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Should Early Use of Chemotherapy Be Avoided in the Treatment of Metastatic Prostate Cancer?

pjoshea13 profile image
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Interesting editorial in JMA [Japan Medical Association] Journal:

"The therapeutic strategy for advanced prostate cancer has dramatically changed recently. Previously, docetaxel was the only drug with evidences showing improved overall survival (OS) in metastatic castration-resistant prostate cancer (CRPC). However, androgen receptor pathway inhibitors (ARPI), such as abiraterone acetate and enzalutamide, cabazitaxel, radium-223, and olaparib, have emerged since the 2010s. In addition, early use of docetaxel or ARPIs with androgen deprivation therapy for castration-sensitive prostate cancer has also shown significant survival benefit over the last several years. Under certain circumstances, appropriate sequence of the drugs has been one of the important clinical questions in this field.

"Matsumoto et al retrospectively compared the efficacy of second-line ARPI, docetaxel, and radium-223 in patients with CRPC who received ARPI as first-line treatment. The results indicated that docetaxel showed significantly better progression-free survival (PFS) than second-line ARPI and radium-223, and OS was not different among them (1). The results of this study were consistent with those of previous retrospective studies (2), (3). The cause of the difference in efficacy between drugs as second-line treatment is thought to be cross-resistance among ARPIs, which was reported in several prospective and retrospective studies in metastatic CRPC. In the prospective randomized crossover trial to assess the optimal sequencing of enzalutamide and abiraterone acetate, time to prostate-specific antigen (PSA) progression of second-line enzalutamide and abiraterone acetate was 3.5 and 1.7 months (4), respectively, which was consistent with the results of Matsumoto’s study; median PFS of second-line ARPI was 2.8 months.

"Another interesting finding of Matsumoto’s study was that PFS of second-line docetaxel was significantly better than that of second-line ARPI even in the subgroup with maximum PSA response of first-line ARPI > 50%. Generally, docetaxel is recommended as second-line treatment after progression of first-line ARPI. However, second-line ARPI is thought to be effective in patients who show a good response to first-line ARPI. Nevertheless, the results of this study revealed that the efficacy of second-line ARPI was limited even in good responders of first-line ARPI. Therefore, using drugs with a different mechanism of action in appropriate timing is an important treatment strategy for metastatic CRPC.

"According to the evidences so far, including this study, docetaxel should be recommended as second-line treatment for metastatic CRPC patients who received first-line ARPI. However, docetaxel is selected as second-line treatment only for limited patients in real-world clinical practice. In a retrospective study of the Veterans Health Administration database, including 3,174 metastatic CRPC patients treated with first-line ARPI from 2014 to 2018, 1229 and 1945 patients were treated with enzalutamide and abiraterone acetate, respectively. Among then, 45% and 54% of patients were received second-line therapy during the observation period, but only 6% and 9% were administrated docetaxel, whereas 23% and 26% were administrated second-line ARPI, respectively (5). Prostate cancer is relatively slow growing even when in the metastatic state. In addition, both ARPI and chemotherapy are similarly effective. On the other hand, chemotherapy is more toxic than ARPI due to severe adverse events, such as neutropenia, febrile neutropenia, alopecia, and neuropathy. Thus, patients tend to prefer ARPIs than chemotherapy. However, the efficacy of second-line ARPI is limited and most of the patients need to change the treatment a couple of months later. In addition, patients might lose the chance to receive chemotherapy due to progression of the disease in later-line treatment sequences. Clinicians must explain the fact and prospect of the treatment strategy to patients during the early phase of treatment.

"Several clinical trials of new drugs for metastatic CRPC with different modes of action are ongoing. Under such circumstances, we must provide an appropriate therapeutic strategy based on the evidences. In addition, further studies are required to assess whether the current evidences of CRPC can be adapted to CRPC after combined treatment of ARPI and androgen deprivation therapy for metastatic castration-sensitive prostate cancer."

-Patrick

[1] jmaj.jp/detail.php?id=10.31...

