DNA repair gene alterations and PARP inhibitor response in patients with metastatic castration-resistant prostate cancer

Eric Lu; George V. Thomas; Yiyi Chen; Alexander W. Wyatt; Paul Lloyd; Jack Youngren; David Quigley; Raymond Bergan; Shawna Bailey; Tomasz M. Beer; Felix Y. Feng; Eric J. Small; Joshi J. Alumkal

doi:10.6004/jnccn.2018.7020

DNA repair gene alterations and PARP inhibitor response in patients with metastatic castration-resistant prostate cancer

Eric Lu, George V. Thomas, Yiyi Chen, Alexander W. Wyatt, Paul Lloyd, Jack Youngren, David Quigley, Raymond Bergan, Shawna Bailey, Tomasz M. Beer, Felix Y. Feng, Eric J. Small, Joshi J. Alumkal

Research output: Contribution to journal › Article › peer-review

7 Scopus citations

Abstract

Background: PARP inhibition is a promising therapeutic strategy for the treatment of men with metastatic castration-resistant prostate cancer whose tumors harbor homologous recombination DNA repair gene alterations. However, questions remain for many practicing clinicians about which patients are ideally suited for PARP inhibitor treatment. This report details our institutional experience using PARP inhibitor therapy in patients whose tumors harbored specific DNA repair gene alterations. Patients and Methods: We performed a retrospective chart review to identify patients at Oregon Health & Science University who were treated with PARP inhibition. We identified 8 patients and determined the impact of the specific DNA repair gene alterations on tumor response and time on treatment with PARP inhibition. Results: A number of DNA repair gene alterations were identified. Three patients had pathogenic BRCA2 mutations and one had a BRCA2 mutation of uncertain significance. Conversely, the 4 other patients' tumors harbored alterations in other DNA repair genes, none of which were clearly pathogenic. A statistically significant difference in benefit was seen between patients whose tumors harbored BRCA2 gene alterations and those whose tumors did not, as measured by >50% decline in prostate-specific antigen levels (100% vs 0%; P=.03) and duration on therapy (31.4 vs 6.4 weeks; P=.03). Conclusions: Our results demonstrate that not all DNA repair alterations are equally predictive of PARP inhibitor response. Importantly, all responding patients had tumors harboring BRCA2 DNA repair alterations, including one without a known pathogenic mutation. Conversely, among the 4 nonresponders, several DNA repair alterations in genes other than BRCA2 were identified that were not clearly pathogenic. This demonstrates the need to carefully examine the functional relevance of the DNA repair alterations identified, especially in genes other than BRCA2, when considering patients for PARP inhibitor treatment.

Original language	English (US)
Pages (from-to)	933-937
Number of pages	5
Journal	JNCCN Journal of the National Comprehensive Cancer Network
Volume	16
Issue number	8
DOIs	https://doi.org/10.6004/jnccn.2018.7020
State	Published - Aug 1 2018

ASJC Scopus subject areas

Oncology

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Lu, E., Thomas, G. V., Chen, Y., Wyatt, A. W., Lloyd, P., Youngren, J., Quigley, D., Bergan, R., Bailey, S., Beer, T. M., Feng, F. Y., Small, E. J., & Alumkal, J. J. (2018). DNA repair gene alterations and PARP inhibitor response in patients with metastatic castration-resistant prostate cancer. JNCCN Journal of the National Comprehensive Cancer Network, 16(8), 933-937. https://doi.org/10.6004/jnccn.2018.7020

Lu, E, Thomas, GV, Chen, Y, Wyatt, AW, Lloyd, P, Youngren, J, Quigley, D, Bergan, R, Bailey, S, Beer, TM, Feng, FY, Small, EJ & Alumkal, JJ 2018, 'DNA repair gene alterations and PARP inhibitor response in patients with metastatic castration-resistant prostate cancer', JNCCN Journal of the National Comprehensive Cancer Network, vol. 16, no. 8, pp. 933-937. https://doi.org/10.6004/jnccn.2018.7020

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title = "DNA repair gene alterations and PARP inhibitor response in patients with metastatic castration-resistant prostate cancer",

abstract = "Background: PARP inhibition is a promising therapeutic strategy for the treatment of men with metastatic castration-resistant prostate cancer whose tumors harbor homologous recombination DNA repair gene alterations. However, questions remain for many practicing clinicians about which patients are ideally suited for PARP inhibitor treatment. This report details our institutional experience using PARP inhibitor therapy in patients whose tumors harbored specific DNA repair gene alterations. Patients and Methods: We performed a retrospective chart review to identify patients at Oregon Health & Science University who were treated with PARP inhibition. We identified 8 patients and determined the impact of the specific DNA repair gene alterations on tumor response and time on treatment with PARP inhibition. Results: A number of DNA repair gene alterations were identified. Three patients had pathogenic BRCA2 mutations and one had a BRCA2 mutation of uncertain significance. Conversely, the 4 other patients' tumors harbored alterations in other DNA repair genes, none of which were clearly pathogenic. A statistically significant difference in benefit was seen between patients whose tumors harbored BRCA2 gene alterations and those whose tumors did not, as measured by >50% decline in prostate-specific antigen levels (100% vs 0%; P=.03) and duration on therapy (31.4 vs 6.4 weeks; P=.03). Conclusions: Our results demonstrate that not all DNA repair alterations are equally predictive of PARP inhibitor response. Importantly, all responding patients had tumors harboring BRCA2 DNA repair alterations, including one without a known pathogenic mutation. Conversely, among the 4 nonresponders, several DNA repair alterations in genes other than BRCA2 were identified that were not clearly pathogenic. This demonstrates the need to carefully examine the functional relevance of the DNA repair alterations identified, especially in genes other than BRCA2, when considering patients for PARP inhibitor treatment.",

