([C@@H](OC(=O)\C=C\C(=C\C(=C\C=C\C(=C\[C@H](O)[C@@H](O)C[C@@H](O)C)C)C)C)CCC1)C)C)[C@@H](C)CC(=C/[C@@H](C)[C@H](O)C[C@H](O)C)/C
| MeSHName=Mycolactone
}}
|Section2={{Chembox Properties
| Formula=C44H70O9
| MolarMass=743.021
| Appearance=
| Density=
| MeltingPt=
| BoilingPt=
| Solubility=
}}
|Section3={{Chembox Hazards
| MainHazards=
| FlashPt=
| AutoignitionPt =
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}}
Mycolactone is a polyketide-derived macrolide produced and secreted by a group of very closely related pathogenic mycobacteria species including M. ulcerans, M. liflandii (an unofficial designation), M. pseudoshottsii, and some strains of M. marinum. These mycobacteria are collectively referred to as mycolactone-producing mycobacteria or MPM.{{cite journal
|vauthors=Yip MJ, Porter JL, Fyfe JA, Lavender CJ, etal | title = Evolution of Mycobacterium ulcerans and other mycolactone-producing mycobacteria from a common Mycobacterium marinum progenitor.
| journal = J. Bacteriol.
| date=March 2007
| volume = 189
| pages = 2021–29
| pmid = 17172337
| doi = 10.1128/JB.01442-06
| issue = 5
| pmc = 1855710}}{{cite journal
|author1=Käser M |author2=Hauser J |author3=Small P |author4=Pluschke G. | title = Large sequence polymorphisms unveil the phylogenetic relationship of environmental and pathogenic mycobacteria related to "Mycobacterium ulcerans".
| journal = Appl Environ Microbiol
| date=September 2009
| volume = 75
| pages = 5667–75
| pmid = 19592526
| doi = 10.1128/AEM.00446-09
| issue = 17
| pmc = 2737907|bibcode=2009ApEnM..75.5667K }}
In humans, mycolactone is the toxin responsible for Buruli ulcers, doing so by damaging tissues and inhibiting the immune response.{{cite web|url=https://www.who.int/mediacentre/factsheets/fs199/en/|title=Buruli ulcer disease|date=March 2007|work=Fact sheets|publisher=WHO|access-date=24 March 2012}}
__TOC__
Variants
Five distinct, naturally occurring mycolactone structural variants have been described so far:
- Mycolactone A/B (M. ulcerans from Africa, Malaysia, Japan{{cite journal
|vauthors=Pidot SJ, Hong H, Seemann T, Porter JL, etal | title = Deciphering the genetic basis for polyketide variation among mycobacteria producing mycolactones.
| journal = BMC Genomics
| date=October 2008
| volume = 9
| pages = 462
| pmc=2569948
| doi = 10.1186/1471-2164-9-462
| pmid = 18840298
| doi-access = free
}}
- Mycolactone C (M. ulcerans from Australia){{cite journal |last1=Mve-Obiang |first1=Armand |last2=Lee |first2=Richard E. |last3=Portaels |first3=Françoise |last4=Small |first4=P. L. C. |title=Heterogeneity of Mycolactones Produced by Clinical Isolates of Mycobacterium ulcerans : Implications for Virulence |journal=Infection and Immunity |date=February 2003 |volume=71 |issue=2 |pages=774–783 |doi=10.1128/IAI.71.2.774-783.2003 |pmid=12540557 |pmc=145382 }}
- Mycolactone D (M. ulcerans from China)
- Mycolactone E (M. liflandii from Sub-Saharan Africa){{cite journal
|vauthors=Mve-Obiang A, Lee RE, Umstot ES, Trott KA, etal | title = A newly discovered mycobacterial pathogen isolated from laboratory colonies of Xenopus species with lethal infections produces a novel form of mycolactone, the Mycobacterium ulcerans macrolide toxin.
| journal = Infect. Immun.
