What Is 2-methylcitrate dehydratase
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Last updated: April 15, 2026
Key Facts
- 2-methylcitrate dehydratase catalyzes the dehydration of 2-methylcitrate to 2-methyl-*cis*-aconitate with <strong>Km = 0.3 mM</strong> in *Salmonella*.
- The enzyme is encoded by the <strong>prpD gene</strong>, first identified in <strong>1999</strong> in *Salmonella enterica*.
- It functions in the <strong>propionyl-CoA catabolic pathway</strong>, essential for metabolizing odd-chain fatty acids and branched-chain amino acids.
- Defects in this pathway are linked to <strong>propionic acidemia</strong>, a rare metabolic disorder in humans.
- The enzyme is structurally related to <strong>aconitase</strong> but shows substrate specificity for methyl-substituted citrates.
Overview
2-methylcitrate dehydratase is a key enzyme in the 2-methylcitric acid cycle, a metabolic pathway used by various organisms to break down propionyl-CoA. This compound arises from the catabolism of odd-chain fatty acids, cholesterol, and several amino acids like isoleucine and valine.
The enzyme specifically catalyzes the third step in the methylcitrate cycle, converting 2-methylcitrate into 2-methyl-*cis*-aconitate through a dehydration reaction. It is essential for energy production and detoxification in microbes such as *Salmonella enterica* and *Aspergillus nidulans*.
- Substrate specificity: The enzyme acts exclusively on 2-methylcitrate, showing no activity toward citrate or isocitrate, which ensures pathway fidelity.
- Kinetic efficiency: In *Salmonella*, the enzyme has a Km of 0.3 mM for 2-methylcitrate, indicating high affinity under physiological conditions.
- Gene origin: The prpD gene encodes this enzyme and was first cloned and characterized in 1999 during studies on propionate metabolism.
- Organism distribution: Found in bacteria like *E. coli* and fungi including *Candida albicans*, indicating evolutionary conservation across kingdoms.
- pH optimum: The enzyme functions optimally at pH 7.5–8.0, consistent with cytosolic enzyme activity in most microbial systems.
How It Works
2-methylcitrate dehydratase operates via a metal-independent mechanism, removing a water molecule from 2-methylcitrate to form the unsaturated intermediate 2-methyl-*cis*-aconitate. This step is analogous to the aconitase-catalyzed reaction in the TCA cycle but tailored for methylated substrates.
- Reaction type: The enzyme catalyzes a dehydration reaction, eliminating the –OH group from C3 and a hydrogen from C2 of 2-methylcitrate.
- Catalytic residues: Mutagenesis studies show that histidine 143 and aspartate 147 in *Salmonella* are essential for proton abstraction and catalysis.
- Intermediate stability: The product, 2-methyl-*cis*-aconitate, is unstable and is rapidly hydrated by 2-methylisocitrate lyase in the next pathway step.
- Enzyme class: Classified as a lyase (EC 4.2.1.87), it belongs to the enolase superfamily, sharing structural motifs with other dehydratases.
- Temperature sensitivity: Activity peaks at 37°C in mesophilic bacteria, with sharp decline above 45°C, indicating thermal instability.
- Inhibitors:Phosphonoacetate acts as a competitive inhibitor with a Ki of 0.1 mM, useful in experimental studies of the pathway.
Comparison at a Glance
The following table compares 2-methylcitrate dehydratase with related enzymes in structure, function, and biological role:
| Feature | 2-Methylcitrate Dehydratase | Aconitase | Isocitrate Dehydrogenase |
|---|---|---|---|
| EC Number | 4.2.1.87 | 4.2.1.3 | 1.1.1.42 |
| Primary Substrate | 2-methylcitrate | Citrate | Isocitrate |
| Reaction Type | Dehydration | Dehydration | Oxidative decarboxylation |
| Metabolic Pathway | Methylcitrate cycle | TCA cycle | TCA cycle |
| Gene (in E. coli) | prpD | acnA/acnB | icd |
While all three enzymes process citrate derivatives, 2-methylcitrate dehydratase is specialized for methylated substrates, preventing interference with central carbon metabolism. Its presence allows microbes to utilize propionate as a carbon source, a capability absent in organisms lacking the *prp* operon.
Why It Matters
Understanding 2-methylcitrate dehydratase has implications for microbial physiology, biotechnology, and human health. Its role in propionate detoxification is critical for pathogens surviving in host environments rich in fatty acids and amino acids.
- Antifungal targets: In *Candida albicans*, disruption of the methylcitrate pathway reduces virulence, making prpD a potential drug target.
- Bioremediation: Engineered bacteria with enhanced 2-methylcitrate dehydratase activity can degrade environmental propionates and industrial byproducts.
- Metabolic engineering: Used in synthetic biology to reroute carbon flux in biofuel-producing microbes utilizing odd-chain substrates.
- Human disease link: Defects in analogous pathways cause propionic acidemia, a disorder with neurological and metabolic symptoms.
- Diagnostic marker: Elevated 2-methylcitrate in urine is a biomarker for propionic acidemia, detectable via mass spectrometry.
- Evolutionary insight: Gene duplication events from aconitase ancestors suggest divergent evolution driven by substrate specialization.
Further research into the enzyme’s structure and regulation may lead to new antimicrobial strategies and improved metabolic disease diagnostics.
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Sources
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