author = "Eric Lu and Thomas, {George V.} and Yiyi Chen and Wyatt, {Alexander W.} and Paul Lloyd and Jack Youngren and David Quigley and Raymond Bergan and Shawna Bailey and Beer, {Tomasz M.} and Feng, {Felix Y.} and Small, {Eric J.} and Alumkal, {Joshi J.}",

note = "Publisher Copyright: {\textcopyright} 2018 JNCCN-Journal of the National Comprehensive Cancer Network.",

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doi = "10.6004/jnccn.2018.7020",

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T1 - DNA repair gene alterations and PARP inhibitor response in patients with metastatic castration-resistant prostate cancer

AU - Lu, Eric

AU - Thomas, George V.

AU - Chen, Yiyi

AU - Wyatt, Alexander W.

AU - Lloyd, Paul

AU - Youngren, Jack

AU - Quigley, David

AU - Bergan, Raymond

AU - Bailey, Shawna

AU - Beer, Tomasz M.

AU - Feng, Felix Y.

AU - Small, Eric J.

AU - Alumkal, Joshi J.

PY - 2018/8/1

Y1 - 2018/8/1

N2 - Background: PARP inhibition is a promising therapeutic strategy for the treatment of men with metastatic castration-resistant prostate cancer whose tumors harbor homologous recombination DNA repair gene alterations. However, questions remain for many practicing clinicians about which patients are ideally suited for PARP inhibitor treatment. This report details our institutional experience using PARP inhibitor therapy in patients whose tumors harbored specific DNA repair gene alterations. Patients and Methods: We performed a retrospective chart review to identify patients at Oregon Health & Science University who were treated with PARP inhibition. We identified 8 patients and determined the impact of the specific DNA repair gene alterations on tumor response and time on treatment with PARP inhibition. Results: A number of DNA repair gene alterations were identified. Three patients had pathogenic BRCA2 mutations and one had a BRCA2 mutation of uncertain significance. Conversely, the 4 other patients' tumors harbored alterations in other DNA repair genes, none of which were clearly pathogenic. A statistically significant difference in benefit was seen between patients whose tumors harbored BRCA2 gene alterations and those whose tumors did not, as measured by >50% decline in prostate-specific antigen levels (100% vs 0%; P=.03) and duration on therapy (31.4 vs 6.4 weeks; P=.03). Conclusions: Our results demonstrate that not all DNA repair alterations are equally predictive of PARP inhibitor response. Importantly, all responding patients had tumors harboring BRCA2 DNA repair alterations, including one without a known pathogenic mutation. Conversely, among the 4 nonresponders, several DNA repair alterations in genes other than BRCA2 were identified that were not clearly pathogenic. This demonstrates the need to carefully examine the functional relevance of the DNA repair alterations identified, especially in genes other than BRCA2, when considering patients for PARP inhibitor treatment.

AB - Background: PARP inhibition is a promising therapeutic strategy for the treatment of men with metastatic castration-resistant prostate cancer whose tumors harbor homologous recombination DNA repair gene alterations. However, questions remain for many practicing clinicians about which patients are ideally suited for PARP inhibitor treatment. This report details our institutional experience using PARP inhibitor therapy in patients whose tumors harbored specific DNA repair gene alterations. Patients and Methods: We performed a retrospective chart review to identify patients at Oregon Health & Science University who were treated with PARP inhibition. We identified 8 patients and determined the impact of the specific DNA repair gene alterations on tumor response and time on treatment with PARP inhibition. Results: A number of DNA repair gene alterations were identified. Three patients had pathogenic BRCA2 mutations and one had a BRCA2 mutation of uncertain significance. Conversely, the 4 other patients' tumors harbored alterations in other DNA repair genes, none of which were clearly pathogenic. A statistically significant difference in benefit was seen between patients whose tumors harbored BRCA2 gene alterations and those whose tumors did not, as measured by >50% decline in prostate-specific antigen levels (100% vs 0%; P=.03) and duration on therapy (31.4 vs 6.4 weeks; P=.03). Conclusions: Our results demonstrate that not all DNA repair alterations are equally predictive of PARP inhibitor response. Importantly, all responding patients had tumors harboring BRCA2 DNA repair alterations, including one without a known pathogenic mutation. Conversely, among the 4 nonresponders, several DNA repair alterations in genes other than BRCA2 were identified that were not clearly pathogenic. This demonstrates the need to carefully examine the functional relevance of the DNA repair alterations identified, especially in genes other than BRCA2, when considering patients for PARP inhibitor treatment.

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DNA repair gene alterations and PARP inhibitor response in patients with metastatic castration-resistant prostate cancer

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