Identification using phage display of peptides promoting targeting and internalization into HPV‐transformed cell lines
Identifieur interne : 000991 ( Istex/Corpus ); précédent : 000990; suivant : 000992Identification using phage display of peptides promoting targeting and internalization into HPV‐transformed cell lines
Auteurs : Philip Robinson ; Denise Stuber ; François Deryckère ; Philip Tedbury ; Magali Lagrange ; Georges OrfanoudakisSource :
- Journal of Molecular Recognition [ 0952-3499 ] ; 2005-03.
English descriptors
- Teeft :
- Alexa fluor1, Amersham biosciences, Amino, Amino acid sequence, Biopanning, Bioscience, Carcinoma, Caski, Caski cells, Cell line, Cell lines, Cell surface, Cervical, Cervical cancer, Chloroquine, Clone, Copyright, Disulphide bond, Egfp, Focal plane medial, Fusion products, Hela, Hela cells, Human papillomavirus, Human transferrin, Individual clones, Internalization, Internalizing, Internalizing peptides, Invitrogen, Ivanenkov, John wiley sons, Keratinocytes, Mammalian cells, Other cell lines, Papillomavirus, Peptide, Phage, Phage display, Phage display technology, Phage particles, Phagemid, Phagemid library, Pviii, Receptor, Recognit, Room temperature, Sequence coding, Siha, Siha cells, Target cells, Transferrin, Tumour.
Abstract
‘High‐risk’ human papilloma viruses (HPVs) cause cervical tumours. In order to treat these tumours therapeutic approaches must be developed that efficiently target the tumour cells. Using phage display, we selected tumour‐targeting peptides from a library of constrained nonamer peptides presented multivalently on pVIII of M13. Three different consensus peptide sequences were isolated by biopanning on HPV16‐transformed SiHa cells. The corresponding phage‐peptides targeted and were internalized in HPV16 transformed SiHa and CaSki cells as well as in HPV18‐transformed HeLa cells, but failed to bind a panel of normal or transformed cell lines. Two of the three selected peptides targeted cells only when presented on phage particles in a constrained conformation. However, all three peptides retained their targeting capacity when presented on the reporter protein enhanced green fluorescent protein (EGFP) in a monovalent form. These peptides may be useful for the design of drug or gene delivery vectors for the treatment of cervical cancer. Copyright © 2004 John Wiley & Sons, Ltd.
Url:
DOI: 10.1002/jmr.723
Links to Exploration step
ISTEX:6C9216CF604FD78D06604E6B689FDA71BD7EE31CLe document en format XML
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1995</json:string><json:string>Cheng et al., 2002</json:string><json:string>Grifman et al., 2001</json:string><json:string>Alvarez-Salas et al., 2003</json:string><json:string>Zhang et al., 2001</json:string><json:string>WangJohanning et al., 1998</json:string><json:string>Wolf et al., 2003</json:string><json:string>Jaafari and Foldvari, 2002</json:string><json:string>Oyama et al., 2003</json:string><json:string>Nicklin and Baker, 2002</json:string><json:string>Ivanenkov et al., 1999a,b</json:string><json:string>Aina et al., 2002</json:string><json:string>Horner et al., 2004</json:string><json:string>Wattiaux et al., 2000</json:string><json:string>Klausner et al., 1983</json:string><json:string>Nees et al., 1998</json:string><json:string>Butz et al., 2003</json:string><json:string>Park et al., 2001</json:string><json:string>Felici et al., 1991</json:string><json:string>Kempf et al., 2001</json:string><json:string>Wang-Johanning et al., 1998</json:string><json:string>zur Hausen, 1996</json:string><json:string>Poul et al., 2000</json:string><json:string>Ivanenkov et al., 1999b</json:string><json:string>Rey et al., 1999</json:string><json:string>Garland, 2003</json:string><json:string>Mazzucchelli et al., 1999</json:string><json:string>reviewed in [Landon and Deutscher, 2003</json:string></ref_bibl><bibl></bibl></unitex></namedEntities><ark><json:string>ark:/67375/WNG-0QVXH7W8-4</json:string></ark><categories><wos><json:string>1 - science</json:string><json:string>2 - biophysics</json:string><json:string>2 - biochemistry & molecular biology</json:string></wos><scienceMetrix><json:string>1 - health sciences</json:string><json:string>2 - biomedical research</json:string><json:string>3 - biophysics</json:string></scienceMetrix><scopus><json:string>1 - Life Sciences</json:string><json:string>2 - Biochemistry, Genetics and Molecular