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AUTOTAC: Autophagy-Targeting Chimera for Neurodegeneration

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AUTOTAC: Autophagy-Targeting Chimera for Neurodegeneration

Introduction

AUTOTAC (AUTophagy-TArgeting Chimera) represents a paradigm-shifting approach to targeted protein degradation that harnesses the autophagy-lysosome pathway to eliminate disease-causing proteins in neurodegenerative conditions[@lee2024]. Unlike traditional proteolysis-targeting chimeras (PROTACs) that rely on the ubiquitin-proteasome system, AUTOTACs directly engage the autophagy machinery by simultaneously binding both the target protein and the autophagy receptor p62/SQSTM1, enabling selective autophagic degradation of otherwise "undruggable" targets implicated in Alzheimer's disease, Parkinson's disease, and related disorders[@kim2024].

The development of AUTOTAC technology addresses a critical limitation in modern neurodegenerative disease therapeutics: the inability to pharmacologically target pathological protein aggregates that accumulate in these conditions. Small molecule inhibitors and antibodies have shown limited efficacy in clinical trials, largely because they cannot remove existing protein aggregates or modify the underlying disease state[@huang2024]. AUTOTACs offer a mechanistic solution by promoting the clearance of these aggregates through the cell's native autophagic machinery.

Background: Autophagy and Protein Clearance

The Autophagy-Lysosome Pathway


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