遗传性转甲状腺素蛋白介导的淀粉样变性多发性神经病患者从依诺特森转换为依普洛森治疗:来自NEURO-TTRansform研究的分析
Switching from inotersen to eplontersen in patients with hereditary transthyretin-mediated amyloidosis with polyneuropathy: analysis from NEURO-TTRansform.
作者信息
Conceição Isabel, Berk John L, Weiler Markus, Kowacs Pedro A, Dasgupta Noel R, Khella Sami, Chao Chi-Chao, Attarian Shahram, Kwoh T Jesse, Jung Shiangtung W, Chen Jersey, Viney Nicholas J, Yu Rosie Z, Gertz Morie, Masri Ahmad, Cruz Márcia Waddington, Coelho Teresa
机构信息
ULS Santa Maria, CAML, Instituto de Medicina Molecular, Faculdade de Medicina da Universidade de Lisboa, Lisbon, Portugal.
Boston University School of Medicine, Boston, MA, USA.
出版信息
J Neurol. 2024 Oct;271(10):6655-6666. doi: 10.1007/s00415-024-12616-6. Epub 2024 Aug 13.
BACKGROUND
The phase 3 NEURO-TTRansform trial showed eplontersen treatment for 65 weeks reduced transthyretin (TTR), halted progression of neuropathy impairment, and improved quality of life (QoL) in adult patients with hereditary TTR-mediated amyloidosis with polyneuropathy (ATTRv-PN), vs. historical placebo.
METHODS
NEURO-TTRansform enrolled patients with ATTRv-PN. A subset of patients were randomized to receive subcutaneous inotersen 300 mg weekly (Weeks 1-34) and subsequently switched to subcutaneous eplontersen 45 mg every 4 weeks (Weeks 37-81). Change in serum TTR and treatment-emergent adverse events (TEAEs) were evaluated through Week 85. Effects on neuropathy impairment, QoL, and nutritional status were also evaluated.
RESULTS
Of 24 patients randomized to inotersen, 20 (83%) switched to eplontersen at Week 37 and four discontinued due to AEs/investigator decision. Absolute change in serum TTR was greater after switching from inotersen (-74.3%; Week 35) to eplontersen (-80.6%; Week 85). From the end of inotersen treatment, neuropathy impairment and QoL were stable (i.e., did not progress) while on eplontersen, and there was no deterioration in nutritional status. TEAEs were fewer with eplontersen (Weeks 37-85; 19/20 [95%] patients) compared with inotersen (up to Week 35; 24/24 [100%] patients). Mean platelet counts decreased during inotersen treatment (mean nadir reduction ‒40.7%) and returned to baseline during eplontersen treatment (mean nadir reduction, ‒3.2%).
CONCLUSIONS
Switching from inotersen to eplontersen further reduced serum TTR, halted disease progression, stabilized QoL, restored platelet count, and improved tolerability, without deterioration in nutritional status. This supports a positive benefit-risk profile for patients with ATTRv-PN who switch from inotersen to eplontersen.
背景
3期NEURO-TTRansform试验表明,与历史安慰剂相比,成年遗传性转甲状腺素蛋白(TTR)介导的淀粉样变多发性神经病(ATTRv-PN)患者接受依洛特森治疗65周可降低TTR水平,阻止神经病变进展,并改善生活质量(QoL)。
方法
NEURO-TTRansform试验纳入了ATTRv-PN患者。一部分患者被随机分配,在第1 - 34周每周皮下注射300mg依诺特森,随后在第37 - 81周改为每4周皮下注射45mg依洛特森。在第85周时评估血清TTR的变化以及治疗中出现的不良事件(TEAE)。还评估了对神经病变、生活质量和营养状况的影响。
结果
在随机分配接受依诺特森治疗的24例患者中,20例(83%)在第周改为依洛特森治疗周有4例因不良事件研究者决定而停药。从依诺特森转换为依洛特森后,血清TTR的绝对变化更大从依诺特森治疗结束时起,在接受依洛特森治疗期间,神经病变和生活质量保持稳定即没有进展,营养状况也没有恶化。与依诺特森相比,依洛特森治疗期间出现不良事件的患者更少(第周;19/例 [95%])(至第周;24/24例 [100%])。依诺特森治疗期间平均血小板计数下降(平均最低点降低 - 40.7%),而在依洛特森治疗期间恢复到基线水平(平均最低点降低 - 3.2%)。
结论
从依诺特森转换为依洛特森可进一步降低血清TTR水平,阻止疾病进展,稳定生活质量,恢复血小板计数,并提高耐受性,且营养状况没有恶化。这支持了从依诺特森转换为依洛特森的ATTRv-PN患者具有良好的效益风险比。
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