Decyanation of vitamin B
            <sub>12</sub>
            by a trafficking chaperone

Kim, Jihoe; Gherasim, Carmen; Banerjee, Ruma

doi:10.1073/pnas.0805989105

Cited by 194 publications

(190 citation statements)

References 29 publications

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“…Hence, it is possible that M. barkeri strain Fusaro and the Sporomusa isolates provided the D. mccartyi strains with not yet identified compounds that enhance growth yields. Another possible explanation for the lower growth yields observed with CN-Cbl is the cell's energetic burden associated with the replacement of the upper cyanide ligand [33].…”

Section: Discussionmentioning

confidence: 99%

Guided cobalamin biosynthesis supports Dehalococcoides mccartyi reductive dechlorination activity

Yan

Yang

et al. 2013

Phil. Trans. R. Soc. B

132

101

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Dehalococcoides mccartyi strains are corrinoid-auxotrophic Bacteria and axenic cultures that require vitamin B 12 (CN-Cbl) to conserve energy via organohalide respiration. Cultures of D. mccartyi strains BAV1, GT and FL2 grown with limiting amounts of 1 µg l −1 CN-Cbl quickly depleted CN-Cbl, and reductive dechlorination of polychlorinated ethenes was incomplete leading to vinyl chloride (VC) accumulation. In contrast, the same cultures amended with 25 µg l −1 CN-Cbl exhibited up to 2.3-fold higher dechlorination rates, 2.8–9.1-fold increased growth yields, and completely consumed growth-supporting chlorinated ethenes. To explore whether known cobamide-producing microbes supply Dehalococcoides with the required corrinoid cofactor, co-culture experiments were performed with the methanogen Methanosarcina barkeri strain Fusaro and two acetogens, Sporomusa ovata and Sporomusa sp. strain KB-1, as Dehalococcoides partner populations. During growth with H 2 /CO 2 , M. barkeri axenic cultures produced 4.2 ± 0.1 µg l −1 extracellular cobamide (factor III), whereas the Sporomusa cultures produced phenolyl- and p -cresolyl-cobamides. Neither factor III nor the phenolic cobamides supported Dehalococcoides reductive dechlorination activity suggesting that M. barkeri and the Sporomusa sp. cannot fulfil Dehalococcoides ' nutritional requirements. Dehalococcoides dechlorination activity and growth occurred in M. barkeri and Sporomusa sp. co-cultures amended with 10 µM 5′,6′-dimethylbenzimidazole (DMB), indicating that a cobalamin is a preferred corrinoid cofactor of strains BAV1, GT and FL2 when grown with chlorinated ethenes as electron acceptors. Even though the methanogen and acetogen populations tested did not produce cobalamin, the addition of DMB enabled guided biosynthesis and generated a cobalamin that supported Dehalococcoides ' activity and growth. Guided cobalamin biosynthesis may offer opportunities to sustain and enhance Dehalococcoides activity in contaminated subsurface environments.

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Section: Discussionmentioning

confidence: 99%

Guided cobalamin biosynthesis supports Dehalococcoides mccartyi reductive dechlorination activity

Yan

Yang

et al. 2013

Phil. Trans. R. Soc. B

132

101

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“…The reductive decyanation of CNCbl is catalyzed by the MMACHC protein in the presence of a flavoprotein reductase and NADPH [ 36 ]. The authors reported that cblC bound both MeCbl and AdoCbl inducing their base-off conformation [ 36 ]; however, it did not catalyze the dealkylation of MeCbl and AdoCbl, the two major dietary forms of Cbl. This intriguing finding was re-examined via ex vivo studies [ 37 ], and a new function was uncovered for the cblC protein: MMACHC is also a Cbl dealkylase [ 37 ].…”

Section: Biophysical and Structural Characterization Of The B 12 -Promentioning

confidence: 99%

“…The mystery of how decyanation of cyanocobalamin (CNCbl) occurs was recently solved by the in vitro studies of Kim et al [ 36 ]. The reductive decyanation of CNCbl is catalyzed by the MMACHC protein in the presence of a flavoprotein reductase and NADPH [ 36 ].…”

Section: Biophysical and Structural Characterization Of The B 12 -Promentioning

confidence: 99%

Proteomics of vitamin B12 processing

Hannibal

DiBello

Jacobsen³

2013

Clinical Chemistry and Laboratory Medicine

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The causes of cobalamin (B 12 , Cbl) deficiency are multifactorial. Whether nutritional due to poor dietary intake, or functional due to impairments in absorption or intracellular processing and trafficking events, the major symptoms of Cbl deficiency include megaloblastic anemia, neurological deterioration and in extreme cases, failure to thrive and death. The common biomarkers of Cbl deficiency (hyperhomocysteinemia and methylmalonic acidemia) are extremely valuable diagnostic indicators of the condition, but little is known about the changes that occur at the protein level. A mechanistic explanation bridging the physiological changes associated with functional B 12 deficiency with its intracellular processers and carriers is lacking. In this article, we will cover the effects of B 12 deficiency in a cblC -disrupted background (also referred to as MMACHC) as a model of functional Cbl deficiency. As will be shown, major protein changes involve the cytoskeleton, the neurological system as well as signaling and detoxification pathways. Supplementation of cultured MMACHC-mutant cells with hydroxocobalamin (HOCbl) failed to restore these variants to the normal phenotype, suggesting that a defective Cbl processing pathway produces irreversible changes at the protein level.

