CUTS RNA Biosensor for the Real-Time Detection of TDP-43 Loss-of-Function

Author:

Xie Longxin123,Merjane Jessica13,Bergmann Cristian A13ORCID,Xu Jiazhen134,Hurtle Bryan135,Donnelly Christopher J13456ORCID

Affiliation:

1. Department of Neurobiology, University of Pittsburgh School of Medicine

2. School of Medicine, Tsinghua University

3. LiveLikeLou Center for ALS Research, University of Pittsburgh School of Medicine

4. Interdisciplinary Biomedical Graduate Program Cellular and Molecular Pathology, University of Pittsburgh

5. Center for Neuroscience at the University of Pittsburgh

6. Pittsburgh Institute for Neurodegeneration, University of Pittsburgh

Abstract

Given the mounting evidence implicating TDP-43 dysfunction in several neurodegenerative diseases, there is a pressing need to establish accessible tools to sense and quantify TDP-43 loss-of-function (LOF). These tools are crucial for assessing potential disease contributors and exploring therapeutic candidates in TDP-43 proteinopathies. Here, we develop a sensitive and accurate real-time sensor for TDP-43 LOF: the CUTS (CFTR UNC13A TDP-43 Loss-of-Function) system. This system combines previously reported cryptic exons regulated by TDP-43 with a reporter, enabling the tracking of TDP-43 LOF through live microscopy and RNA/protein-based assays. We demonstrate CUTS’ effectiveness in detecting LOF caused by TDP-43 mislocalization and RNA binding dysfunction, and pathological aggregation. Our results highlight the sensitivity and accuracy of the CUTS system in detecting and quantifying TDP-43 LOF, opening avenues to explore unknown TDP-43 interactions that regulate its function. In addition, by replacing the fluorescent tag in the CUTS system with the coding sequence for TDP-43, we show significant recovery of its function under TDP-43 LOF conditions, highlighting CUTS’ potential for self-regulating gene therapy applications. In summary, CUTS represents a versatile platform for evaluating TDP-43 LOF in real-time and advancing gene-replacement therapies in neurodegenerative diseases associated with TDP-43 dysfunction.

Publisher

eLife Sciences Publications, Ltd

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