Lentivirus-mediated gene therapy for Fabry disease: 5-year End-of-Study results from the Canadian FACTs trial

IF 6.8 1区医学 Q1 MEDICINE, RESEARCH & EXPERIMENTAL Clinical and Translational Medicine Pub Date : 2025-01-10 DOI:10.1002/ctm2.70073

Aneal Khan, Dwayne L. Barber, William M. McKillop, C. Anthony Rupar, Christiane Auray-Blais, Graeme Fraser, Daniel H. Fowler, Alexandra Berger, Ronan Foley, Armand Keating, Michael L. West, Jeffrey A. Medin

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Abstract

Background

Fabry disease is an X-linked lysosomal storage disorder due to a deficiency of α-galactosidase A (α-gal A) activity. Our goal was to correct the enzyme deficiency in Fabry patients by transferring the cDNA for α-gal A into their CD34+ hematopoietic stem/progenitor cells (HSPCs). Overexpression of α-gal A leads to secretion of the hydrolase; which can be taken up and used by uncorrected bystander cells. Gene-augmented HSPCs can circulate and thus provide sustained systemic correction. Interim results from this ‘first-in-the-world’ Canadian FACTs (Fabry Disease Clinical Research and Therapeutics) trial were published in 2021. Herein we report 5-year ‘End-of-Study’ results.

Methods

Five males with classical Fabry disease were treated. Their HSPCs were mobilized, enriched, and transduced with a recombinant lentivirus engineering expression of α-gal A. Autologous transduced cells were infused after conditioning with a nonmyeloablative, reduced dose, melphalan regimen. Safety monitoring was performed. α-Gal A activity was measured in plasma and peripheral blood (PB) leucocytes. Globotriaosylceramide (Gb3) and lyso-Gb3 levels in urine and plasma were assessed by mass spectrometry. qPCR assays measured vector copy number in PB leucocytes. Antibody titers were measured by ELISA. Body weight, blood pressure, urinary protein levels, eGFR, troponin levels, and LVMI were tracked.

Results

Four out of 5 patients went home the same day as their infusions; one was kept overnight for observation. Circulating α-gal A activity was observed at Day 6–8 in each patient following infusion and has remained durable for 5+ years. LV marking of peripheral blood cells has remained durable and polyclonal. All 5 patients were eligible to come off biweekly enzyme therapy; 3 patients did so. Plasma lyso-Gb3 was significantly lower in 4 of 5 patients. There was no sustained elevation of anti-α-gal A antibodies. Patient weight was stable in 4 of the 5 patients. All blood pressures were in the normal range. Kidney symptoms were stabilized in all patients.

Conclusions

This treatment was well tolerated as only two SAEs occurred (during the treatment phase) and only two AEs were reported since 2021. We demonstrate that this therapeutic approach has merit, is durable, and should be explored in a larger clinical trial.

Highlights

This was the first gene therapy clinical trial to be completed for Fabry disease.
There were no adverse events of any grade attributable to the cellular gene therapy intervention or host conditioning throughout the follow-up interval of 5 years.
After reduced-intensity melphalan treatment, all patients engrafted their autologous modified α-gal A expressing cells.
All patients synthesized and secreted α-gal A throughout the course of the study.
Expression of α-gal A resulted in a decrease in plasma lyso-Gb3 in four of five patients and stabilization of kidney symptoms in all patients.

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慢病毒介导的法布里病基因治疗：加拿大FACTs试验的5年研究结束结果

背景：Fabry病是一种由α-半乳糖苷酶a （α-gal a）活性缺乏引起的x连锁溶酶体贮积症。我们的目标是通过将α-半胱氨酸A的cDNA转移到他们的CD34+造血干细胞/祖细胞（HSPCs）中来纠正Fabry患者的酶缺乏症。α-gal A过表达导致水解酶分泌；它可以被未纠正的旁观者细胞吸收和利用。基因增强的HSPCs可以循环，从而提供持续的全身纠正。这项“世界首创”的加拿大法布里病临床研究和治疗试验的中期结果于2021年公布。在此，我们报告了5年的“研究结束”结果。方法：对5例男性经典法布里病进行治疗。他们的HSPCs被动员、富集，并通过α-gal a的重组慢病毒工程表达进行转导。将自身转导的细胞在非清髓性、减少剂量的melphalan方案中灌注。进行安全监测。测定α-Gal A在血浆和外周血白细胞中的活性。用质谱法测定尿液和血浆中球三烷基神经酰胺（Gb3）和溶索-Gb3水平。qPCR检测PB白细胞的载体拷贝数。ELISA法检测抗体滴度。追踪体重、血压、尿蛋白水平、eGFR、肌钙蛋白水平和LVMI。结果：5例患者中有4例在输液当天回家；其中一人留院观察。在每位患者输注后第6-8天观察到循环α-gal A活性，并持续5年以上。外周血细胞的LV标记具有持久性和多克隆性。所有5例患者均符合停止双周酶治疗的条件；3名患者接受了治疗。5例患者中有4例血浆溶酶- gb3明显降低。抗α-gal A抗体无持续升高。5例患者中4例体重稳定。所有的血压都在正常范围内。所有患者肾脏症状均稳定。结论：该治疗耐受性良好，仅发生2例急性急性发作（在治疗阶段），自2021年以来仅报告了2例ae。我们证明这种治疗方法有优点，是持久的，应该在更大的临床试验中探索。亮点：这是第一个完成的法布里病基因治疗临床试验。在5年的随访期间，没有任何级别的不良事件可归因于细胞基因治疗干预或宿主调节。在降低强度的美法仑治疗后，所有患者都移植了自体修饰的表达α-gal A的细胞。所有患者在整个研究过程中合成并分泌α-半乳糖A。α-gal A的表达导致5例患者中4例血浆溶酶- gb3水平下降，所有患者肾脏症状稳定。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Clinical and Translational Medicine Multiple-

CiteScore

15.90

自引率

1.90%

发文量

450

审稿时长

4 weeks

期刊介绍： Clinical and Translational Medicine (CTM) is an international, peer-reviewed, open-access journal dedicated to accelerating the translation of preclinical research into clinical applications and fostering communication between basic and clinical scientists. It highlights the clinical potential and application of various fields including biotechnologies, biomaterials, bioengineering, biomarkers, molecular medicine, omics science, bioinformatics, immunology, molecular imaging, drug discovery, regulation, and health policy. With a focus on the bench-to-bedside approach, CTM prioritizes studies and clinical observations that generate hypotheses relevant to patients and diseases, guiding investigations in cellular and molecular medicine. The journal encourages submissions from clinicians, researchers, policymakers, and industry professionals.