Co-transmission MCQs With Answer

Co-transmission MCQs With Answer

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Introduction: Co-transmission is the phenomenon where a single neuron releases two or more chemical messengers—classical neurotransmitters, neuropeptides, or ATP—affecting synaptic transmission and neuromodulation. For B. Pharm students, understanding co-transmission is essential for pharmacology, drug design and therapeutic strategies, since co-release alters receptor targets, synaptic plasticity and drug responses. Key concepts include co-release versus co-transmission, vesicle types (small clear vesicles vs dense-core vesicles), vesicular transporters (VGLUT, VMAT, VAChT, VGAT), and examples such as dopamine–glutamate and GABA–glycine co-release. This topic links molecular mechanisms to clinical implications in neuropsychiatric and pain treatments. Now let’s test your knowledge with 30 MCQs on this topic.

Q1. What does “co-transmission” primarily describe in neuroscience?

  • The release of a single neurotransmitter only
  • Simultaneous release of multiple chemical messengers from one neuron
  • Electrical coupling between two neurons
  • Long-term potentiation at excitatory synapses

Correct Answer: Simultaneous release of multiple chemical messengers from one neuron

Q2. Which term specifically refers to release of different transmitters from the same synaptic vesicle?

  • Co-transmission
  • Co-release
  • Autocrine signaling
  • Paracrine signaling

Correct Answer: Co-release

Q3. Which vesicle type typically contains neuropeptides rather than classical small-molecule neurotransmitters?

  • Small clear synaptic vesicles
  • Dense-core vesicles
  • Endosomes
  • Exosomes

Correct Answer: Dense-core vesicles

Q4. Which vesicular transporter is responsible for loading glutamate into synaptic vesicles?

  • VMAT
  • VGLUT
  • VGAT
  • VAChT

Correct Answer: VGLUT

Q5. Co-transmission involving a classical neurotransmitter and a neuropeptide commonly shows which release difference?

  • Neuropeptides are released at lower frequency than classical transmitters
  • Neuropeptides are released only after high-frequency stimulation
  • Classical transmitters require more Ca2+ than peptides for release
  • Peptides are immediately reuptaken like monoamines

Correct Answer: Neuropeptides are released only after high-frequency stimulation

Q6. Which of the following is an example of co-transmission reported in midbrain neurons?

  • Dopamine and glutamate co-release
  • Acetylcholine and glycine co-release
  • Serotonin and ATP co-release in cerebellum
  • Norepinephrine and GABA co-release in retina

Correct Answer: Dopamine and glutamate co-release

Q7. Vesicular synergy describes which phenomenon?

  • Competition between vesicles for docking sites
  • One transmitter’s vesicular uptake enhancing uptake of another transmitter
  • Vesicle fusion preventing subsequent release
  • Loss of vesicle proton gradient due to reuptake

Correct Answer: One transmitter’s vesicular uptake enhancing uptake of another transmitter

Q8. Which transporter loads monoamines into synaptic vesicles?

  • VGLUT1
  • VGAT
  • VMAT2
  • EAAT2

Correct Answer: VMAT2

Q9. Which experimental technique is commonly used to directly visualize co-localization of transmitters in terminals?

  • Patch-clamp electrophysiology only
  • Immunohistochemistry with confocal microscopy
  • Behavioral assays
  • Microdialysis without histology

Correct Answer: Immunohistochemistry with confocal microscopy

Q10. ATP often acts as a co-transmitter. Which receptor family mediates rapid ATP signaling?

  • GABA-A receptors
  • Ionotropic P2X receptors
  • Metabotropic muscarinic receptors
  • Tyrosine kinase receptors

Correct Answer: Ionotropic P2X receptors

Q11. In co-transmission, how do neuropeptides typically differ from small-molecule transmitters in termination of action?

  • Neuropeptides are removed by high-affinity transporters
  • Neuropeptides are degraded extracellularly by peptidases
  • Neuropeptides are rapidly reuptaken like glutamate
  • Neuropeptides are endocytosed by postsynaptic neurons

Correct Answer: Neuropeptides are degraded extracellularly by peptidases

Q12. Which pharmacological agent blocks vesicular monoamine transporters and affects co-transmission of monoamines?

  • Reserpine
  • Cocaine
  • Bicuculline

Correct Answer: Reserpine

Q13. Co-transmission can alter drug responses because:

  • Only one transmitter is ever pharmacologically active
  • Multiple co-released messengers can target different receptor classes
  • Co-transmission prevents receptor activation
  • It makes synapses electrically silent

Correct Answer: Multiple co-released messengers can target different receptor classes

Q14. Which pair is a classic example of inhibitory co-release in the spinal cord?

  • Glutamate and dopamine
  • GABA and glycine
  • Serotonin and acetylcholine
  • ATP and substance P

Correct Answer: GABA and glycine

Q15. Which property of dense-core vesicles distinguishes their release compared to small clear vesicles?

  • Dense-core vesicles release at active zones only
  • Dense-core vesicle release is less dependent on intracellular Ca2+
  • Dense-core vesicle release often requires higher-frequency stimulation and broader Ca2+ influx
  • Dense-core vesicles contain only classical neurotransmitters

Correct Answer: Dense-core vesicle release often requires higher-frequency stimulation and broader Ca2+ influx

Q16. Which receptor type mediates fast ionotropic glutamatergic transmission often modulated by co-transmitters?

