Analysis of the three Yersinia pestis CRISPR loci provides new tools for phylogenetic studies and possibly for the investigation of ancient DNA.
Identifieur interne : 004994 ( Main/Exploration ); précédent : 004993; suivant : 004995Analysis of the three Yersinia pestis CRISPR loci provides new tools for phylogenetic studies and possibly for the investigation of ancient DNA.
Auteurs : Gilles Vergnaud [France] ; Yanjun Li ; Olivier Gorgé ; Yujun Cui ; Yajun Song ; Dongsheng Zhou ; Ibtissem Grissa [France] ; Svetlana V. Dentovskaya ; Mikhail E. Platonov ; Alexander Rakin ; Sergey V. Balakhonov ; Heinrich Neubauer ; Christine Pourcel [France] ; Andrey P. Anisimov ; Ruifu YangSource :
- Advances in Experimental Medicine and Biology [ 0065-2598 ] ; 2007.
Abstract
The precise nature of the pathogen having caused early plague pandemics is uncertain. Although Yersinia pestis is a likely candidate for all three plague pandemics, the very rare direct evidence that can be deduced from ancient DNA (aDNA) analysis is controversial. Moreover, which of the three biovars, Antiqua, Medievalis or Orientalis, was associated with these pandemics is still debated. There is a need for phylogenetic analysis performed on Y. pestis strains isolated from countries from which plague probably arose and is still endemic. In addition there exist technical difficulties inherent to aDNA investigations and a lack of appropriate genetic targets. The recently described CRISPRs (clustered regularly interspaced short palindromic repeats) may represent such a target. CRISPR loci consist of a succession of highly conserved regions separated by specific "spacers" usually of viral origin. To be of use, data describing the mechanisms of evolution and diversity of CRISPRs in Y. pestis, its closest neighbors, and other species which might contaminate ancient DNA, are necessary. The investigation of closely related Y. pestis isolates has revealed recent mutation events in which elements constituting CRISPRs were acquired or lost, providing essential insight on their evolution. Rules deduced represent the basis for subsequent interpretation. In the present study, the CRISPR loci from representative Y. pestis and Yersinia pseudotuberculosis strains were investigated by PCR amplification and sequence analysis. The investigation of this wider panel of strains, including other subspecies or ecotypes within Y. pestis and also Y. pseudotuberculosis strains provides a database of the existing CRISPR spacers and helps predict the expected CRISPR structure of the Y. pestis ancestor. This knowledge will open the way to the development of a spoligotyping assay, in which spacers can be amplified even from highly degraded DNA samples. The data obtained show that CRISPR analysis can provide a very powerful typing tool, adapted to the systematic, large-scale genotyping of Y. pestis isolates, and the creation of international typing databases. In addition, CRISPRs do constitute a very promising new tool and genetic target to investigate ancient DNA. The corresponding genetic targets are small (<70bp), present in multiple copies (usually more than 10), highly conserved and specific. In addition, the assay can be run in any laboratory. Interpretation of the data is not dependent on accurate sequence data.
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Dentovskaya</name></author><author><name sortKey="Platonov, Mikhail E" sort="Platonov, Mikhail E" uniqKey="Platonov M" first="Mikhail E" last="Platonov">Mikhail E. Platonov</name></author><author><name sortKey="Rakin, Alexander" sort="Rakin, Alexander" uniqKey="Rakin A" first="Alexander" last="Rakin">Alexander Rakin</name></author><author><name sortKey="Balakhonov, Sergey V" sort="Balakhonov, Sergey V" uniqKey="Balakhonov S" first="Sergey V" last="Balakhonov">Sergey V. Balakhonov</name></author><author><name sortKey="Neubauer, Heinrich" sort="Neubauer, Heinrich" uniqKey="Neubauer H" first="Heinrich" last="Neubauer">Heinrich Neubauer</name></author><author><name sortKey="Pourcel, Christine" sort="Pourcel, Christine" uniqKey="Pourcel C" first="Christine" last="Pourcel">Christine Pourcel</name><affiliation wicri:level="1"><hal:affiliation type="laboratory" xml:id="struct-1361" status="OLD"> <orgName>Institut de génétique et microbiologie [Orsay]</orgName> <orgName type="acronym">IGM</orgName> <date type="end">2014-12-31</date> <desc> <address> <addrLine>Bâtiments 400 et 409UFR des Sciences - Université Paris-Sud 1115, rue Georges Clémenceau - F 91405 ORSAY Cedex</addrLine> <country key="FR"></country> </address> <ref type="url">http://www.igmors.u-psud.fr</ref> </desc> <listRelation> <relation name="UMR8621" active="#struct-441569" type="direct"></relation> <relation active="#struct-92966" type="direct"></relation> </listRelation> <tutelles><tutelle name="UMR8621" active="#struct-441569" type="direct"><org type="institution" xml:id="struct-441569" status="VALID"> <idno type="IdRef">02636817X</idno> <idno type="ISNI">0000000122597504</idno> <orgName>Centre National de la Recherche Scientifique</orgName> <orgName type="acronym">CNRS</orgName> <date type="start">1939-10-19</date> <desc> <address> <country key="FR"></country> </address> <ref type="url">http://www.cnrs.fr/</ref> </desc> </org></tutelle><tutelle active="#struct-92966" type="direct"><org type="institution" xml:id="struct-92966" status="VALID"> <orgName>Université Paris-Sud - Paris 11</orgName> <orgName type="acronym">UP11</orgName> <desc> <address> <addrLine>Bâtiment 300 - 91405 Orsay cedex</addrLine> <country