Pain

Question 1

What is pain?

Answer 1

An unpleasent sensory and emotional experience associated with real or potential tissue damage, or described in terms of tissue damage.

Question 2

What are the types of pain?

Answer 2

• Fast, stabbing pain: Result of Aδ fibres due to faster conduction velocities.
• Slow, burning pain: Result of C fibres with lower conduction velocities.

Question 3

What are the types of spinal cord neurones that respond to pain?

Answer 3

• Lamina I neurones only receive inputs from nociceptive fibres and only respond to pain so are known as narrow dynamic range (NDR) cells.
• Lamina V neurones receive inputs from both nociceptive and somoatosensory fibres so respond to touch at low stimuli intensities and pain at high intensities, so are know as wide dynamic range (WDR) cells.

Question 4

What are the main areas of the cortex that respond to pain?

Answer 4

• Somatosensory cortex: Involved with the sensory component of pain detection.
• Anterior cingulate cortex (ACC): Part of the limbic system involved with mediating emotional response to pain. Also involved with empathetic pain (pain caused by seeing other people in pain).
• Insula: Involved in homeostasis and so forms part of the homeostatic response to pain.

Question 5

Which areas of the brain give descending fibres involved in gate-control of pain?

Answer 5

• Periaqueductal grey (PAG)
• Raphe nucleus
• Nuclei of rostral medulla

Question 6

What is nociception?

Answer 6

The neural process of encoding noxious stimuli

Question 7

What channels are associated with noxious heat?

Answer 7

• TRPV1
• TRPV3
• Anoctamin 1 (ANO1)

Question 8

What channels are associated with noxious cold?

Answer 8

• TRPM8
• TRPA1

Question 9

What channels are assciated with protons?

Answer 9

• ASICs (acid-sensing ion channels)
• TRPV1
• TASKS

Question 10

What channels are associated with noxious mechanical stimuli?

Answer 10

Peizol 1/2 (possible TRPV4, ASICs)

Question 11

What channels are associated with noxious ATP?

Answer 11

P2X3

Question 12

What are external noxious stimuli?

Answer 12

• Mechanical
• Temperature
• Chemical

Question 13

What are internal noxious stimuli?

Answer 13

• ATP
• Bradykinins
• Acid

Question 14

What is the pain threshold for heat?

Answer 14

~42^o

Question 15

What are the types of pain sensitisations?

Answer 15

• Allodynia: Reduction in pain threshold
• Hyperalgesia: Same intensity of stimuli causes more pain

Question 16

What are the important sensitisation factors?

Answer 16

1. NGF
2. PGE₂

Question 17

What is the general process of pain sensitisation following tissue injury?

Answer 17

1. When stimulated, nociceptor endings themselves release pro-inflammatory substances such as CGRP (calcitonin gene-related product) and SP (substance P).
2. These chemical mediators cause vasodilation and increased permeability of blood vessels in area of injury.
3. These chemicals also cause degranulation of mast cells, releasing histamine amongst other pro-inflammatory mediators
4. Amongst these inflammatory mediators are prostaglandin E₂ (PGE₂) and nerve growth factor (NGF)
5. PGE₂ and NGF cause sensitisation of local tissues to pain.

Question 18

How does PGE₂ cause pain sensitisation?

Answer 18

1. EP₄ expression in nociceptive fibres is up-regulated during inflammation.
2. It is a GPCR that binds to PGE₂.
3. Associated α_s subunit activates PKA that phosphorylates ion channels such as Na_vs, decreasing firing thresholds for nociceptive fibres.

Question 19

What are the main classes of analgesics?

Answer 19

• NSAIDs
• Opioids

Question 20

What is the mechanism of action of NSAIDs?

Answer 20

Inhibits COX enzymes, and thus disrupts production of PGE₂ which is one of the main pain sensitisers.

Question 21

What are the functional differences between COX-1 and COX-2?

Answer 21

1. COX-1 is a constitutive enzyme present in most tissues and has basic homeostatic (‘house-keeping’) functions. E.g. producing prostaglandins involved in gastric cytoprotection, platelet aggregation…
2. COX-2 is mainly activated during inflammation by pro-inflammatory cytokines and produce pro-inflammatory prostaglandins.

