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95 research outputs found

Molecular alterations in endometrial cancer: implications for clinical management

Author: Stelloo E.
Publication venue
Publication date: 20/04/2017
Field of study

Over the last decades, advances have been made in the treatment of endometrial cancer. The clinicopathological risk stratification for postoperative therapy has considerably reduced overtreatment by refining indications and introducing treatment with fewer side effects. Despite refinement in the use of postoperative radiation therapy in EC, over- and under- treatment remain a clinical problem. This may be caused by the limited accuracy of the clinicopathological risk stratification to select patients of higher risk of recurrence. The lack of reproducibility of pathologists to diagnose tumor type and grade may also limit the accuracy of the clinicopathological risk stratification. Expert gyneco-pathology review and a two-tiered grading system will lead to more accurate and reproducible diagnoses. Nonetheless, there is pressing need to understand tumor behavior and design tailored treatments to further improve risk stratification. The identification of molecular markers predictive of recurrence risk or treatment benefit beyond current clinicopathological factors would represent a major advance. The aims of this thesis were to gain insight in the molecular alterations of endometrial cancer and to identify prognostic markers in endometrial cancer to refine clinicopathological risk assessment and direct adjuvant therapy.LUMC / Geneeskund

Leiden University Scholary Publications

Practical guidance for mismatch repair-deficiency testing in endometrial cancer

Author: Bosse T.
Church D.N.
Creutzberg C.L.
Jansen A.M.L.
Morreau H.
Nout R.A.
Osse E.M.
Ruano D.
Smit V.T.H.B.M.
Stelloo E.
Wezel T. van
Publication venue: 'Oxford University Press (OUP)'
Publication date: 01/01/2016
Field of study

MTG8 - Moleculaire pathologie van gynecologische tumore

Oxford University Research Archive

Leiden University Scholary Publications

Folate receptor-alpha targeted near-infrared fluorescence imaging in high-risk endometrial cancer patients: a tissue microarray and clinical feasibility study

Author: Beltman J.J.
Boogerd L.S.F.
Bosse T.
Burggraaf J.
Gaarenstroom K.N.
Hoogstins C.E.S.
Kroon C.D. de
Low P.S.
Stelloo E.
Vahrmeijer A.L.
Vuyk J.
Publication venue: 'Impact Journals, LLC'
Publication date: 02/01/2018
Field of study

Surgical oncolog

Leiden University Scholary Publications

Androgen receptor profiling predicts prostate cancer outcome

Author: Bergman A.M. (Andries)
de Jong J. (Jeroen)
Jenster G.W. (Guido)
Leenders G.J.H.L. (Geert)
Nevedomskaya E. (Ekaterina)
Stelloo S. (Suzan)
van der Poel H.G. (Henk G.)
Wessels L. (Lodewyk)
Zwart W. (Wilbert)
Publication venue: 'EMBO'
Publication date: 01/01/2015
Field of study

Prostate cancer is the second most prevalent malignancy in men. Biomarkers for outcome prediction are urgently needed, so that high-risk patients could be monitored more closely postoperatively. To identify prognostic markers and to determine causal players in prostate cancer progression, we assessed changes in chromatin state during tumor development and progression. Based on this, we assessed genomewide androgen receptor/chromatin binding and identified a distinct androgen receptor/chromatin binding profile between primary prostate cancers and tumors with an acquired resistance to therapy. These differential androgen receptor/chromatin interactions dictated expression of a distinct gene signature with strong prognostic potential. Further refinement of the signature provided us with a concise list of nine genes that hallmark prostate cancer outcome in multiple independent validation series. In this report, we identified a novel gene expression signature for prostate cancer outcome through generation of multilevel genomic data on chromatin accessibility and transcriptional regulation and integration with publically available transcriptomic and clinical datastreams. By combining existing technologies, we propose a novel pipeline for biomarker discovery that is easily implementable in other fields of oncology

