Department of Protein Science, School of Engineering Sciences in Chemistry, Biotechnology and Health, KTH Royal Institute of Technology, Stockholm, Sweden.
Front Immunol. 2024 Aug 8;15:1437886. doi: 10.3389/fimmu.2024.1437886. eCollection 2024.
Heterozygous loss-of-function mutations in the gene are a common cause of frontotemporal dementia. Such mutations lead to decreased plasma and cerebrospinal fluid levels of progranulin (PGRN), a neurotrophic factor with lysosomal functions. Sortilin is a negative regulator of extracellular PGRN levels and has shown promise as a therapeutic target for frontotemporal dementia, enabling increased extracellular PGRN levels through inhibition of sortilin-mediated PGRN degradation. Here we report the development of a high-affinity sortilin-binding affibody-peptide fusion construct capable of increasing extracellular PGRN levels . By genetic fusion of a sortilin-binding affibody generated through phage display and a peptide derived from the progranulin C-terminus, an affinity protein (A3-PGRN15*) with 185-pM affinity for sortilin was obtained. Treating PGRN-secreting and sortilin-expressing human glioblastoma U-251 cells with the fusion protein increased extracellular PGRN levels up to 2.5-fold, with an EC value of 1.3 nM. Our results introduce A3-PGRN15* as a promising new agent with therapeutic potential for the treatment of frontotemporal dementia. Furthermore, the work highlights means to increase binding affinity through synergistic contribution from two orthogonal polypeptide units.
基因杂合性功能丧失突变是额颞叶痴呆的一个常见原因。此类突变导致颗粒蛋白前体(PGRN)的血浆和脑脊液水平降低,PGRN 是一种具有溶酶体功能的神经营养因子。分选连接蛋白是细胞外 PGRN 水平的负调节剂,已被证明是额颞叶痴呆的一种有前途的治疗靶点,通过抑制分选连接蛋白介导的 PGRN 降解,可增加细胞外 PGRN 水平。在这里,我们报告了一种高亲和力分选连接蛋白结合亲和体肽融合构建体的开发,该构建体能增加细胞外 PGRN 水平。通过噬菌体展示产生的分选连接蛋白结合亲和体与源自颗粒蛋白 C 末端的肽进行基因融合,获得了对分选连接蛋白具有 185-pM 亲和力的亲和蛋白(A3-PGRN15*)。用融合蛋白处理分泌 PGRN 和表达分选连接蛋白的人胶质母细胞瘤 U-251 细胞,可使细胞外 PGRN 水平增加高达 2.5 倍,EC 值为 1.3 nM。我们的研究结果表明,A3-PGRN15*是一种很有前途的新型药物,具有治疗额颞叶痴呆的潜力。此外,这项工作强调了通过两个正交多肽单元的协同贡献来提高结合亲和力的方法。
