Current perspectives on recommendations for BRCA genetic testing in ovarian cancer patients.

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Authors

Vergote, I
Banerjee, S
Gerdes, A-M
van Asperen, C
Marth, C
Vaz, F
Ray-Coquard, I
Stoppa-Lyonnet, D
Gonzalez-Martin, A
Sehouli, J
Colombo, N

Document Type

Journal Article

Date

2016-12-01

Date Accepted

2016-10-05

Abstract

Traditionally, BRCA genetic testing has been undertaken to identify patients and family members at future risk of developing cancer and patients have been referred for testing based on family history. However, the now recognised risk of ovarian cancer (OC) patients, even those with no known family history, harbouring a mutation in BRCA1/2, together with the first poly adenosine diphosphate ribose polymerase inhibitor (PARPi; olaparib [Lynparza]) being licenced for the treatment of BRCA-mutated OC, has led to reconsideration of referral criteria for OC patients. Provided here is a review of the existing data and guidelines in the European Union, relating to recommendations, as well as considerations, for the referral of OC patients for BRCA genetic testing. Based on this review of newly updated guidance and up-to-date evidence, the following is recommended: all patients with invasive epithelial OC (excluding borderline or mucinous), including those with fallopian tube and peritoneal cancers, should be considered as candidates for referral for BRCA genetic testing, irrespective of age; genetic testing should ideally be offered at diagnosis, although patients can be referred at any stage; retrospective testing should be offered to patients in long-term follow-up because of the implications for family members and individual future breast cancer risk; and germline BRCA testing of a blood/saliva sample should initially be conducted and, if negative, tumour tissue should be tested (to identify non-germline [somatic] BRCA PARPi therapy candidates).

Citation

European journal of cancer (Oxford, England : 1990), 2016, 69 pp. 127 - 134

Source Title

Publisher

ELSEVIER SCI LTD

ISSN

0959-8049

eISSN

1879-0852

Research Team

Notes