A dolabralexin-deficient mutant provides insight into specialized diterpenoid metabolism in maize

Author:

Murphy Katherine M1ORCID,Dowd Tyler2ORCID,Khalil Ahmed3ORCID,Char Si Nian4ORCID,Yang Bing24,Endelman Benjamin J1ORCID,Shih Patrick M56,Topp Christopher2ORCID,Schmelz Eric A3ORCID,Zerbe Philipp1ORCID

Affiliation:

1. Department of Plant Biology, University of California-Davis , Davis, CA 95616 , USA

2. Donald Danforth Plant Science Center , St. Louis, MO 63132 , USA

3. Section of Cell and Developmental Biology, University of California San Diego , La Jolla, CA 92093 , USA

4. Division of Plant Science and Technology, University of Missouri , Columbia, MO 65211 , USA

5. Environmental Genomics and Systems Biology Division, Lawrence Berkeley National Laboratory , Berkeley, CA 94720 , USA

6. Department of Plant and Microbial Biology, UC Berkeley , Berkeley, CA 94720 , USA

Abstract

Abstract Two major groups of specialized metabolites in maize (Zea mays), termed kauralexins and dolabralexins, serve as known or predicted diterpenoid defenses against pathogens, herbivores, and other environmental stressors. To consider the physiological roles of the recently discovered dolabralexin pathway, we examined dolabralexin structural diversity, tissue-specificity, and stress-elicited production in a defined biosynthetic pathway mutant. Metabolomics analyses support a larger number of dolabralexin pathway products than previously known. We identified dolabradienol as a previously undetected pathway metabolite and characterized its enzymatic production. Transcript and metabolite profiling showed that dolabralexin biosynthesis and accumulation predominantly occur in primary roots and show quantitative variation across genetically diverse inbred lines. Generation and analysis of CRISPR-Cas9-derived loss-of-function Kaurene Synthase-Like 4 (Zmksl4) mutants demonstrated dolabralexin production deficiency, thus supporting ZmKSL4 as the diterpene synthase responsible for the conversion of geranylgeranyl pyrophosphate precursors into dolabradiene and downstream pathway products. Zmksl4 mutants further display altered root-to-shoot ratios and root architecture in response to water deficit. Collectively, these results demonstrate dolabralexin biosynthesis via ZmKSL4 as a committed pathway node biochemically separating kauralexin and dolabralexin metabolism, and suggest an interactive role of maize dolabralexins in plant vigor during abiotic stress.

Funder

National Science Foundation

NSF Graduate Research Fellowship Program

UC Davis Innovation Institute for Food and Health

USDA NIFA Predoctoral Fellowship Program

Publisher

Oxford University Press (OUP)

Subject

Plant Science,Genetics,Physiology

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