What Is 3-dehydroquinate hydro-lyase

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Last updated: April 15, 2026

Quick Answer: 3-Dehydroquinate hydro-lyase (DHQH) is an enzyme that catalyzes the third step in the shikimate pathway, converting 3-dehydroquinate into 3-dehydroshikimate. This reaction is essential for aromatic amino acid biosynthesis in plants, fungi, and bacteria.

Key Facts

3-Dehydroquinate hydro-lyase catalyzes the third step in the shikimate pathway, a critical metabolic route.
The enzyme converts 3-dehydroquinate into 3-dehydroshikimate through a dehydration reaction.
DHQH is absent in humans, making it a potential target for antibiotic and herbicide development.
The enzyme is encoded by the aroD gene in Escherichia coli and other bacteria.
Structural studies show DHQH has a TIM barrel fold, common in enzymes involved in carbohydrate metabolism.

Overview

3-Dehydroquinate hydro-lyase (DHQH) is a key enzyme in the shikimate pathway, which is responsible for the biosynthesis of aromatic amino acids such as phenylalanine, tyrosine, and tryptophan. This pathway is absent in animals but vital in plants, fungi, and most bacteria, making DHQH a strategic target for antimicrobial and herbicide research.

The enzyme functions by catalyzing the reversible dehydration of 3-dehydroquinate to form 3-dehydroshikimate, a necessary intermediate in the pathway. Because this step is not present in mammals, inhibitors of DHQH do not affect human metabolism, enhancing its appeal for drug development.

Reaction catalyzed: DHQH converts 3-dehydroquinate into 3-dehydroshikimate through the elimination of water, a key step in the seven-step shikimate pathway.
Gene origin: In Escherichia coli, the aroD gene encodes DHQH, and mutations in this gene disrupt aromatic amino acid synthesis, leading to bacterial auxotrophy.
Enzyme class: It belongs to the hydro-lyase family (EC 4.2.1.10), which cleaves C–O bonds via elimination reactions without hydrolysis.
Structural motif: DHQH exhibits a β/α-barrel (TIM barrel) fold, a conserved protein architecture seen in many enzymes involved in metabolic pathways.
Thermostability: Studies on Mycobacterium tuberculosis DHQH show it remains active up to 50°C, indicating moderate thermal resilience.

How It Works

DHQH operates through a precise mechanism involving acid-base catalysis and metal ion coordination, depending on the organism. The active site facilitates proton abstraction and stabilization of reaction intermediates to enable efficient dehydration.

Substrate:3-Dehydroquinate binds to the active site, where its hydroxyl groups coordinate with a divalent metal ion, typically Mg²⁺ or Mn²⁺, enhancing reactivity.
Catalytic residues:Glutamate and lysine residues act as proton donors and acceptors, facilitating the removal of water from the substrate in a stereospecific manner.
Reaction type: The enzyme performs a syn-elimination of water, forming a double bond between C2 and C3 of the ring structure in 3-dehydroshikimate.
Reversibility: The reaction is reversible under physiological conditions, allowing the enzyme to function bidirectionally depending on substrate concentration.
Quaternary structure: In E. coli, DHQH functions as a homodimer, with each subunit contributing to the stability and catalytic efficiency of the enzyme.
Inhibitors:Carbaphosphonate analogs mimic the transition state and inhibit DHQH activity, showing promise as lead compounds for antibiotic development.

Comparison at a Glance

Below is a comparison of DHQH across different organisms, highlighting structural and functional variations:

Organism	Gene	Protein Length (aa)	Optimal pH	Function in Pathway
Escherichia coli	aroD	229	7.5	Catalyzes step 3 of shikimate pathway
Mycobacterium tuberculosis	aroD	234	8.0	Essential for pathogen survival in host
Saccharomyces cerevisiae	ARO3/ARO4	245	7.0	Regulated by feedback inhibition
Arabidopsis thaliana	At4g39980	258	7.8	Targeted by glyphosate adjuvants
Plasmodium falciparum	PF3D7_1313800	267	7.2	Potential antimalarial drug target

These variations reflect evolutionary adaptations in different kingdoms. While bacterial and fungal forms are well-characterized, plant and protozoan versions show increased regulatory complexity and potential for selective targeting in disease control.

Why It Matters

Understanding 3-dehydroquinate hydro-lyase has significant implications for medicine, agriculture, and biotechnology. Its absence in humans makes it a safe target for antimicrobial agents, and its role in essential biosynthesis pathways underscores its biological importance.

Antibiotic development: Inhibiting DHQH in M. tuberculosis could lead to novel anti-TB drugs with minimal human toxicity.
Herbicide design: Compounds targeting plant DHQH can disrupt growth, offering selective weed control without harming animals.
Metabolic engineering: Engineered E. coli strains with modified DHQH are used to overproduce aromatic compounds for industrial applications.
Drug resistance: Monitoring aroD mutations helps track resistance development in bacterial pathogens exposed to experimental inhibitors.
Structural biology: DHQH’s TIM barrel structure provides insights into enzyme evolution and catalytic mechanism conservation.
Antimalarial research:Plasmodium relies on the shikimate pathway in its apicoplast, making DHQH a promising target for new antimalarials.