评估在一项评估利妥昔单抗(EXPLORER)治疗狼疮患者的 II/III 期研究中入组的患者的疾病 flares。
Assessment of flares in lupus patients enrolled in a phase II/III study of rituximab (EXPLORER).
机构信息
Oklahoma Medical Research Foundation, Oklahoma City 73104,USA.
出版信息
Lupus. 2011 Jun;20(7):709-16. doi: 10.1177/0961203310395802. Epub 2011 Apr 8.
The EXPLORER study was designed to assess the response to rituximab versus placebo in patients with moderate to severe extrarenal systemic lupus erythematosus (SLE) receiving background immunosuppression. The definition of response required reduced clinical activity without subsequent flares over 52 weeks, and the study did not meet its efficacy endpoint. The current exploratory analysis assessed flare rates in patients who achieved initial low disease activity response (British Isles Lupus Assessment Group [BILAG] C or better in all organs) during the study. Exploratory reanalysis of data from the EXPLORER trial was conducted, considering alternative definitions for flare. No difference was found between rituximab and placebo in preventing or delaying moderate to severe flares. However, when severe (BILAG A) flares alone were examined, rituximab reduced the risk of a subsequent first A flare (hazard ratio = 0.61; p = 0.052) and lowered mean ± SD annualized A flare rates (0.86 ± 1.47 vs. 1.41 ± 2.14; p = 0.038). Eighty-four (49.7%) rituximab-treated patients achieved low disease activity without subsequent A flares versus 31 (35.2%) placebo-treated patients (p = 0.027). Prednisone rescue for A flares was similar in rituximab- (24%) and placebo-treated (14%) patients (p = 0.204). This post hoc analysis evaluates the hypothesis that assessment of BILAG A flares may distinguish potential treatment effects with greater sensitivity than assessment of BILAG B flares.
EXPLORER 研究旨在评估利妥昔单抗与安慰剂在接受背景免疫抑制治疗的中重度肾外系统性红斑狼疮 (SLE) 患者中的疗效。反应的定义需要在 52 周内没有临床活动恶化和随后的复发,该研究未达到其疗效终点。本探索性分析评估了在研究期间达到初始低疾病活动反应(所有器官均为英国狼疮评估组 [BILAG] C 或更好)的患者的复发率。对 EXPLORER 试验的数据进行了探索性重新分析,并考虑了复发的替代定义。利妥昔单抗与安慰剂在预防或延迟中重度复发方面无差异。然而,当单独检查严重(BILAG A)复发时,利妥昔单抗降低了随后首次 A 复发的风险(风险比=0.61;p=0.052),并降低了平均±SD 年化 A 复发率(0.86±1.47 与 1.41±2.14;p=0.038)。与安慰剂治疗组(31 例,35.2%)相比,84 例(49.7%)利妥昔单抗治疗患者在无后续 A 复发的情况下达到低疾病活动(p=0.027)。利妥昔单抗治疗组(24%)和安慰剂治疗组(14%)的 A 复发患者接受泼尼松解救治疗的比例相似(p=0.204)。本事后分析评估了这样一种假设,即 BILAG A 复发的评估可能比 BILAG B 复发的评估更敏感地区分潜在的治疗效果。
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