Department of Gastroenterology, Royal Devon University Healthcare NHS Foundation Trust, Exeter, UK; Exeter IBD and Pharmacogenetics Research Group, University of Exeter, Exeter, UK.
Exeter IBD and Pharmacogenetics Research Group, University of Exeter, Exeter, UK.
Lancet Gastroenterol Hepatol. 2024 Jun;9(6):521-538. doi: 10.1016/S2468-1253(24)00044-X. Epub 2024 Apr 16.
We sought to report the effectiveness of infliximab and adalimumab over the first 3 years of treatment and to define the factors that predict anti-TNF treatment failure and the strategies that prevent or mitigate loss of response.
Personalised Anti-TNF therapy in Crohn's disease (PANTS) is a UK-wide, multicentre, prospective observational cohort study reporting the rates of effectiveness of infliximab and adalimumab in anti-TNF-naive patients with active luminal Crohn's disease aged 6 years and older. At the end of the first year, sites were invited to enrol participants still receiving study drug into the 2-year PANTS-extension study. We estimated rates of remission across the whole cohort at the end of years 1, 2, and 3 of the study using a modified survival technique with permutation testing. Multivariable regression and survival analyses were used to identify factors associated with loss of response in patients who had initially responded to anti-TNF therapy and with immunogenicity. Loss of response was defined in patients who initially responded to anti-TNF therapy at the end of induction and who subsequently developed symptomatic activity that warranted an escalation of steroid, immunomodulatory, or anti-TNF therapy, resectional surgery, or exit from study due to treatment failure. This study was registered with ClinicalTrials.gov, NCT03088449, and is now complete.
Between March 19, 2014, and Sept 21, 2017, 389 (41%) of 955 patients treated with infliximab and 209 (32%) of 655 treated with adalimumab in the PANTS study entered the PANTS-extension study (median age 32·5 years [IQR 22·1-46·8], 307 [51%] of 598 were female, and 291 [49%] were male). The estimated proportion of patients in remission at the end of years 1, 2, and 3 were, for infliximab 40·2% (95% CI 36·7-43·7), 34·4% (29·9-39·0), and 34·7% (29·8-39·5), and for adalimumab 35·9% (95% CI 31·2-40·5), 32·9% (26·8-39·2), and 28·9% (21·9-36·3), respectively. Optimal drug concentrations at week 14 to predict remission at any later timepoints were 6·1-10·0 mg/L for infliximab and 10·1-12·0 mg/L for adalimumab. After excluding patients who had primary non-response, the estimated proportions of patients who had loss of response by years 1, 2, and 3 were, for infliximab 34·4% (95% CI 30·4-38·2), 54·5% (49·4-59·0), and 60·0% (54·1-65·2), and for adalimumab 32·1% (26·7-37·1), 47·2% (40·2-53·4), and 68·4% (50·9-79·7), respectively. In multivariable analysis, loss of response at year 2 and 3 for patients treated with infliximab and adalimumab was predicted by low anti-TNF drug concentrations at week 14 (infliximab: hazard ratio [HR] for each ten-fold increase in drug concentration 0·45 [95% CI 0·30-0·67], adalimumab: 0·39 [0·22-0·70]). For patients treated with infliximab, loss of response was also associated with female sex (vs male sex; HR 1·47 [95% CI 1·11-1·95]), obesity (vs not obese 1·62 [1·08-2·42]), baseline white cell count (1·06 [1·02-1·11) per 1 × 10 increase in cells per L), and thiopurine dose quartile. Among patients treated with adalimumab, carriage of the HLA-DQA105 risk variant was associated with loss of response (HR 1·95 [95% CI 1·17-3·25]). By the end of year 3, the estimated proportion of patients who developed anti-drug antibodies associated with undetectable drug concentrations was 44·0% (95% CI 38·1-49·4) among patients treated with infliximab and 20·3% (13·8-26·2) among those treated with adalimumab. The development of anti-drug antibodies associated with undetectable drug concentrations was significantly associated with treatment without concomitant immunomodulator use for both groups (HR for immunomodulator use: infliximab 0·40 [95% CI 0·31-0·52], adalimumab 0·42 [95% CI 0·24-0·75]), and with carriage of HLA-DQA105 risk variant for infliximab (HR for carriage of risk variant: infliximab 1·46 [1·13-1·88]) but not for adalimumab (HR 1·60 [0·92-2·77]). Concomitant use of an immunomodulator before or on the day of starting infliximab was associated with increased time without the development of anti-drug antibodies associated with undetectable drug concentrations compared with use of infliximab alone (HR 2·87 [95% CI 2·20-3·74]) or introduction of an immunomodulator after anti-TNF initiation (1·70 [1·11-2·59]). In years 2 and 3, 16 (4%) of 389 patients treated with infliximab and 11 (5%) of 209 treated with adalimumab had adverse events leading to treatment withdrawal. Nine (2%) patients treated with infliximab and two (1%) of those treated with adalimumab had serious infections in years 2 and 3.
Only around a third of patients with active luminal Crohn's disease treated with an anti-TNF drug were in remission at the end of 3 years of treatment. Low drug concentrations at the end of the induction period predict loss of response by year 3 of treatment, suggesting higher drug concentrations during the first year of treatment, particularly during induction, might lead to better long-term outcomes. Anti-drug antibodies associated with undetectable drug concentrations of infliximab, but not adalimumab, can be predicted by carriage of HLA-DQA1*05 and mitigated by concomitant immunomodulator use for both drugs.
Guts UK, Crohn's and Colitis UK, Cure Crohn's Colitis, AbbVie, Merck Sharp and Dohme, Napp Pharmaceuticals, Pfizer, and Celltrion Healthcare.
