Evolution of instability at coding and non-coding repeat sequences in human MSI-H colorectal cancers
Identifieur interne : 00BD34 ( Main/Exploration ); précédent : 00BD33; suivant : 00BD35Evolution of instability at coding and non-coding repeat sequences in human MSI-H colorectal cancers
Auteurs : Alex Duval [France] ; Sandra Rolland [France] ; Aurore Compoint [France] ; Emmanuel Tubacher [France] ; Barry Lacopetta [Australie] ; Gilles Thomas [France] ; Richard Hamelin [France]Source :
- Human molecular genetics [ 0964-6906 ] ; 2001.
Descripteurs français
- Pascal (Inist)
- Wicri :
- topic : Homme.
English descriptors
- KwdEn :
Abstract
A number of human genes containing coding mononucleotide repeat sequences are particularly prone to mutations in tumors with defects in mismatch repair (MMR) genes (MSI-H cancers). In a large series of MSI-H colorectal tumors, we looked for mutations in 25 coding repeats contained in eight genes already known to be mutated in these cancers or in 17 other genes with an expected role in carcinogenesis. Mutations were found in 19 of the 25 candidate genes. Using a maximum likelihood statistical method, they were separated into two different groups that differed significantly in their mutation frequencies, and were likely to represent mutations that do or do not provide selective pressures during MSI-H tumoral progression, respectively. Three new target genes were found (GRB-14, RHAMM, RAD50). Our results provide evidence that MSI-H tumoral progression involves the cumulative mutations of a large number of genes. For each MSI-H tumor we calculated indexes representing the number of mutations found in genes of these groups. We also evaluated a shortening index at both the Bat-25 and Bat-26 non-coding mononucleotide tracts that are known to be almost always unstable in MSI-H cancers. A significant correlation was observed between instability at both coding and non-coding repeats, suggesting that Bat-25 and Bat-26 could be used as simple phenotypical markers of the tumoral evolution. A preferential order of mutations was deduced. During this process, hMSH3 alterations, a target gene encoding for a MMR protein, was found to play an important role by increasing the instability phenomenon characterizing these cancers.
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sequences in human MSI-H colorectal cancers</title><author><name sortKey="Duval, Alex" sort="Duval, Alex" uniqKey="Duval A" first="Alex" last="Duval">Alex Duval</name><affiliation wicri:level="3"><inist:fA14 i1="01"><s1>INSERM U434, CEPH, 27 rue Juliette Dodu</s1><s2>75010 Paris</s2><s3>FRA</s3><sZ>1 aut.</sZ><sZ>2 aut.</sZ><sZ>3 aut.</sZ><sZ>4 aut.</sZ><sZ>6 aut.</sZ><sZ>7 aut.</sZ></inist:fA14><country>France</country><placeName><region type="region" nuts="2">Île-de-France</region><settlement type="city">Paris</settlement></placeName></affiliation></author><author><name sortKey="Rolland, Sandra" sort="Rolland, Sandra" uniqKey="Rolland S" first="Sandra" last="Rolland">Sandra Rolland</name><affiliation wicri:level="3"><inist:fA14 i1="01"><s1>INSERM U434, CEPH, 27 rue Juliette Dodu</s1><s2>75010 Paris</s2><s3>FRA</s3><sZ>1 aut.</sZ><sZ>2 aut.</sZ><sZ>3 aut.</sZ><sZ>4 aut.</sZ><sZ>6 aut.</sZ><sZ>7 aut.</sZ></inist:fA14><country>France</country><placeName><region type="region" 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aut.</sZ></inist:fA14><country>France</country><wicri:noRegion>75010 Paris</wicri:noRegion><placeName><settlement type="city">Paris</settlement><region type="région" nuts="2">Île-de-France</region></placeName></affiliation></author><author><name sortKey="Hamelin, Richard" sort="Hamelin, Richard" uniqKey="Hamelin R" first="Richard" last="Hamelin">Richard Hamelin</name><affiliation wicri:level="1"><inist:fA14 i1="01"><s1>INSERM U434, CEPH, 27 rue Juliette Dodu</s1><s2>75010 Paris</s2><s3>FRA</s3><sZ>1 aut.</sZ><sZ>2 aut.</sZ><sZ>3 aut.</sZ><sZ>4 aut.</sZ><sZ>6 aut.</sZ><sZ>7 aut.</sZ></inist:fA14><country>France</country><wicri:noRegion>75010 Paris</wicri:noRegion><placeName><settlement type="city">Paris</settlement><region type="région" nuts="2">Île-de-France</region></placeName></affiliation></author></analytic><series><title level="j" type="main">Human molecular genetics</title><title level="j" type="abbreviated">Hum. mol. genet.