Tau variants in FUS-mediated ALS
NINDS - National Institute of Neurological Disorders and Stroke
About This Grant
Amyotrophic lateral sclerosis (ALS) is a neurodegenerative disease with no effective treatment. Among the identified ALS-causing genes, several encode RNA binding proteins including FUsed in Sarcoma (FUS). Mutant FUS protein is mis-localized to the cytoplasm where it forms inclusions, a pathological hallmark of ALS. We and others have studied the FUS protein under physiological and pathological conditions in various models. Notably, we recently identified six individuals in an extended ALS kindred who carry the ALS-linked FUS R521G mutation but remain free of ALS well into their 60s and beyond (Unaffected Mutation Carriers, UMCs). We generated induced pluripotent stem cell (iPSC) lines from four UMCs, six FUS ALS patients, and four healthy controls, differentiated them to motor neurons (iMNs), and measured their electrophysiological properties. FUS ALS iMNs demonstrated disease-related hyperexcitability, whereas UMC and control iMNs displayed normal electrophysiological properties. Using an integrated analysis of whole genome sequencing and RNA-Seq data, we identified a cluster of variants in the 3’ untranslated region (3’-UTR) of the microtubule- associated protein tau (MAPT) gene. This set of linked variants was highly expressed in all UMCs but was absent in all ALS patients. More excitingly, an isogenic line with these variants incorporated into MAPT 3’-UTR of an ALS iPSC showed normal electrophysiological properties, supporting that these variants are critical to mitigating the hyperexcitability phenotype. iMNs from FUS ALS patients had increased Tau protein levels as compared to those from UMCs with the MAPT variants. In addition, overexpression of Tau induced neuronal hyperexcitability whereas Tau knockdown restored neuronal excitability to normal. We thus hypothesize that the MAPT variants reduce Tau protein expression, mitigate iMN hyperexcitability, and ultimately protect UMCs from developing ALS. Three specific aims are designed to test the hypothesis. Aim 1 is to establish the causative role of the MAPT 3’-UTR variants in reducing the hyperexcitability phenotype. We will generate additional isogenic lines by introducing the wild-type MAPT allele to UMC iPSCs to solidify the causative role of the MAPT variants in determining ALS or UMC phenotypes. We will generate and characterize two isogenic lines carrying 4 rare variants or 10 common variants to delineate their contributions. Aim 2 is to determine how the FUS mutation increases Tau expression and alters other properties, and how the MAPT variants prevent these abnormalities. Aim 3 is to determine which ion channel or receptor is responsible for the ALS-related hyperexcitability phenotype, and to examine whether up- and down-regulation of Tau expression changes the specific ion channel or receptor activity. The proposed studies are highly innovative conceptually and technically. The results will provide insights into the mechanisms underlying the protective effects of the MAPT variants and identify potential novel therapeutic targets. This project has a broader impact beyond ALS since Tau plays a critical role in other neurodegenerative diseases.
Grant Summary
Tau variants in FUS-mediated ALS is a NINDS - National Institute of Neurological Disorders and Stroke grant providing up to $645K for university, nonprofit, healthcare org. Applications are due 2031-06-30 (open). Check eligibility and apply with FindGrants.
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Up to $645K
2031-06-30
- 1Confirm your organization is eligible for Tau variants in FUS-mediated ALS from NINDS - National Institute of Neurological Disorders and Stroke, checking organization type, location, and any population or project requirements.
- 2Gather the required documents and information, including your organization details, project plan, and budget figures.
- 3Draft your application narrative and budget addressing the funder's priorities and review criteria. FindGrants can draft each section for you to review and edit.
- 4Review every section against the requirements checklist, then export a submission-ready application pack and submit it to NINDS - National Institute of Neurological Disorders and Stroke before the deadline.
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Tau variants in FUS-mediated ALS: Frequently Asked Questions
Who is eligible for the Tau variants in FUS-mediated ALS?
Tau variants in FUS-mediated ALS is offered by NINDS - National Institute of Neurological Disorders and Stroke and is generally open to university, nonprofit, healthcare org. It is open to organizations nationwide unless the funder specifies otherwise. Review the specific eligibility terms before applying, since funders set their own requirements around organization type, location, and the population or project being served.
How much funding does the Tau variants in FUS-mediated ALS provide?
Tau variants in FUS-mediated ALS provides up to $645K per award from NINDS - National Institute of Neurological Disorders and Stroke. Actual award sizes depend on the scope of your project, available program funds, and the number of applicants, so build a budget that reflects realistic, allowable costs rather than the maximum figure.
When is the Tau variants in FUS-mediated ALS deadline?
Applications for Tau variants in FUS-mediated ALS are due 2031-06-30 (open). Because deadlines can change, verify the date with the funder, NINDS - National Institute of Neurological Disorders and Stroke, and give yourself enough time to prepare a complete, competitive application before the close date.
How do you apply for the Tau variants in FUS-mediated ALS?
To apply for Tau variants in FUS-mediated ALS, confirm your eligibility, gather the required documents, and prepare a narrative and budget that address the funder's priorities. FindGrants guides you step by step and can draft each section, then exports a submission-ready application pack for this grant from NINDS - National Institute of Neurological Disorders and Stroke.