Coenzyme M
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| Names | |
|---|---|
|  IUPAC name
 2-Sulfanylethanesulfonate  | |
|  Systematic IUPAC name
 2-Sulfanylethanesulfonate  | |
|  Other names
 2-mercaptoethylsulfonate; 2-mercaptoethanesulfonate; coenzyme M anion; H-S-CoM; AC1L1HCY; 2-sulfanylethane-1-sulfonate; CTK8A8912  | |
| Identifiers | |
| ChEBI |  CHEBI:58319  | 
| ChemSpider |  3935  | 
| Jmol interactive 3D | Image | 
| PubChem | 4077 | 
 
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| Properties | |
| C2H5O3S2 | |
| Molar mass | 141.18 g·mol−1 | 
|   Except where otherwise noted, data are given for materials in their standard state (at 25 °C [77 °F], 100 kPa).  | |
| Infobox references | |
Coenzyme M is a coenzyme required for methyl-transfer reactions in the metabolism of methanogens.[1][2] The coenzyme is an anion with the formula HSCH
2CH
2SO−
3.  It is named 2-mercaptoethanesulfonate and abbreviated HS–CoM.  The cation is unimportant, but the sodium salt is most available.  Mercaptoethanesulfonate contains both a thiol, which is the main site of reactivity, and a sulfonate group, which confers solubility in aqueous media.
Biochemical role
The coenzyme is the C1 donor in methanogenesis.  It is converted to propyl coenzyme M-thioester, the thioether CH
3SCH
2CH
2SO−
3, in the penultimate step to methane formation.[3]  Coenzyme M reacts with coenzyme B, 7-thioheptanoylthreoninephosphate, to give a homodisulfide, releasing methane:
- CH
3–S–CoM + HS–CoB → CH
4 + CoB–S–S–CoM 
This induction is catalyzed by the enzyme methyl-coenzyme M reductase, which restricts cofactor F430 as the prosthetic group.
See also
- Mesna – a cancer chemotherapy adjuvant with the same parent structure
 
References
- ↑ Balch WE, Wolfe RS (1979). "Specificity and biological distribution of coenzyme M (2-mercaptoethanesulfonic acid)". J. Bacteriol. 137 (1): 256–63. PMC 218444. PMID 104960.
 - ↑  Taylor CD, Wolfe RS (10 August 1974). "Structure and methylation of coenzyme M(HSCH
2CH
2SO
3)". J. Biol. Chem. 249 (15): 4879–85. PMID 4367810. - ↑ Thauer RK (1998). "Biochemistry of Methanogenesis: a Tribute to Marjory Stephenson". Microbiology 144 (9): 2377–2406. doi:10.1099/00221287-144-9-2377. PMID 9782487.
 
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