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Anne-Marie Duchêne

Bio: Anne-Marie Duchêne is an academic researcher from University of Strasbourg. The author has contributed to research in topics: Transfer RNA & Mitochondrion. The author has an hindex of 25, co-authored 38 publications receiving 1673 citations. Previous affiliations of Anne-Marie Duchêne include Institut national de la recherche agronomique & Centre national de la recherche scientifique.

Papers
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Journal ArticleDOI
TL;DR: A systematic analysis of the targeting of organellar aminoacyl-tRNA synthetases in the model plant Arabidopsis thaliana indicates that extensive exchange of aaRSs has occurred during evolution and that many are now shared between two or even three compartments.
Abstract: In plants, protein synthesis occurs in the cytosol, mitochondria, and plastids. Each compartment requires a full set of tRNAs and aminoacyl-tRNA synthetases. We have undertaken a systematic analysis of the targeting of organellar aminoacyl-tRNA synthetases in the model plant Arabidopsis thaliana. Dual targeting appeared to be a general rule. Among the 24 identified organellar aminoacyl-tRNA synthetases (aaRSs), 15 (and probably 17) are shared between mitochondria and plastids, and 5 are shared between cytosol and mitochondria (one of these aaRSs being present also in chloroplasts). Only two were shown to be uniquely chloroplastic and none to be uniquely mitochondrial. Moreover, there are no examples where the three aaRS genes originating from the three ancestral genomes still coexist. These results indicate that extensive exchange of aaRSs has occurred during evolution and that many are now shared between two or even three compartments. The findings have important implications for studies of the translation machinery in plants and on protein targeting and gene transfer in general.

248 citations

Journal ArticleDOI
TL;DR: All mitochondrial aminoacyl-tRNA synthetases and many tRNAs are imported from the cytosol into the mitochondria in eukaryotic cells and their origin and their import into the organelle have been studied in evolutionary distinct organisms.
Abstract: During evolution, most of the bacterial genes from the ancestral endosymbiotic α-proteobacteria at the origin of mitochondria have been either lost or transferred to the nuclear genome. A crucial evolutionary step was the establishment of macromolecule import systems to allow the come back of proteins and RNAs into the organelle. Paradoxically, the few mitochondria-encoded protein genes remain essential and must be translated by a mitochondrial translation machinery mainly constituted by nucleus-encoded components. Two crucial partners of the mitochondrial translation machinery are the aminoacyl-tRNA synthetases and the tRNAs. All mitochondrial aminoacyl-tRNA synthetases and many tRNAs are imported from the cytosol into the mitochondria in eukaryotic cells. During the last few years, their origin and their import into the organelle have been studied in evolutionary distinct organisms and we review here what is known in this field.

133 citations

Journal ArticleDOI
TL;DR: The characterization of both direct and co-import mechanisms involving distinct protein-import factors is in agreement with a polyphyletic origin of tRNA import.

122 citations

Journal ArticleDOI
TL;DR: These findings identify unexpected components of the tRNA import machinery and suggest that the plant tRNAs import pathway has evolved by recruiting multifunctional proteins.
Abstract: In plants, as in most eukaryotic cells, import of nuclear-encoded cytosolic tRNAs is an essential process for mitochondrial biogenesis. Despite its broad occurrence, the mechanisms governing RNA transport into mitochondria are far less understood than protein import. This article demonstrates by Northwestern and gel-shift experiments that the plant mitochondrial voltage-dependent anion channel (VDAC) protein interacts with tRNA in vitro. It shows also that this porin, known to play a key role in metabolite transport, is a major component of the channel involved in the tRNA translocation step through the plant mitochondrial outer membrane, as supported by inhibition of tRNA import into isolated mitochondria by VDAC antibodies and Ruthenium red. However VDAC is not a tRNA receptor on the outer membrane. Rather, two major components from the TOM (translocase of the outer mitochondrial membrane) complex, namely TOM20 and TOM40, are important for tRNA binding at the surface of mitochondria, suggesting that they are also involved in tRNA import. Finally, we show that proteins and tRNAs are translocated into plant mitochondria by different pathways. Together, these findings identify unexpected components of the tRNA import machinery and suggest that the plant tRNA import pathway has evolved by recruiting multifunctional proteins.

110 citations

Journal ArticleDOI
TL;DR: It is demonstrated that the Arabidopsis RNases T2, called RNS, are key players of both long and short tRFs biogenesis, and an evolutionary conserved feature of these enzymes in eukaryotes is suggested.
Abstract: RNA fragments deriving from tRNAs (tRFs) exist in all branches of life and the repertoire of their biological functions regularly increases. Paradoxically, their biogenesis remains unclear. The human RNase A, Angiogenin, and the yeast RNase T2, Rny1p, generate long tRFs after cleavage in the anticodon region. The production of short tRFs after cleavage in the D or T regions is still enigmatic. Here, we show that the Arabidopsis Dicer-like proteins, DCL1-4, do not play a major role in the production of tRFs. Rather, we demonstrate that the Arabidopsis RNases T2, called RNS, are key players of both long and short tRFs biogenesis. Arabidopsis RNS show specific expression profiles. In particular, RNS1 and RNS3 are mainly found in the outer tissues of senescing seeds where they are the main endoribonucleases responsible of tRNA cleavage activity for tRFs production. In plants grown under phosphate starvation conditions, the induction of RNS1 is correlated with the accumulation of specific tRFs. Beyond plants, we also provide evidence that short tRFs can be produced by the yeast Rny1p and that, in vitro, human RNase T2 is also able to generate long and short tRFs. Our data suggest an evolutionary conserved feature of these enzymes in eukaryotes.

