Hong Lauren, Ye Tianzheng, Wang Tian Z, Srijay Divya, Liu Howard, Zhao Lin, Watson Rio, Vincoff Sophia, Chen Tianlai, Kholina Kseniia, Goel Shrey, DeLisa Matthew P, Chatterjee Pranam
Department of Biomedical Engineering, Duke University, Durham, NC, USA.
Robert F. Smith School of Chemical and Biomolecular Engineering, Cornell University, Ithaca, NY, USA.
Nat Commun. 2025 Apr 15;16(1):3555. doi: 10.1038/s41467-025-58872-6.
Dysregulated protein degradation via the ubiquitin-proteasomal pathway can induce numerous disease phenotypes, including cancer, neurodegeneration, and diabetes. While small molecule-based targeted protein degradation (TPD) and targeted protein stabilization (TPS) platforms can address this dysregulation, they rely on structured and stable binding pockets, which do not exist to classically "undruggable" targets. Here, we expand the TPS target space by engineering "deubiquibodies" (duAbs) via fusion of computationally-designed peptide binders to the catalytic domain of the potent OTUB1 deubiquitinase. In human cells, duAbs effectively stabilize exogenous and endogenous proteins in a DUB-dependent manner. Using protein language models to generate target-binding peptides, we engineer duAbs to conformationally diverse target proteins, including key tumor suppressor proteins p53 and WEE1, and heavily-disordered fusion oncoproteins, such as PAX3::FOXO1. We further encapsulate p53-targeting duAbs as mRNA in lipid nanoparticles and demonstrate effective intracellular delivery, p53 stabilization, and apoptosis activation, motivating further in vivo translation.
通过泛素-蛋白酶体途径的蛋白质降解失调可引发多种疾病表型,包括癌症、神经退行性疾病和糖尿病。虽然基于小分子的靶向蛋白质降解(TPD)和靶向蛋白质稳定化(TPS)平台可以解决这种失调问题,但它们依赖于结构化且稳定的结合口袋,而经典的“不可成药”靶点并不存在这样的口袋。在此,我们通过将计算设计的肽结合物与强效OTUB1去泛素酶的催化结构域融合来构建“去泛素抗体”(duAbs),从而扩展TPS的靶点空间。在人类细胞中,duAbs以一种依赖去泛素化酶的方式有效稳定外源和内源蛋白质。利用蛋白质语言模型生成靶向结合肽,我们构建了针对构象多样的靶蛋白的duAbs,包括关键肿瘤抑制蛋白p53和WEE1,以及高度无序的融合癌蛋白,如PAX3::FOXO1。我们进一步将靶向p53的duAbs作为mRNA封装在脂质纳米颗粒中,并证明其能有效实现细胞内递送、p53稳定化和凋亡激活,这为进一步的体内转化研究提供了动力。
Zotero 插件
