LOVASTATIN INSENSITIVE 1, a novel pentatricopeptide repeat protein, is a potential regulatory factor of isoprenoid biosynthesis in Arabidopsis

Higher plants have two metabolic pathways for isoprenoid biosynthesis: the cytosolic mevalonate (MVA) pathway and the plastidal non-mevalonate (MEP) pathway. Despite the compartmentalization of these two pathways, metabolic flow occurs between them. However, little is known about the mechanisms that...

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Bibliographic Details
Published in:Plant and cell physiology 2007-02, Vol.48 (2), p.322-331
Main Authors: Kobayashi, K.(Institute of Physical and Chemical Research, Yokohama (Japan). Plant Science Center), Suzuki, M, Tang, J, Nagata, N, Ohyama, K, Seki, H, Kiuchi, R, Kaneko, Y, Nakazawa, M, Matsui, M, Matsumoto, S, Yoshida, S, Muranaka, T
Format: Article
Language:English
Subjects:
Arabidopsis
Arabidopsis - genetics
Arabidopsis - metabolism
Arabidopsis Proteins - genetics
Arabidopsis Proteins - physiology
ARABIDOPSIS THALIANA
Base Sequence
CHLOROPHYLLE
CHLOROPHYLLS
CLOROFILAS
DNA Primers
DNA, Bacterial
ISOPRENOIDE
ISOPRENOIDES
ISOPRENOIDS
MITOCHONDRIA
MITOCHONDRIE
MITOCONDRIA
MUTANT
MUTANTES
MUTANTS
PHYSIOLOGICAL REGULATION
Polyisoprenyl Phosphates - biosynthesis
Promoter Regions, Genetic
REGULACION FISIOLOGICA
REGULATION PHYSIOLOGIQUE
TRANSCRIPCION
TRANSCRIPTION
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Summary:Higher plants have two metabolic pathways for isoprenoid biosynthesis: the cytosolic mevalonate (MVA) pathway and the plastidal non-mevalonate (MEP) pathway. Despite the compartmentalization of these two pathways, metabolic flow occurs between them. However, little is known about the mechanisms that regulate the two pathways and the metabolic cross-talk. To identify such regulatory mechanisms, we isolated and characterized the Arabidopsis T-DNA insertion mutant lovastatin insensitive 1 (loi1), which is resistant to lovastatin and clomazone, inhibitors of the MVA and MEP pathways, respectively. The accumulation of the major products of these pathways, i.e. sterols and chlorophyll, was less affected by lovastatin and clomazone, respectively, in loi1 than in the wild type. Furthermore, the 3-hydroxy-3-methylglutaryl coenzyme A reductase (HMGR) activity analysis showed higher activity of HMGR in loi1-1 treated with lovastatin than that in the WT. We consider that the lovastatin-resistant phenotype of loi1-1 was derived from this post-transcriptional up-regulation of HMGR. The LOI1 gene encodes a novel pentatricopeptide repeat (PPR) protein. PPR proteins are thought to regulate the expression of genes encoded in organelle genomes by post-transcriptional regulation in mitochondria or plastids. Our results demonstrate that LOI1 is predicted to localize in mitochondria and has the ability to bind single-stranded nucleic acids. Our investigation revealed that the post-transcriptional regulation of mitochondrial RNA may be involved in isoprenoid biosynthesis in both the MVA and MEP pathways.
ISSN:0032-0781
1471-9053
DOI:10.1093/pcp/pcm005