JMA Journal

Editorial

Should Early Use of Chemotherapy Be Avoided in the Treatment of Metastatic Prostate Cancer?

Takahiro Kimura

Author affiliations

Corresponding author: Takahiro Kimura, tkimura@jikei.ac.jp

DOI: 10.31662/jmaj.2021-0207

Received: November 9, 2021

Accepted: November 11, 2021

Advance Publication: December 24, 2021

Published: January 17, 2022

Cite this article as:

Kimura T. Should Early Use of Chemotherapy Be Avoided in the Treatment of Metastatic Prostate Cancer?. JMA J. 2022;5(1):91-92.

Key words: prostate cancer, castration-resistant, docetaxel

The therapeutic strategy for advanced prostate cancer has dramatically changed recently. Previously, docetaxel was the only drug with evidences showing improved overall survival (OS) in metastatic castration-resistant prostate cancer (CRPC). However, androgen receptor pathway inhibitors (ARPI), such as abiraterone acetate and enzalutamide, cabazitaxel, radium-223, and olaparib, have emerged since the 2010s. In addition, early use of docetaxel or ARPIs with androgen deprivation therapy for castration-sensitive prostate cancer has also shown significant survival benefit over the last several years. Under certain circumstances, appropriate sequence of the drugs has been one of the important clinical questions in this field.

Matsumoto et al retrospectively compared the efficacy of second-line ARPI, docetaxel, and radium-223 in patients with CRPC who received ARPI as first-line treatment. The results indicated that docetaxel showed significantly better progression-free survival (PFS) than second-line ARPI and radium-223, and OS was not different among them (1). The results of this study were consistent with those of previous retrospective studies (2), (3). The cause of the difference in efficacy between drugs as second-line treatment is thought to be cross-resistance among ARPIs, which was reported in several prospective and retrospective studies in metastatic CRPC. In the prospective randomized crossover trial to assess the optimal sequencing of enzalutamide and abiraterone acetate, time to prostate-specific antigen (PSA) progression of second-line enzalutamide and abiraterone acetate was 3.5 and 1.7 months (4), respectively, which was consistent with the results of Matsumoto’s study; median PFS of second-line ARPI was 2.8 months.

Another interesting finding of Matsumoto’s study was that PFS of second-line docetaxel was significantly better than that of second-line ARPI even in the subgroup with maximum PSA response of first-line ARPI > 50%. Generally, docetaxel is recommended as second-line treatment after progression of first-line ARPI. However, second-line ARPI is thought to be effective in patients who show a good response to first-line ARPI. Nevertheless, the results of this study revealed that the efficacy of second-line ARPI was limited even in good responders of first-line ARPI. Therefore, using drugs with a different mechanism of action in appropriate timing is an important treatment strategy for metastatic CRPC.

According to the evidences so far, including this study, docetaxel should be recommended as second-line treatment for metastatic CRPC patients who received first-line ARPI. However, docetaxel is selected as second-line treatment only for limited patients in real-world clinical practice. In a retrospective study of the Veterans Health Administration database, including 3,174 metastatic CRPC patients treated with first-line ARPI from 2014 to 2018, 1229 and 1945 patients were treated with enzalutamide and abiraterone acetate, respectively. Among then, 45% and 54% of patients were received second-line therapy during the observation period, but only 6% and 9% were administrated docetaxel, whereas 23% and 26% were administrated second-line ARPI, respectively (5). Prostate cancer is relatively slow growing even when in the metastatic state. In addition, both ARPI and chemotherapy are similarly effective. On the other hand, chemotherapy is more toxic than ARPI due to severe adverse events, such as neutropenia, febrile neutropenia, alopecia, and neuropathy. Thus, patients tend to prefer ARPIs than chemotherapy. However, the efficacy of second-line ARPI is limited and most of the patients need to change the treatment a couple of months later. In addition, patients might lose the chance to receive chemotherapy due to progression of the disease in later-line treatment sequences. Clinicians must explain the fact and prospect of the treatment strategy to patients during the early phase of treatment.

