The University of Melbourne, Melbourne, VIC.
Parkville Familial Cancer Centre, Peter MacCallum Cancer Centre and Royal Melbourne Hospital, Melbourne, VIC.
Med J Aust. 2023 May 1;218(8):368-373. doi: 10.5694/mja2.51906. Epub 2023 Apr 2.
To determine the feasibility of universal genetic testing of women with newly diagnosed breast cancer, to estimate the incidence of pathogenic gene variants and their impact on patient management, and to evaluate patient and clinician acceptance of universal testing.
DESIGN, SETTING, PARTICIPANTS: Prospective study of women with invasive or high grade in situ breast cancer and unknown germline status discussed at the Parkville Breast Service (Melbourne) multidisciplinary team meeting. Women were recruited to the pilot (12 June 2020 - 22 March 2021) and expansion phases (17 October 2021 - 8 November 2022) of the Mutational Assessment of newly diagnosed breast cancer using Germline and tumour genomICs (MAGIC) study.
Germline testing by DNA sequencing, filtered for nineteen hereditary breast and ovarian cancer genes that could be classified as actionable; only pathogenic variants were reported. Surveys before and after genetic testing assessed pilot phase participants' perceptions of genetic testing, and psychological distress and cancer-specific worry. A separate survey assessed clinicians' views on universal testing.
Pathogenic germline variants were identified in 31 of 474 expanded study phase participants (6.5%), including 28 of 429 women with invasive breast cancer (6.5%). Eighteen of the 31 did not meet current genetic testing eligibility guidelines (probability of a germline pathogenic variant ≥ 10%, based on CanRisk, or Manchester score ≥ 15). Clinical management was changed for 24 of 31 women after identification of a pathogenic variant. Including 68 further women who underwent genetic testing outside the study, 44 of 542 women carried pathogenic variants (8.1%). Acceptance of universal testing was high among both patients (90 of 103, 87%) and clinicians; no decision regret or adverse impact on psychological distress or cancer-specific worry were reported.
Universal genetic testing following the diagnosis of breast cancer detects clinically significant germline pathogenic variants that might otherwise be missed because of testing guidelines. Routine testing and reporting of pathogenic variants is feasible and acceptable for both patients and clinicians.
确定对新诊断乳腺癌女性进行普遍基因检测的可行性,估计致病基因突变的发生率及其对患者管理的影响,并评估患者和临床医生对普遍检测的接受程度。
设计、地点和参与者:对在帕克维尔乳房服务中心(墨尔本)多学科团队会议上讨论的患有浸润性或高级别原位乳腺癌且种系状态未知的女性进行前瞻性研究。招募女性参加 Mutational Assessment of newly diagnosed breast cancer using Germline and tumour genomICs(MAGIC)研究的试点(2020 年 6 月 12 日至 2021 年 3 月 22 日)和扩展阶段(2021 年 10 月 17 日至 2022 年 11 月 8 日)。
通过 DNA 测序进行种系检测,筛选出 19 种可归类为可操作的遗传性乳腺癌和卵巢癌基因的致病变体;仅报告致病性变体。基因检测前后的调查评估了试点阶段参与者对基因检测的看法,以及心理困扰和癌症特异性担忧。一项单独的调查评估了临床医生对普遍检测的看法。
在扩展研究阶段的 474 名参与者中,有 31 名(6.5%)发现了致病性种系变体,其中 429 名患有浸润性乳腺癌的女性中有 28 名(6.5%)。18 名女性不符合当前基因检测的合格标准(基于 CanRisk 或曼彻斯特评分≥15%,种系致病性变异的概率≥10%)。在确定致病性变体后,31 名女性中的 24 名改变了临床管理。包括 68 名在研究之外接受基因检测的女性,542 名女性中有 44 名携带致病性变体(8.1%)。患者(103 名中的 90 名,87%)和临床医生都对普遍检测的接受度很高;没有决策后悔或对心理困扰或癌症特异性担忧产生不利影响的报告。
在诊断乳腺癌后进行普遍的基因检测可以检测到临床上有意义的种系致病性变体,如果不根据检测指南进行检测,这些变体可能会被遗漏。对患者和临床医生来说,常规检测和报告致病性变体是可行且可接受的。
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