AI Article Synopsis

  • Ferredoxin (Fd) is crucial for photosynthesis and reductive metabolism in chloroplasts, with the Chlamydomonas reinhardtii genome having six distinct ferredoxins (Fd, Fdx2-Fdx6).
  • A study analyzed the localization and gene expression of these ferredoxins in response to different nutritional and stress conditions, using specific antibodies and monitoring factors like iron and copper levels.
  • The findings suggest that each FDX gene responds uniquely to nutrient changes, with Fdx2 being a more efficient electron donor under certain conditions, indicating the importance of having multiple ferredoxin isoforms for tailored metabolic functions in chloroplasts.

Article Abstract

Ferredoxin (Fd) is the major iron-containing protein in photosynthetic organisms and is central to reductive metabolism in the chloroplast. The Chlamydomonas reinhardtii genome encodes six plant type [Fe2S2] ferredoxins, products of PETF, FDX2-FDX6. We performed the functional analysis of these ferredoxins by localizing Fd, Fdx2, Fdx3, and Fdx6 to the chloroplast by using isoform-specific antibodies and monitoring the pattern of gene expression by iron and copper nutrition, nitrogen source, and hydrogen peroxide stress. In addition, we also measured the midpoint redox potentials of Fd and Fdx2 and determined the kinetic parameters of their reactions with several ferredoxin-interacting proteins, namely nitrite reductase, Fd:NADP+ oxidoreductase, and Fd:thioredoxin reductase. We found that each of the FDX genes is differently regulated in response to changes in nutrient supply. Moreover, we show that Fdx2 (Em = -321 mV), whose expression is regulated by nitrate, is a more efficient electron donor to nitrite reductase relative to Fd. Overall, the results suggest that each ferredoxin isoform has substrate specificity and that the presence of multiple ferredoxin isoforms allows for the allocation of reducing power to specific metabolic pathways in the chloroplast under various growth conditions.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2757988PMC
http://dx.doi.org/10.1074/jbc.M109.023622DOI Listing

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