一种针对日本初诊骨转移激素初治前列腺癌患者的新型预后模型。
A novel prognostic model for Japanese patients with newly diagnosed bone-metastatic hormone-naïve prostate cancer.
作者信息
Miyoshi Yasuhide, Yasui Masato, Yoneyama Shuko, Kawahara Takashi, Nakagami Yoshihiro, Ohno Yoshimasa, Iizuka Junpei, Tanabe Kazunari, Hashimoto Yasunobu, Tsumura Hideyasu, Tabata Ken-Ichi, Iwamura Masatsugu, Yano Akihiro, Kawakami Satoru, Uemura Hiroji
机构信息
Department of Urology and Renal Transplantation Yokohama City University Medical Center Yokohama Japan.
Department of Urology Tokyo Medical University Tokyo Japan.
出版信息
BJUI Compass. 2020 Sep 18;2(2):105-114. doi: 10.1002/bco2.46. eCollection 2021 Mar.
OBJECTIVES
To evaluate the prognosis of newly diagnosed patients with metastatic hormone-naïve prostate cancer (mHNPC) and develop a novel prognostic model based on ChemoHormonal Therapy Versus Androgen Ablation Randomized Trial for Extensive Disease in Prostate Cancer (CHAARTED) risk classifications.
PATIENTS AND METHODS
We retrospectively analyzed the data of 578 newly diagnosed mHNPC patients initially treated with androgen deprivation therapy. We evaluated three clinical factors, namely, CHAARTED risk classifications (high-volume disease [HVD] vs low-volume disease [LVD]), Gleason scores (GS, 9-10 vs ≤8), and hemoglobin (Hb, ≤13.0 g/dL vs >13.0 g/dL), for their prognostic potential in predicting time to castration-resistant prostate cancer (TTC) and overall survival (OS) of mHNPC patients by multivariate analysis. Moreover, we developed a novel prognostic model that consisted of significant prognostic factors.
RESULTS
Of the entire cohort, the median TTC and OS values were 18.3 and 67.5 months, respectively. HVD, GS 9-10, and Hb ≤13.0 g/dL were independent poor prognostic factors for both TTC and OS. We developed a novel prognostic model which could stratify mHNPC patients into four risk groups according to the numbers of poor prognostic factors: group 1, LVD with low-risk (LVD patients without GS 9-10 and Hb ≤13.0 g/dL); group 2, LVD with high-risk (LVD patients with GS 9-10, Hb ≤13.0 g/dL, or both); group 3, HVD with low-risk (HVD patients without GS 9-10 with or without Hb ≤13.0 g/dL); and group 4, HVD with high-risk (HVD patients with GS 9-10 with or without Hb ≤13.0 g/dL). The median TTC and OS of groups 1, 2, 3, and 4 were 124.8, 36.4, 17.9, and 11.2 months, and 117.2, 94.2, 67.9, and 46.2 months, respectively. A significant difference in TCC and OS was found between all groups.
CONCLUSION
We developed a prognostic model for mHNPC patients that consisted of CHAARTED risk classifications, GS, and Hb. Our prognostic model could significantly stratify the prognosis of patients with LVD and HVD into two groups each. This model might be a good reference for shared decision making between patients and physicians on the initial treatment for mHNPC.
目的
评估新诊断的转移性激素初治前列腺癌(mHNPC)患者的预后,并基于前列腺癌广泛疾病的化疗激素治疗与雄激素剥夺随机试验(CHAARTED)风险分类开发一种新的预后模型。
患者与方法
我们回顾性分析了578例最初接受雄激素剥夺治疗的新诊断mHNPC患者的数据。我们评估了三个临床因素,即CHAARTED风险分类(高瘤负荷疾病 [HVD] 与低瘤负荷疾病 [LVD])、 Gleason评分(GS,9 - 10分与≤8分)以及血红蛋白(Hb,≤13.0 g/dL与>13.0 g/dL),通过多变量分析评估它们在预测mHNPC患者去势抵抗性前列腺癌发生时间(TTC)和总生存期(OS)方面的预后潜力。此外,我们开发了一种由显著预后因素组成的新预后模型。
结果
在整个队列中,TTC和OS的中位数值分别为18.3个月和67.5个月。HVD、GS 9 - 10分以及Hb≤13.0 g/dL是TTC和OS的独立不良预后因素。我们开发了一种新的预后模型,该模型可根据不良预后因素的数量将mHNPC患者分为四个风险组:第1组,低风险LVD(无GS 9 - 10分且Hb>13.0 g/dL的LVD患者);第2组,高风险LVD(有GS 9 - 10分、Hb≤13.0 g/dL或两者皆有的LVD患者);第3组,低风险HVD(无GS 9 - 10分且有或无Hb≤13.0 g/dL的HVD患者);第4组,高风险HVD(有GS 9 - 10分且有或无Hb≤13.0 g/dL的HVD患者)。第1、2、3和4组的TTC中位数值分别为124.8、36.4、17.9和11.2个月,OS中位数值分别为117.2、94.2、67.9和46.2个月。所有组之间在TCC和OS方面均存在显著差异。
结论
我们为mHNPC患者开发了一种由CHAARTED风险分类、GS和Hb组成的预后模型。我们的预后模型可以将LVD和HVD患者的预后显著分为两组。该模型可能为患者和医生在mHNPC初始治疗的共同决策中提供良好参考。
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