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PHRM30002_2025_SM2 PHRM30002 MST 2- Requires Respondus LockDown Browser

Single choice

What is the primary mechanism of mercury-induced neurotoxicity?

Options
A.Mercury disrupts GTP binding to microtubules, leading to impaired axonal transport and synaptic transmission.
B.Mercury prevents the assembly of beta tubulin subunits, leading to destabilization of microtubules and dendritic atrophy.
C.Mercury enhances GTP binding to microtubules, resulting in hyperactive axonal growth and excessive synaptic signalling.
D.Mercury promotes the assembly of beta tubulin subunits, causing microtubule hyperstability and increased neuronal excitability.
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Step-by-Step Analysis
Mercury neurotoxicity primarily stems from its high affinity for sulfhydryl (thiol) groups in proteins, including tubulin, which interferes with the normal polymerization of microtubules in neurons. This disruption impairs axonal transport and structural integrity of dendrites, contributing to neurotoxic effects. Option 1: 'Mercury disrupts GTP binding......Login to view full explanation

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