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AuthorJütte, Hendrikdc.contributor.author
AuthorReike, Moritzdc.contributor.author
AuthorWirtz, Ralph M.dc.contributor.author
AuthorKriegmair, Maximiliandc.contributor.author
AuthorErben, Philippdc.contributor.author
AuthorTully, Karldc.contributor.author
AuthorWeyerer, Veronikadc.contributor.author
AuthorEckstein, Markusdc.contributor.author
AuthorHartmann, Arndtdc.contributor.author
AuthorEidt, Sebastiandc.contributor.author
AuthorWezel, Felixdc.contributor.author
AuthorBolenz, Christiandc.contributor.author
AuthorTannapfel, Andreadc.contributor.author
AuthorNoldus, Joachimdc.contributor.author
AuthorRoghmann, Floriandc.contributor.author
Date of accession2022-11-07T13:57:54Zdc.date.accessioned
Available in OPARU since2022-11-07T13:57:54Zdc.date.available
Date of first publication2021-05-26dc.date.issued
AbstractPatients with muscle-invasive bladder cancer (MIBC) that underwent neoadjuvant chemotherapy (NAC) prior to radical cystectomy (RC) show improved overall survival, especially those with pathological complete response (pCR). The response to NAC according to molecular subtypes has been discussed. Molecular targets such as estrogen receptor (ESR1) and human epidermal growth factor receptor 2 (ERBB2) play an important role in breast cancer management and have also been associated with urothelial bladder cancer. Hence, the association of Keratin 20 (KRT20) Keratin 5 (KRT5), ESR1, and ERBB2 mRNA expression in MIBC at transurethral resection (TUR-BT) with pCR after NAC was analyzed retrospectively. Formalin-fixed paraffin-embedded tumour tissue samples from TUR-BT of 54 patients (42 males, 12 females, median age of 64) with MIBC were analyzed for KRT20, KRT5, ESR1, and ERBB2 mRNA expression. After NAC, RC was performed, and the specimens were evaluated for pCR. Statistical analyses comprised nonparametric and chi2 testing, partition models, and Spearman correlation analyses. After NAC, 22 out of 54 patients (40.7%) had pCR. Tumours with an elevated expression of markers associated with luminal differentiation (KRT20, ERBB2, ESR1) were associated with a higher chance of pCR (55% vs. 15.8%, p = 0.009). Elevated ERBB2 expression was positively correlated with luminal expression features such as KRT20, and negatively with basal characteristics such as KRT5. Patients with MIBC showing a high expression of ERBB2, ESR1, or KRT20 have a significantly higher chance of pCR following NAC. These findings might improve patient selection for NAC in MIBC.dc.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
Keywordchemotherapydc.subject
Keywordmuscle invasivedc.subject
Keywordrisk stratificationdc.subject
Keywordsubtypedc.subject
Dewey Decimal GroupDDC 610 / Medicine & healthdc.subject.ddc
LCSHBladder; Cancerdc.subject.lcsh
LCSHBladder; Cancer; Adjuvant treatmentdc.subject.lcsh
MeSHUrinary bladder neoplasms; Drug therapydc.subject.mesh
TitleKRT20, KRT5, ESR1 and ERBB2 expression can predict pathologic outcome in patients undergoing neoadjuvant chemotherapy and radical cystectomy for muscle-invasive bladder cancerdc.title
Resource typeWissenschaftlicher Artikeldc.type
SWORD Date2021-06-12T04:11:45Zdc.date.updated
VersionpublishedVersiondc.description.version
DOIhttp://dx.doi.org/10.18725/OPARU-45707dc.identifier.doi
URNhttp://nbn-resolving.de/urn:nbn:de:bsz:289-oparu-45783-0dc.identifier.urn
GNDBlasenkrebsdc.subject.gnd
GNDChemotherapiedc.subject.gnd
InstitutionUKU. Klinik für Urologie und Kinderurologieuulm.affiliationSpecific
Peer reviewjauulm.peerReview
DCMI TypeTextuulm.typeDCMI
CategoryPublikationenuulm.category
DOI of original publication10.3390/jpm11060473dc.relation1.doi
Source - Title of sourceJournal of Personalized Medicinesource.title
Source - Place of publicationMDPIsource.publisher
Source - Volume11source.volume
Source - Issue6source.issue
Source - Year2021source.year
Source - Article number473source.articleNumber
Source - eISSN2075-4426source.identifier.eissn
Open AccessDOAJ Gold, Green Publisheduulm.OA
WoS000666438100001uulm.identifier.wos
Bibliographyuulmuulm.bibliographie


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