Biology</json:string><json:string>3 - Molecular Biology</json:string><json:string>1 - Life Sciences</json:string><json:string>2 - 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type="article"><analytic><title level="a" type="main">Identification using phage display of peptides promoting targeting and internalization into HPV‐transformed cell lines</title><title level="a" type="short" xml:lang="en">INTERNALIZING PEPTIDES FOR HPV‐TRANSFORMED CELLS</title><author xml:id="author-0000"><persName><forename type="first">Philip</forename><surname>Robinson</surname></persName><affiliation><orgName type="department">UMR7100‐CNRS Ecole Supérieure de Biotechnologie de Strasbourg</orgName><orgName type="institution">Université Louis Pasteur</orgName><address><addrLine>boulevard Sébastien Brandt</addrLine><addrLine>67400‐Illkirch, France</addrLine><country key="FR" xml:lang="en">FRANCE</country></address></affiliation></author><author xml:id="author-0001"><persName><forename type="first">Denise</forename><surname>Stuber</surname></persName><affiliation><orgName type="department">UMR7100‐CNRS Ecole Supérieure de Biotechnologie de Strasbourg</orgName><orgName type="institution">Université Louis Pasteur</orgName><address><addrLine>boulevard Sébastien Brandt</addrLine><addrLine>67400‐Illkirch, France</addrLine><country key="FR" xml:lang="en">FRANCE</country></address></affiliation></author><author xml:id="author-0002"><persName><forename type="first">François</forename><surname>Deryckère</surname></persName><affiliation><orgName type="department">UMR7100‐CNRS Ecole Supérieure de Biotechnologie de Strasbourg</orgName><orgName type="institution">Université Louis Pasteur</orgName><address><addrLine>boulevard Sébastien Brandt</addrLine><addrLine>67400‐Illkirch, France</addrLine><country key="FR" xml:lang="en">FRANCE</country></address></affiliation></author><author xml:id="author-0003"><persName><forename type="first">Philip</forename><surname>Tedbury</surname></persName><affiliation><orgName type="department">UMR7100‐CNRS Ecole Supérieure de Biotechnologie de Strasbourg</orgName><orgName type="institution">Université Louis Pasteur</orgName><address><addrLine>boulevard Sébastien Brandt</addrLine><addrLine>67400‐Illkirch, France</addrLine><country key="FR" xml:lang="en">FRANCE</country></address></affiliation></author><author xml:id="author-0004"><persName><forename type="first">Magali</forename><surname>Lagrange</surname></persName><affiliation><orgName type="department">UMR7100‐CNRS Ecole Supérieure de Biotechnologie de Strasbourg</orgName><orgName type="institution">Université Louis Pasteur</orgName><address><addrLine>boulevard Sébastien Brandt</addrLine><addrLine>67400‐Illkirch, France</addrLine><country key="FR" xml:lang="en">FRANCE</country></address></affiliation></author><author xml:id="author-0005" role="corresp"><persName><forename type="first">Georges</forename><surname>Orfanoudakis</surname></persName><email>orfanoud@esbs.u‐strasbg.fr</email><affiliation><orgName type="department">UMR7100‐CNRS Ecole Supérieure de Biotechnologie de Strasbourg</orgName><orgName type="institution">Université Louis 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However, all three peptides retained their targeting capacity when presented on the reporter protein enhanced green fluorescent protein (EGFP) in a monovalent form. These peptides may be useful for the design of drug or gene delivery vectors for the treatment of cervical cancer. Copyright © 2004 John Wiley & Sons, Ltd.</p></abstract><textClass><keywords xml:lang="en"><term xml:id="kwd1">phage display</term><term xml:id="kwd2">HPV</term><term xml:id="kwd3">cervical cancer</term><term xml:id="kwd4">cell internalization</term><term xml:id="kwd5">targeting</term></keywords><keywords rend="articleCategory"><term>Research Article</term></keywords><keywords rend="tocHeading1"><term>Research Articles</term></keywords></textClass><langUsage><language ident="en"></language></langUsage></profileDesc><revisionDesc><change when="2019-12-20" who="#istex" xml:id="pub2tei">formatting</change></revisionDesc></teiHeader></istex:fulltextTEI><json:item><extension>txt</extension><original>false</original><mimetype>text/plain</mimetype><uri>https://api.istex.fr/ark:/67375/WNG-0QVXH7W8-4/fulltext.txt</uri></json:item></fulltext><metadata><istex:metadataXml wicri:clean="Wiley, elements deleted: body"><istex:xmlDeclaration>version="1.0" encoding="UTF-8" standalone="yes"</istex:xmlDeclaration><istex:document><component version="2.0" type="serialArticle" xml:lang="en"><header><publicationMeta level="product"><publisherInfo><publisherName>John Wiley & Sons, Ltd.