Zaorsky Nicholas G, Churilla Thomas M, Ruth Karen, Hayes Shelly B, Sobczak Mark L, Hallman Mark A, Smaldone Marc C, Chen David Yt, Horwitz Eric M
Department of Radiation Oncology,
Department of Radiation Oncology.
Am J Clin Nutr. 2016 Dec;104(6):1583-1593. doi: 10.3945/ajcn.115.119958. Epub 2016 Oct 26.
Approximately 50% of newly diagnosed cancer patients start taking dietary supplements. Men's health supplements (MHSs), which we define as supplements that are specifically marketed with the terms men's health and prostate health (or similar permutations), are often mislabeled as having potential anticancer benefits.
We evaluated the effects of MHSs on patient outcomes and toxicities in patients who were undergoing definitive intensity-modulated radiation therapy (IMRT) for localized prostate cancer.
This retrospective analysis included patients who were being treated at a National Cancer Institute-designated comprehensive cancer center and consented to have information stored in a prospective database. MHSs were queried online. Outcome measures were freedom from biochemical failure (FFBF) (biochemical failure was defined with the use of the prostate-specific antigen nadir + 2-ng/mL definition), freedom from distant metastasis (FFDM), cancer-specific survival (CSS), and overall survival (OS) as well as toxicities. Kaplan-Meier analysis, log-rank tests, Fine and Gray competing-risk regression (to adjust for patient and lifestyle factors), and Cox models were used.
From 2001 to 2012, 2207 patients were treated with IMRT with a median dose of 78 Gy, and a median follow-up of 46 mo. Of these patients, 43% were low risk, 37% were intermediate risk, and 20% were high risk; 10% used MHSs. MHSs contained a median of 3 identifiable ingredients (range: 0-78 ingredients). Patients who were taking an MHS compared with those who were not had improved 5-y OS (97% compared with 92%, respectively; P = 0.01), but there were no differences in the FFBF (94% compared with 89%, respectively; P = 0.12), FFDM (96% compared with 97%, respectively; P = 0.32), or CSS (100% compared with 99%, respectively; P = 0.22). The unadjusted association between MHS use and improved OS was attenuated after adjustment for patient lifestyle factors and comorbidities. There was no difference in toxicities between the 2 groups (late-grade 3-4 genitourinary <3%; gastrointestinal <4%).
The use of MHSs is not associated with outcomes or toxicities.
约50%新确诊的癌症患者开始服用膳食补充剂。男性健康补充剂(MHS),我们将其定义为专门以男性健康和前列腺健康(或类似表述)为营销术语的补充剂,常常被错误地标示为具有潜在抗癌益处。
我们评估了MHS对接受局限性前列腺癌根治性调强放疗(IMRT)患者的预后和毒性反应的影响。
这项回顾性分析纳入了在美国国立癌症研究所指定的综合癌症中心接受治疗且同意将信息存储在前瞻性数据库中的患者。通过在线查询MHS的使用情况。观察指标包括无生化失败生存(FFBF)(生化失败定义为前列腺特异性抗原最低点加2 ng/mL)、无远处转移生存(FFDM)、癌症特异性生存(CSS)和总生存(OS)以及毒性反应。采用Kaplan-Meier分析、对数秩检验、Fine和Gray竞争风险回归(以调整患者和生活方式因素)以及Cox模型。
2001年至2012年,2207例患者接受了IMRT治疗,中位剂量为78 Gy,中位随访时间为46个月。这些患者中,43%为低风险,37%为中风险,20%为高风险;10%使用MHS。MHS中可识别成分的中位数为3种(范围:0 - 78种成分)。与未使用MHS的患者相比,使用MHS的患者5年总生存率有所提高(分别为97%和92%;P = 0.01),但在FFBF(分别为94%和89%;P = 0.12)、FFDM(分别为96%和97%;P = 0.32)或CSS(分别为100%和99%;P = 0.22)方面无差异。在调整患者生活方式因素和合并症后,使用MHS与总生存率提高之间的未调整关联减弱。两组之间的毒性反应无差异(晚期3 - 4级泌尿生殖系统毒性反应<3%;胃肠道毒性反应<4%)。
使用MHS与预后或毒性反应无关。