输血依赖型重度基因型β-地中海贫血(HGB-212)患者的 Betibeglogene autotemcel 基因疗法:一项非随机、多中心、单臂、开放标签、单剂量的 3 期试验

Janet L Kwiatkowski, Mark C Walters, Suradej Hongeng, Evangelia Yannaki, Andreas E Kulozik, Joachim B Kunz, Martin G Sauer, Adrian J Thrasher, Isabelle Thuret, Ashutosh Lal, Ge Tao, Shamshad Ali, Himal L Thakar, Heidi Elliot, Ankit Lodaya, Ji Lee, Richard A Colvin, Franco Locatelli, Alexis A Thompson
{"title":"输血依赖型重度基因型β-地中海贫血(HGB-212)患者的 Betibeglogene autotemcel 基因疗法:一项非随机、多中心、单臂、开放标签、单剂量的 3 期试验","authors":"Janet L Kwiatkowski, Mark C Walters, Suradej Hongeng, Evangelia Yannaki, Andreas E Kulozik, Joachim B Kunz, Martin G Sauer, Adrian J Thrasher, Isabelle Thuret, Ashutosh Lal, Ge Tao, Shamshad Ali, Himal L Thakar, Heidi Elliot, Ankit Lodaya, Ji Lee, Richard A Colvin, Franco Locatelli, Alexis A Thompson","doi":"10.1016/s0140-6736(24)01884-1","DOIUrl":null,"url":null,"abstract":"<h3>Background</h3>Transfusion-dependent β-thalassaemia (TDT) is a severe disease, resulting in lifelong blood transfusions, iron overload, and associated complications. Betibeglogene autotemcel (beti-cel) gene therapy uses autologous haematopoietic stem and progenitor cells (HSPCs) transduced with BB305 lentiviral vector to enable transfusion independence.<h3>Methods</h3>HGB-212 was a non-randomised, multicentre, single-arm, open-label, phase 3 study of beti-cel in patients with TDT conducted at eight centres in France, Germany, Greece, Italy, the UK, and the USA. Patients with β<sup>0</sup>/β<sup>0</sup>, β<sup>0</sup>/β<sup>+IVS-I-110</sup>, or β<sup>+IVS-I-110</sup>/β<sup>+IVS-I-110</sup> genotypes, clinically stable TDT, and a transfusion history of at least 100 mL/kg per year of packed red blood cells (pRBCs) or at least eight transfusions of pRBCs per year in the 2 years before enrolment were eligible for participation. After undergoing HSPC mobilisation and busulfan-based, pharmacokinetic-adjusted myeloablative conditioning, patients were infused with beti-cel and followed up for 24 months. The primary efficacy outcome was transfusion independence, defined as weighted average haemoglobin level of 9 g/dL or above without pRBC transfusions for 12 or more months. The primary outcome was measured in all patients who received an infusion of beti-cel (transplant population); safety was evaluated in all patients who initiated study treatment (intention-to-treat population). Patients were eligible to enrol in the ongoing 13-year long-term follow-up study (for a total of 15 years), LTF-303 (registered at <span><span>ClinicalTrials.gov</span><svg aria-label=\"Opens in new window\" focusable=\"false\" height=\"20\" viewbox=\"0 0 8 8\"><path d=\"M1.12949 2.1072V1H7V6.85795H5.89111V2.90281L0.784057 8L0 7.21635L5.11902 2.1072H1.12949Z\"></path></svg></span>, <span><span>NCT02633943</span><svg aria-label=\"Opens in new window\" focusable=\"false\" height=\"20\" viewbox=\"0 0 8 8\"><path d=\"M1.12949 2.1072V1H7V6.85795H5.89111V2.90281L0.784057 8L0 7.21635L5.11902 2.1072H1.12949Z\"></path></svg></span>). This trial, HGB-212, was registered at <span><span>ClinicalTrials.gov</span><svg aria-label=\"Opens in new window\" focusable=\"false\" height=\"20\" viewbox=\"0 0 8 8\"><path d=\"M1.12949 2.1072V1H7V6.85795H5.89111V2.90281L0.784057 8L0 7.21635L5.11902 2.1072H1.12949Z\"></path></svg></span> (<span><span>NCT03207009</span><svg aria-label=\"Opens in new window\" focusable=\"false\" height=\"20\" viewbox=\"0 0 8 8\"><path d=\"M1.12949 2.1072V1H7V6.85795H5.89111V2.90281L0.784057 8L0 7.21635L5.11902 2.1072H1.12949Z\"></path></svg></span>), and is complete.