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卡介苗膀胱灌注在降低高危浅表性膀胱癌肿瘤复发方面优于丝裂霉素C:一项随机试验的荟萃分析

Intravesical bacillus Calmette-Guérin is superior to mitomycin C in reducing tumour recurrence in high-risk superficial bladder cancer: a meta-analysis of randomized trials.

作者信息

Shelley M D, Wilt T J, Court J, Coles B, Kynaston H, Mason M D

机构信息

Cochrane Prostatic Diseases and Urologic Cancers Group, Velindre NHS Trust, Cardiff, UK.

出版信息

BJU Int. 2004 Mar;93(4):485-90. doi: 10.1111/j.1464-410x.2003.04655.x.

Abstract

OBJECTIVE

To assess, in a systematic review and meta-analysis, the relative effectiveness of intravesical mitomycin C and bacillus Calmette-Guérin (BCG) for tumour recurrence, disease progression and overall survival in patients with medium- to high-risk Ta and T1 bladder cancer.

METHODS

The major medical databases were searched comprehensively up to June 2003, and relevant journals hand-searched for randomized controlled trials, in any language, that compared intravesical mitomycin C with BCG in medium- to high-risk patients with Ta or T1 bladder cancer.

RESULTS

Twenty-five articles were identified but only seven were considered eligible for the analysis. This represented 1901 evaluable patients in all, 820 randomized to mitomycin C and 1081 to BCG. Six trials had sufficient data for meta-analysis and included 1527 patients, 693 in the mitomycin and 834 in the BCG arm. There was no significant difference between mitomycin C and BCG for tumour recurrence in the six trials, with a weighted mean log hazard ratio, LHR, (variance) of -0.022 (0.005). However, there was significant heterogeneity between trials (P = 0.001). A subgroup analysis of three trials that included only high-risk Ta and T1 patients indicated no heterogeneity (P = 0.25) and a LHR for recurrence of -0.371 (0.012). With mitomycin C used as the control in the meta-analysis, a negative ratio is in favour of BCG and, in this case, was highly significant (P < 0.001). The seventh trial (in abstract form only) used BCG in low doses for two arms of the trial (27 mg and 13.5 mg) compared with a standard dose of mitomycin C (30 mg), and reported a significantly lower recurrence rate with BCG (27 mg) than for mitomycin C (P = 0.001). Only two trials included sufficient data to analyse disease progression and survival, representing 681 patients (338 randomized to BCG and 343 to mitomycin C). There was no significant difference between mitomycin C and BCG for disease progression, with a LHR of 0.044 (0.04) (P = 0.16), or survival, at -0.112 (0.03) (P = 0.50). Adverse events were slightly more frequent with BCG. Local toxicity (dysuria, cystitis, frequency and haematuria) were associated with both mitomycin C (30%) and BCG (44%). Systemic toxicity, e.g. chills, fever and malaise, occurred with both agents (12% and 19%, respectively) although skin rash was more common with mitomycin C.

CONCLUSION

Tumour recurrence was significantly lower with intravesical BCG than with mitomycin C only in those patients at high risk of tumour recurrence. However, there was no difference in disease progression or survival, and the decision to use either agent might be based on adverse events and cost.

摘要

目的

通过一项系统评价和荟萃分析,评估膀胱内注射丝裂霉素C和卡介苗(BCG)对中高危Ta和T1期膀胱癌患者肿瘤复发、疾病进展及总生存期的相对疗效。

方法

全面检索主要医学数据库至2003年6月,并手工检索相关期刊,查找以任何语言发表的、比较膀胱内注射丝裂霉素C与BCG治疗中高危Ta或T1期膀胱癌患者的随机对照试验。

结果

共识别出25篇文章,但仅7篇被认为符合分析条件。这些文章共纳入1901例可评估患者,其中820例随机接受丝裂霉素C治疗,1081例接受BCG治疗。6项试验有足够数据进行荟萃分析,共纳入1527例患者,丝裂霉素C组693例,BCG组834例。在这6项试验中,丝裂霉素C与BCG在肿瘤复发方面无显著差异,加权平均对数风险比(LHR,方差)为-0.022(0.005)。然而,试验间存在显著异质性(P = 0.001)。对仅纳入高危Ta和T1期患者的3项试验进行亚组分析,结果显示无异质性(P = 0.25),复发的LHR为-0.371(0.012)。在荟萃分析中以丝裂霉素C作为对照,负比值有利于BCG,在这种情况下具有高度显著性(P < 0.001)。第7项试验(仅摘要形式)在试验的两个组中使用低剂量BCG(27 mg和13.5 mg)与标准剂量丝裂霉素C(30 mg)进行比较,报告BCG(27 mg)组的复发率显著低于丝裂霉素C组(P = 0.001)。仅有2项试验有足够数据分析疾病进展和生存期,共纳入681例患者(338例随机接受BCG治疗,343例接受丝裂霉素C治疗)。丝裂霉素C与BCG在疾病进展方面无显著差异,LHR为0.044(0.04)(P = 0.16),在生存期方面也无显著差异,LHR为-0.112(0.03)(P = 0.50)。BCG的不良事件略多。局部毒性(排尿困难、膀胱炎、尿频和血尿)在丝裂霉素C组(30%)和BCG组(44%)中均有发生。全身毒性,如寒战、发热和不适,两种药物均有发生(分别为12%和19%),尽管皮疹在丝裂霉素C组更常见。

结论

仅在肿瘤复发高危患者中,膀胱内注射BCG的肿瘤复发率显著低于丝裂霉素C。然而,在疾病进展或生存期方面无差异,选择使用这两种药物中的任何一种可能基于不良事件和成本。

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