Bladder cancer diagnosis and identification of clinically significant disease by combined urinary detection of Mcm5 and nuclear matrix protein 22.

Bladder cancer diagnosis and identification of clinically significant disease by combined urinary detection of Mcm5 and nuclear matrix protein 22.

Urinary biomarkers for bladder cancer detection are constrained by inadequate sensitivity or specificity. Here we evaluate the diagnostic accuracy of Mcm5, a novel cell cycle biomarker of aberrant growth, alone and in combination with NMP22.1677 consecutive patients under investigation for urinary t...

Full description

Bibliographic Details
Main Authors: John D Kelly, Tim J Dudderidge, Alex Wollenschlaeger, Odu Okoturo, Keith Burling, Fiona Tulloch, Ian Halsall, Teresa Prevost, Andrew Toby Prevost, Joana C Vasconcelos, Wendy Robson, Hing Y Leung, Nikhil Vasdev, Robert S Pickard, Gareth H Williams, Kai Stoeber
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2012-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3392249?pdf=render
id doaj-932ab7c6a77c4ff793140bcf000429db
record_format Article
spelling doaj-932ab7c6a77c4ff793140bcf000429db2020-11-25T01:46:07ZengPublic Library of Science (PLoS)PLoS ONE1932-62032012-01-0177e4030510.1371/journal.pone.0040305Bladder cancer diagnosis and identification of clinically significant disease by combined urinary detection of Mcm5 and nuclear matrix protein 22.John D KellyTim J DudderidgeAlex WollenschlaegerOdu OkoturoKeith BurlingFiona TullochIan HalsallTeresa PrevostAndrew Toby PrevostJoana C VasconcelosWendy RobsonHing Y LeungNikhil VasdevRobert S PickardGareth H WilliamsKai StoeberUrinary biomarkers for bladder cancer detection are constrained by inadequate sensitivity or specificity. Here we evaluate the diagnostic accuracy of Mcm5, a novel cell cycle biomarker of aberrant growth, alone and in combination with NMP22.1677 consecutive patients under investigation for urinary tract malignancy were recruited to a prospective blinded observational study. All patients underwent ultrasound, intravenous urography, cystoscopy, urine culture and cytologic analysis. An immunofluorometric assay was used to measure Mcm5 levels in urine cell sediments. NMP22 urinary levels were determined with the FDA-approved NMP22® Test Kit.Genito-urinary tract cancers were identified in 210/1564 (13%) patients with an Mcm5 result and in 195/1396 (14%) patients with an NMP22 result. At the assay cut-point where sensitivity and specificity were equal, the Mcm5 test detected primary and recurrent bladder cancers with 69% sensitivity (95% confidence interval = 62-75%) and 93% negative predictive value (95% CI = 92-95%). The area under the receiver operating characteristic curve for Mcm5 was 0.75 (95% CI = 0.71-0.79) and 0.72 (95% CI = 0.67-0.77) for NMP22. Importantly, Mcm5 combined with NMP22 identified 95% (79/83; 95% CI = 88-99%) of potentially life threatening diagnoses (i.e. grade 3 or carcinoma in situ or stage ≥pT1) with high specificity (72%, 95% CI = 69-74%).The Mcm5 immunoassay is a non-invasive test for identifying patients with urothelial cancers with similar accuracy to the FDA-approved NMP22 ELISA Test Kit. The combination of Mcm5 plus NMP22 improves the detection of UCC and identifies 95% of clinically significant disease. Trials of a commercially developed Mcm5 assay suitable for an end-user laboratory alongside NMP22 are required to assess their potential clinical utility in improving diagnostic and surveillance care pathways.http://europepmc.org/articles/PMC3392249?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author John D Kelly
Tim J Dudderidge
Alex Wollenschlaeger
Odu Okoturo
Keith Burling
Fiona Tulloch
Ian Halsall
Teresa Prevost
Andrew Toby Prevost
Joana C Vasconcelos
Wendy Robson
Hing Y Leung
Nikhil Vasdev
Robert S Pickard
Gareth H Williams
Kai Stoeber
spellingShingle John D Kelly
Tim J Dudderidge
Alex Wollenschlaeger
Odu Okoturo
Keith Burling
Fiona Tulloch
Ian Halsall
Teresa Prevost
Andrew Toby Prevost
Joana C Vasconcelos
Wendy Robson
Hing Y Leung
Nikhil Vasdev
Robert S Pickard
Gareth H Williams
Kai Stoeber
Bladder cancer diagnosis and identification of clinically significant disease by combined urinary detection of Mcm5 and nuclear matrix protein 22.
PLoS ONE
author_facet John D Kelly
Tim J Dudderidge
Alex Wollenschlaeger
Odu Okoturo
Keith Burling
Fiona Tulloch
Ian Halsall
Teresa Prevost
Andrew Toby Prevost
Joana C Vasconcelos
Wendy Robson
Hing Y Leung
Nikhil Vasdev
Robert S Pickard
Gareth H Williams
Kai Stoeber
author_sort John D Kelly
title Bladder cancer diagnosis and identification of clinically significant disease by combined urinary detection of Mcm5 and nuclear matrix protein 22.
title_short Bladder cancer diagnosis and identification of clinically significant disease by combined urinary detection of Mcm5 and nuclear matrix protein 22.
