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MSA Neurotransmitter Dysfunction

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Neurotransmitter Dysfunction in Multiple System Atrophy

Multiple System Atrophy (MSA) is characterized by widespread neurotransmitter dysfunction affecting multiple systems simultaneously. Unlike Parkinson's disease, where dopaminergic loss is primary, MSA involves early and severe damage to autonomic and non-dopaminergic neurotransmitter systems.

Overview

MSA results from progressive degeneration of neuronal populations producing:

  • Dopamine (substantia nigra, ventral tegmental area)
  • Noradrenaline (locus coeruleus)
  • Serotonin (raphe nuclei)
  • Acetylcholine (basal forebrain, pedunculopontine nucleus)
  • GABA (Purkinje cells, striatal interneurons)

This multi-system involvement explains the diverse clinical features beyond parkinsonism.

Autonomic Nervous System Failure

Sympathetic Noradrenergic Dysfunction

MSA produces severe sympathetic noradrenergic dysfunction that distinguishes it from other Parkinsonian disorders. Postganglionic sympathetic neurons undergo progressive degeneration, leading to:

  • Norepinephrine depletion: Loss of sympathetic nerve terminals in heart, blood vessels, and skin results in profound norepinephrine deficiency. This manifests as severe orthostatic hypotension due to inability to compensate for upright posture.
  • Cardiac denervation: [¹²³I]metaiodobenzylguanidine (MIBG) scintigraphy reveals complete cardiac sympathetic denervation in MSA, contrasting with partial denervation seen in Parkinson's disease.

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