DAT blockade

What it is

Cocaine’s primary psychopharmacological mechanism. It’s a competitive, use-dependent triple monoamine reuptake inhibitor — highest affinity for DAT (dopamine transporter), then NET (norepinephrine transporter), then SERT (serotonin transporter).

Why it matters

DAT blockade → cytosolic DA accumulates → cannot be cleared → overflows into synaptic cleft → nucleus accumbens DA surge → euphoria
NET blockade → synaptic NE accumulation → sympathetic overdrive → tachycardia, hypertension, hyperthermia
SERT blockade → 5-HT accumulation → modulatory effect on mood, impulse control

The relative DAT:NET:SERT affinity explains cocaine’s profile: strong reward (DAT) + strong autonomic activation (NET) + modest serotonergic modulation (SERT).

Secondary mechanism: Na⁺ channel blockade

Cocaine also blocks voltage-gated sodium channels (local anaesthetic effect). This is mechanistically distinct from the DAT/NET/SERT effects and is the primary driver of cardiac arrhythmia risk.

Use-dependent kinetics: higher HR (from catecholamine surge) worsens Na⁺ blockade → pro-arrhythmic positive feedback loop.

Crash not driven by DAT per se

DAT itself doesn’t change acutely. The crash is driven by:

D2 autoreceptor-mediated vesicular redistribution → functional presynaptic deficit
PKC-mediated DAT dysregulation (cocaine blocks PKC phosphorylation of DAT → keeps DAT levels high → pulls DA out of synapse faster during recovery)
See Cocaine crash

Cocaine, Cocaine crash, Cardiovascular signatures, Cocaethylene

Vitals Knowledge Vault

Explorer

DAT blockade

DAT blockade

What it is

Why it matters

Secondary mechanism: Na⁺ channel blockade

Crash not driven by DAT per se

Graph View

Table of Contents

Backlinks

Vitals Knowledge Vault

Explorer

DAT blockade

DAT blockade

What it is

Why it matters

Secondary mechanism: Na⁺ channel blockade

Crash not driven by DAT per se

Related

Graph View

Table of Contents

Backlinks