<h3>Findings</h3>From June 8, 2017, to March 12, 2020, 20 patients were screened for eligibility. One patient was ineligible and one withdrew consent before HSPC mobilisation and myeloablative conditioning. Of the 18 patients who received beti-cel, ten (56%) were male and eight (44%) were female; 13 (72%) were younger than 18 years at the time of informed consent, and five (28%) were older than 18 years. 12 (67%) patients had β<sup>0</sup>/β<sup>0</sup> genotypes, three (17%) had β<sup>0</sup>/ β<sup>+IVS-I-110</sup>, and three (17%) had β<sup>+IVS-I-110</sup>/β<sup>+IVS-I-110</sup>. As of Jan 30, 2023, all patients enrolled in the long-term follow-up study and the median follow-up was 47·9 months (range 23·8–59·0). All 18 patients were evaluable for transfusion independence, with 16 (89%) of 18 reaching and maintaining transfusion independence to last follow=up (estimated effect size 89·9% [95% CI 65·3–98·6]). All patients had at least one adverse event after beti-cel infusion. There were no serious adverse events considered to be related to beti-cel, and no deaths.<h3>Interpretation</h3>These data demonstrate that beti-cel can allow patients with genotypes that cause severe β-thalassaemia (β<sup>0</sup>/β<sup>0</sup>, β<sup>0</sup>/β<sup>+IVS-I-110</sup>, or β<sup>+IVS-I-110</sup>/β<sup>+IVS-I-110</sup>) to reach transfusion independence. Beti-cel offers the potential to attain near-normal haemoglobin levels for those with severe forms of TDT, and a potentially curative option without the risks and limitations of allogeneic HSPC transplantation. Patients are being followed up for a total of 15 years to assess the durability of transfusion independence and long-term safety profile of beti-cel.<h3>Funding</h3>Bluebird Bio, Somerville, MA, USA.","PeriodicalId":22898,"journal":{"name":"The Lancet","volume":"1 1","pages":""},"PeriodicalIF":0.0000,"publicationDate":"2024-11-08","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"Betibeglogene autotemcel gene therapy in patients with transfusion-dependent, severe genotype β-thalassaemia (HGB-212): a non-randomised, multicentre, single-arm, open-label, single-dose, phase 3 trial\",\"authors\":\"Janet L Kwiatkowski, Mark C Walters, Suradej Hongeng, Evangelia Yannaki, Andreas E Kulozik, Joachim B Kunz, Martin G Sauer, Adrian J Thrasher, Isabelle Thuret, Ashutosh Lal, Ge Tao, Shamshad Ali, Himal L Thakar, Heidi Elliot, Ankit Lodaya, Ji Lee, Richard A Colvin, Franco Locatelli, Alexis A Thompson\",\"doi\":\"10.1016/s0140-6736(24)01884-1\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<h3>Background</h3>Transfusion-dependent β-thalassaemia (TDT) is a severe disease, resulting in lifelong blood transfusions, iron overload, and associated complications. Betibeglogene autotemcel (beti-cel) gene therapy uses autologous haematopoietic stem and progenitor cells (HSPCs) transduced with BB305 lentiviral vector to enable transfusion independence.<h3>Methods</h3>HGB-212 was a non-randomised, multicentre, single-arm, open-label, phase 3 study of beti-cel in patients with TDT conducted at eight centres in France, Germany, Greece, Italy, the UK, and the USA. Patients with β<sup>0</sup>/β<sup>0</sup>, β<sup>0</sup>/β<sup>+IVS-I-110</sup>, or β<sup>+IVS-I-110</sup>/β<sup>+IVS-I-110</sup> genotypes, clinically stable TDT, and a transfusion history of at least 100 mL/kg per year of packed red blood cells (pRBCs) or at least eight transfusions of pRBCs per year in the 2 years before enrolment were eligible for participation. After undergoing HSPC mobilisation and busulfan-based, pharmacokinetic-adjusted myeloablative conditioning, patients were infused with beti-cel and followed up for 24 months. 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引用次数: 0

