# Mechanisms of Brain Manganese Homeostasis and Manganese-induced Parkinsonism

> **NIH NIH F99** · UNIVERSITY OF TEXAS AT AUSTIN · 2021 · $31,777

## Abstract

PROJECT SUMMARY
 Manganese (Mn) is an essential metal required for normal neural development and function; however,
at elevated levels, it is neurotoxic. Adults and children exposed to Mn through environmental or occupational
sources exhibit incurable motor and cognitive deficits. Mn overexposure is also associated with a-synuclein
aggregation and increased risk for developing Parkinson’s Disease. Mn presents an environmental health
concern, but the mechanisms of brain Mn homeostasis and the effects of Mn on brain function remain are not
fully understood. Upon overexposure, Mn builds up in the basal ganglia; however, the specific neuronal targets
of Mn are unclear. A major question in the field is whether Mn primarily effects catecholaminergic, particularly
dopaminergic, or GABAergic neurons in the basal ganglia. The proposed study aims to address this question
by selectively increasing Mn in catecholaminergic and GABAergic neurons which was not previously possible.
 Homozygous mutations in the Mn efflux transporter, SLC30A10, resulted in increased brain Mn and
Mn-induced parkinsonism. The current proposal leverages the discovery of SLC30A10 to understand the
mechanisms of brain Mn homeostasis and the effects of increased Mn in all or some neurons. Using full-body,
pan/neuronal/glial, liver-, and endoderm-specific Slc30a10 knockout mice, we discovered that under basal
conditions, brain Mn levels are primarily regulated by activity of SLC30A10 in the digestive system, while its
activity in the brain protected against neurotoxicity during Mn overexposure. This work established the
predominance of SLC30A10 in regulating brain Mn levels and presented a novel method for studying Mn
neurotoxicity. Subsequent work will use pan-neuronal/glial, catecholaminergic, and GABAergic Slc30a10
knockouts to selectively increase Mn in all, catecholaminergic, or GABAergic neurons. This study will test the
hypothesis that catecholaminergic, but not GABAergic, Slc30a10 knockouts mimic the phenotype observed in
pan-neuronal/glial knockouts. Proposed experiments will assay for Mn-induced changes in motor function,
neurodegeneration, neurotransmission, and gene expression under normal conditions and during an oral Mn
exposure relevant to human disease. The proposed study uses a multidisciplinary approach to further elucidate
how brain Mn homeostasis is regulated and how excess brain Mn impacts the catecholaminergic and
GABAergic systems. Proposed studies will be performed under the supervision of sponsor, Dr. Somshuvra
Mukhopadhyay and co-sponsor, Dr. Robert Messing at the University of Texas at Austin (UT Austin). Dr.
Mukhopadhyay is an expert in Mn toxicology, and Dr. Messing has a well-established career in neuroscience.
Their combined expertise and the collaborative environment at UT Austin are critical for the successful
completion of the proposed study and for providing the training and mentorship necessary for the applicant’s
goals of a career in academia and neur...

## Key facts

- **NIH application ID:** 10318895
- **Project number:** 1F99NS124142-01
- **Recipient organization:** UNIVERSITY OF TEXAS AT AUSTIN
- **Principal Investigator:** Cherish A Taylor
- **Activity code:** F99 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2021
- **Award amount:** $31,777
- **Award type:** 1
- **Project period:** 2021-07-01 → 2022-05-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/10318895

## Citation

> US National Institutes of Health, RePORTER application 10318895, Mechanisms of Brain Manganese Homeostasis and Manganese-induced Parkinsonism (1F99NS124142-01). Retrieved via AI Analytics 2026-05-22 from https://api.ai-analytics.org/grant/nih/10318895. Licensed CC0.

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