title_full Bladder cancer diagnosis and identification of clinically significant disease by combined urinary detection of Mcm5 and nuclear matrix protein 22.
title_fullStr Bladder cancer diagnosis and identification of clinically significant disease by combined urinary detection of Mcm5 and nuclear matrix protein 22.
title_full_unstemmed Bladder cancer diagnosis and identification of clinically significant disease by combined urinary detection of Mcm5 and nuclear matrix protein 22.
title_sort bladder cancer diagnosis and identification of clinically significant disease by combined urinary detection of mcm5 and nuclear matrix protein 22.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2012-01-01
description Urinary biomarkers for bladder cancer detection are constrained by inadequate sensitivity or specificity. Here we evaluate the diagnostic accuracy of Mcm5, a novel cell cycle biomarker of aberrant growth, alone and in combination with NMP22.1677 consecutive patients under investigation for urinary tract malignancy were recruited to a prospective blinded observational study. All patients underwent ultrasound, intravenous urography, cystoscopy, urine culture and cytologic analysis. An immunofluorometric assay was used to measure Mcm5 levels in urine cell sediments. NMP22 urinary levels were determined with the FDA-approved NMP22® Test Kit.Genito-urinary tract cancers were identified in 210/1564 (13%) patients with an Mcm5 result and in 195/1396 (14%) patients with an NMP22 result. At the assay cut-point where sensitivity and specificity were equal, the Mcm5 test detected primary and recurrent bladder cancers with 69% sensitivity (95% confidence interval = 62-75%) and 93% negative predictive value (95% CI = 92-95%). The area under the receiver operating characteristic curve for Mcm5 was 0.75 (95% CI = 0.71-0.79) and 0.72 (95% CI = 0.67-0.77) for NMP22. Importantly, Mcm5 combined with NMP22 identified 95% (79/83; 95% CI = 88-99%) of potentially life threatening diagnoses (i.e. grade 3 or carcinoma in situ or stage ≥pT1) with high specificity (72%, 95% CI = 69-74%).The Mcm5 immunoassay is a non-invasive test for identifying patients with urothelial cancers with similar accuracy to the FDA-approved NMP22 ELISA Test Kit. The combination of Mcm5 plus NMP22 improves the detection of UCC and identifies 95% of clinically significant disease. Trials of a commercially developed Mcm5 assay suitable for an end-user laboratory alongside NMP22 are required to assess their potential clinical utility in improving diagnostic and surveillance care pathways.
url http://europepmc.org/articles/PMC3392249?pdf=render
work_keys_str_mv AT johndkelly bladdercancerdiagnosisandidentificationofclinicallysignificantdiseasebycombinedurinarydetectionofmcm5andnuclearmatrixprotein22
AT timjdudderidge bladdercancerdiagnosisandidentificationofclinicallysignificantdiseasebycombinedurinarydetectionofmcm5andnuclearmatrixprotein22
AT alexwollenschlaeger bladdercancerdiagnosisandidentificationofclinicallysignificantdiseasebycombinedurinarydetectionofmcm5andnuclearmatrixprotein22
AT oduokoturo bladdercancerdiagnosisandidentificationofclinicallysignificantdiseasebycombinedurinarydetectionofmcm5andnuclearmatrixprotein22
AT keithburling bladdercancerdiagnosisandidentificationofclinicallysignificantdiseasebycombinedurinarydetectionofmcm5andnuclearmatrixprotein22
AT fionatulloch bladdercancerdiagnosisandidentificationofclinicallysignificantdiseasebycombinedurinarydetectionofmcm5andnuclearmatrixprotein22
AT ianhalsall bladdercancerdiagnosisandidentificationofclinicallysignificantdiseasebycombinedurinarydetectionofmcm5andnuclearmatrixprotein22
AT teresaprevost bladdercancerdiagnosisandidentificationofclinicallysignificantdiseasebycombinedurinarydetectionofmcm5andnuclearmatrixprotein22
AT andrewtobyprevost bladdercancerdiagnosisandidentificationofclinicallysignificantdiseasebycombinedurinarydetectionofmcm5andnuclearmatrixprotein22
AT joanacvasconcelos bladdercancerdiagnosisandidentificationofclinicallysignificantdiseasebycombinedurinarydetectionofmcm5andnuclearmatrixprotein22
AT wendyrobson bladdercancerdiagnosisandidentificationofclinicallysignificantdiseasebycombinedurinarydetectionofmcm5andnuclearmatrixprotein22
AT hingyleung bladdercancerdiagnosisandidentificationofclinicallysignificantdiseasebycombinedurinarydetectionofmcm5andnuclearmatrixprotein22
AT nikhilvasdev bladdercancerdiagnosisandidentificationofclinicallysignificantdiseasebycombinedurinarydetectionofmcm5andnuclearmatrixprotein22
AT robertspickard bladdercancerdiagnosisandidentificationofclinicallysignificantdiseasebycombinedurinarydetectionofmcm5andnuclearmatrixprotein22
AT garethhwilliams bladdercancerdiagnosisandidentificationofclinicallysignificantdiseasebycombinedurinarydetectionofmcm5andnuclearmatrixprotein22
AT kaistoeber bladdercancerdiagnosisandidentificationofclinicallysignificantdiseasebycombinedurinarydetectionofmcm5andnuclearmatrixprotein22
_version_ 1725020809365291008

Similar Items