4.5 Article

Rim2, a pyrimidine nucleotide exchanger, is needed for iron utilization in mitochondria

Journal

BIOCHEMICAL JOURNAL
Volume 440, Issue -, Pages 137-146

Publisher

PORTLAND PRESS LTD
DOI: 10.1042/BJ20111036

Keywords

haem; iron; iron-sulfur; mitochondrial carrier protein; mitochondrion; pyrimidine

Funding

  1. National Institutes of Health [R37DK053953]
  2. National Institute on Aging [AG030504]
  3. American Heart Association [09GRNT2260364]

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Mitochondria transport and utilize iron for the synthesis of haem and Fe-S clusters. Although many proteins are known to be involved in these processes, additional proteins are likely to participate. To test this hypothesis, in the present study we used a genetic screen looking for yeast mutants that are synthetically lethal with the mitochondrial iron carriers Mrs3 and Mrs4. Several genes were identified, including an isolate mutated for Yfh1, the yeast frataxin homologue. All such triple mutants were complemented by increased expression of Rim2, another mitochondrial carrier protein. Rim2 overexpression was able to enhance haem and Fe-S cluster synthesis in wildtype or Delta mrs3/Delta mrs4 backgrounds. Conversely Rim2 depletion impaired haem and Fe-S cluster synthesis in wild-type or Delta mrs3/Delta mrs4 backgrounds, indicating a unique requirement for this mitochondrial transporter for these processes. Rim2 was previously shown to mediate pyrimidine exchange in and out of vesicles. In the present study we found that isolated mitochondria lacking Rim2 exhibited concordant iron defects and pyrimidine transport defects, although the connection between these two functions is not explained. When organellar membranes were ruptured to bypass iron transport, ham synthesis from added iron and porphyrin was still markedly deficient in Rim2-depleted mitochondrial lysate. The results indicate that Rim2 is a pyrimidine exchanger with an additional unique function in promoting mitochondrial iron utilization.

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