A 60-year-old man has resting tremor, pill-rolling movements, rigidity, and bradykinesia. Which of the following is most likely to be decreased in this man?

Dopamine neurons in the substantia nigra

GABA neurons in the caudate nucleus and putamen

Serotonin neurons in the raphe nuclei

Acetylcholine neurons in the forebrain

What are nitrergic neurons?

First-order neurons releasing nitric oxide.

Postganglionic neurons releasing nitric oxide.

Postganglionic neurons releasing substance P.

First-order neurons releasing calcitonin gene-related peptide.

Neurobiology of Addiction for FMGE: High-Yield Internal Medicine Lessons

Key Players - Brain's Chemical Crew

Dopamine (DA): The "pleasure chemical." Central to reward, motivation, and reinforcement. Key in drug-seeking.
Serotonin (5-HT): Modulates mood, sleep patterns, and impulsivity. Imbalances contribute to craving and relapse.
GABA (Gamma-aminobutyric acid): Primary inhibitory neurotransmitter. Reduces neuronal excitability; alcohol & sedatives potentiate its effects.
Glutamate: Main excitatory neurotransmitter. Involved in learning, memory, and addiction-related synaptic plasticity.
Endogenous Opioids (Endorphins, Enkephalins): Provide natural pain relief and euphoria. Opioid drugs mimic their action.

⭐ Dopamine release in the nucleus accumbens is a common final pathway for the rewarding effects of most drugs of abuse.

Neurobiology of Addiction: Opiate effects on VTA neurons

Reward Pathway - Pleasure's Superhighway

Mesolimbic Pathway: Key reward circuit; Dopamine (DA) is main neurotransmitter.
- Ventral Tegmental Area (VTA): DA synthesis.
- Nucleus Accumbens (NAc): Reward, pleasure.
- Prefrontal Cortex (PFC): Craving, compulsion.
Drug Hijack: All addictive drugs ↑ DA in NAc.
- Stimulants (cocaine, amphetamine): Block DA reuptake.
- Opioids: Disinhibit VTA DA neurons.
- Alcohol, Nicotine, Cannabis: ↑ DA release via various mechanisms.
NAc DA Receptors:
- D1: "Go" signal (promotes drug-seeking).
- D2: "No-Go" signal (signals satiety, inhibits seeking).

⭐ Chronic drug use leads to neuroadaptations like ↓ D2 receptor density in NAc, contributing to anhedonia and compulsive use.

Mesolimbic Reward Pathway Diagram 📌 VTA Nudges PFC with Dopamine (Ventral Tegmental Area, Nucleus Accumbens, Prefrontal Cortex, Dopamine).

Adaptation & Tolerance - The New Normal

Brain adapts to persistent drug presence, establishing a new "normal" state.
Mechanisms of Tolerance:
- Pharmacokinetic (Metabolic): ↑ drug metabolism (e.g., enzyme induction by alcohol, barbiturates).
- Pharmacodynamic (Cellular/Functional): Neuronal adaptation at the drug's site of action.
  - Receptor changes: Downregulation (e.g., for agonists like opioids) or upregulation (for antagonists).
  - Receptor desensitization: ↓ response despite binding.
  - Altered gene expression: e.g., CREB, ΔFosB.
Allostasis: Shift in hedonic set point; reward pathways become less sensitive (↓ reward), anti-reward systems become overactive.

⭐ ΔFosB is a highly stable transcription factor that accumulates with chronic drug exposure, mediating long-lasting neural and behavioral plasticity related to addiction.

Withdrawal Signs - Brain's Payback Time

Withdrawal: Brain's counter-adaptation when drug use ceases.

Neurochemical Basis: Opponent-process theory.
- Drug suppresses system → brain upregulates it.
- Cessation → unopposed hyperactivity (e.g., ↑ noradrenaline in opioid withdrawal).
Key Brain Regions:
- Locus Coeruleus (LC): Central to opioid withdrawal (↑ noradrenergic activity).
- Amygdala: Mediates anxiety, dysphoria.
Dependence Link:
- Physical: Body adapts; withdrawal upon cessation.
- Psychological: Compulsive use, craving.

⭐ Locus Coeruleus hyperactivity (↑ noradrenaline) is a major driver of opioid withdrawal symptoms like anxiety, tremors, and autonomic signs.

Craving & Relapse - Addiction's Echo

Key Brain Regions:
- Amygdala: Heightened cue-reactivity, emotional drug memories.
- Hippocampus: Context-dependent craving (people, places).
- Prefrontal Cortex (PFC): Impaired judgment, ↓ impulse control, relapse vulnerability.
Neurobiology:
- Glutamatergic dysregulation: Underpins intense, persistent craving.
- Incentive Salience: Cues acquire exaggerated motivational importance ("wanting").

Neurochemical neurocircuits in drug reward

⭐ The amygdala's heightened response to drug cues, coupled with impaired PFC control, forms a critical neurobiological loop driving craving and relapse.

High‑Yield Points - ⚡ Biggest Takeaways

The mesolimbic pathway (VTA to NAc, PFC) is central, mediating reward and motivation.

Dopamine (DA) is the primary neurotransmitter for pleasure, reinforcement, and salience.

Chronic substance use causes neuroadaptations, like ↓ D2 receptor density, leading to tolerance and withdrawal.

Glutamate system dysregulation, especially in PFC-NAc projections, drives craving and drug-seeking.

GABAergic system alterations contribute to withdrawal symptoms, anxiety, and loss of control.

Prefrontal Cortex (PFC) dysfunction results in impaired executive functions like decision-making and impulsivity.

Stress, acting via the HPA axis and CRF system, significantly increases relapse vulnerability and drug-seeking behavior.

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