One of the main challenges for medicine in the early part of 21st century is to incorporate knowledge of the
human genome into the medical management of patients, thereby yielding more precise diagnoses and
mechanism-based deployment of therapy. Nowhere is this need more pressing than in the treatment of men
with prostate cancer. Prostate cancer is a major cause of death and morbidity, yet large numbers of men are
believed to harbor tumors that are indolent even in the absence of therapy. As such, many men receive
unnecessary treatment with its attendant effects, and others die of disease despite aggressive therapy. We
hypothesize that the variability in the natural history of CaP is determined by heretofore unrecognized
molecular heterogeneity of the disease. We therefore propose here to identify a gene expression signature
that distinguishes indolent from lethal disease.
This Project has 3 Specific Aims:
Aim 1: Collect, register, and process archival formalin-fixed paraffin embedded (FFPE) samples from the
Swedish Watchful Waiting (WW) cohorts with up to 30 years clinical follow up.
Aim 2: Develop molecular signatures of lethal and indolent prostate cancer on the Watchful Waiting FFPE
samples using an Illumina expression array platform with over 6000 genes developed specifically for
molecular signature discovery.
Aim 3: Validate the signatures on Swedish WW cases not used in Aim 2 and test for the presence of these
profiles in tumor samples (n=100) from the Physicians' Health Study (PHS).
At the conclusion of this proposal, we expect to have discovered and validated molecular predictors of
prostate cancer outcome that are appropriate for further clinical development. To accomplish these goals, we
have assembled a multidisciplinary team of investigators with a long track record of collaboration, and with
particular expertise in the clinical, pathological and epidemiological aspects of prostate cancer, in the
development and deployment of genomics technologies, and in advanced computational and statistical
analysis.
Public Health Relevance Statement
Data not available.
NIH Spending Category
No NIH Spending Category available.
Project Terms
AddressArchivesBiochemicalCancer SurvivorCaringCause of DeathCellsCessation of lifeClinicalClinical TrialsCollaborationsCore BiopsyDana-Farber Cancer InstituteData SetDecision MakingDevelopmentDiagnosisDiagnosticDiseaseEnd PointFailureFormalinGene Expression ProfileGene Expression ProfilingGenerationsGenesGenomeGenomicsGoalsHealthHeterogeneityHospitalsHuman GenomeIndolentInstitutesInstitutionInternationalInterventionKnowledgeLocalizedMalignant neoplasm of prostateMassachusettsMedicalMedicineMethodsMolecularMolecular AnalysisMolecular ProfilingMorbidity - disease rateNatural HistoryNeoplasm MetastasisNumbersOperative Surgical ProceduresOutcomeParaffin EmbeddingPatient observationPatientsPhysiciansProcessProstatectomyPublic DomainsPublic Health SchoolsRadiationRecurrenceResearch PersonnelRiskSamplingSpecimenStandards of Weights and MeasuresSwedenTechnologyTestingTherapeutic InterventionTimeTissue SampleTissuesUniversity HospitalsWomanWorkbasecohortfollow-upmenmultidisciplinaryneoplastic cellnew technologynovelprogramstumor
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