</title><idno type="ISSN">0964-6906</idno><imprint><date when="2001">2001</date></imprint></series></biblStruct></sourceDesc><seriesStmt><title level="j" type="main">Human molecular genetics</title><title level="j" type="abbreviated">Hum. mol. genet.</title><idno type="ISSN">0964-6906</idno></seriesStmt></fileDesc><profileDesc><textClass><keywords scheme="KwdEn" xml:lang="en"><term>Base mismatching</term><term>Carcinogenesis</term><term>Cell line</term><term>Colon</term><term>Gene</term><term>Human</term><term>Malignant tumor</term><term>Mutation</term><term>Nucleotide sequence</term><term>Rectum</term><term>Targeting</term></keywords><keywords scheme="Pascal" xml:lang="fr"><term>Homme</term><term>Lignée cellulaire</term><term>Gène</term><term>Séquence nucléotide</term><term>Côlon</term><term>Rectum</term><term>Tumeur maligne</term><term>Mutation</term><term>Carcinogenèse</term><term>Ciblage</term><term>Mésappariement base</term></keywords><keywords scheme="Wicri" type="topic" xml:lang="fr"><term>Homme</term></keywords></textClass></profileDesc></teiHeader><front><div type="abstract" xml:lang="en">A number of human genes containing coding mononucleotide repeat sequences are particularly prone to mutations in tumors with defects in mismatch repair (MMR) genes (MSI-H cancers). In a large series of MSI-H colorectal tumors, we looked for mutations in 25 coding repeats contained in eight genes already known to be mutated in these cancers or in 17 other genes with an expected role in carcinogenesis. Mutations were found in 19 of the 25 candidate genes. Using a maximum likelihood statistical method, they were separated into two different groups that differed significantly in their mutation frequencies, and were likely to represent mutations that do or do not provide selective pressures during MSI-H tumoral progression, respectively. Three new target genes were found (GRB-14, RHAMM, RAD50). Our results provide evidence that MSI-H tumoral progression involves the cumulative mutations of a large number of genes. For each MSI-H tumor we calculated indexes representing the number of mutations found in genes of these groups. We also evaluated a shortening index at both the Bat-25 and Bat-26 non-coding mononucleotide tracts that are known to be almost always unstable in MSI-H cancers. A significant correlation was observed between instability at both coding and non-coding repeats, suggesting that Bat-25 and Bat-26 could be used as simple phenotypical markers of the tumoral evolution. A preferential order of mutations was deduced. During this process, hMSH3 alterations, a target gene encoding for a MMR protein, was found to play an important role by increasing the instability phenomenon characterizing these cancers.</div></front></TEI><affiliations><list><country><li>Australie</li><li>France</li></country><region><li>Île-de-France</li></region><settlement><li>Paris</li></settlement></list><tree><country name="France"><region name="Île-de-France"><name sortKey="Duval, Alex" sort="Duval, Alex" uniqKey="Duval A" first="Alex" last="Duval">Alex Duval</name></region><name sortKey="Compoint, Aurore" sort="Compoint, Aurore" uniqKey="Compoint A" first="Aurore" last="Compoint">Aurore Compoint</name><name sortKey="Hamelin, Richard" sort="Hamelin, Richard" uniqKey="Hamelin R" first="Richard" last="Hamelin">Richard Hamelin</name><name sortKey="Rolland, Sandra" sort="Rolland, Sandra" uniqKey="Rolland S" first="Sandra" last="Rolland">Sandra Rolland</name><name sortKey="Thomas, Gilles" sort="Thomas, Gilles" uniqKey="Thomas G" first="Gilles" last="Thomas">Gilles Thomas</name><name sortKey="Tubacher, Emmanuel" sort="Tubacher, Emmanuel" uniqKey="Tubacher E" first="Emmanuel" last="Tubacher">Emmanuel Tubacher</name></country><country name="Australie"><noRegion><name sortKey="Lacopetta, Barry" sort="Lacopetta, Barry" uniqKey="Lacopetta B" first="Barry" last="Lacopetta">Barry Lacopetta</name></noRegion></country></tree></affiliations></record>Pour manipuler ce document sous Unix (Dilib)
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