| date=June 2005
| volume = 73
| pages = 3307–12
| pmc = 1111873
| doi = 10.1128/IAI.73.6.3307-3312.2005
| pmid = 15908356
| issue = 6}}{{cite journal
|author1=Hong H |author2=Stinear T |author3=Skelton P |author4=Spencer JB |author5=Leadlay PF. | title = Structure elucidation of a novel family of mycolactone toxins from the frog pathogen Mycobacterium sp. MU128FXT by mass spectrometry.
| journal = Chem Commun
| date=Sep 2005
| volume = 34
| pages = 4306–8
| doi = 10.1039/b506835e
| pmid = 16113730
| issue = 34}}
{{cite journal
|vauthors=Ranger BS, Mahrous EA, Mosi L, etal | title = Globally distributed mycobacterial fish pathogens produce a novel plasmid-encoded toxic macrolide, mycolactone F.
| journal = Infect. Immun.
| date=November 2006
| volume =74
| issue =11
| pages =6037–45
| url= | doi = 10.1128/IAI.00970-06
| pmid = 16923788 |pmc=1695495}}
|author1=Stragier P |author2=Hermans K |author3=Stinear T |author4=Portaels F. | title = First report of a mycolactone-producing Mycobacterium infection in fish agriculture in Belgium.
| journal = FEMS Microbiol. Lett.
| date=September 2008
| volume = 286
| pages = 93–5
| pmid = 18631185
| doi = 10.1111/j.1574-6968.2008.01264.x
| issue = 1| doi-access = free}}
Biosynthesis
Mycolactone consists of a 12-membered macrolide core with an ester-linked polyketide chain. Three plasmid-encoded polyketide synthase (PKS) enzymes are responsible for its production: MLSA 1 and MLSA 2 which generate the core, and MLSB is responsible for the synthesis of the polyketide chain. As shown in Figure 1, MLSB (1.2 MDa) contains seven consecutive extension modules and MLSA 1 (1.8 MDa) consists of eight. The remaining PKS enzyme, MLSA 2, contains the ninth module of MLSA.{{cite journal
|vauthors=Stinear TP, Mve-Obiang A, Small PL, Frigui W, etal | title = Giant plasmid-encoded polyketide synthases produce the macrolide toxin of "Mycobacterium ulcerans".
| journal = PNAS
| date=February 2004
| volume = 101
| issue = 6
| pages = 1345–9
| pmid = 14736915
| doi = 10.1073/pnas.0305877101
| pmc = 337055| doi-access = free
}} The C-terminal domains of both MLSA2 and MLSB includes a thioesterase (TE) that was thought to catalyze the formation of the mycolactone core but appears inactive.{{cite journal |last1=Meier |first1=Jordan L. |last2=Barrows-Yano |first2=Tiffany |last3=Foley |first3=Timothy L. |last4=Wike |first4=Candice L. |last5=Burkart |first5=Michael D. |title=The unusual macrocycle forming thioesterase of mycolactone |journal=Molecular BioSystems |date=2008 |volume=4 |issue=6 |pages=663–671 |doi=10.1039/b801397g |pmid=18493665 }} Each module consists of either malonyl-CoA or methylmalonyl-CoA Acyltransferase (AT) that allows for chain extension, a ketosynthase (KS), which catalyzes chain elongation, and an Acyl carrier protein (ACP) where the growing polyketide chain is attached. Modules may also consist of any of the following modifying domains: a dehydratase (DH), an enoyl reductase (ER) and one of two types of ketoreductase (KR) domains. Type A and B KRs refer to the two directions of ketoreduction that are correlated with specific amino acids in the active site. Four of the DH domains are predicted to be inactive based on a point mutation found in the active site sequence.{{cite journal |last1=Bali |first1=Shilpa |last2=Weissman |first2=Kira J. |title=Ketoreduction in Mycolactone Biosynthesis: Insight into Substrate Specificity and Stereocontrol from Studies of Discrete Ketoreductase Domains in vitro |journal=ChemBioChem |date=4 December 2006 |volume=7 |issue=12 |pages=1935–1942 |doi=10.1002/cbic.200600285 |pmid=17031885 |s2cid=40596187 }}
{{wide image|Mycolactone3.jpg|1266px|Domain organization of mycolactone.}}