</publisherName><publisherLoc>Chichester, UK</publisherLoc></publisherInfo><doi registered="yes">10.1002/(ISSN)1099-1352</doi><issn type="print">0952-3499</issn><issn type="electronic">1099-1352</issn><idGroup><id type="product" value="JMR"></id></idGroup><titleGroup><title type="main" xml:lang="en" sort="JOURNAL OF MOLECULAR RECOGNITION">Journal of Molecular Recognition</title><title type="subtitle">An Interdisciplinary Journal</title><title type="short">J. 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In order to treat these tumours therapeutic approaches must be developed that efficiently target the tumour cells. Using phage display, we selected tumour‐targeting peptides from a library of constrained nonamer peptides presented multivalently on pVIII of M13. Three different consensus peptide sequences were isolated by biopanning on HPV16‐transformed SiHa cells. The corresponding phage‐peptides targeted and were internalized in HPV16 transformed SiHa and CaSki cells as well as in HPV18‐transformed HeLa cells, but failed to bind a panel of normal or transformed cell lines. Two of the three selected peptides targeted cells only when presented on phage particles in a constrained conformation. However, all three peptides retained their targeting capacity when presented on the reporter protein enhanced green fluorescent protein (EGFP) in a monovalent form. These peptides may be useful for the design of drug or gene delivery vectors for the treatment of cervical cancer. Copyright © 2004 John Wiley & Sons, Ltd.</p></abstract></abstractGroup></contentMeta></header></component></istex:document></istex:metadataXml><mods version="3.6"><titleInfo lang="en"><title>Identification using phage display of peptides promoting targeting and internalization into HPV‐transformed cell lines</title></titleInfo><titleInfo type="abbreviated" lang="en"><title>INTERNALIZING PEPTIDES FOR HPV‐TRANSFORMED CELLS</title></titleInfo><titleInfo type="alternative" contentType="CDATA" lang="en"><title>Identification using phage display of peptides promoting targeting and internalization into HPV‐transformed cell lines</title></titleInfo><name type="personal"><namePart type="given">Philip</namePart><namePart type="family">Robinson</namePart><affiliation>UMR7100‐CNRS Ecole Supérieure de Biotechnologie de Strasbourg, Université Louis Pasteur, boulevard Sébastien Brandt, 67400‐Illkirch, France</affiliation><role><roleTerm type="text">author</roleTerm></role></name><name type="personal"><namePart type="given">Denise</namePart><namePart type="family">Stuber</namePart><affiliation>UMR7100‐CNRS Ecole Supérieure de Biotechnologie de Strasbourg, Université Louis Pasteur, boulevard Sébastien Brandt, 67400‐Illkirch, France</affiliation><role><roleTerm type="text">author</roleTerm></role></name><name type="personal"><namePart type="given">François</namePart><namePart type="family">Deryckère</namePart><affiliation>UMR7100‐CNRS Ecole Supérieure de Biotechnologie de Strasbourg, Université Louis Pasteur, boulevard Sébastien Brandt, 67400‐Illkirch, France</affiliation><role><roleTerm type="text">author</roleTerm></role></name><name type="personal"><namePart type="given">Philip</namePart><namePart type="family">Tedbury</namePart><affiliation>UMR7100‐CNRS Ecole Supérieure de Biotechnologie de Strasbourg, Université Louis Pasteur, boulevard Sébastien Brandt, 67400‐Illkirch, France</affiliation><role><roleTerm type="text">author</roleTerm></role></name><name type="personal"><namePart type="given">Magali</namePart><namePart type="family">Lagrange</namePart><affiliation>UMR7100‐CNRS Ecole Supérieure de Biotechnologie de Strasbourg, Université Louis Pasteur, boulevard Sébastien Brandt, 67400‐Illkirch, France</affiliation><role><roleTerm type="text">author</roleTerm></role></name><name type="personal"><namePart type="given">Georges</namePart><namePart type="family">Orfanoudakis</namePart><affiliation>UMR7100‐CNRS Ecole Supérieure de Biotechnologie de Strasbourg, Université Louis Pasteur, boulevard Sébastien Brandt, 67400‐Illkirch, France</affiliation><affiliation>E-mail: orfanoud@esbs.u‐strasbg.fr</affiliation><affiliation>Correspondence address: UMR7100‐CNRS, Ecole Supérieure de Biotechnologie de Strasbourg, Université Louis Pasteur, boulevard Sébastien Brandt, 67400‐Illkirch, France.