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Treatment-induced anaemia and its potential clinical impact in patients receiving sequential high dose chemotherapy for metastatic testicular cancer

机译:序贯高剂量化疗治疗转移性睾丸癌患者的治疗性贫血及其潜在临床影响

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First-line sequential high dose chemotherapy is under investigation in patients with ‘poor prognosis’ metastatic germ cell tumours in order to improve survival. Despite the use of autologous peripheral blood stem cell transplantation and granulocyte colony stimulating factor chemotherapy dose intensification is associated with severe haematotoxicity including anaemia, which may significantly affect quality of life and tolerability of chemotherapy. This study investigates the frequency and degree of anaemia in patients receiving first-line sequential high dose chemotherapy for metastatic testicular cancer and the impact of anaemia on treatment outcome. A total of 101 newly diagnosed patients with ‘poor prognosis’ metastatic nonseminomatous germ cell tumours were treated with one cycle of standard VIP followed by three cycles of HD-VIP-chemotherapy (etoposide, ifosfamide, cisplatin) within a large phase I/II study. Differential blood cell counts were taken prior, during and after every cycle of chemotherapy. Additionally, the numbers of red blood cell and platelet transfusions were recorded. Kaplan–Meier analyses were performed to correlate pre-treatment and post-treatment haemoglobin values to response and overall survival. Forty-eight per cent of the patients were classified anaemic (haemoglobin <12 g dl−1) prior to the start of chemotherapy. The application of sequential HD-VIP resulted in median haemoglobin nadirs between 7.8 g dl−1 (range 5.5–11.1 g dl−1) in the first cycle and 7.6 g dl−1 (range 6.0–11.4 g dl−1) in the third cycle despite the frequent use of red blood cell transfusions. Almost all patients (99%) had haemoglobin levels <10 g dl−1 at some timepoint during first-line sequential high dose chemotherapy. Overall, 97 patients received red blood cell transfusions with a median of 10 units (range 2–25) per patient during the four consecutive cycles of therapy. The time to first transfusion was shortest in patients with the lowest initial haemoglobin values. While there was no prediction of response or outcome by baseline haemoglobin-levels, a significant survival difference in favour of patients with a haemoglobin value >10.5 g dl−1 after completion of four cycles of therapy (at leukocyte recovery after the last cycle) compared to those with haemoglobin values <10.5 g dl−1 was found with 3-year overall survival rates of 87% vs 68%, respectively (P<0.05). Severe anaemia is a very frequent side effect of sequential dose intensive therapy in patients with germ cell cancer, with almost all patients becoming transfusion dependent. Despite the frequent use of red blood cell transfusions, median haemoglobin nadirs remained about 7.5–8 g dl−1 during therapy. A correlation of haemoglobin-values after completion of therapy to overall treatment outcome was found.British Journal of Cancer (2002) >87, 1066–1071. doi: © 2002
机译:一线序贯高剂量化疗正在研究“预后不良”的转移性生殖细胞肿瘤患者,以提高生存率。尽管使用了自体外周血干细胞移植和粒细胞集落刺激因子化疗,但剂量增加仍与包括贫血在内的严重血液毒性有关,这可能会显着影响化疗的生活质量和耐受性。这项研究调查了接受转移性睾丸癌一线序贯高剂量化疗的患者出现贫血的频率和程度,以及贫血对治疗结果的影响。在一项大型的I / II期研究中,共对101例新诊断为“预后差”的转移性非精原细胞性生殖细胞肿瘤患者进行了一个周期的标准VIP治疗,随后进行了三个周期的HD-VIP化学疗法(依托泊苷,异环磷酰胺,顺铂)治疗。在化学疗法的每个周期之前,期间和之后进行差异血细胞计数。另外,记录红细胞和血小板输注的次数。进行Kaplan–Meier分析以将治疗前和治疗后血红蛋白值与反应和总体生存率相关联。在开始化疗之前,有48%的患者被分类为贫血(血红蛋白<12 g dl -1 )。连续HD-VIP的应用导致第一个周期的中位数血红蛋白最低点在7.8 g dl -1 (范围5.5–11.1 g dl -1 )和7.6 g dl之间尽管频繁使用红细胞输注,但在第三周期的 -1 (范围6.0–11.4 g dl -1 )。一线序贯高剂量化疗期间的某个时间点,几乎所有患者(99%)的血红蛋白水平<10 -1 。总体而言,在连续四个治疗周期中,有97名患者接受了红细胞输血,每位患者的中位数为10 8个单位(范围2至25)。初始血红蛋白值最低的患者首次输血时间最短。尽管不能通过基线血红蛋白水平预测疗效或预后,但在完成四个疗程后(在白血球处)血红蛋白值> 10.5 g dl -1 的患者生存率差异显着与血红蛋白值<10.5 g dl -1 的人相比,其3年总生存率分别为87%和68%(P <0.05)。严重贫血是生殖细胞癌患者序贯强化治疗的非常常见的副作用,几乎所有患者都依赖输血。尽管经常使用红细胞输血,但治疗期间中位血红蛋白最低点仍约为7.5–8 g dl -1 。发现完成治疗后血红蛋白值与总体治疗结果之间的相关性。《英国癌症杂志》(2002年,> 87 ,1066-1071)。 doi:©2002

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