NeuroNexus Research/Hunter Neurology, Franklin, TN, USA.
The University of Texas Health Science Center, Houston, TX, USA.
Mult Scler Relat Disord. 2024 Nov;91:105912. doi: 10.1016/j.msard.2024.105912. Epub 2024 Sep 30.
Multiple sclerosis (MS) has not been well studied in racial and ethnic minorities, as these populations are typically underrepresented in clinical trials. Black or African Americans comprise ∼13 % of the US population, yet are represented by as little as 5 % in clinical trials. Differences in disease course and progression have been reported between races and ethnicities, so there is a need to understand the safety and efficacy of disease-modifying therapies (DMTs) in Black patients, to inform evidence-based approaches to treatment in this population.
EVOLVE-MS-1 (NCT0234307) was an open-label, single-arm, phase 3 study assessing the long-term safety, tolerability, and efficacy of diroximel fumarate (DRF) over 96 weeks in adults with relapsing-remitting multiple sclerosis (RRMS). Patients were either newly initiated to DRF or rolled over from completing EVOLVE-MS-2 (NCT03093324). In this post-hoc analysis of the phase 3 EVOLVE-MS-1 study, we evaluate the safety and exploratory efficacy outcomes for DRF in Black and non-Black patient subgroups.
Of 1057 patients enrolled, 72 (6.8 %) were Black. In Black vs non-Black patients, mean age was 42 vs 43 years and 75 % vs 72 % were female, respectively. In both groups, median (range) duration of DRF exposure was 1.8 (0.0-2.0) years and mean Expanded Disability Status Scale (EDSS) was 2.7. The most common prior DMTs for both Black vs non-Black patients were interferons (47 % vs 37 %) and glatiramer acetate (36 % vs 24 %). DRF treatment was discontinued in 33 (46 %) Black and 224 (23 %) non-Black patients; most common reasons for discontinuation were withdrawal by patient (n = 11, 15.3 %), adverse events (AEs; n = 7, 9.7 %), and lost to follow-up (n = 7, 9.7 %) in Black patients; AEs (8.2 %) and withdrawal by patient (7.0 %) in non-Black patients. AEs were reported in 90 % Black and 89 % non-Black patients; most AEs were mild or moderate in both groups. Gastrointestinal (GI) AEs were reported in 36 % Black and 32 % non-Black patients; no Black patients discontinued due to GI AEs, vs 7 (0.7 %) non-Black patients. The most commonly reported AE was flushing (18 % Black and 28 % non-Black patients). No AEs of lymphopenia were reported in Black patients compared with 13 % of non-Black patients. Mean absolute lymphocyte count declined from baseline to week 48 by 15 % in Black patients and 29 % in non-Black patients, then plateaued and remained above the lower limit of normal (LLN; 0.91 × 10/L). Adjusted annualized relapse rate (95 % confidence interval) was reduced by 78.2 % (54.6 - 89.5; p < 0.0001) in Black patients, from 12 months before to 96 weeks after DRF treatment; similar to 81.7 % (78.5 - 84.5 %; p < 0.0001) reduction in non-Black patients. Mean number of patients free from confirmed disability progression was 93.4 % by week 48, then 86.2 % vs 90.4 % by week 96 in Black vs non-Black patients, respectively.
This study presents the first analysis of safety and efficacy of DRF in Black patients. Relapse rates remained low in Black patients on DRF, consistent with non-Black patients, and there were no new safety signals identified in the Black patient subgroup in EVOLVE-MS-1. Together, these outcomes support DRF as an effective treatment option in Black patients with RRMS.
多发性硬化症(MS)在少数民族和种族中研究不足,因为这些人群在临床试验中的代表性通常较低。黑人和非裔美国人约占美国人口的 13%,但在临床试验中仅占 5%。不同种族和族裔之间的疾病过程和进展存在差异,因此需要了解疾病修饰疗法(DMT)在黑人患者中的安全性和疗效,为该人群的循证治疗提供依据。
EVOLVE-MS-1(NCT0234307)是一项开放标签、单臂、3 期研究,评估了二羟甲基富马酸(DRF)在 96 周内对复发缓解型多发性硬化症(RRMS)成年患者的长期安全性、耐受性和疗效。患者新开始使用 DRF 或从 EVOLVE-MS-2(NCT03093324)完成研究后转入。在这项 3 期 EVOLVE-MS-1 研究的事后分析中,我们评估了黑人和非黑人患者亚组中 DRF 的安全性和探索性疗效结果。
在 1057 名入组患者中,72 名(6.8%)为黑人。与非黑人患者相比,黑人患者的平均年龄为 42 岁 vs 43 岁,分别有 75%和 72%为女性。两组患者的中位(范围)DRF 暴露时间均为 1.8(0.0-2.0)年,平均扩展残疾状况量表(EDSS)为 2.7。两组患者最常见的既往 DMT 均为干扰素(47% vs 37%)和聚乙二醇干扰素(36% vs 24%)。33 名(46%)黑人患者和 224 名(23%)非黑人患者停用 DRF;最常见的停药原因是患者停药(n=11,15.3%)、不良事件(AE;n=7,9.7%)和失访(n=7,9.7%),在黑人患者中;AE(8.2%)和患者停药(7.0%)在非黑人患者中。90%的黑人患者和 89%的非黑人患者报告了 AE;两组患者的 AE 均为轻度或中度。黑人患者中有 36%报告胃肠道(GI)AE,非黑人患者中有 32%报告 GI AE;没有黑人患者因 GI AE 停药,而非黑人患者有 7 人(0.7%)。最常见的 AE 是潮红(18%黑人患者和 28%非黑人患者)。与 13%的非黑人患者相比,没有黑人患者报告淋巴细胞减少相关的 AE。与基线相比,黑人患者的绝对淋巴细胞计数在第 48 周时下降了 15%,而非黑人患者下降了 29%,然后稳定在正常值下限(LLN;0.91×10/L)之上。调整后的年度复发率(95%置信区间)在黑人患者中降低了 78.2%(54.6-89.5;p<0.0001),从 DRF 治疗前 12 个月到 96 周;非黑人患者的降幅相似,为 81.7%(78.5-84.5%;p<0.0001)。在第 48 周时,有 93.4%的患者没有确认残疾进展,在第 96 周时,黑人患者和非黑人患者分别为 86.2%和 90.4%。
这项研究首次分析了 DRF 在黑人患者中的安全性和疗效。DRF 治疗的黑人患者的复发率保持较低水平,与非黑人患者一致,并且在 EVOLVE-MS-1 中没有发现黑人患者亚组的新安全性信号。这些结果共同支持 DRF 作为治疗 RRMS 黑人患者的有效治疗选择。