</affiliation><role><roleTerm type="text">author</roleTerm></role></name><typeOfResource>text</typeOfResource><genre type="article" displayLabel="article" authority="ISTEX" authorityURI="https://content-type.data.istex.fr" valueURI="https://content-type.data.istex.fr/ark:/67375/XTP-6N5SZHKN-D">article</genre><originInfo><publisher>John Wiley & Sons, Ltd.</publisher><place><placeTerm type="text">Chichester, UK</placeTerm></place><dateIssued encoding="w3cdtf">2005-03</dateIssued><dateCaptured encoding="w3cdtf">2004-05-27</dateCaptured><dateValid encoding="w3cdtf">2004-07-07</dateValid><copyrightDate encoding="w3cdtf">2005</copyrightDate></originInfo><language><languageTerm type="code" authority="rfc3066">en</languageTerm><languageTerm type="code" authority="iso639-2b">eng</languageTerm></language><physicalDescription><extent unit="figures">4</extent><extent unit="tables">1</extent><extent unit="references">35</extent></physicalDescription><abstract lang="en">‘High‐risk’ human papilloma viruses (HPVs) cause cervical tumours. In order to treat these tumours therapeutic approaches must be developed that efficiently target the tumour cells. Using phage display, we selected tumour‐targeting peptides from a library of constrained nonamer peptides presented multivalently on pVIII of M13. Three different consensus peptide sequences were isolated by biopanning on HPV16‐transformed SiHa cells. The corresponding phage‐peptides targeted and were internalized in HPV16 transformed SiHa and CaSki cells as well as in HPV18‐transformed HeLa cells, but failed to bind a panel of normal or transformed cell lines. Two of the three selected peptides targeted cells only when presented on phage particles in a constrained conformation. However, all three peptides retained their targeting capacity when presented on the reporter protein enhanced green fluorescent protein (EGFP) in a monovalent form. These peptides may be useful for the design of drug or gene delivery vectors for the treatment of cervical cancer. Copyright © 2004 John Wiley & Sons, Ltd.</abstract><note type="funding">Association pour la Recherche sur le Cancer</note><note type="funding">La Ligue Nationale Contre le Cancer</note><subject lang="en"><genre>keywords</genre><topic>phage display</topic><topic>HPV</topic><topic>cervical cancer</topic><topic>cell internalization</topic><topic>targeting</topic></subject><relatedItem type="host"><titleInfo><title>Journal of Molecular Recognition</title><subTitle>An Interdisciplinary Journal</subTitle></titleInfo><titleInfo type="abbreviated"><title>J. Mol. Recognit.</title></titleInfo><genre type="journal" authority="ISTEX" authorityURI="https://publication-type.data.istex.fr" valueURI="https://publication-type.data.istex.fr/ark:/67375/JMC-0GLKJH51-B">journal</genre><subject><genre>article-category</genre><topic>Research Article</topic><topic>Research Articles</topic></subject><identifier type="ISSN">0952-3499</identifier><identifier type="eISSN">1099-1352</identifier><identifier type="DOI">10.1002/(ISSN)1099-1352</identifier><identifier type="PublisherID">JMR</identifier><part><date>2005</date><detail type="volume"><caption>vol.</caption><number>18</number></detail><detail type="issue"><caption>no.</caption><number>2</number></detail><extent unit="pages"><start>175</start><end>182</end><total>8</total></extent></part></relatedItem><relatedItem type="references" displayLabel="cit1"><titleInfo><title>Therapeutic cancer targeting peptides</title></titleInfo><name type="personal"><namePart type="given">OH</namePart><namePart type="family">Aina</namePart><role><roleTerm type="text">author</roleTerm></role></name><name type="personal"><namePart type="given">TC</namePart><namePart type="family">Sroka</namePart><role><roleTerm type="text">author</roleTerm></role></name><name type="personal"><namePart type="given">ML</namePart><namePart type="family">Chen</namePart><role><roleTerm type="text">author</roleTerm></role></name><name type="personal"><namePart type="given">KS</namePart><namePart type="family">Lam</namePart><role><roleTerm type="text">author</roleTerm></role></name><genre>journal-article</genre><note type="citation/reference">Aina OH, Sroka TC, Chen ML, Lam KS. 2002. 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