Subcellular tracking reveals the location of dimethylsulfoniopropionate in microalgae and visualises its uptake by marine bacteria

Jean Baptiste Raina*, Peta L. Clode, Soshan Cheong, Jeremy Bougoure, Matt R. Kilburn, Anthony Reeder, Sylvain Forêt, Michael Stat, Victor Beltran, Peter Thomas-Hall, Dianne Tapiolas, Cherie M. Motti, Bill Gong, Mathieu Pernice, Christopher E. Marjo, Justin R. Seymour, Bette L. Willis, David G. Bourne

*Corresponding author for this work

    Research output: Contribution to journalArticlepeer-review

    69 Citations (Scopus)

    Abstract

    Phytoplankton-bacteria interactions drive the surface ocean sulfur cycle and local climatic processes through the production and exchange of a key compound: dimethylsulfoniopropionate (DMSP). Despite their large-scale implications, these interactions remain unquantified at the cellular-scale. Here we use secondary-ion mass spectrometry to provide the first visualization of DMSP at sub-cellular levels, tracking the fate of a stable sulfur isotope (34S) from its incorporation by microalgae as inorganic sulfate to its biosynthesis and exudation as DMSP, and finally its uptake and degradation by bacteria. Our results identify for the first time the storage locations of DMSP in microalgae, with high enrichments present in vacuoles, cytoplasm and chloroplasts. In addition, we quantify DMSP incorporation at the single-cell level, with DMSPdegrading bacteria containing seven times more 34S than the control strain. This study provides an unprecedented methodology to label, retain, and image small diffusible molecules, which can be transposable to other symbiotic systems.

    Original languageEnglish
    Article numbere23008
    JournaleLife
    Volume6
    DOIs
    Publication statusPublished - 4 Apr 2017

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