92 citations


Cited by
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Journal ArticleDOI
Sabeeha S. Merchant1, Simon E. Prochnik2, Olivier Vallon3, Elizabeth H. Harris4, Steven J. Karpowicz1, George B. Witman5, Astrid Terry2, Asaf Salamov2, Lillian K. Fritz-Laylin6, Laurence Maréchal-Drouard7, Wallace F. Marshall8, Liang-Hu Qu9, David R. Nelson10, Anton A. Sanderfoot11, Martin H. Spalding12, Vladimir V. Kapitonov13, Qinghu Ren, Patrick J. Ferris14, Erika Lindquist2, Harris Shapiro2, Susan Lucas2, Jane Grimwood15, Jeremy Schmutz15, Pierre Cardol3, Pierre Cardol16, Heriberto Cerutti17, Guillaume Chanfreau1, Chun-Long Chen9, Valérie Cognat7, Martin T. Croft18, Rachel M. Dent6, Susan K. Dutcher19, Emilio Fernández20, Hideya Fukuzawa21, David González-Ballester22, Diego González-Halphen23, Armin Hallmann, Marc Hanikenne16, Michael Hippler24, William Inwood6, Kamel Jabbari25, Ming Kalanon26, Richard Kuras3, Paul A. Lefebvre11, Stéphane D. Lemaire27, Alexey V. Lobanov17, Martin Lohr28, Andrea L Manuell29, Iris Meier30, Laurens Mets31, Maria Mittag32, Telsa M. Mittelmeier33, James V. Moroney34, Jeffrey L. Moseley22, Carolyn A. Napoli33, Aurora M. Nedelcu35, Krishna K. Niyogi6, Sergey V. Novoselov17, Ian T. Paulsen, Greg Pazour5, Saul Purton36, Jean-Philippe Ral7, Diego Mauricio Riaño-Pachón37, Wayne R. Riekhof, Linda A. Rymarquis38, Michael Schroda, David B. Stern39, James G. Umen14, Robert D. Willows40, Nedra F. Wilson41, Sara L. Zimmer39, Jens Allmer42, Janneke Balk18, Katerina Bisova43, Chong-Jian Chen9, Marek Eliáš44, Karla C Gendler33, Charles R. Hauser45, Mary Rose Lamb46, Heidi K. Ledford6, Joanne C. Long1, Jun Minagawa47, M. Dudley Page1, Junmin Pan48, Wirulda Pootakham22, Sanja Roje49, Annkatrin Rose50, Eric Stahlberg30, Aimee M. Terauchi1, Pinfen Yang51, Steven G. Ball7, Chris Bowler25, Carol L. Dieckmann33, Vadim N. Gladyshev17, Pamela J. Green38, Richard A. Jorgensen33, Stephen P. Mayfield29, Bernd Mueller-Roeber37, Sathish Rajamani30, Richard T. Sayre30, Peter Brokstein2, Inna Dubchak2, David Goodstein2, Leila Hornick2, Y. Wayne Huang2, Jinal Jhaveri2, Yigong Luo2, Diego Martinez2, Wing Chi Abby Ngau2, Bobby Otillar2, Alexander Poliakov2, Aaron Porter2, Lukasz Szajkowski2, Gregory Werner2, Kemin Zhou2, Igor V. Grigoriev2, Daniel S. Rokhsar6, Daniel S. Rokhsar2, Arthur R. Grossman22 
University of California, Los Angeles1, United States Department of Energy2, University of Paris3, Duke University4, University of Massachusetts Medical School5, University of California, Berkeley6, Centre national de la recherche scientifique7, University of California, San Francisco8, Sun Yat-sen University9, University of Tennessee Health Science Center10, University of Minnesota11, Iowa State University12, Genetic Information Research Institute13, Salk Institute for Biological Studies14, Stanford University15, University of Liège16, University of Nebraska–Lincoln17, University of Cambridge18, Washington University in St. Louis19, University of Córdoba (Spain)20, Kyoto University21, Carnegie Institution for Science22, National Autonomous University of Mexico23, University of Münster24, École Normale Supérieure25, University of Melbourne26, University of Paris-Sud27, University of Mainz28, Scripps Research Institute29, Ohio State University30, University of Chicago31, University of Jena32, University of Arizona33, Louisiana State University34, University of New Brunswick35, University College London36, University of Potsdam37, Delaware Biotechnology Institute38, Boyce Thompson Institute for Plant Research39, Macquarie University40, Oklahoma State University Center for Health Sciences41, İzmir University of Economics42, Academy of Sciences of the Czech Republic43, Charles University in Prague44, St. Edward's University45, University of Puget Sound46, Hokkaido University47, Tsinghua University48, Washington State University49, Appalachian State University50, Marquette University51
12 Oct 2007-Science
TL;DR: Analyses of the Chlamydomonas genome advance the understanding of the ancestral eukaryotic cell, reveal previously unknown genes associated with photosynthetic and flagellar functions, and establish links between ciliopathy and the composition and function of flagella.
Abstract: Chlamydomonas reinhardtii is a unicellular green alga whose lineage diverged from land plants over 1 billion years ago. It is a model system for studying chloroplast-based photosynthesis, as well as the structure, assembly, and function of eukaryotic flagella (cilia), which were inherited from the common ancestor of plants and animals, but lost in land plants. We sequenced the approximately 120-megabase nuclear genome of Chlamydomonas and performed comparative phylogenomic analyses, identifying genes encoding uncharacterized proteins that are likely associated with the function and biogenesis of chloroplasts or eukaryotic flagella. Analyses of the Chlamydomonas genome advance our understanding of the ancestral eukaryotic cell, reveal previously unknown genes associated with photosynthetic and flagellar functions, and establish links between ciliopathy and the composition and function of flagella.

