| Literature DB >> 24804229 |
Gautier Chene1, Gery Lamblin1, Karine Le Bail-Carval1, Philippe Chabert1, Naoual Bakrin1, Georges Mellier1.
Abstract
Faced with the catastrophic prognosis for ovarian cancer due to the fact that it is most often diagnosed late at the peritoneal carcinomatosis stage, screening and early detection could probably reduce the mortality rate. A better understanding of the molecular characteristics of the different ovarian cancer subtypes and their specific molecular signatures is indispensable prior to development of new screening strategies. We discuss here the early natural history of ovarian cancer and its origins.Entities:
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Year: 2014 PMID: 24804229 PMCID: PMC3997076 DOI: 10.1155/2014/639252
Source DB: PubMed Journal: Biomed Res Int Impact factor: 3.411
Figure 1Comparison of the tubal pathway versus the ovarian pathway. The potential serous carcinogenic tubal sequence in comparison with the potential serous carcinogenic ovarian sequence. Note that SCOUT lesions (the earliest precursor lesion) could develop into other types of preinvasive lesions, p53 signature, and then STIL and STIC. The STIC would then easily metastasize in the ovary and adjacent peritoneum. By contrast, only the ovarian epithelial dysplasia is described as an ovarian preinvasive lesion. This figure raises the question of the interaction and molecular mechanisms between the fallopian tube and the ovary.
Figure 3Precursor and invasive lesions in high-grade serous, clear cell, and endometrioid carcinoma. Note. Normal fallopian tube (A) and ovarian surface epithelium (B). High-grade serous ovarian carcinoma (G) may arise from ovarian dysplasia (inclusion cysts in C, deep cortical invaginations in D) and/or from tubal preinvasive lesions (STIC, H&E in E, and high immunohistochemical expression of P53 in F). On the other side, endometriosis (H) may develop in endometrioid carcinoma (J) or clear cell carcinoma (I). With this picture, we would like to show the thin anatomical connection between ovary and fallopian tube and their implications in ovarian carcinogenesis.