PROREPAIR-B: A Prospective Cohort Study of the Impact of Germline DNA Repair Mutations on the Outcomes of Patients With Metastatic Castration-Resistant Prostate Cancer

被引:307
作者
Castro, Elena [1 ,2 ]
Romero-Laorden, Nuria [1 ,3 ]
del Pozo, Angela [4 ,5 ]
Lozano, Rebeca [1 ,6 ]
Medina, Ana [7 ]
Puente, Javier [8 ]
Maria Piulats, Josep [9 ]
Lorente, David [10 ]
Isabel Saez, Maria [6 ,11 ]
Morales-Barrera, Rafael [12 ]
Gonzalez-Billalabeitia, Enrique [13 ]
Cendon, Ylenia [1 ,14 ]
Garcia-Carbonero, Iciar [15 ]
Borrega, Pablo [16 ]
Mendez Vidal, M. Jose [17 ]
Montesa, Alvaro [6 ,11 ]
Nombela, Paz [1 ]
Fernandez-Parra, Eva [18 ]
Gonzalez del Alba, Aranzazu [19 ]
Carlos Villa-Guzman, Jose [20 ]
Ibanez, Kristina [4 ,5 ]
Rodriguez-Vida, Alejo [21 ]
Magraner-Pardo, Lorena [1 ]
Perez-Valderrama, Begona [22 ]
Vallespin, Elena [4 ,5 ]
Gallardo, Enrique [23 ]
Vazquez, Sergio [24 ]
Pritchard, Colin C. [25 ]
Lapunzina, Pablo [4 ,5 ]
Olmos, David [1 ,6 ]
机构
[1] Spanish Natl Canc Res Ctr, Prostate Canc Clin Unit, Madrid, Spain
[2] Hosp Univ Quiron, Madrid, Spain
[3] Hosp Univ La Princesa, Madrid, Spain
[4] Hosp Univ La Paz, Inst Med & Mol Genet, Madrid, Spain
[5] CIBERER Inst Salud Carlos III, Madrid, Spain
[6] Inst Biomed Res Malaga, CNIO IBIMA Genitourinary Canc Res Unit, Malaga, Spain
[7] Ctr Oncol Galicia, Coruna, Spain
[8] Hosp Clin San Carlos, Inst Invest Sanitaria, Madrid, Spain
[9] Bellvitge Biomed Res Inst, Inst Catala Oncol, Barcelona, Spain
[10] Hosp Univ La Fe, Valencia, Spain
[11] Hosp Univ Virgen Victoria & Reg Malaga, Malaga, Spain
[12] Univ Autonoma Barcelona, Vail dHebron Univ Hosp, Vail dHebron Inst Oncol, Barcelona, Spain
[13] UCAM, Hosp Morales Messeguer IMIB, Murcia, Spain
[14] Univ Autonoma Madrid, Madrid, Spain
[15] Hosp Virgen Salud, Toledo, Spain
[16] Hosp San Pedro Alcantara, Caceres, Spain
[17] Hosp Univ Reina Sofia, Cordoba, Spain
[18] Hosp Univ Valme, Seville, Spain
[19] Hosp Univ Son Espases, Palma De Mallorca, Spain
[20] Hosp Gen Univ Ciudad Real, Ciudad Real, Spain
[21] Hosp del Mar, Barcelona, Spain
[22] Hosp Univ Virgen Rocio, Seville, Spain
[23] Univ Autonoma Barcelona, I3PT, Parc Tauli Hosp Univ, Sabadell, Spain
[24] Hosp Univ Lucus Augusti, Lugo, Spain
[25] Univ Washington, Med Ctr, Seattle, WA 98195 USA
关键词
CELL-FREE DNA; BRCA2; GENE; CHEMOTHERAPY; ASSOCIATION; VARIANTS; TUMOR; RISK; MEN;
D O I
10.1200/JCO.18.00358
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
PurposeGermline mutations in DNA damage repair (DDR) genes are identified in a significant proportion of patients with metastatic prostate cancer, but the clinical implications of these genes remain unclear. This prospective multicenter cohort study evaluated the prevalence and effect of germline DDR (gDDR) mutations on metastatic castration-resistance prostate cancer (mCRPC) outcomes.Patients and MethodsUnselected patients were enrolled at diagnosis of mCRPC and were screened for gDDR mutations in 107 genes. The primary aim was to assess the impact of ATM/BRCA1/BRCA2/PALB2 germline mutations on cause-specific survival (CSS) from diagnosis of mCRPC. Secondary aims included the association of gDDR subgroups with response outcomes for mCRPC treatments. Combined progression-free survival from the first systemic therapy (PFS) until progression on the second systemic therapy (PFS2) was also explored.ResultsWe identified 68 carriers (16.2%) of 419 eligible patients, including 14 with BRCA2, eight with ATM, four with BRCA1, and none with PALB2 mutations. The study did not reach its primary end point, because the difference in CSS between ATM/BRCA1/BRCA2/PALB2 carriers and noncarriers was not statistically significant (23.3 v 33.2 months; P = .264). CSS was halved in germline BRCA2 (gBRCA2) carriers (17.4 v 33.2 months; P = .027), and gBRCA2 mutations were identified as an independent prognostic factor for CCS (hazard ratio [HR], 2.11; P = .033). Significant interactions between gBRCA2 status and treatment type (androgen signaling inhibitor v taxane therapy) were observed (CSS adjusted P = .014; PFS2 adjusted P = .005). CSS (24.0 v 17.0 months) and PFS2 (18.9 v 8.6 months) were greater in gBRCA2 carriers treated in first line with abiraterone or enzalutamide compared with taxanes. Clinical outcomes did not differ by treatment type in noncarriers.ConclusiongBRCA2 mutations have a deleterious impact on mCRPC outcomes that may be affected by the first line of treatment used. Determination of gBRCA2 status may be of assistance for the selection of the initial treatment in mCRPC. Nonetheless, confirmatory studies are required before these results can support a change in clinical practice.
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收藏
页码:490 / +
页数:29
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