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Home NEWS Science News Cancer

UCLA Study Finds Hormone Therapy Often Ineffective for Men Undergoing Radiotherapy Post-Prostate Surgery

Bioengineer by Bioengineer
February 26, 2026
in Cancer
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A groundbreaking study led by researchers at UCLA Health Jonsson Comprehensive Cancer Center brings new clarity to the role of hormone therapy when combined with post-operative radiotherapy in men diagnosed with prostate cancer. Prostate cancer, one of the most common malignancies among men worldwide, often requires a multifaceted treatment approach. This study, published recently in the prestigious journal The Lancet, meticulously dissects the survival benefits and potential detriments of adding hormonal interventions to standard radiotherapy after prostatectomy, particularly focusing on the significance of PSA (prostate-specific antigen) levels prior to radiation treatment.

Hormone therapy, also known as androgen deprivation therapy (ADT), has traditionally been used to suppress testosterone’s influence, as testosterone is a key driver of prostate cancer cell growth. While previous clinical trials have affirmed hormone therapy’s benefit in men with intact prostates undergoing radiotherapy, the efficacy of this approach in the post-surgical setting has remained inconclusive until now. The UCLA-led investigation specifically delves into this uncertainty by analyzing data from over 6,000 men across six randomized controlled trials, employing a sophisticated individual patient data meta-analysis methodology through the MARCAP Consortium.

The researchers meticulously stratified patients based on their PSA levels measured immediately before radiotherapy initiation following prostatectomy. Their detailed analyses reveal that men exhibiting low PSA levels (≤0.5 ng/mL) before radiation treatment do not derive any appreciable overall survival advantage from the addition of hormone therapy, regardless of whether it is administered short-term or long-term. This finding challenges previously held assumptions and highlights the potent efficacy of radiotherapy alone in controlling microscopic residual disease in low-PSA patients, suggesting a potential pause in prescribing hormone therapy in this subgroup.

Conversely, men with elevated PSA levels prior to commencing radiotherapy seem to benefit moderately from hormone therapy. For these higher-risk individuals, hormone treatment not only extends overall survival but also reduces the likelihood of metastatic disease, a critical factor impacting quality of life and long-term prognosis. These insights carve a pathway toward more personalized prostate cancer treatment protocols, ensuring that hormone therapy is reserved primarily for those patients who stand to gain the most while sparing others from unnecessary side effects.

One of the study’s strengths lies in its nuanced examination of hormone therapy duration. The investigation assessed short-term treatment lasting between four and six months alongside long-term administration spanning up to two years. Interestingly, short-term hormone therapy, while not significantly improving overall survival, did marginally decrease metastatic risk. Long-term therapy offered a slight survival benefit for patients with higher PSA pre-radiotherapy but was not conclusively superior to short-term therapy in improving mortality outcomes. This crucial distinction may influence clinical decisions regarding the length of hormone therapy required to optimize patient outcomes, balancing efficacy with quality of life considerations.

The team’s extensive follow-up period averaging nine years provided robust data for evaluating long-term effects, allowing for a comprehensive understanding of survival, recurrence, and metastasis trends over time. Such prolonged observation underscores the rigor and depth of the research, offering a rare window into the enduring impacts of combining hormone therapy with radiotherapy after prostatectomy. This long-term perspective is essential for guiding treatment paradigms in prostate cancer, a disease characterized by variable and often protracted clinical courses.

Importantly, the research underscores the significant side-effect burden associated with hormone therapy, which includes debilitating fatigue, hot flashes, sexual dysfunction, weight gain, and metabolic derangements that elevate cardiovascular risk. These adverse effects can profoundly diminish a patient’s quality of life, reinforcing the imperative to precisely identify those who truly benefit from hormone therapy. The findings advocate for a careful risk-benefit assessment, steering away from blanket hormone therapy use toward more judicious, personalized care strategies.

Dr. Amar Kishan, the study’s lead author and a radiation oncology expert at UCLA’s David Geffen School of Medicine, emphasized the transformative potential of these findings. He highlighted that precise patient stratification based on PSA levels prior to radiation could serve as a pivotal biomarker in clinical decision-making, allowing physicians to spare men with low PSA from unnecessary and potentially harmful treatments. This approach aligns with the broader trend in oncology toward de-escalation of therapy where appropriate, minimizing harm without compromising efficacy.

The researchers utilized a meta-analytic approach that pooled individual patient data across multiple randomized controlled trials, an advanced technique that enhances statistical power and granularity beyond conventional meta-analyses relying on published summary results. This method allowed for more detailed subgroup analyses, providing high-resolution insights into which patients benefit from hormone therapy and under which clinical circumstances. International collaboration through the MARCAP Consortium was integral to this success, exemplifying the value of cooperative data sharing in advancing cancer research.

Ongoing investigations seek to build on these results by integrating molecular and genetic biomarkers to further refine patient selection for hormone therapy post-prostatectomy. Trials such as the BALANCE Trial aim to unravel the biological underpinnings determining hormone therapy responsiveness, promising even more tailored treatment strategies in the future. Such advancements could revolutionize the management of prostate cancer by combining clinical indicators like PSA with molecular signatures to maximize treatment efficacy while safeguarding patient quality of life.

This pioneering study marks a significant step forward in prostate cancer treatment, encouraging clinicians to reconsider the routine use of hormone therapy in all post-operative radiotherapy cases. By identifying which subsets of patients truly benefit, it is possible to enhance survival outcomes selectively, reduce unnecessary toxicity, and pave the way for personalized medicine in urologic oncology. As further research refines these findings, patients and providers alike may anticipate smarter, less burdensome treatment paradigms that optimize both longevity and well-being.

In summary, the evidence emerging from this meta-analysis robustly supports the notion that hormone therapy should not be indiscriminately combined with post-operative radiotherapy, particularly in men with low PSA levels where radiotherapy alone suffices. For those with higher PSA levels, hormone therapy remains a valuable adjunct, although the optimal duration continues to be an open question. These insights hold promise for reshaping clinical guidelines, highlighting the centrality of PSA stratification in therapeutic decision-making and exemplifying the ongoing evolution toward precision oncology.

Subject of Research: Prostate cancer treatment optimization following prostatectomy
Article Title: Hormone Therapy Addition to Post-Prostatectomy Radiotherapy Provides Limited Survival Benefit Except for High PSA Patients
News Publication Date: 2024
Web References:

The Lancet Article
BALANCE Trial
References: Published study in The Lancet, MARCAP Consortium clinical trial data
Keywords: Prostate cancer, hormone therapy, androgen deprivation therapy, radiotherapy, PSA levels, post-operative treatment, metastasis-free survival, personalized oncology, cancer treatment side effects, randomized controlled trials, meta-analysis, BALANCE trial

Tags: androgen deprivation therapy in prostate cancerhormone therapy effectiveness post-prostatectomyhormone therapy limitations after prostatectomyMARCAP Consortium meta-analysispost-operative prostate cancer treatment outcomesprostate-specific antigen role in treatmentPSA levels impact on cancer treatmentradiotherapy after prostate surgeryrandomized controlled trials prostate cancersurvival benefits hormone therapy radiotherapytestosterone suppression in cancer therapyUCLA prostate cancer research

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