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An enzyme-trap approach allows isolation of intermediates in cobalamin biosynthesis
Journal article

An enzyme-trap approach allows isolation of intermediates in cobalamin biosynthesis

Evelyne Deery, Susanne Schroeder, Andrew D. Lawrence, Samantha L. Taylor, Arefeh Seyedarabi, Jitka Waterman, Keith S. Wilson, David Brown, Michael A. Geeves, Mark J. Howard, …
Nature chemical biology, Vol.8(11), pp.933-940
2012
PMCID: PMC3480714
PMID: 23042036

Abstract

Biochemistry & Molecular Biology Life Sciences & Biomedicine Science & Technology
The biosynthesis of many vitamins and coenzymes has often proven difficult to elucidate owing to a combination of low abundance and kinetic lability of the pathway intermediates. Through a serial reconstruction of the cobalamin (vitamin B-12) pathway in Escherichia coli and by His tagging the terminal enzyme in the reaction sequence, we have observed that many unstable intermediates can be isolated as tightly bound enzyme-product complexes. Together, these approaches have been used to extract intermediates between precorrin-4 and hydrogenobyrinic acid in their free acid form and permitted the delineation of the overall reaction catalyzed by CobL, including the formal elucidation of precorrin-7 as a metabolite. Furthermore, a substrate-carrier protein, CobE, that can also be used to stabilize some of the transient metabolic intermediates and enhance their onward transformation, has been identified. The tight association of pathway intermediates with enzymes provides evidence for a form of metabolite channeling.

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Collaboration types
Domestic collaboration
Citation topics
3 Agriculture, Environment & Ecology
3.171 Photoproductivity
3.171.1776 Acute Intermittent Porphyria
Web Of Science research areas
Biochemistry & Molecular Biology
ESI research areas
Biology & Biochemistry
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