key="FR"></country> </address> <ref type="url">http://www.u-psud.fr/</ref> </desc> </org></tutelle></tutelles></hal:affiliation><country>France</country></affiliation></author><author><name sortKey="Anisimov, Andrey P" sort="Anisimov, Andrey P" uniqKey="Anisimov A" first="Andrey P" last="Anisimov">Andrey P. Anisimov</name></author><author><name sortKey="Yang, Ruifu" sort="Yang, Ruifu" uniqKey="Yang R" first="Ruifu" last="Yang">Ruifu Yang</name></author></analytic><series><title level="j">Advances in Experimental Medicine and Biology</title><idno type="ISSN">0065-2598</idno><imprint><date type="datePub">2007</date></imprint></series></biblStruct></sourceDesc></fileDesc><profileDesc><textClass></textClass></profileDesc></teiHeader><front><div type="abstract" xml:lang="en"> <p>The precise nature of the pathogen having caused early plague pandemics is uncertain. Although Yersinia pestis is a likely candidate for all three plague pandemics, the very rare direct evidence that can be deduced from ancient DNA (aDNA) analysis is controversial. Moreover, which of the three biovars, Antiqua, Medievalis or Orientalis, was associated with these pandemics is still debated. There is a need for phylogenetic analysis performed on Y. pestis strains isolated from countries from which plague probably arose and is still endemic. In addition there exist technical difficulties inherent to aDNA investigations and a lack of appropriate genetic targets. The recently described CRISPRs (clustered regularly interspaced short palindromic repeats) may represent such a target. CRISPR loci consist of a succession of highly conserved regions separated by specific "spacers" usually of viral origin. To be of use, data describing the mechanisms of evolution and diversity of CRISPRs in Y. pestis, its closest neighbors, and other species which might contaminate ancient DNA, are necessary. The investigation of closely related Y. pestis isolates has revealed recent mutation events in which elements constituting CRISPRs were acquired or lost, providing essential insight on their evolution. Rules deduced represent the basis for subsequent interpretation. In the present study, the CRISPR loci from representative Y. pestis and Yersinia pseudotuberculosis strains were investigated by PCR amplification and sequence analysis. The investigation of this wider panel of strains, including other subspecies or ecotypes within Y. pestis and also Y. pseudotuberculosis strains provides a database of the existing CRISPR spacers and helps predict the expected CRISPR structure of the Y. pestis ancestor. This knowledge will open the way to the development of a spoligotyping assay, in which spacers can be amplified even from highly degraded DNA samples. The data obtained show that CRISPR analysis can provide a very powerful typing tool, adapted to the systematic, large-scale genotyping of Y. pestis isolates, and the creation of international typing databases. In addition, CRISPRs do constitute a very promising new tool and genetic target to investigate ancient DNA. The corresponding genetic targets are small (<70bp), present in multiple copies (usually more than 10), highly conserved and specific. In addition, the assay can be run in any laboratory. Interpretation of the data is not dependent on accurate sequence data.</p> </div></front></TEI><affiliations><list><country><li>France</li></country></list><tree><noCountry><name sortKey="Anisimov, Andrey P" sort="Anisimov, Andrey P" uniqKey="Anisimov A" first="Andrey P" last="Anisimov">Andrey P. Anisimov</name><name sortKey="Balakhonov, Sergey V" sort="Balakhonov, Sergey V" uniqKey="Balakhonov S" first="Sergey V" last="Balakhonov">Sergey V. Balakhonov</name><name sortKey="Cui, Yujun" sort="Cui, Yujun" uniqKey="Cui Y" first="Yujun" last="Cui">Yujun Cui</name><name sortKey="Dentovskaya, Svetlana V" sort="Dentovskaya, Svetlana V" uniqKey="Dentovskaya S" first="Svetlana V" last="Dentovskaya">Svetlana V. Dentovskaya</name><name sortKey="Gorge, Olivier" sort="Gorge, Olivier" uniqKey="Gorge O" first="Olivier" last="Gorgé">Olivier Gorgé</name><name sortKey="Li, Yanjun" sort="Li, Yanjun" uniqKey="Li Y" first="Yanjun" last="Li">Yanjun Li</name><name sortKey="Neubauer, Heinrich" sort="Neubauer, Heinrich" uniqKey="Neubauer H" first="Heinrich" last="Neubauer">Heinrich Neubauer</name><name sortKey="Platonov, Mikhail E" sort="Platonov, Mikhail E" uniqKey="Platonov M" first="Mikhail E" last="Platonov">Mikhail E. Platonov</name><name sortKey="Rakin, Alexander" sort="Rakin, Alexander" uniqKey="Rakin A" first="Alexander" last="Rakin">Alexander Rakin</name><name sortKey="Song, Yajun" sort="Song, Yajun" uniqKey="Song Y" first="Yajun" last="Song">Yajun Song</name><name sortKey="Yang, Ruifu" sort="Yang, Ruifu" uniqKey="Yang R" first="Ruifu" last="Yang">Ruifu Yang</name><name sortKey="Zhou, Dongsheng" sort="Zhou, Dongsheng" uniqKey="Zhou D" first="Dongsheng" last="Zhou">Dongsheng Zhou</name></noCountry><country name="France"><noRegion><name sortKey="Vergnaud, Gilles" sort="Vergnaud, Gilles" uniqKey="Vergnaud G" first="Gilles" last="Vergnaud">Gilles Vergnaud</name></noRegion><name sortKey="Grissa, Ibtissem" sort="Grissa, Ibtissem" uniqKey="Grissa I" first="Ibtissem" last="Grissa">Ibtissem Grissa</name><name sortKey="Pourcel, Christine" sort="Pourcel, Christine" uniqKey="Pourcel C" first="Christine" last="Pourcel">Christine Pourcel</name></country></tree></affiliations></record>Pour manipuler ce document sous Unix (Dilib)
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