What question did this study set out to answer?

The research aims to clarify how the loss of α2δ4 leads to photoreceptor degeneration by exploring synaptic dysfunction and mitochondrial health.

March 25, 2026Open Access

Dysfunction of α2δ4 leads to photoreceptor degeneration through disrupted synaptic mitochondria and calcium crosstalk

Key Points

The research aims to clarify how the loss of α2δ4 leads to photoreceptor degeneration by exploring synaptic dysfunction and mitochondrial health.
Used α2δ4 knockout mice to study degeneration onset and development.
Conducted proteomic analyses to assess changes in metabolic pathways.
Applied transmission electron microscopy to evaluate mitochondrial structure.
Performed immunohistochemistry to observe protein levels in retinas.
Photoreceptor degeneration onset was observed around 7 months in α2δ4 KO mice.
Diminished mitochondrial size and quantity in synaptic terminals of α2δ4 KO retinas were documented.
Downregulation of caloric and calcium-handling proteins was evident in the outer plexiform layer of retinas.

Abstract

Abstract Synaptic deficit has emerged as a key early hallmark for neurodegeneration in the visual pathway. The molecular pathway connecting local synaptic deficit with global cell dysfunction and death remains unclear. We have previously shown that α2δ4, an auxiliary subunit of the voltage-gated calcium channel, is targeted to photoreceptor synapses and required for their formation and function. Notably, α2δ4 mutations have been identified in patients with retinal dystrophy. However, how loss of synaptic α2δ4 leads to overall photoreceptor degeneration remains unknown. Here, we showed that α2δ4 loss in mice leads to a late onset photoreceptor degeneration around 7 months. Consistent with clinical observation, the progression of degeneration is minimal until 17 months, as supported by ERG, OCT imaging and histology. We found that Cav1.4 KO mice, where the calcium channel is missing, display an earlier degeneration onset than α2δ4 KO mice, where calcium channel is partially preserved. Proteomic studies revealed that tricarboxylic acid (TCA) cycle is significantly downregulated in the young α2δ4 KO retinas prior to degeneration. Transmission electron microscopy study demonstrated significant reduction in mitochondrial size and number in photoreceptor synaptic terminals, but not in the inner segment (IS), of the young α2δ4 KO retinas. Consistently, immunohistochemistry (IHC) studies showed significant reduction of mitochondrial proteins in the outer plexiform layer (OPL). IHC studies on ER and mitochondrial proteins revealed that ryanodine receptor (RyR2) and mitochondrial calcium uniporter (MCU) are downregulated in the OPL, but not in the IS. Together, our results propose a model where α2δ4 dysfunction impairs Cav1.4 channel activity, leading to disrupted calcium crosstalk among the plasma membrane, ER, and mitochondria, as well as mitochondrial damage and metabolic deficits. Importantly, our study underscores the critical role of synaptic calcium homeostasis and mitochondrial integrity in connecting the early stages of synaptic dysfunction with the later stages of cell degeneration.

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Cite This Study

Amieghemen et al. (Mon,) studied this question.

synapsesocial.com/papers/69c37afeb34aaaeb1a67d0a3 https://doi.org/https://doi.org/10.1038/s41419-026-08587-3

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