# Transmission deficits in spinal muscular atrophy and a potential novel treatment

> **NIH NIH F31** · UNIVERSITY OF PITTSBURGH AT PITTSBURGH · 2020 · $34,958

## Abstract

Abstract
Spinal Muscular Atrophy (SMA) is the leading genetic cause of premature death in children. SMA patients
gradually succumb to muscle paralysis as a result of massive motor neuron degeneration. Patients with severe
and intermediate forms of SMA experience lifelong physical disability and markedly shorter lifespans, with
death as soon as one year (in severe patients). In Dec. 2016, the FDA approved the first and only treatment for
SMA, which utilizes intrathecally-administered antisense oligonucleotides (ASOs) upon SMA diagnosis, usually
after motor symptoms appear well into the disease progression. ASOs increase SMN (Survival of Motor
Neuron) protein expression, which is deleteriously low in SMA patients and is the underlying cause of motor
neuron degeneration. ASOs seem to improve motor function and lifespan in patients, but clinical data are still
being collected to conclusively determine ASO benefits in humans. Evaluation of ASO efficacy in SMA mouse
models support these clinical conjectures, however. Treated mice have improved motor function and longer
lifespans, though they remain weaker than healthy littermates and still succumb to eventual motor neuron
degeneration and premature death. This is likely because ASO therapy occurs well after the first deficits are
established, and central administration of ASO treatment may have reduced access to the peripheral
neuromuscular synapses. Without treatment, low levels of SMN produce severe neuromuscular defects that
result in up to 50% depression in neurotransmission in SMA model mice. Structural defects include reduced
calcium channel expression and clustering (MN cultures & SMA model mice) and fewer neurotransmitter
release sites (SMA model mice) in neuromuscular junctions. These deficits contribute to reduced calcium entry
into motor nerve terminals (SMA model zebrafish, preliminary data) and reduced calcium transients in growth
cones (MN cultures). Because neurotransmission is a calcium-triggered process, these reductions in calcium
channels and calcium entry likely explain transmission deficits in SMA model systems. We hypothesize that
defective calcium entry underlies reduced neurotransmission in SMA neuromuscular synapses, and that ASO
treatment incompletely rescues reduced neurotransmission. This lingering dysfunction ultimately leads to
muscular weakness, which precedes motor neuron degeneration. Therefore, an SMN-independent approach
that directly targets neuromuscular function by increasing neurotransmission would complement current
therapy. We propose to investigate a combination of ASOs (to prolong motor neuron degeneration and overall
survival) plus a calcium channel agonist combined with a potassium channel blocker (to increase
neurotransmission). We will evaluate these treatments by measuring 1) calcium entry using fluorescent
calcium imaging, 2) transmitter release using electrophysiology, and 3) motor function using strength assays.

## Key facts

- **NIH application ID:** 9881187
- **Project number:** 5F31NS106753-02
- **Recipient organization:** UNIVERSITY OF PITTSBURGH AT PITTSBURGH
- **Principal Investigator:** Kristine Ojala
- **Activity code:** F31 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2020
- **Award amount:** $34,958
- **Award type:** 5
- **Project period:** 2019-02-28 → 2020-09-30

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/9881187

## Citation

> US National Institutes of Health, RePORTER application 9881187, Transmission deficits in spinal muscular atrophy and a potential novel treatment (5F31NS106753-02). Retrieved via AI Analytics 2026-05-24 from https://api.ai-analytics.org/grant/nih/9881187. Licensed CC0.

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