遗传增强
干细胞
造血
病毒载体
生物
造血干细胞
基因
病毒学
医学
遗传学
重组DNA
作者
Pilar Puig-Serra,Ana Hinckley-Boned,María Tristán‐Manzano,Paula Rı́o,Raúl Torres,Sandra Rodríguez,Francisco Martı́n
出处
期刊:Human Gene Therapy
[Mary Ann Liebert, Inc.]
日期:2025-09-01
卷期号:36 (17-18): 1159-1172
被引量:1
标识
DOI:10.1177/10430342251372474
摘要
Seven cases of hematological malignancy reported in recipients of Skysona™ (elivaldogene autotemcel) have reignited long-standing concerns about insertional mutagenesis in lentiviral vector (LV)-based gene therapy. Here, we dissect the molecular and clinical evidence underlying these events, place them in the broader context of over 300 patients treated with LV-modified hematopoietic stem and progenitor cells (HSPCs), and review the real-world safety record of LV-engineered chimeric antigen receptor T cells. We show that cancers associated with Skysona are mechanistically linked to the use of a potent viral MNDU3 promoter probably combined with intensive conditioning and growth-factor support, whereas LV products employing weak or physiological promoters continue to display an excellent safety profile. With event rates <0.6/100 patient-years, lower than those after autologous HSCT, the therapeutic index of approved LV-HSPC advanced therapy medicinal products remains favorable. Ongoing optimization of vector design, conditioning, and long-term surveillance, together with emerging genome-editing platforms, is expected to further mitigate residual risk.
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