AUTHOR=Hamdi Yosr , Mighri Najah , Boujemaa Maroua , Mejri Nesrine , Ben Nasr Sonia , Ben Rekaya Mariem , Messaoud Olfa , Bouaziz Hanen , Berrazega Yosra , Rachdi Haifa , Jaidane Olfa , Daoud Nouha , Zribi Aref , Ayari Jihene , El Benna Houda , Labidi Soumaya , Ben Hassouna Jamel , Haddaoui Abderazzek , Rahal Khaled , Benna Farouk , Mrad Ridha , Ben Ahmed Slim , Boussen Hamouda , Boubaker Samir , Abdelhak Sonia 

TITLE=Identification of Eleven Novel BRCA Mutations in Tunisia: Impact on the Clinical Management of BRCA Related Cancers

JOURNAL=Frontiers in Oncology

VOLUME=11

YEAR=2021

URL=https://www.frontiersin.org/journals/oncology/articles/10.3389/fonc.2021.674965

DOI=10.3389/fonc.2021.674965

ISSN=2234-943X

ABSTRACT=<sec><title>Background</title><p>Breast cancer is the world’s most common cancer among women. It is becoming an increasingly urgent problem in low- and middle-income countries (LMICs) where a large fraction of women is diagnosed with advanced-stage disease and have no access to treatment or basic palliative care. About 5-10% of all breast cancers can be attributed to hereditary genetic components and up to 25% of familial cases are due to mutations in <italic>BRCA1</italic>/2 genes. Since their discovery in 1994 and 1995, as few as 18 mutations have been identified in <italic>BRCA</italic> genes in the Tunisian population. The aim of this study is to identify additional <italic>BRCA</italic> mutations, to estimate their contribution to the hereditary breast and ovarian cancers in Tunisia and to investigate the clinicopathological signatures associated with <italic>BRCA</italic> mutations.</p></sec><sec><title>Methods</title><p>A total of 354 patients diagnosed with breast and ovarian cancers, including 5 male breast cancer cases, have been investigated for <italic>BRCA1/2</italic> mutations using traditional and/or next generation sequencing technologies. Clinicopathological signatures associated with <italic>BRCA</italic> mutations have also been investigated.</p></sec><sec><title>Results</title><p>In the current study, 16 distinct mutations were detected: 10 in <italic>BRCA1</italic> and 6 in <italic>BRCA2</italic>, of which 11 are described for the first time in Tunisia including 3 variations that have not been reported previously in public databases namely <italic>BRCA1</italic>_c.915T&gt;A; <italic>BRCA2</italic>_c.-227-?_7805+? and <italic>BRCA2</italic>_c.249delG. Early age at onset, family history of ovarian cancer and high tumor grade were significantly associated with <italic>BRCA</italic> status. <italic>BRCA1</italic> carriers were more likely to be triple negative breast cancer compared to <italic>BRCA2</italic> carriers. A relatively high frequency of contralateral breast cancer and ovarian cancer occurrence was observed among <italic>BRCA</italic> carriers and was more frequent in patients carrying <italic>BRCA1</italic> mutations.</p></sec><sec><title>Conclusion</title><p>Our study provides new insights into breast and ovarian cancer genetic landscape in the under-represented North African populations. The prevalence assessment of novel and recurrent <italic>BRCA1/2</italic> pathogenic mutations will enhance the use of personalized treatment and precise screening strategies by both affected and unaffected North African cancer cases.</p></sec>