Question 22

What are the consequences of inhibition of different types of COX enzymes?

Answer 22

• Inhibition of COX-2 causes main pharmacological effects.
• Inhibition of COX-1 causes main side-effects.

Question 23

How do NSAIDs inhibit COX?

Answer 23

They ener hydrophobic channel in enzyme and form H-bond with Arg120 residue and blocks entry of fatty acid substrate. Prevents catalysis of AA → PGG₂ step in PGE production only.

Question 24

What is the mechanism of action of aspirin?

Answer 24

Enters active site and acetylates Ser530 and irreversibly inactivates both COX-1 and COX-2.

Question 25

What are examples of NSAIDs?

Answer 25

- Aspirin - Ibuprofen - Paracetamol (no anti-inflammatory effects) - Celecoxib

Question 26

What are the side effects of NSAIDs?

Answer 26

1. GI bleeds: PGs have inhibitory effect on gastric acid secretion and stimulatory effect on secretion of protective mucin. 2. Renal insufficiency: PGE₂/PGI₂ involved in maintenance of renal blood flow. 3. Stroke/MI (COX-2 selective inhibitors): COX-2 has constitutive role in VSM, producing PGI₂, which cause vasodilation, and prevents platelet aggregation. 4. Bronchospasms: Reasons unclear.

Question 27

What are the opioid receptors in the body?

Answer 27

μ, κ, δ, ORL₁

Question 28

What types of receptors are opioid receptors?

Answer 28

G_i/o GPCRs

Question 29

Which type of opioid receptor is mainly responsible for mediating analgesic effects of opioids?

Answer 29

μ

Question 30

What are the structural features of opioids that are important to their function?

Answer 30

1. -OH group on 4th benzene ring (clockwise) 2. N- atom linked to 2 carbons on 1st benzene ring

Question 31

What are the effects of opioids on peripheral nociceptive fibres?

Answer 31

1. α_i subunit inhibits adenylyl cyclase activity, which counteracts sensitising effects of PGE₂. - **Peripheral effect** 2. βγ subunit activates GIRK channels, causing hyperpolarisation of neurones and decreased NT release at from pain fibres in spinal cord. - **Central effect**

Question 32

What are the central analgesic mechanisms of opioids?

Answer 32

1. Inhibits transmission of nociceptive nerve impulses through the dorsal horn of the spinal cord, either pre-synaptically by inhibiting NT release, or post-synaptically by decreasing the excitability of dorsal horn projecting neurones. 2. Stimulates areas of the brain such as the periaqueductal grey, involved in central modulation of pain.

Question 33

What are examples of opioids?

Answer 33

- Morphine - Codeine - Etorphine - Naloxone

Question 34

What are the side effects of opioids and opioid receptors responsible?

Answer 34

- Respiratory depression: Mediated by μ opioid receptors and is a result of suppression of central breathing rhythm. - Nausea/vomiting: Mediated by μ/δ receptors. - Constipation: Mediated by μ, κ and σ receptors.

Question 35

What is placebo analgesia?

Answer 35

Phenomenon whereby a substance which is known not to have any analgesic effects produces analgesic response in subject when given as an analgesic.

Question 36

What is the mechanism behind placebo analgesia?

Answer 36

- Release of endogenous opioids in area where subject believes placebo analgesic is acting causes suppression of pain - There may be a somatotopic representation in the PAG that controls release of endogenous opioids in specific areas of the body.

Question 37

What is the mechanism of analgesic action of gabapentin/pregabalin?

Answer 37

Decreases density of Ca_v α₂δ₁ subunit localisation in PM, thus decreasing inward Ca²⁺ current and spinal cord NT release from nociceptive fibres.

Question 38

What is the mechanism of analgesic action of lidocaine?

Answer 38

Blocks Na_vs and decreases the spontaneous discharge of nociceptive fibres.

Question 39

What is the mechanism of analgesic action of ziconotide?

Answer 39

Antagonism of N-type Ca_vs and decreases NT release at spinal cord from nociceptive fibres.

Question 40

What is the mechanism of transcutaneous electrical nerve stimulation (TENS) in pain relief?

Answer 40

Stimulation of Aβ in the area around source of pain causes inhibition of WDR pain response by gate control theory.