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  3. A Prostate Cancer "Nimbosus": Genomic Instability and SChLAP1 Dysregulation Underpin Aggression of Intraductal and Cribriform Subpathologies.
 

A Prostate Cancer "Nimbosus": Genomic Instability and SChLAP1 Dysregulation Underpin Aggression of Intraductal and Cribriform Subpathologies.

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BORIS DOI
10.7892/boris.109890
Publisher DOI
10.1016/j.eururo.2017.04.034
PubMed ID
28511883
Description
BACKGROUND

Intraductal carcinoma (IDC) and cribriform architecture (CA) represent unfavorable subpathologies in localized prostate cancer. We recently showed that IDC shares a clonal ancestry with the adjacent glandular adenocarcinoma.

OBJECTIVE

We investigated for the co-occurrence of "aggression" factors, genomic instability and hypoxia, and performed gene expression profiling of these tumors.

DESIGN, SETTING, AND PARTICIPANTS

A total of 1325 men were treated for localized prostate cancer from four academic institutions (University Health Network, CHU de Québec-Université Laval, Memorial Sloan Kettering Cancer Center [MSKCC], and Erasmus Medical Center). Pathological specimens were centrally reviewed. Gene copy number and expression, and intraprostatic oxygenation were assessed.

OUTCOME MEASUREMENTS AND STATISTICAL ANALYSIS

IDC/CA was separately assessed for biochemical relapse risk in the Canadian and MSKCC cohorts. Both cohorts were pooled for analyses on metastasis.

RESULTS AND LIMITATION

Presence of IDC/CA independently predicted for increased risks of biochemical relapse (HRCanadian 2.17, p<0.001; HRMSKCC 2.32, p=0.0035) and metastasis (HRpooled 3.31, p<0.001). IDC/CA+ cancers were associated with an increased percentage of genome alteration (PGA [median] 7.2 vs 3.0, p<0.001), and hypoxia (64.0% vs 45.5%, p=0.17). Combinatorial genomic-pathological indices offered the strongest discrimination for metastasis (C-index 0.805 [clinical+IDC/CA+PGA] vs 0.786 [clinical+IDC/CA] vs 0.761 [clinical]). Profiling of mRNA abundance revealed that long noncoding RNA, SChLAP1, was the only gene expressed at >3-fold higher (p<0.0001) in IDC/CA+ than in IDC/CA- tumors, independently corroborated by increased SChLAP1 RNA in situ hybridization signal. Optimal treatment intensification for IDC/CA+ prostate cancer requires prospective testing.

CONCLUSIONS

The poor outcome associated with IDC and CA subpathologies is associated with a constellation of genomic instability, SChLAP1 expression, and hypoxia. We posit a novel concept in IDC/CA+ prostate cancer, "nimbosus" (gathering of stormy clouds, Latin), which manifests as increased metastatic capacity and lethality.

PATIENT SUMMARY

A constellation of unfavorable molecular characteristics co-occur with intraductal and cribriform subpathologies in prostate cancer. Modern imaging for surveillance and treatment intensification trials should be considered in this adverse subgroup.
Date of Publication
2017-11
Publication Type
Article
Subject(s)
600 Technology > 610 Medicine & health
Keyword(s)
Cribriform architecture Genomic instability Hypoxia Intraductal carcinoma Prognosis SChLAP1
Language(s)
en
Contributor(s)
Chua, Melvin L K
Lo, Winnie
Pintilie, Melania
Murgic, Jure
Lalonde, Emilie
Bhandari, Vinayak
Mahamud, Osman
Gopalan, Anuradha
Kweldam, Charlotte F
van Leenders, Geert J L H
Verhoef, Esther I
Hoogland, Agnes Marije
Livingstone, Julie
Berlin, Alejandro
Dal Pra, Alan
Universitätsklinik für Radio-Onkologie
Meng, Alice
Zhang, Junyan
Orain, Michèle
Picard, Valérie
Hovington, Hélène
Bergeron, Alain
Lacombe, Louis
Fradet, Yves
Têtu, Bernard
Reuter, Victor E
Fleshner, Neil
Fraser, Michael
Boutros, Paul C
van der Kwast, Theodorus H
Bristow, Robert G
Additional Credits
Universitätsklinik für Radio-Onkologie
Series
European urology
Publisher
Elsevier
ISSN
0302-2838
Access(Rights)
restricted
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