贝伐单抗能增加癌症患者的重症蛋白尿风险
2011-06-07 Wu S;Kim C;Baer L;Zhu X MedSci原创
采用化学治疗药物(贝伐单抗,是中和血管内皮生长因子的人源化抗体)治疗可导致蛋白尿和肾功能损害。尚未完全理解肾功能不良事件的风险因素和临床结果。我们对已发表的随机、对照试验进行一项系统性回顾和荟萃分析,以评估应用贝伐单抗治疗引起重症蛋白尿的整体风险。我们分析了来自16个研究(包括12,268例患有多种肿瘤的患者)的数据。应用贝伐单抗治疗的大量(3或4级)蛋白尿发病率为2.2%(95%置信区间 [CI
采用化学治疗药物(贝伐单抗,是中和血管内皮生长因子的人源化抗体)治疗可导致蛋白尿和肾功能损害。尚未完全理解肾功能不良事件的风险因素和临床结果。我们对已发表的随机、对照试验进行一项系统性回顾和荟萃分析,以评估应用贝伐单抗治疗引起重症蛋白尿的整体风险。我们分析了来自16个研究(包括12,268例患有多种肿瘤的患者)的数据。应用贝伐单抗治疗的大量(3或4级)蛋白尿发病率为2.2%(95%置信区间 [CI]为1.2至4.3%)。相比于单纯化疗,贝伐单抗联合化疗明显的增加大量蛋白尿(相对危险度4.79;95%CI为2.71至8.46)和肾病综合症(相对危险度7.78,95%CI为1.80至33.62)的风险;较高剂量的贝伐单抗与蛋白尿风险增加的相关。关于肿瘤类型,肾细胞癌与最高的风险相关(累积发生率10.2%)。我们在大量蛋白尿风险方面未检测到铂和非铂为基础的同步化疗间显著的差异(P=0.39)。总之,贝伐单抗与化疗联合应用显著的增加大量蛋白尿和肾病综合征的风险。
Treatment with the chemotherapeutic agent bevacizumab, a humanized mAb that neutralizes vascular endothelial growth factor, can lead to proteinuria and renal damage. The risk factors and clinical outcomes of renal adverse events are not well understood. We performed a systematic review and meta-analysis of published randomized, controlled trials to assess the overall risk for severe proteinuria with bevacizumab. We analyzed data from 16 studies comprising 12,268 patients with a variety of tumors. The incidence of high-grade (grade 3 or 4) proteinuria with bevacizumab was 2.2% (95% confidence interval [CI] 1.2 to 4.3%). Compared with chemotherapy alone, bevacizumab combined with chemotherapy significantly increased the risk for high-grade proteinuria (relative risk 4.79; 95% CI 2.71 to 8.46) and nephrotic syndrome (relative risk 7.78; 95% CI 1.80 to 33.62); higher dosages of bevacizumab associated with increased risk for proteinuria. Regarding tumor type, renal cell carcinoma associated with the highest risk (cumulative incidence 10.2%). We did not detect a significant difference between platinum- and non-platinum-based concurrent chemotherapy with regard to risk for high-grade proteinuria (P = 0.39). In conclusion, the addition of bevacizumab to chemotherapy significantly increases the risk for high-grade proteinuria and nephrotic syndrome.
专家评价:
Michael Mayr and
Jurg Schifferli
Medizinische Universitaetsklinik Basel, Switzerland
Nephrology
In this study, the authors not only confirm that the vascular endothelial growth factor (VEGF)-neutralizing antibody bevacizumab (avastin) can cause proteinuria but also point out its role as a risk factor for severe proteinuria in cancer patients. Interestingly, there seems to be a dose-dependent effect whereby patients treated for renal cell carcinoma (RCC) are at highest risk of developing severe proteinuria.
VEGF plays an important role in tumor angiogenesis, growth, progression, invasion and metastasis. This led to the development and successful introduction of a new class of drugs in cancer therapy that are characterized by inhibiting VEGF signaling pathways at different levels. In the current meta-analysis of 16 randomized controlled trials, 6482 patients treated with bevacizumab in combination with chemotherapy were compared to 5786 patients treated with chemotherapy alone. The patients suffered either from colorectal cancer, non-small cell lung cancer, breast cancer, pancreatic cancer, renal cell carcinoma or malignant mesothelioma. The summary incidence rate of high-grade proteinuria in patients treated with bevacizumab was 2.2%, whereby the addition of bevacizumab increased the risk of severe proteinuria and nephrotic syndrome by a factor of 5 and 8, respectively. Furthermore and clinically important, patients suffering from RCC had the highest risk for severe proteinuria with an incidence rate of 12%. When low versus high bevacizumab dosages were compared (arbitrarily determined as a weekly dosage of 2.5mg/kg compared to 5mg/kg), a dose-dependent effect on the development of severe proteinuria could be observed. At the moment, it is unclear whether the development of severe proteinuria has any impact on the clinical outcome of cancer patients. At least at the study level, no correlation between high-grade proteinuria and progression-free survival or overall survival could be found. However, this does not exclude clinically relevant implications at the patient level. Therefore, patients treated with bevacizumab and, assuming a class effect, other VEGF signaling pathway inhibitors, such as axitinib, VEGF Trap, sorafenib, and sunitinib, should be closely monitored to prevent undesired renal and cardiovascular side effects. Finally, the degree of proteinuria in relation to the tumor type needs further exploration. It is unclear whether the effect seen in patients with RCC is simply explainable by secondary effects due to the loss of renal mass since almost all patients are nephrectomised?
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