Angelozzi Marco, Molin Arnaud, Karvande Anirudha, Fernández-Iglesias Ángela, Whipple Samantha, Bloh Andrew M, Lefebvre Véronique
J Clin Invest. 2025 Jan 16;135(2):e184929. doi: 10.1172/JCI184929.
Achondroplasia, the most prevalent short-stature disorder, is caused by missense variants overactivating the fibroblast growth factor receptor 3 (FGFR3). As current surgical and pharmaceutical treatments only partially improve some disease features, we sought to explore a genetic approach. We show that an enhancer located 29 kb upstream of mouse Fgfr3 (-29E) is sufficient to confer a transgenic mouse reporter with a domain of expression in cartilage matching that of Fgfr3. Its CRISPR/Cas9-mediated deletion in otherwise WT mice reduced Fgfr3 expression in this domain by half without causing adverse phenotypes. Importantly, its deletion in mice harboring the ortholog of the most common human achondroplasia variant largely normalized long bone and vertebral body growth, markedly reduced spinal canal and foramen magnum stenosis, and improved craniofacial defects. Consequently, mouse achondroplasia is no longer lethal, and adults are overall healthy. These findings, together with high conservation of -29E in humans, open a path to develop genetic therapies for people with achondroplasia.
软骨发育不全是最常见的身材矮小疾病,由错义变体过度激活成纤维细胞生长因子受体3(FGFR3)引起。由于目前的手术和药物治疗只能部分改善某些疾病特征,我们试图探索一种基因治疗方法。我们发现,位于小鼠Fgfr3上游29 kb处的一个增强子(-29E)足以使转基因小鼠报告基因在软骨中的表达域与Fgfr3的表达域相匹配。在野生型小鼠中,通过CRISPR/Cas9介导删除该增强子,该区域的Fgfr3表达减少了一半,且未引起不良表型。重要的是,在携带最常见人类软骨发育不全变体直系同源基因的小鼠中删除该增强子,可使长骨和椎体生长基本恢复正常,显著减轻椎管和枕大孔狭窄,并改善颅面缺陷。因此,小鼠软骨发育不全不再致命,成年小鼠总体健康。这些发现,再加上-29E在人类中的高度保守性,为开发针对软骨发育不全患者的基因疗法开辟了一条道路。
