Does Androgen-deprivation therapy accelerate the development of frailty in older men with prostate cancer? A conceptual review

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Abstract

The majority of men with prostate cancer are aged ≥65 years. Men, as they age, are more likely to suffer from impaired physical function. The standard treatment for recurrent prostate cancer is androgen-deprivation therapy (ADT). Well-established toxicities from ADT include lean weight loss or sarcopenia, muscle weakness, fatigue, and reduced activity levels. Frailty is a term from geriatrics that describes older individuals with limited physiologic reserve who are at significant risk for adverse outcomes, including falls, disability, hospitalization, and death. An increasingly accepted definition of frailty is a syndrome in which ≥3 of the following are present: unintentional (lean) weight loss ≥10 pounds in the past year, weakness (measured by grip strength), slow walking speed, self-reported exhaustion, and low physical activity. This clinical syndrome overlaps closely with the known toxicities of ADT. In addition, alterations in the inflammatory system, neuroendocrine system, and energy production are associated with this syndrome, as evidenced by biomarkers such as C-reactive protein, interleukin-6, and tumor necrosis factor-α. For this article, the authors reviewed the evidence for the effect of ADT on each of the 5 frailty components plus the identified biomarkers, and the evidence indicates that ADT may accelerate the development of frailty in vulnerable older men with prostate cancer. Given the association of frailty with important clinical outcomes such as hospitalization and death, this potential consequence of ADT should be considered carefully when initiating therapy in older patients with recurrent prostate cancer. © 2007 American Cancer Society.

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Bylow, K., Mohile, S. G., Stadler, W. M., & Dale, W. (2007, December 15). Does Androgen-deprivation therapy accelerate the development of frailty in older men with prostate cancer? A conceptual review. Cancer. https://doi.org/10.1002/cncr.23084

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