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AuthorFast, Laura A.dc.contributor.author
AuthorMikuličić, Snježanadc.contributor.author
AuthorFritzen, Annadc.contributor.author
AuthorSchwickert, Jonasdc.contributor.author
AuthorBoukhallouk, Fatimadc.contributor.author
AuthorHochdorfer, Danieldc.contributor.author
AuthorSinzger, Christiandc.contributor.author
AuthorSuarez, Henardc.contributor.author
AuthorMonk, Peter N.dc.contributor.author
AuthorYáñez-Mó, Maríadc.contributor.author
AuthorLieber, Dianadc.contributor.author
AuthorFlorin, Luisedc.contributor.author
Date of accession2023-03-20T12:47:28Zdc.date.accessioned
Available in OPARU since2023-03-20T12:47:28Zdc.date.available
Date of first publication2018-10-02dc.date.issued
AbstractTetraspanins are suggested to regulate the composition of cell membrane components and control intracellular transport, which leaves them vulnerable to utilization by pathogens such as human papillomaviruses (HPV) and cytomegaloviruses (HCMV) to facilitate host cell entry and subsequent infection. In this study, by means of cellular depletion, the cluster of differentiation (CD) tetraspanins CD9, CD63, and CD151 were found to reduce HPV16 infection in HeLa cells by 50 to 80%. Moreover, we tested recombinant proteins or peptides of specific tetraspanin domains on their effect on the most oncogenic HPV type, HPV16, and HCMV. We found that the C-terminal tails of CD63 and CD151 significantly inhibited infections of both HPV16 and HCMV. Although CD9 was newly identified as a key cellular factor for HPV16 infection, the recombinant CD9 C-terminal peptide had no effect on infection. Based on the determined half-maximal inhibitory concentration (IC50), we classified CD63 and CD151 C-terminal peptides as moderate to potent inhibitors of HPV16 infection in HeLa and HaCaT cells, and in EA.hy926, HFF (human foreskin fibroblast) cells, and HEC-LTT (human endothelial cell-large T antigen and telomerase) cells for HCMV, respectively. These results indicate that HPV16 and HCMV share similar cellular requirements for their entry into host cells and reveal the necessity of the cytoplasmic CD151 and CD63 C-termini in virus infections. Furthermore, this highlights the suitability of these peptides for functional investigation of tetraspanin domains and as inhibitors of pathogen infectionsdc.description.abstract
Languageendc.language.iso
PublisherUniversität Ulmdc.publisher
LicenseCC BY 4.0 Internationaldc.rights
Link to license texthttps://creativecommons.org/licenses/by/4.0/dc.rights.uri
Keywordhuman papillomavirusdc.subject
KeywordHPV16dc.subject
Keywordhuman cytomegalovirusdc.subject
Keywordtetraspanindc.subject
Keywordvirus entrydc.subject
Keywordblocking peptidedc.subject
KeywordIC 50dc.subject
Dewey Decimal GroupDDC 610 / Medicine & healthdc.subject.ddc
MeSHHuman papillomavirus virusesdc.subject.mesh
MeSHCytomegalovirusdc.subject.mesh
MeSHTetraspaninsdc.subject.mesh
MeSHVirus internalizationdc.subject.mesh
TitleInhibition of tetraspanin functions impairs human papillomavirus and cytomegalovirus infectionsdc.title
Resource typeWissenschaftlicher Artikeldc.type
SWORD Date2022-09-06T17:02:29Zdc.date.updated
VersionpublishedVersiondc.description.version
DOIhttp://dx.doi.org/10.18725/OPARU-47809dc.identifier.doi
URNhttp://nbn-resolving.de/urn:nbn:de:bsz:289-oparu-47885-9dc.identifier.urn
GNDHumanes Papillomavirusdc.subject.gnd
GNDCytomegalie-Virusdc.subject.gnd
InstitutionUKU. Institut für Virologieuulm.affiliationSpecific
Peer reviewjauulm.peerReview
DCMI TypeTextuulm.typeDCMI
CategoryPublikationenuulm.category
DOI of original publication10.3390/ijms19103007dc.relation1.doi
Source - Title of sourceInternational Journal of Molecular Sciencessource.title
Source - Place of publicationMDPIsource.publisher
Source - Volume19source.volume
Source - Issue10source.issue
Source - Year2018source.year
Source - Article number3007source.articleNumber
Source - eISSN1422-0067source.identifier.eissn
WoS000448951000162uulm.identifier.wos
Bibliographyuulmuulm.bibliographie


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