ACTIONABILITY KNOWLEDGE REPOSITORY ACTIONABILITY CURATION INTERFACE

Adult Summary Report Secondary Findings in Adult Subjects Non-diagnostic, excludes newborn screening & prenatal testing/screening A Current Version Rule-Out Dashboard Release History Status (Adult): Passed (Consensus scoring is Complete) Curation Status (Adult): Released 1.1.1

GENE/GENE PANEL: RAD51C, RAD51D, BRIP1
Condition: Ovarian cancer
Mode(s) of Inheritance: Autosomal Dominant
Actionability Assertion
Gene Condition Pairs(s)
Final Assertion
RAD51C0016248 (breast-ovarian cancer, familial, susceptibility to, 3; brovca3)
Assertion Pending
RAD51D0016248 (breast-ovarian cancer, familial, susceptibility to, 4; brovca4)
Assertion Pending
BRIP10016248 (breast cancer)
Assertion Pending
Actionability Rationale
This topic was initially scored prior to development of the process for making actionability assertions. The Actionability Working Group decided to defer making an assertion until after the topic could be reviewed through the update process.
Final Consensus Scoresa
Outcome / Intervention Pair
Severity
Likelihood
Effectiveness
Nature of the
Intervention
Total
Score
Ovarian cancer / Oophorectomy
2
1C
3B
1
7CB

 
Topic
Narrative Description of Evidence
Ref
1. What is the nature of the threat to health for an individual carrying a deleterious allele?
Prevalence of the Genetic Condition
The prevalence of familial breast-ovarian cancer associated with heterozygous germline pathogenic variants in the RAD51C, RAD51D, or BRIP1 genes in the general population is not clear. A recent review estimated that altogether, RAD51C pathogenic variants have been identified in 29 breast or ovarian cancer probands with a family history of ovarian cancer, with an overall prevalence of 0.84%. A study of 1915 women with ovarian cancer with available germline DNA, unselected for age or family history, reported a frequency of 0.6% of RAD51C and RAD51D and 1.4% of BRIP1 pathogenic variants.
1 2
Clinical Features
(Signs / symptoms)
Pathogenic variants in RAD51C , RAD51D, and BRIP1 are associated with an increased risk of ovarian cancer. However, there is currently insufficient evidence for the risk of breast cancer associated with these genes.
3 4 5
Natural History
(Important subgroups & survival / recovery)
A study of 6 unrelated German pedigrees indicated that the mean age of onset of ovarian cancer associated with RAD51C was 60 years, 8 years younger than the mean age of onset of ovarian cancer of 68 years in the general population. A US-based study of 1915 women with ovarian cancer with available germline DNA, unselected for age or family history, reported mean ages of onset of 64, 54, and 65.5 for individuals with pathogenic variants in RAD51C, RAD51D, and BRIP1, respectively. Individuals in the same study without an identified mutation had a median age of onset of 62 years.
2 3
2. How effective are interventions for preventing harm?
Information on the effectiveness of the recommendations below was not provided unless otherwise stated.
Patient Management
Based on estimates from available studies, the lifetime risk of ovarian cancer in carriers of pathogenic variants in RAD51C, RAD51D , and BRIP1 appears to be sufficient to justify consideration of risk-reducing salpingo-oophorectomy (RRSO). However, the current evidence is insufficient to make a firm recommendation as to the optimal age for RRSO. The argument has been made that RRSO should not be considered until a woman’s expected lifetime risk of developing ovarian cancer exceeds 2.6%, the expected lifetime risk of a woman with a BRCA-negative family history of ovarian cancer. The cumulative risk for developing ovarian cancer does not approach 2.6% until ages 60 to 64 for RAD51C, ages 50 to 54 for RAD51D, and ages 50 to 55 years for BRIP1. However, some women may have additive risk factors and delaying the discussion of RRSO until these age ranges may miss some cases of early-onset ovarian cancer. Therefore, based on the current, limited evidence base, it has been recommended for carriers of RAD51C, RAD51D, and BRIP1 pathogenic variants that a discussion about RRSO should be held around age 45–50 years or earlier based on a specific family history of an earlier onset ovarian cancer. (Tier 2)
4 6
Evidence on the effectiveness of reducing risk of ovarian cancer following RRSO in patients with pathogenic variants in RAD51C, RAD51C, and BRIP1 was not available. However, studies in women who are at high risk, including those with BRCA1 an BRCA2 mutations, show a reduction in risk of ovarian cancer by 69-100%. (Tier 1)
7 8
Surveillance
Screening for ovarian cancer in high risk groups, including carriers of pathogenic variants in RAD51C and RAD51D, should only be offered in the context of a research study. (Tier 2)
6
A similar recommendation was not identified for BRIP1.
 
Circumstances to Avoid
No circumstances-to-avoid recommendations have been provided for the Adult context.
 
3. What is the chance that this threat will materialize?
Mode of Inheritance
Autosomal Dominant
 
Prevalence of Genetic Variants
The prevalence of pathogenic mutations associated with an increased risk of ovarian cancer in RAD51C, RAD51D, and BRIP1 in the general population is unknown.
 