摘要

背景输血依赖型β-地中海贫血(TDT)是一种严重疾病,会导致终身输血、铁超载和相关并发症。Betibeglogene autotemcel(beti-cel)基因疗法使用BB305慢病毒载体转导的自体造血干细胞和祖细胞(HSPCs)来实现输血独立。方法HGB-212是一项非随机、多中心、单臂、开放标签的3期研究,在法国、德国、希腊、意大利、英国和美国的8个中心进行。患者基因型为β0/β0、β0/β+IVS-I-110 或 β+IVS-I-110/β+IVS-I-110/β+IVS-I-110 ,TDT 临床病情稳定,每年至少输注 100 毫升/千克包装红细胞(pRBCs),或在入组前 2 年内每年至少输注 8 次包装红细胞(pRBCs)。患者在接受HSPC动员和基于丁硫、药代动力学调整的髓脱落调理后,输注beti-cel,并随访24个月。主要疗效指标是输血独立性,即加权平均血红蛋白水平达到或超过 9 g/dL 且 12 个月或更长时间内未输注 pRBC。主要疗效在所有接受贝特类药物输注的患者(移植人群)中进行测定;安全性在所有开始接受研究治疗的患者(意向治疗人群)中进行评估。患者有资格参加正在进行的13年长期随访研究(共计15年)LTF-303(已在ClinicalTrials.gov注册,NCT02633943)。这项名为HGB-212的试验已在ClinicalTrials.gov(NCT03207009)上注册,并已完成。研究结果从2017年6月8日至2020年3月12日,共筛选出20名符合条件的患者。1名患者不符合条件,1名患者在HSPC动员和髓鞘脱落调理前撤回同意书。在接受贝特细胞治疗的18名患者中,10名(56%)为男性,8名(44%)为女性;13名(72%)在知情同意时年龄小于18岁,5名(28%)年龄大于18岁。12名患者(67%)的基因型为β0/β0,3名患者(17%)的基因型为β0/β+IVS-I-110,3名患者(17%)的基因型为β+IVS-I-110/β+IVS-I-110。截至 2023 年 1 月 30 日,所有患者都参加了长期随访研究,中位随访时间为 47-9 个月(23-8-59-0)。所有18名患者均可接受输血独立评估,其中16名患者(89%)在最后一次随访时达到并保持了输血独立(估计效应大小为89-9% [95% CI 65-3-98-6])。所有患者在输注贝特类药物后都至少出现过一次不良反应。这些数据表明,贝特类凝胶可使基因型为重型β地中海贫血(β0/β0、β0/β+IVS-I-110或β+IVS-I-110/β+IVS-I-110)的患者实现输血独立。Beti-cel为严重TDT患者提供了达到接近正常血红蛋白水平的可能性,同时也是一种潜在的治疗方案,没有异体HSPC移植的风险和局限性。目前正在对患者进行长达15年的随访,以评估输血独立的持久性和beti-cel的长期安全性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Betibeglogene autotemcel gene therapy in patients with transfusion-dependent, severe genotype β-thalassaemia (HGB-212): a non-randomised, multicentre, single-arm, open-label, single-dose, phase 3 trial

Background

Transfusion-dependent β-thalassaemia (TDT) is a severe disease, resulting in lifelong blood transfusions, iron overload, and associated complications. Betibeglogene autotemcel (beti-cel) gene therapy uses autologous haematopoietic stem and progenitor cells (HSPCs) transduced with BB305 lentiviral vector to enable transfusion independence.

Methods

HGB-212 was a non-randomised, multicentre, single-arm, open-label, phase 3 study of beti-cel in patients with TDT conducted at eight centres in France, Germany, Greece, Italy, the UK, and the USA. Patients with β00, β0+IVS-I-110, or β+IVS-I-110+IVS-I-110 genotypes, clinically stable TDT, and a transfusion history of at least 100 mL/kg per year of packed red blood cells (pRBCs) or at least eight transfusions of pRBCs per year in the 2 years before enrolment were eligible for participation. After undergoing HSPC mobilisation and busulfan-based, pharmacokinetic-adjusted myeloablative conditioning, patients were infused with beti-cel and followed up for 24 months. The primary efficacy outcome was transfusion independence, defined as weighted average haemoglobin level of 9 g/dL or above without pRBC transfusions for 12 or more months. The primary outcome was measured in all patients who received an infusion of beti-cel (transplant population); safety was evaluated in all patients who initiated study treatment (intention-to-treat population). Patients were eligible to enrol in the ongoing 13-year long-term follow-up study (for a total of 15 years), LTF-303 (registered at ClinicalTrials.gov, NCT02633943). This trial, HGB-212, was registered at ClinicalTrials.gov (NCT03207009), and is complete.

Findings

From June 8, 2017, to March 12, 2020, 20 patients were screened for eligibility. One patient was ineligible and one withdrew consent before HSPC mobilisation and myeloablative conditioning. Of the 18 patients who received beti-cel, ten (56%) were male and eight (44%) were female; 13 (72%) were younger than 18 years at the time of informed consent, and five (28%) were older than 18 years. 12 (67%) patients had β00 genotypes, three (17%) had β0/ β+IVS-I-110, and three (17%) had β+IVS-I-110+IVS-I-110. As of Jan 30, 2023, all patients enrolled in the long-term follow-up study and the median follow-up was 47·9 months (range 23·8–59·0). All 18 patients were evaluable for transfusion independence, with 16 (89%) of 18 reaching and maintaining transfusion independence to last follow=up (estimated effect size 89·9% [95% CI 65·3–98·6]). All patients had at least one adverse event after beti-cel infusion. There were no serious adverse events considered to be related to beti-cel, and no deaths.

Interpretation

These data demonstrate that beti-cel can allow patients with genotypes that cause severe β-thalassaemia (β00, β0+IVS-I-110, or β+IVS-I-110+IVS-I-110) to reach transfusion independence. Beti-cel offers the potential to attain near-normal haemoglobin levels for those with severe forms of TDT, and a potentially curative option without the risks and limitations of allogeneic HSPC transplantation. Patients are being followed up for a total of 15 years to assess the durability of transfusion independence and long-term safety profile of beti-cel.

Funding

Bluebird Bio, Somerville, MA, USA.
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