Bioinformatic identification of FGF, p38-MAPK, and calcium signalling pathways associated with carcinoma in situ in the urinary bladder

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Bioinformatic identification of FGF, p38-MAPK, and calcium signalling pathways associated with carcinoma in situ in the urinary bladder. / Herbsleb, Malene; Christensen, Ole F.; Thykjaer, Thomas; Wiuf, Carsten; Borre, Michael; Ørntoft, Torben F.; Dyrskjøt, Lars.

In: BMC Cancer, Vol. 8, 37, 31.01.2008.

Research output: Contribution to journalJournal articleResearchpeer-review

Harvard

Herbsleb, M, Christensen, OF, Thykjaer, T, Wiuf, C, Borre, M, Ørntoft, TF & Dyrskjøt, L 2008, 'Bioinformatic identification of FGF, p38-MAPK, and calcium signalling pathways associated with carcinoma in situ in the urinary bladder', BMC Cancer, vol. 8, 37. https://doi.org/10.1186/1471-2407-8-37

APA

Herbsleb, M., Christensen, O. F., Thykjaer, T., Wiuf, C., Borre, M., Ørntoft, T. F., & Dyrskjøt, L. (2008). Bioinformatic identification of FGF, p38-MAPK, and calcium signalling pathways associated with carcinoma in situ in the urinary bladder. BMC Cancer, 8, [37]. https://doi.org/10.1186/1471-2407-8-37

Vancouver

Herbsleb M, Christensen OF, Thykjaer T, Wiuf C, Borre M, Ørntoft TF et al. Bioinformatic identification of FGF, p38-MAPK, and calcium signalling pathways associated with carcinoma in situ in the urinary bladder. BMC Cancer. 2008 Jan 31;8. 37. https://doi.org/10.1186/1471-2407-8-37

Author

Herbsleb, Malene ; Christensen, Ole F. ; Thykjaer, Thomas ; Wiuf, Carsten ; Borre, Michael ; Ørntoft, Torben F. ; Dyrskjøt, Lars. / Bioinformatic identification of FGF, p38-MAPK, and calcium signalling pathways associated with carcinoma in situ in the urinary bladder. In: BMC Cancer. 2008 ; Vol. 8.

Bibtex

@article{779de31acb074057a9bab059c2459c9e,
title = "Bioinformatic identification of FGF, p38-MAPK, and calcium signalling pathways associated with carcinoma in situ in the urinary bladder",
abstract = "Background: Carcinoma in situ (CIS) is believed to be a precursor of invasive bladder cancer. Identification of CIS is a valuable prognostic factor since radical treatment strategies can be offered these patients before the disease becomes invasive. Methods: We developed a pathway based classifier approach to predict presence or absence of CIS in patients suffering from non muscle invasive bladder cancer. From Ingenuity Pathway Analysis we considered four canonical signalling pathways (p38 MAPK, FGF, Calcium, and cAMP pathways) with most coherent expression of transcription factors (TFs) across samples in a set of twenty-eight non muscle invasive bladder carcinomas. These pathways contained twelve TFs in total. We used the expression of the TFs to predict presence or absence of CIS in a Leave-One-Out Cross Validation classification. Results: We showed that TF expression levels in three pathways (FGF, p38 MAPK, and calcium signalling) or the expression of the twelve TFs together could be used to predict presence or absence of concomitant CIS. A cluster analysis based on expression of the twelve TFs separated the samples in two main clusters: one branch contained 11 of the 15 patients without concomitant CIS and with the majority of the genes being down regulated; the other branch contained 10 of 13 patients with concomitant CIS, and here genes were mostly up regulated. The expression in the CIS group was comparable to the expression of twenty-three patients suffering from muscle-invasive bladder carcinoma. Finally, we validated our results in an independent test set and found that prediction of CIS status was possible using TF expression of the p38 MAPK pathway. Conclusion: We conclude that it is possible to use pathway analysis for molecular classification of bladder tumors.",
author = "Malene Herbsleb and Christensen, {Ole F.} and Thomas Thykjaer and Carsten Wiuf and Michael Borre and {\O}rntoft, {Torben F.} and Lars Dyrskj{\o}t",
year = "2008",
month = jan,
day = "31",
doi = "10.1186/1471-2407-8-37",
language = "English",
volume = "8",
journal = "B M C Cancer",
issn = "1471-2407",
publisher = "BioMed Central Ltd.",

}

RIS

TY - JOUR

T1 - Bioinformatic identification of FGF, p38-MAPK, and calcium signalling pathways associated with carcinoma in situ in the urinary bladder

AU - Herbsleb, Malene

AU - Christensen, Ole F.