  • Metabotropic GABA-B receptors
  • NMDA and AMPA receptors
  • Muscarinic acetylcholine receptors
  • Dopamine D2 receptors

Correct Answer: NMDA and AMPA receptors

Q17. Which of the following best explains how co-transmission contributes to synaptic plasticity?

  • Co-transmission makes synapses static and unchangeable
  • Different co-released agents activate distinct signaling cascades that modulate receptor trafficking and gene expression
  • Co-transmission reduces postsynaptic receptor sensitivity permanently
  • Co-transmission solely increases vesicle recycling speed

Correct Answer: Different co-released agents activate distinct signaling cascades that modulate receptor trafficking and gene expression

Q18. Which technique can demonstrate functional co-release by measuring postsynaptic currents from identified receptors?

  • Western blotting
  • Patch-clamp electrophysiology with pharmacological blockers
  • Genome sequencing
  • Ultracentrifugation

Correct Answer: Patch-clamp electrophysiology with pharmacological blockers

Q19. Substance P is commonly co-released with which classical transmitter in nociceptive pathways?

  • GABA
  • Glutamate
  • Glycine
  • Acetylcholine

Correct Answer: Glutamate

Q20. Which statement about co-transmission and drug targeting is true?

  • Drugs targeting one receptor type can fully predict therapeutic outcome without considering co-transmitters
  • Co-transmission can create off-target effects via secondary receptor systems, affecting efficacy and side effects
  • Co-transmission only matters in invertebrates
  • Co-transmission prevents any pharmacological modulation

Correct Answer: Co-transmission can create off-target effects via secondary receptor systems, affecting efficacy and side effects

Q21. Which transporter is responsible for loading GABA into synaptic vesicles?

  • VGLUT2
  • VGAT (also called VIAAT)
  • VAChT
  • NET

Correct Answer: VGAT (also called VIAAT)

Q22. Which of the following is a likely consequence when a neuron co-releases an excitatory transmitter and a peptide neuromodulator?

  • Immediate short-term excitation only, with no lasting change
  • Fast postsynaptic excitation combined with slower modulatory effects that alter receptor sensitivity or gene expression
  • Complete inhibition of synaptic transmission
  • Peptide prevents any receptor binding

Correct Answer: Fast postsynaptic excitation combined with slower modulatory effects that alter receptor sensitivity or gene expression

Q23. Which molecule is NOT typically considered a classical neurotransmitter co-released with peptides?

  • Glutamate
  • Dopamine
  • Neuropeptide Y
  • GABA

Correct Answer: Neuropeptide Y

Q24. How does co-release of glutamate with dopamine in mesencephalic neurons influence signaling?

  • It only inhibits postsynaptic targets
  • It allows rapid excitatory signaling via glutamate and modulatory dopaminergic signaling over longer timescales
  • It prevents dopamine synthesis
  • It causes vesicles to shrink

Correct Answer: It allows rapid excitatory signaling via glutamate and modulatory dopaminergic signaling over longer timescales

Q25. Which pharmacological approach can help isolate peptide-mediated effects in co-transmission studies?

  • Using selective antagonists for peptide receptors or inhibiting peptidases
  • Blocking all ion channels nonspecifically
  • Removing extracellular Ca2+ only
  • Using electrical stimulation without blockers

Correct Answer: Using selective antagonists for peptide receptors or inhibiting peptidases

Q26. Which statement about vesicular proton gradient is relevant to co-transmission?

  • Vesicular proton gradient has no role in transmitter uptake
  • Proton gradient drives uptake of many transmitters via vesicular transporters, influencing co-packaging
  • Proton gradient only affects peptide synthesis
  • Proton gradient is irrelevant to VMAT function

Correct Answer: Proton gradient drives uptake of many transmitters via vesicular transporters, influencing co-packaging

Q27. Which clinical area might benefit from understanding co-transmission for better drug design?

  • Neuropsychiatric disorders like depression and schizophrenia
  • Only dermatological conditions
  • Bone fracture healing exclusively
  • Hair growth regulation only

Correct Answer: Neuropsychiatric disorders like depression and schizophrenia

Q28. Which evidence supports the existence of co-release rather than sequential release?

  • Distinct postsynaptic effects that cannot occur simultaneously
  • Immunogold electron microscopy showing two transmitters in the same vesicle
  • Behavioral changes without synaptic recordings
  • Absence of vesicular transporters

Correct Answer: Immunogold electron microscopy showing two transmitters in the same vesicle

Q29. Which is true regarding regulation of receptor responses during co-transmission?

  • Activation of metabotropic receptors by a co-transmitter cannot influence ionotropic receptor function
  • Metabotropic co-transmitters can modulate ionotropic receptor phosphorylation and trafficking
  • Ionotropic receptors are immune to intracellular signaling changes
  • Receptor regulation only occurs at the transcriptional level

Correct Answer: Metabotropic co-transmitters can modulate ionotropic receptor phosphorylation and trafficking

Q30. Which is a common method to pharmacologically separate co-released fast and slow signals in slice physiology?

  • Apply receptor-specific antagonists for fast ionotropic receptors and separate blockers or peptidase inhibitors for slower modulatory pathways
  • Use only tonic electrical stimulation
  • Ignore postsynaptic responses and record only presynaptic potentials
  • Apply broad-spectrum protease inhibitors only

Correct Answer: Apply receptor-specific antagonists for fast ionotropic receptors and separate blockers or peptidase inhibitors for slower modulatory pathways

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