The ERF Transcription Factor LTF1 Activates DIR1 to Control Stereoselective Synthesis of Antiviral Lignans and Stress Defense in Roots

Overview

Journal Acta Pharm Sin B

Publisher Elsevier

Specialty Pharmacology

Date 2024 Jan 23

PMID 38261810

Authors

Ruibing Chen

Jian Yu

Luyao Yu

Liang Xiao

Ying Xiao

Junfeng Chen

Shouhong Gao

Xianghui Chen

Qing Li

Henan Zhang

Wansheng Chen

Lei Zhang

Affiliations

Soon will be listed here.

Abstract

Lignans are a powerful weapon for plants to resist stresses and have diverse bioactive functions to protect human health. Elucidating the mechanisms of stereoselective biosynthesis and response to stresses of lignans is important for the guidance of plant improvement. Here, we identified the complete pathway to stereoselectively synthesize antiviral (-)-lariciresinol glucosides in roots, which consists of three-step sequential stereoselective enzymes DIR1/2, PLR, and UGT71B2. DIR1 was further identified as the key gene in respoJanuary 2024nse to stresses and was able to trigger stress defenses by mediating the elevation in lignan content. Mechanistically, the phytohormone-responsive ERF transcription factor LTF1 colocalized with DIR1 in the cell periphery of the vascular regions in mature roots and helped resist biotic and abiotic stresses by directly regulating the expression of DIR1. These systematic results suggest that DIR1 as the first common step of the lignan pathway cooperates with PLR and UGT71B2 to stereoselectively synthesize (-)-lariciresinol derived antiviral lignans in roots and is also a part of the LTF1-mediated regulatory network to resist stresses. In conclusion, the LTF1-DIR1 module is an ideal engineering target to improve plant Defenses while increasing the content of valuable lignans in plants.

Citing Articles

Construction of lignan glycosides biosynthetic network in Escherichia coli using mutltienzyme modules.

Qiao Y, Huang D, Li Y, Jiang S, Chen X, Chen J Microb Cell Fact. 2024; 23(1):193.

PMID: 38970026 PMC: 11225284. DOI: 10.1186/s12934-024-02467-1.

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