Crossref

PubMed Central

Erasmus University Digital Repository

Multilevel genomics of colorectal cancers with microsatellite instability—clinical impact of JAK1 mutations and consensus molecular subtype 1

Author: A Duval
A Sottoriva
A Untergasser
AL Børresen
Anita Sveen
Arild Nesbakken
B Efron
B Mlecnik
B Niu
B Vogelstein
Bjarne Johannessen
C Chen
CA Miller
CE Bronner
CG Kim
CJ Punt
CT Saunders
David Kerr
DH Ghoneim
DJ Kerr
DS Shin
DT Le
E Becht
E Rayner
E Stelloo
EC Røyrvik
Edward Leithe
Enric Domingo
F Supek
FS Leach
Guro E. Lind
H Li
H Rajagopalan
I Hoof
Ian Tomlinson
Ina A. Eilertsen
J Bruun
J Ferlay
J Guinney
JG Herman
JM Cunningham
JM Mullaney
JM Zaretsky
JS Gehring
K Andresen
K Cibulskis
K Wang
K Wang
K Yoshihara
Kaja C. G. Berg
L Marisa
LA Aaltonen
LB Alexandrov
Leonardo A. Meza-Zepeda
LG Morris
LL Myeroff
LQM Chow
M Angelova
M Berg
M Buchert
M Giannakis
M Giannakis
M Guidoboni
M Nielsen
MF Kane
MS Lawrence
N Andor
N Andor
N Papadopoulos
Ola Myklebost
P Charoentong
P Loo Van
P Peltomaki
P Sansone
R Fishel
R Parsons
R Sanz-Pamplona
R Wooster
RA Lothe
RA Lothe
Ragnhild A. Lothe
RJ Hause
Rolf I. Skotheim
S Hanzelmann
S Markowitz
S Popat
SA McCarroll
SA Shukla
SD Brown
SN Thibodeau
Stine A. Danielsen
The Cancer Genome Atlas Network
TM Kim
TN Schumacher
Torstein Tengs
W Hugo
WE Johnson
Y Ionov
Y Ren
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2017
Field of study

Background Approximately 15% of primary colorectal cancers have DNA mismatch repair deficiency, causing a complex genome with thousands of small mutations—the microsatellite instability (MSI) phenotype. We investigated molecular heterogeneity and tumor immunogenicity in relation to clinical endpoints within this distinct subtype of colorectal cancers. Methods A total of 333 primary MSI+ colorectal tumors from multiple cohorts were analyzed by multilevel genomics and computational modeling—including mutation profiling, clonality modeling, and neoantigen prediction in a subset of the tumors, as well as gene expression profiling for consensus molecular subtypes (CMS) and immune cell infiltration. Results Novel, frequent frameshift mutations in four cancer-critical genes were identified by deep exome sequencing, including in CRTC1, BCL9, JAK1, and PTCH1. JAK1 loss-of-function mutations were validated with an overall frequency of 20% in Norwegian and British patients, and mutated tumors had up-regulation of transcriptional signatures associated with resistance to anti-PD-1 treatment. Clonality analyses revealed a high level of intra-tumor heterogeneity; however, this was not associated with disease progression. Among the MSI+ tumors, the total mutation load correlated with the number of predicted neoantigens (P = 4 × 10−5), but not with immune cell infiltration—this was dependent on the CMS class; MSI+ tumors in CMS1 were highly immunogenic compared to MSI+ tumors in CMS2-4. Both JAK1 mutations and CMS1 were favorable prognostic factors (hazard ratios 0.2 [0.05–0.9] and 0.4 [0.2–0.9], respectively, P = 0.03 and 0.02). Conclusions Multilevel genomic analyses of MSI+ colorectal cancer revealed molecular heterogeneity with clinical relevance, including tumor immunogenicity and a favorable patient outcome associated with JAK1 mutations and the transcriptomic subgroup CMS1, emphasizing the potential for prognostic stratification of this clinically important subtype. See related research highlight by Samstein and Chan 10.1186/s13073-017-0438-

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