Penetrance
(Include any high risk racial or ethnic subgroups)
The cumulative risk of developing ovarian cancer in carriers of a RAD51C pathogenic variant approaches 2.6% around ages 60 to 64 years, with the cumulative risk between the ages of 55 to 59 being 1.5%. (Tier 3)
4
For RAD51D, carriers approach a cumulative risk of 2.6% around age 50 to 54. (Tier 3)
4
The cumulative lifetime risk of developing ovarian cancer by age 80 in carriers of BRIP1 pathogenic variants is estimated to be 5.8%. (Tier 3)
4
Relative Risk
(Include any high risk racial or ethnic subgroups)
The relative risk of ovarian cancer for RAD51C and RAD51D has been estimated as 5.88 (95% CI: 2.91–11.88) and 6.30 (95% CI: 2.86–13.85), respectively. However, literature related to risk of ovarian cancer and BRIP1 is odds ratios estimated from case-control studies, which are likely similar to relative risks given the rarity of this outcome in the general population: 8.13 (95% CI: 4.74-13.95) to 11.22 (95% CI: 3.22–34.10). (Tier 3)
3 4 5 9
Expressivity
There may be the presence of additive risk factors that may increase the risk of early onset ovarian cancer. (Tier 4)
4
4. What is the Nature of the Intervention?
Nature of Intervention
In women with BRCA1 and/or BRCA2 mutations who underwent an RRSO, 5% of women with a personal history of breast cancer expirenced a surgical complication. In a second study women with BRCA1 and/or BRCA2 mutations who underwent surgery at a mean age of 47 (47% with a personal history of breast cancer), most women reported worsening of vasomotor symptoms, and decreased sexual functioning after surgery. Guidelines state that the decision to carry out RRSO should not be made lightly, given the impact of premature menopause.
4 7
5. Would the underlying risk or condition escape detection prior to harm in the settting of recommended care?
Chance to Escape Clinical Detection
There are currently no ovarian cancer surveillance in the general population. Ovarian cancer is typically metastatic when diagnosed, thus RRSO is the only effective strategy to reduce the risk of dying from ovarian cancer. (Tier 1)
7 8
Description of sources of evidence:
Tier 1: Evidence from a systematic review, or a meta-analysis or clinical practice guideline clearly based on a systematic review.
Tier 2: Evidence from clinical practice guidelines or broad-based expert consensus with non-systematic evidence review.
Tier 3: Evidence from another source with non-systematic review of evidence with primary literature cited.
Tier 4: Evidence from another source with non-systematic review of evidence with no citations to primary data sources.
Tier 5: Evidence from a non-systematically identified source.

 
Gene Condition Associations
Gene
Condition Associations
OMIM Identifier
Primary MONDO Identifier
Additional MONDO Identifiers
Reference List
1. Sopik V, Akbari MR, Narod SA. Genetic testing for RAD51C mutations: in the clinic and community. Clin Genet. (2015) 88(4):303-12.
2. Norquist BM, Harrell MI, Brady MF, Walsh T, Lee MK, Gulsuner S, Bernards SS, Casadei S, Yi Q, Burger RA, Chan JK, Davidson SA, Mannel RS, DiSilvestro PA, Lankes HA, Ramirez NC, King MC, Swisher EM, Birrer MJ. Inherited Mutations in Women With Ovarian Carcinoma. JAMA Oncol. (2016) 2(4):482-90.
3. Online Medelian Inheritance in Man, OMIM®. Johns Hopkins University, Baltimore, MD. BREAST-OVARIAN CANCER, FAMILIAL, SUSCEPTIBILITY TO, 3; BROVCA3. MIM: 613399: 2012 May 16. World Wide Web URL: http://omim.org.
4. Daly MB, Pilarski R, Berry M, Buys SS, Farmer M, Friedman S, Garber JE, Kauff ND, Khan S, Klein C, Kohlmann W, Kurian A, Litton JK, Madlensky L, Merajver SD, Offit K, Pal T, Reiser G, Shannon KM, Swisher E, Vinayak S, Voian NC, Weitzel JN, Wick MJ, Wiesner GL, Dwyer M, Darlow S. NCCN Guidelines Insights: Genetic/Familial High-Risk Assessment: Breast and Ovarian, Version 2.2017. J Natl Compr Canc Netw. (2017) 15(1):9-20.
5. Online Medelian Inheritance in Man, OMIM®. Johns Hopkins University, Baltimore, MD. BREAST-OVARIAN CANCER, FAMILIAL, SUSCEPTIBILITY TO, 4; BROVCA4. MIM: 614291: 2011 Oct 17. World Wide Web URL: http://omim.org.
6. Scottish Intercollegiate Guidelines Network (SIGN). Management of epithelial ovarian cancer. A national clinical guideline. SIGN publication no. 135. (2013) Website: http://www.sign.ac.uk/assets/sign135.pdf
7. Moyer VA. Risk assessment, genetic counseling, and genetic testing for BRCA-related cancer in women: U.S. Preventive Services Task Force recommendation statement. Ann Intern Med. (2014) 160(4):271-81.
8. Nelson, H.D., Fu, R., Goddard, K., Mitchell, J.P., Okinaka-Hu, L., Pappas, M., Zakher, B. Risk Assessment, Genetic Couseling, And Genetic Testing for BRCA-Related Cancer: Systematic Review to Update the U.S. Preventive Servicies Task Force Recommendation. Evidence Synthesis Number 101. Report No.: AHRQ Publication No. 12-05164-EF-1. (2013) Website: https://www.ncbi.nlm.nih.gov/books/NBK179201/
9. Online Medelian Inheritance in Man, OMIM®. Johns Hopkins University, Baltimore, MD. RAD51, S. CEREVISIAE, HOMOLOG OF, C; RAD51C. MIM: 602774: 2013 Dec 04. World Wide Web URL: http://omim.org.
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