Several clinical trials of new drugs for metastatic CRPC with different modes of action are ongoing. Under such circumstances, we must provide an appropriate therapeutic strategy based on the evidences. In addition, further studies are required to assess whether the current evidences of CRPC can be adapted to CRPC after combined treatment of ARPI and androgen deprivation therapy for metastatic castration-sensitive prostate cancer.

Article Information

Conflicts of Interest

Takahiro Kimura is a paid consultant/advisor of Astellas, Bayer, Janssen, and Sanofi.

Author Contributions

TK wrote this manuscript.

Approval by Institutional Review Board (IRB)

NA

References

1.

Matsumoto T, Shiota M, Yamada S, et al. Anticancer effect of second-line treatment for castration-resistant prostate cancer following first-line treatment with androgen receptor pathway inhibitors. JMA J. 2022;5(1):83-90.

View Article

2.

Miyake H, Sugiyama T, Aki R, et al. Comparison of alternative androgen receptor-axis-targeted agent (ARATA) and docetaxel as second-line therapy for patients with metastatic castration-resistant prostate cancer with progression after initial ARATA in real-world clinical practice in Japan. Clin Genitourin Cancer. 2018;16(3):219-25.

View Article PubMed

3.

Matsubara N, Yamada Y, Tabata K-I, et al. Comparison of sequential treatment with androgen receptor-targeted agent followed by another androgen receptor-targeted agent versus androgen receptor-targeted agent followed by docetaxel in chemotherapy-naive patients with metastatic castration-resistant prostate cancer. Clin Genitourin Cancer. 2017;15(6):e1073-80.

View Article PubMed

4.

Khalaf DJ, Annala M, Taavitsainen S, et al. Optimal sequencing of enzalutamide and abiraterone acetate plus prednisone in metastatic castration-resistant prostate cancer: a multicentre, randomised, open-label, phase 2, crossover trial. Lancet Oncol. 2019;20(12):1730-9.

View Article PubMed

5.

Tagawa ST, Ramaswamy K, Huang A, et al. Survival outcomes in patients with chemotherapy-naive metastatic castration-resistant prostate cancer treated with enzalutamide or abiraterone acetate. Prostate Cancer Prostatic Dis. Forthcoming 2021.

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5 Replies

"Should Early Use of Chemotherapy Be Avoided in the Treatment of Metastatic Prostate Cancer?"

IMO, not until phase 3 trials prove otherwise. So far in the US, we have CHAARTED and STAMPEDE in the UK that proved a survival advantage. PEACE 1 confirmed the 4.1 year overall survival shown in CHAARTED.

The latest science shows that not only is Docetaxel beneficial when used early, but adding Abiraterone plus Docetaxel to ADT further increases the benefit.

I think dropping a Docetaxel bomb ASAP is the way to start the show. Saved my miserable life.

Brysonal profile image
Brysonal in reply to

Thanks for sharing. I am about to drop 3 x Docetaxel bombs on my hormone sensitive metastatic cancer so hope it’s the right thing.Currently been on Degarelix since 25th November 2021 when PSA was 17.6 and multiple mets to the spine started Lu-177 on 10th December and 18 days after third Lu-177 my PSA was 0.46 today.

Bloods got signed off today to drop the first Docetaxel bomb on 7th March. Not looking forward of course as side effects of treatment to date very low but 3 lots better than a full course.

Discussion on which advanced hormone therapy to add in continue but neither MO seems in a rush for me to start immediately though it’s meant to be part of my slightly none standard ‘triplet’ of:

Degarelix

3x Lu-177 plus 3 x Docetaxel

Advanced HT - type to be agreed

I hope early Docetaxel is the way to go!

Schwah profile image
Schwah

That study seems absurd given the latest clinical trial showing early chemo extends life….a lot.

Schwah

leebeth profile image
leebeth

I am no expert at reading trials, but to me the conclusion seems erroneous. The data cited definitely support not going from one “ARPI” to another without a course of docetaxel in between. This opinion piece is based on retrospective trials, unlike well designed RCTs like PEACE-1 and ARASENS which clearly show the value of early triplet therapy.

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