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Serous papillary peritoneal carcinoma: Unknown primary tumour, ovarian cancer counterpart or a distinct entity? A systematic review

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Date
2010
Author
ORCID logoPentheroudakis, George
ORCID logoPavlidis, Nicholas
Source
Critical reviews in oncology/hematology
Volume
75
Issue
1
Pages
27-42

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Keyword(s):
Cisplatin
Cyclophosphamide
Doxorubicin
Human
Neoplasms
Humans
Female
Cancer combination chemotherapy
Cancer survival
Ovarian neoplasms
Ovary cancer
Paclitaxel
Taxane derivative
Platinum
Cancer staging
Cytoreductive surgery
Review
Overall survival
Systematic review
Carcinoma
Gene frequency
Genotype
Clinical feature
Immunohistochemistry
Protein bcl 2
Protein p53
Heterozygosity loss
Monoclonal antibody
Unclassified drug
Pathology
Treatment response
Alkylating agent
Cancer of unknown primary site
Tumor localization
Unknown primary
Cancer regression
Metabolism
Treatment duration
Oncoprotein
Unspecified side effect
Ca 125 antigen
Protein s 100
Gene mutation
Cancer of unknown primary
Gene overexpression
Polymerase chain reaction
Ki 67 antigen
Epidermal growth factor receptor 2
Gene deletion
Treatment indication
Gene function
Membrane protein
Peritoneal neoplasms
Papillary
Brca1 protein
Cell adhesion molecule
Epithelial membrane antigen
Gene locus
Genomic instability
Monoclonal antibody b.72.3
Pancytokeratine
Peritoneal carcinomatosis
Peritoneum
Protein ln1
Protein ln21
Serous papillary carcinoma
Serous peritoneal papillary carcinoma
Tumor suppresor wilms tumor 1

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Abstract
Introduction: Serous peritoneal papillary carcinoma (SPPC), though managed according to ovarian cancer therapeutic principles, has been variably considered as an ovarian cancer counterpart, a peritoneal malignancy with distinct characteristics or a cancer of unknown primary (CUP). Patients and methods: We systematically reviewed all publications studying molecular pathophysiology, clinical presentation, management and outcome of at least 10 patients with SPPC from 1980 to 2008 in anglophone medical journals and critically analysed the data. Results: Molecular profiling of CUP was performed in eight papers reporting on 211 patients with stage III/IV SPPC by means of immunohistochemistry or PCR-based assays. Twenty-five clinical series, mostly retrospetive, reported management and outcome of 579 patiens with SPPC, in several cases matched to advanced ovarian cancer controls. Though we did not identify statistically significant differences in molecular biology, clinical presentation, management and outcome of SPPC and ovarian cancer cases, some subtle differences emerged: patterns of loss of heterozygosity at several chromosomal loci differed from those seen in ovarian cancer, while the overexpression of the HER2 oncogene was encountered more often. Serous peritoneal tumours affected older patients and were more frequently multifocal or exhibited virulent clonal expansion in metastatic sites. Diffuse micronodular spread formed a high total load of malignancy in omental, peritoneal surfaces, difficult to debulk optimally. Despite effective chemotherapeutic cytoreduction and occasional long-term remissions, SPPC patients survived 2-6 months less than ovarian cancer patients. Conclusions: Patients with SPPC should not be classified in the poor-risk CUP category, in view of the therapeutic and prognostic differences. Still, the assimilation of the SPPC entity by ovarian cancer hindered further research into its genotypic and phenotypic characteristics that may differ from ovarian cancer. Subgroup analyses of large ovarian cancer trials may shed light in this issue. © 2009 Elsevier Ireland Ltd.
DOI
10.1016/j.critrevonc.2009.10.003
URI
https://gnosis.library.ucy.ac.cy/handle/7/42374
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