Welcome to the new version of CaltechAUTHORS. Login is currently restricted to library staff. If you notice any issues, please email coda@library.caltech.edu
CaltechAUTHORS
Published August 25, 2020 | Submitted
Report Open

Modular metabolite assembly in C. elegans lysosome-related organelles

Le, Henry H. ORCID icon
Wrobel, Chester J. ORCID icon
Cohen, Sarah M. ORCID icon
Yu, Jingfang ORCID icon
Park, Heenam ORCID icon
Helf, Maximilian J. ORCID icon
Curtis, Brian J.
Rodrigues, Pedro R.
Sternberg, Paul W. ORCID icon
Schroeder, Frank C. ORCID icon

Abstract

Signaling molecules derived from attachment of diverse primary metabolic building blocks to ascarosides play a central role in the life history of C. elegans and other nematodes; however, many aspects of their biogenesis remain unclear. Using comparative metabolomics, we show that lysosome-related organelles (LROs) are required for biosynthesis of most modular ascarosides as well as previously undescribed modular glucosides. Both modular glucosides and ascarosides are derived from highly selective assembly of moieties from nucleoside, amino acid, neurotransmitter, and lipid metabolism. We further show that cholinesterase (cest) homologs that localize to the LROs are required for assembly of both modular ascarosides and glucosides, mediating formation of ester and amide linkages between subsets of building blocks. Their specific biosynthesis suggests that modular glucosides, like ascarosides, serve dedicated signaling functions. Further exploration of LRO function and cest homologs in C. elegans and other animals may reveal additional new compound families and signaling paradigms.

Additional Information

The copyright holder for this preprint is the author/funder, who has granted bioRxiv a license to display the preprint in perpetuity. All rights reserved. No reuse allowed without permission. Posted August 24, 2020. This research was funded by an NIH Chemical Biology Interface (CBI) Training Grant 5T32GM008500 (to B.C.), National Institutes of Health grants R35 GM131877 (to F.C.S.), and R24OD023041 (to P.W.S.). F.C.S. is a Faculty Scholar of the Howard Hughes Medical Institute. We thank WormBase for sequences, Tsui-Fen Chou for Cas9 protein, Ying (Kitty) Zhang for assistance with NMR spectroscopy, and Navid Movahed for assistance with mass spectrometry. Author Contributions: The manuscript was written through contributions of all authors and all authors have given approval to the final version of the manuscript. The authors declare no competing interests.

Attached Files

Submitted - 2020.08.22.262956v1.full.pdf

Files

2020.08.22.262956v1.full.pdf
Files (1.5 MB)
Name Size Download all
md5:18f042978ea66590799e6b48d8bff65f
1.5 MB Preview Download

Additional details

Identifiers Funding Dates Caltech Custom Metadata
Created:
August 19, 2023
Modified:
December 13, 2023