Abstract:
Introduction: Every year, worldwide, are registered 10 million new cases of cancer and 6.2
million deaths over the cancer. About 5 to 40 % of malignant tumors of all anatomical locations have a
genetic etiology, and this percentage is growing due to increased general morbidity. So far, in the
literature there are described over 200 hereditary cancer syndromes, for 35% of which are fully described
the primary molecular defects or localisation of chromosomal mutation, and DNA diagnosis has become
a routine method of investigation for genetic diagnosis. Ovarian cancer also refers to these pathologies.
Ovarian cancer ranks 7th in the incidence of malignant tumors that can occur in women, with peak
incidence between 40 and 65 years. A woman's risk of developing ovarian cancer is 1,4 - 1,8%, with an
annual incidence of approximately 57.3 / 100,000 women who reach the age of 75-79 years, representing
the fifth leading cause of death cancer in women, and 5-year survival rate for all stages is between 35-
38%.
Materials and methods: we study the articles, publications and scientific literature specific for
this topic.
Discussion and results: Morphological obvious of the intraepithelial carcinoma in fallopian
tubes showed that glandular serous epithelium of the distal fallopian tube is the origin of anatomical
primary disease in most hereditary ovarian carcinomas type II, then, it seems that the identification of
intraepithelial tubal carcinoma with relatively non - invasive and in situ methods, by molecular imaging
could lead to an improvement in primary and secondary prevention of diseases. Approximately 5-10%
of ovarian cancers develop due to genetic predisposition, by mutations of the BRCA1 gene (17q) and
BRCA2 gene (13q) - forming a combination of ovarian and breast cancer, hereditary breast-ovarian
cancer (HBOC) syndrome. Other genetic mutations involved in the pathogenesis of ovarian cancer are
changes in metalloproteinases, in PTEN, TP53. Around 60% of cases of serous ovarian cancer in stage
III and IV are related to have mutations in the TP53 tumor suppressor gene.
Conclusion: By investigating mutations in ovarian cancers genetically determined, we could
increase survival by performing prophylactic salpingo-oophorectomy to susceptible persons.
Description:
Department of Molecular Biology and Human genetics, Nicolae Testemitanu State University of Medicine and Pharmacy, Chisinau, Republic of Moldova, The 6th International Medical Congress for Students and Young Doctors