Cysteine: an ancestral Cu binding ligand in green algae?

Author:

Strenkert DanielaORCID,Schmollinger StefanORCID,Hu YuntaoORCID,Hofmann Christian,Holbrook Kristen,Liu Helen W.,Purvine Samuel O.,Nicora Carrie D.,Chen Si,Lipton Mary S.,Northen Trent R.,Clemens Stephan,Merchant Sabeeha S.ORCID

Abstract

ABSTRACTGrowth ofChlamydomonas reinhardtiiin zinc (Zn) limited medium leads to disruption of copper (Cu) homeostasis, resulting in up to 40-fold Cu over-accumulation relative to its typical Cu quota. We show that Chlamydomonas controls its Cu quota by balancing Cu import and export, which is disrupted in a Zn deficient cell, thus establishing a mechanistic connection between Cu and Zn homeostasis. Transcriptomics, proteomics and elemental profiling revealed that Zn-limited Chlamydomonas cells up-regulate a subset of genes encoding “first responder” proteins involved in sulfur (S) assimilation and consequently accumulate more intracellular S, which is incorporated into L-cysteine, γ-glutamylcysteine and homocysteine. Most prominently, in the absence of Zn, free L-cysteine is increased ~80-fold, corresponding to ~ 2.8 × 109molecules/cell. Interestingly, classic S-containing metal binding ligands like glutathione and phytochelatins do not increase. X-ray fluorescence microscopy showed foci of S accumulation in Zn-limited cells that co-localize with Cu, phosphorus and calcium, consistent with Cu-thiol complexes in the acidocalcisome, the site of Cu(I) accumulation. Notably, cells that have been previously starved for Cu do not accumulate S or Cys, causally connecting cysteine synthesis with Cu accumulation. We suggest that cysteine is anin vivoCu(I) ligand, perhaps ancestral, that buffers cytosolic Cu.

Publisher

Cold Spring Harbor Laboratory

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