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“…Similarly, in the CblC-catalyzed dealkylation reaction, the glutathione thioether forms upon transfer of the alkyl group in addition to cob(I)alamin. When CNCbl is in the active site, electrons provided by free or protein-bound reduced flavin promote reductive homolytic cleavage, leading to cyanide elimination (13,35). Based on UV-visible and EPR spectroscopy, baseoff cob(II)alamin has been identified as the other product of the reductive elimination, consistent with a homolytic cleavage reaction mechanism.…”

Section: Early Steps In the Cytosolic Processing Of Cobalaminmentioning

confidence: 73%

“…The identity of the upper or ␤-axial ligand varies and includes cyano, aquo, methyl, and 5Ј-deoxyadenosyl groups. Ironically, 6 decades after its discovery, the origin and biological relevance of the cyano group remain unknown, although we have recently described a decyanase activity in the processing pathway (13), which allows utilization of CNCbl used in vitamin supplements. As the cobalt oxidation state decreases from 3 ϩ 3 2 ϩ 3 1 ϩ , the coordination number typically decreases from 6 3 5 3 4.…”

Section: B 12 Chemistry and Catalysismentioning

confidence: 99%

Navigating the B12 Road: Assimilation, Delivery, and Disorders of Cobalamin

Gherasim

Lofgren

Banerjee

2013

Journal of Biological Chemistry

Self Cite

177

123

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The reactivity of the cobalt-carbon bond in cobalamins is the key to their chemical versatility, supporting both methyl transfer and isomerization reactions. During evolution of higher eukaryotes that utilize vitamin B 12 , the high reactivity of the cofactor coupled with its low abundance pressured development of an efficient system for uptake, assimilation, and delivery of the cofactor to client B 12 -dependent enzymes. Although most proteins suspected to be involved in B 12 trafficking were discovered by 2009, the recent identification of a new protein reveals that the quest for elucidating the intracellular B 12 highway is still far from complete. Herein, we review the biochemistry of cobalamin trafficking.Cofactors are variously deployed in nature to stabilize macromolecular structures, expand catalytic functionality, transport gases, transduce signals, and function as sensors. Due to their relative rarity and/or reactivity, cells have evolved strategies for sequestering and regulating the movement of cofactors from their point of entry into the cell to their point of docking in target proteins (1). A subset of cofactors, i.e. the vitamins, is obtained in a precursor form from the diet. Reactions catalyzing the assimilation of inactive cofactors into their active forms are integral to their trafficking pathways. Similarly, elaboration of metals into clusters often occurs on chaperones that subsequently transfer the cofactor to target proteins. The interprotein transfer of metals can occur via ligand exchange reactions that are driven by differences in metal coordination geometry and affinity between the donor and acceptor proteins (2, 3). Seclusion of cofactors in chaperones during assembly/processing into their active forms minimizes unwanted side reactions, whereas guided delivery averts dilution and promotes specificity of cofactor docking.In contrast to our understanding of cellular strategies used for trafficking metals (4 -6) and metal clusters (7), significantly less is known about strategies for shepherding organic and organometallic cofactors to target proteins. This picture has been changing, however, with the convergence of clinical genetics and biochemical approaches that are beginning to illuminate an elaborate pathway for assimilation and delivery of dietary vitamin B 12 or cobalt-containing cobalamin, a complex organometallic cofactor (8 -10). Much less is known about how the tetrapyrrolic cousins of B 12 , e.g. iron protoporphyrin (heme), nickel corphin (F430), and magnesium chlorin (chlorophyll), are guided to specific destinations.In this minireview, we describe a model for mammalian cobalamin trafficking, which includes strategies for conversion of inactive precursors to the active cofactor forms methylcobalamin (MeCbl) 3 and 5Ј-deoxyadenosylcobalamin (AdoCbl; coenzyme B 12 ) and discuss the human diseases that result from impairments along the trafficking highway. We posit that the navigation strategy for B 12 , in which a rare, reactive, and high value cofactor is sequestered and targ...

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Decyanation of vitamin B ₁₂ by a trafficking chaperone

Cited by 194 publications

References 29 publications

Guided cobalamin biosynthesis supports Dehalococcoides mccartyi reductive dechlorination activity

Guided cobalamin biosynthesis supports Dehalococcoides mccartyi reductive dechlorination activity

Proteomics of vitamin B12 processing

Navigating the B12 Road: Assimilation, Delivery, and Disorders of Cobalamin

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Decyanation of vitamin B 12 by a trafficking chaperone

Cited by 194 publications

References 29 publications

Guided cobalamin biosynthesis supports Dehalococcoides mccartyi reductive dechlorination activity

Guided cobalamin biosynthesis supports Dehalococcoides mccartyi reductive dechlorination activity

Proteomics of vitamin B12 processing

Navigating the B12 Road: Assimilation, Delivery, and Disorders of Cobalamin

Contact Info

Product

Resources

About

Decyanation of vitamin B ₁₂ by a trafficking chaperone