我们旨在报告英夫利昔单抗和阿达木单抗在治疗的前 3 年内的有效性,并确定预测抗 TNF 治疗失败的因素以及预防或减轻应答丧失的策略。
克罗恩病的个体化抗 TNF 治疗(PANTS)是一项英国范围内的、多中心的、前瞻性观察性队列研究,报告了在年龄为 6 岁及以上的活动性腔肠内克罗恩病的抗 TNF 初治患者中使用英夫利昔单抗和阿达木单抗的有效性。在第一年结束时,邀请各站点招募仍在接受研究药物治疗的患者进入为期 2 年的 PANTS 扩展研究。我们使用修改后的生存技术(具有置换检验)来估计整个队列在研究的第 1、2 和 3 年末的缓解率。多变量回归和生存分析用于识别在最初对抗 TNF 治疗有反应的患者中与应答丧失相关的因素,以及与免疫原性相关的因素。在诱导结束时最初对抗 TNF 治疗有反应的患者中,定义应答丧失为随后出现需要皮质类固醇、免疫调节剂或抗 TNF 治疗、切除术或因治疗失败而退出研究的症状性活动。这项研究在 ClinicalTrials.gov 上注册,NCT03088449,现已完成。
2014 年 3 月 19 日至 2017 年 9 月 21 日,在 PANTS 研究中接受英夫利昔单抗治疗的 389 名(41%)和接受阿达木单抗治疗的 209 名(32%)患者进入 PANTS 扩展研究(中位年龄 32.5 岁[IQR 22.1-46.8],307 名[51%]为女性,291 名[49%]为男性)。在第 1、2 和 3 年末,预计缓解的患者比例分别为英夫利昔单抗 40.2%(95%CI 36.7-43.7)、34.4%(29.9-39.0)和 34.7%(29.8-39.5),阿达木单抗 35.9%(95%CI 31.2-40.5)、32.9%(26.8-39.2)和 28.9%(21.9-36.3)。预测任何后续时间点缓解的最佳药物浓度为英夫利昔单抗为 6.1-10.0mg/L,阿达木单抗为 10.1-12.0mg/L。排除原发性无应答患者后,在第 1、2 和 3 年末,英夫利昔单抗的应答丧失率分别为 34.4%(95%CI 30.4-38.2)、54.5%(49.4-59.0)和 60.0%(54.1-65.2),阿达木单抗为 32.1%(26.7-37.1)、47.2%(40.2-53.4)和 68.4%(50.9-79.7)。多变量分析表明,英夫利昔单抗和阿达木单抗治疗的患者在第 2 年和第 3 年的应答丧失与第 14 周时的低抗 TNF 药物浓度相关(英夫利昔单抗:药物浓度每增加十倍,风险比[HR]为 0.45[95%CI 0.30-0.67],阿达木单抗:0.39[0.22-0.70])。对于接受英夫利昔单抗治疗的患者,应答丧失还与女性(与男性相比;HR 1.47[95%CI 1.11-1.95])、肥胖(与非肥胖相比 1.62[1.08-2.42])、基线白细胞计数(每 1×10 个细胞增加 1.06[1.02-1.11))和硫嘌呤剂量四分位有关。在接受阿达木单抗治疗的患者中,携带 HLA-DQA105 风险变体与应答丧失相关(HR 1.95[95%CI 1.17-3.25])。到第 3 年末,在接受英夫利昔单抗治疗的患者中,与药物浓度不可检测相关的抗药物抗体的发生率为 44.0%(95%CI 38.1-49.4),在接受阿达木单抗治疗的患者中为 20.3%(13.8-26.2)。与药物浓度不可检测相关的抗药物抗体的发展与两组均不使用伴随免疫调节剂(英夫利昔单抗:免疫调节剂使用的 HR 0.40[95%CI 0.31-0.52],阿达木单抗:0.42[95%CI 0.24-0.75])和与 HLA-DQA105 风险变体携带有关(与携带风险变体相比,英夫利昔单抗的 HR 为 1.46[1.13-1.88]),但与阿达木单抗无关(HR 1.60[0.92-2.77])。在开始英夫利昔单抗治疗之前或当天开始使用免疫调节剂与单独使用英夫利昔单抗相比,与不可检测药物浓度相关的抗药物抗体无发展的时间更长(HR 2.87[95%CI 2.20-3.74])或在抗 TNF 起始后引入免疫调节剂(1.70[1.11-2.59])。在第 2 年和第 3 年,389 名接受英夫利昔单抗治疗的患者中有 16 名(4%)和 209 名接受阿达木单抗治疗的患者中有 11 名(5%)出现导致治疗停止的不良事件。在第 2 年和第 3 年,接受英夫利昔单抗治疗的患者中有 9 名(2%)和接受阿达木单抗治疗的患者中有 2 名(1%)发生严重感染。
只有大约三分之一接受抗 TNF 药物治疗的活动性腔肠内克罗恩病患者在 3 年的治疗后处于缓解状态。在诱导期末期的低药物浓度可预测第 3 年的应答丧失,这表明在治疗的第一年,特别是在诱导期,更高的药物浓度可能会带来更好的长期结果。英夫利昔单抗与不可检测药物浓度相关的抗药物抗体可由 HLA-DQA1*05 预测,并用两种药物的伴随免疫调节剂减轻。
Guts UK、Crohn's and Colitis UK、Cure Crohn's Colitis、AbbVie、Merck Sharp and Dohme、Napp Pharmaceuticals、Pfizer 和 Celltrion Healthcare。