AU - Thykjaer, Thomas

AU - Wiuf, Carsten

AU - Borre, Michael

AU - Ørntoft, Torben F.

AU - Dyrskjøt, Lars

PY - 2008/1/31

Y1 - 2008/1/31

N2 - Background: Carcinoma in situ (CIS) is believed to be a precursor of invasive bladder cancer. Identification of CIS is a valuable prognostic factor since radical treatment strategies can be offered these patients before the disease becomes invasive. Methods: We developed a pathway based classifier approach to predict presence or absence of CIS in patients suffering from non muscle invasive bladder cancer. From Ingenuity Pathway Analysis we considered four canonical signalling pathways (p38 MAPK, FGF, Calcium, and cAMP pathways) with most coherent expression of transcription factors (TFs) across samples in a set of twenty-eight non muscle invasive bladder carcinomas. These pathways contained twelve TFs in total. We used the expression of the TFs to predict presence or absence of CIS in a Leave-One-Out Cross Validation classification. Results: We showed that TF expression levels in three pathways (FGF, p38 MAPK, and calcium signalling) or the expression of the twelve TFs together could be used to predict presence or absence of concomitant CIS. A cluster analysis based on expression of the twelve TFs separated the samples in two main clusters: one branch contained 11 of the 15 patients without concomitant CIS and with the majority of the genes being down regulated; the other branch contained 10 of 13 patients with concomitant CIS, and here genes were mostly up regulated. The expression in the CIS group was comparable to the expression of twenty-three patients suffering from muscle-invasive bladder carcinoma. Finally, we validated our results in an independent test set and found that prediction of CIS status was possible using TF expression of the p38 MAPK pathway. Conclusion: We conclude that it is possible to use pathway analysis for molecular classification of bladder tumors.

AB - Background: Carcinoma in situ (CIS) is believed to be a precursor of invasive bladder cancer. Identification of CIS is a valuable prognostic factor since radical treatment strategies can be offered these patients before the disease becomes invasive. Methods: We developed a pathway based classifier approach to predict presence or absence of CIS in patients suffering from non muscle invasive bladder cancer. From Ingenuity Pathway Analysis we considered four canonical signalling pathways (p38 MAPK, FGF, Calcium, and cAMP pathways) with most coherent expression of transcription factors (TFs) across samples in a set of twenty-eight non muscle invasive bladder carcinomas. These pathways contained twelve TFs in total. We used the expression of the TFs to predict presence or absence of CIS in a Leave-One-Out Cross Validation classification. Results: We showed that TF expression levels in three pathways (FGF, p38 MAPK, and calcium signalling) or the expression of the twelve TFs together could be used to predict presence or absence of concomitant CIS. A cluster analysis based on expression of the twelve TFs separated the samples in two main clusters: one branch contained 11 of the 15 patients without concomitant CIS and with the majority of the genes being down regulated; the other branch contained 10 of 13 patients with concomitant CIS, and here genes were mostly up regulated. The expression in the CIS group was comparable to the expression of twenty-three patients suffering from muscle-invasive bladder carcinoma. Finally, we validated our results in an independent test set and found that prediction of CIS status was possible using TF expression of the p38 MAPK pathway. Conclusion: We conclude that it is possible to use pathway analysis for molecular classification of bladder tumors.

UR - http://www.scopus.com/inward/record.url?scp=41049090396&partnerID=8YFLogxK

U2 - 10.1186/1471-2407-8-37

DO - 10.1186/1471-2407-8-37

M3 - Journal article

C2 - 18237400

AN - SCOPUS:41049090396

VL - 8

JO - B M C Cancer

JF - B M C Cancer

SN - 1471-2407

M1 - 37

ER -

ID: 203905830