Huntingtin contains an ubiquitin-binding domain and regulates lysosomal targeting of mitochondrial and RNA-binding proteins.
Gianna M FoteVinay V EapenRyan G LimClinton YuLisa SalazarNicolette R McClureJharrayne McKnightThai B NguyenMarie C HeathAlice L LauMark A VillamilRicardo MiramontesIan H KratterSteven FinkbeinerJack C ReidlingJoao A PauloPeter KaiserLan HuangDavid E HousmanLeslie M ThompsonJoan S SteffanPublished in: Proceedings of the National Academy of Sciences of the United States of America (2024)
Understanding the normal function of the Huntingtin (HTT) protein is of significance in the design and implementation of therapeutic strategies for Huntington's disease (HD). Expansion of the CAG repeat in the HTT gene, encoding an expanded polyglutamine (polyQ) repeat within the HTT protein, causes HD and may compromise HTT's normal activity contributing to HD pathology. Here, we investigated the previously defined role of HTT in autophagy specifically through studying HTT's association with ubiquitin. We find that HTT interacts directly with ubiquitin in vitro. Tandem affinity purification was used to identify ubiquitinated and ubiquitin-associated proteins that copurify with a HTT N-terminal fragment under basal conditions. Copurification is enhanced by HTT polyQ expansion and reduced by mimicking HTT serine 421 phosphorylation. The identified HTT-interacting proteins include RNA-binding proteins (RBPs) involved in mRNA translation, proteins enriched in stress granules, the nuclear proteome, the defective ribosomal products (DRiPs) proteome and the brain-derived autophagosomal proteome. To determine whether the proteins interacting with HTT are autophagic targets, HTT knockout (KO) cells and immunoprecipitation of lysosomes were used to investigate autophagy in the absence of HTT. HTT KO was associated with reduced abundance of mitochondrial proteins in the lysosome, indicating a potential compromise in basal mitophagy, and increased lysosomal abundance of RBPs which may result from compensatory up-regulation of starvation-induced macroautophagy. We suggest HTT is critical for appropriate basal clearance of mitochondrial proteins and RBPs, hence reduced HTT proteostatic function with mutation may contribute to the neuropathology of HD.
Keyphrases
- oxidative stress
- cell death
- primary care
- small molecule
- healthcare
- endoplasmic reticulum stress
- multiple sclerosis
- drug delivery
- signaling pathway
- genome wide
- mass spectrometry
- gene expression
- amino acid
- functional connectivity
- induced apoptosis
- resting state
- wastewater treatment
- subarachnoid hemorrhage
- stress induced
- brain injury
- dna binding