2,554 citations

01 Jan 2010
TL;DR: It is found that women over 50 are more likely to have a family history of diabetes, especially if they are obese, than women under the age of 50.
Abstract: Hypertension 66 (20.3%) 24 (24.2%) 30 (16.3%) NS Diabetes 20 (6.2%) 7 (7.1%) 10 (5.4%) NS Excess weight 78 (24%) 27 (27.3%) 44 (23.9%) NS Smokers 64 (19.7%) 17 (17.2%) 35 (19.0%) NS Age >50 years 137 (42.2%) 54 (54.5%) 67 (36.4%) <0.02 Kidney disease 7 (2.2%) 1 (1%) 5 (2.7%) NS Family history, DM 102 (31.4%) 28 (28.3%) 66 (35.9%) NS

1,369 citations

Journal ArticleDOI
TL;DR: This updated Arabidopsis genome annotation with a substantially increased resolution of gene models will not only further the understanding of the biological processes of this plant model but also of other species.
Abstract: Summary The flowering plant Arabidopsis thaliana is a dicot model organism for research in many aspects of plant biology. A comprehensive annotation of its genome paves the way for understanding the functions and activities of all types of transcripts, including mRNA, the various classes of non-coding RNA, and small RNA. The TAIR10 annotation update had a profound impact on Arabidopsis research but was released more than 5 years ago. Maintaining the accuracy of the annotation continues to be a prerequisite for future progress. Using an integrative annotation pipeline, we assembled tissue-specific RNA-Seq libraries from 113 datasets and constructed 48 359 transcript models of protein-coding genes in eleven tissues. In addition, we annotated various classes of non-coding RNA including microRNA, long intergenic RNA, small nucleolar RNA, natural antisense transcript, small nuclear RNA, and small RNA using published datasets and in-house analytic results. Altogether, we identified 635 novel protein-coding genes, 508 novel transcribed regions, 5178 non-coding RNAs, and 35 846 small RNA loci that were formerly unannotated. Analysis of the splicing events and RNA-Seq based expression profiles revealed the landscapes of gene structures, untranslated regions, and splicing activities to be more intricate than previously appreciated. Furthermore, we present 692 uniformly expressed housekeeping genes, 43% of whose human orthologs are also housekeeping genes. This updated Arabidopsis genome annotation with a substantially increased resolution of gene models will not only further our understanding of the biological processes of this plant model but also of other species.

769 citations

Journal ArticleDOI
TL;DR: This review highlights new findings on the diverse pathways of tRNA maturation, and on the formation and function of a number of modifications, on the regulation of t RNA biosynthesis, quality control tRNA turnover mechanisms, widespread tRNA cleavage pathways activated in response to stress and other growth conditions.
Abstract: tRNA biology has come of age, revealing an unprecedented level of understanding and many unexpected discoveries along the way. This review highlights new findings on the diverse pathways of tRNA maturation, and on the formation and function of a number of modifications. Topics of special focus include the regulation of tRNA biosynthesis, quality control tRNA turnover mechanisms, widespread tRNA cleavage pathways activated in response to stress and other growth conditions, emerging evidence of signaling pathways involving tRNA and cleavage fragments, and the sophisticated intracellular tRNA trafficking that occurs during and after biosynthesis.

706 citations

Journal ArticleDOI
TL;DR: All animals, some plants, and certain other groups of eukaryotes are mired in profound stases in mitochondrial gene content, whereas other lineages have experienced relatively frequent gene loss.

608 citations