Pain Flashcards
Why is it important for medical students to know about pain ?
- Really common symptom
- Access to pain relief is thought by many to be a human right
- As an FY1 you will be required to (prevent) Recognise, Assess and Treat pain effectively
Define pain.
An unpleasant sensory and emotional experience associated with actual or potential tissue damage or described in terms of such damage
What is the function of pain ?
Protective function, minimises damage by warning body that tissues/cells are getting damaged, or that a structure is not getting enough blood supply (e.g. myocardium).
Identify the main kinds of pain.
IMMEDIATE PAIN (transmitted by A delta fibers) PERSISTING PAIN (transmitted by C fibers)
What happens following immediate pain ?
WITHDRAWAL REFLEX
-Polysynaptic reflex
E.g. Foot injury
APs to nerves which will travel along spinal cord in dorsal horn.
Will then synapse to cause withdrawal of the limb by activating flexors + by relaxing extensors in limb involved + by
activating extensors and relaxing flexors of opposite leg to prepare it to take up weight of the whole body
Give an example of pain where C fibers may be involved.
Polyneuropathy in diabetes, causing loss of sensation to the feet. Due to inability to sense, get repeated trauma to foot which then gets infected.
–> Chronic pain
Describe the general neural pathways of pain in the spinal cord/brain.
- Primary afferents (first oder neuron) from periphery synapse in dorsal horn of spinal cord.
- Second order neurons decussate and ascend in spinothalamic tract to thalamus.
- Third order neuron projects from thalamus to somatosensory cortex.
What is a nociceptor ?
Free nerve endings in the skin and viscera (especially in tissues which can become distended/ischemic/ damaged thermally/chemically /mechanically).
HOWEVER, only respond at extremes of stimuli, where stimuli will cause damage to tissue.
Which types of nerve fibers are involved in pain ?
- A-delta (temperature and pain)
- C (temperature and pain)
Rank the following by velocity of transmission:
- A beta
- A delta
- C
1) A beta
2) A delta
3) C
Identify the main differences between A delta and C fibers.
A-delta fibres:
- Myelinated, thinner
- Faster conduction (6-30 m/s)
- Sharp, localised pain
- Minority of nociceptor
- Polymodal (but usually mechanical and thermal)
- Not usually visceral
C fibers:
- Unmyelinated
- Dull, achy, throbbing, diffuse pain
- Majority of nociceptors
- Slow conduction (0.5-2 m/s)
- Polymodal (thermal, mechanical, chemical stimuli)
What is the management of pain associated with C fibers ?
Imobilise limbs, imobilise joints (to allow healing, esp fracture healing)
Identify the main steps in the physiology of pain (i.e. how noxious stimulus comes from periphery of body to be perceived brain as pain).
- Transduction
• Conversion of a noxious stimulus (heat, mechanical, chemical) into an action potential in a nociceptor
• Pain sensation may extend beyond actual assault
• Primary hyperalgesia effect (when tissue damaged, nerve endings are bathed in chemicals released from damaged tissue, so sensations that may not have been previously perceived can become painful e.g. sunburn under hot water)
(through recruitment of sleeping C fibers) - Transmission
- Modulation
- Perception
Identify examples of thermal, mechanical, and chemical stimuli which may be involved in transduction.
- Heat: >450C or less that 150C
- Chemical: K+, ATP (both of these intracellular, if cell is damaged and empty its contents, K+ activates nociceptors), Bradykinin, histamine (released by inflammatory response in tissue damage), Substance P (generated by nociceptor itself and released at synapses, when AP is getting transmitted up to brain + also releases in retrograde fashion and bathes nociceptors, and sensitises them to other stimuli)
- Mechanical
How do nociceptors adapt ? Why is this useful ?
Nociceptors do NOT adapt (unlike other nerve endings).
Rather than adapting (so that brain ignores it), they get more sensitive and transmit more APs, and your brain perceives pain as getting worse.
USEFUL because protective mechanism, body has to move if sitting in uncomfortable position and foot gets ischemic, and if don’t do anything gets MORE sore so forces you to do something about it.
Which nerve fibers are involved in transduction phase of pain ? Which modalities to they respond to ?
• Nociceptors are free nerve endings of A-delta and C afferent fibres, responding to stimuli (polymodal) that will potentially damage tissue
Identify the main chemical mediators of pain, as well as their source and effect on nociceptor.
MEDIATORS
- K+ (Damaged cells, activates nociceptors)
- Protons (Hypoxic cells, activates nociceptors)
- Serotonin (platelets, activates nociceptors)
- Bradykinin (plasma kininogen, activates nociceptors)
- Histamine (mast cells, activates nociceptors)
- Prostanoids (damaged cells, sensitisation)
- Leukotrienes (damaged cells, sensitisation)
- Substance P (primary afferents, sensitisation)
- CGRP (primary afferents, sensitisation)
- Glutamate (primary afferents, sensitisation)
Explain why MIs are painful.
Ischemia (eg MI, sitting awkwardly so supply to leg cut off), organ involved
become hypoxic an lactic acid is produced, so activates nociceptors and
cause pain.
Why is it clinically important that pain and temperature run together ?
When doing an anesthetic block, instead of testing pain to make sure block is working, can test using temperature sense (e.g. can you feel this ice as cold).
If cannot perceive ice cube as cold, pretty certain that pain is blocked too.
Identify the excitatory substance, and receptors involved in transmission (second step of pain physiology).
Transmission between first and second order neurons
No single excitatory substance
• Glutamate (main one)
• SubstanceP
• CGRP
No single “pain receptor” but glutamate binds to:
• AMPA (when this one gets flooded and noxious stimulus continues, then gets to NMDA receptors and wakes them up)
• NMDA (sleeping but important!)
• G-protein couple receptors
Identify the main components of the anterolateral system, including where they terminate and their main function.
SPINOTHALAMIC
1) Paleo-spinothalamic
- Terminates in the dorsomedial (DM) and intra laminar areas (only provide generalised location for pain)
2) Neo-spinothalamic
- Terminates in the ventral posterior lateral nucleus (VPL, which is somatotopic so there IS local discrimination along this pathway)
SPINOMESENCEPHALIC
-“Terminates in the periaqeductal grey of the midbrain (area that is important to inhibiting or controlling pain sensations)”
SPINORETICULAR
-“Teriminates in the reticular formation in the brainstem. The spinoreticular tract is thought to be important in directing attention toward painful stimuli”
What kind of fibers does the neospinothalamic, and paliospinothalamic tract contrain respectively ?
NEO
-Adelta fibers
PALIO
-C fibers
Where does modulation of pain occur ?
Modulation of pain occurs at the dorsal horn.
Identify the main mechanisms of modulations of pain at the dorsal horn.
3 mechanisms of descending inhibition
- GABA and glycinergic interneurons
- Descending inhibition PAG-RVM-DH (stimulates GABA release)
- Endogenous opioids (e.g. encephalins, released at dorsal horn and minimize transmission of pain upwards to thalamus)
ALSO
• Higher order brain function (distraction, serotonin, NA all have impact at that synapse in dorsal horn)
Describe the gate control theory.
Damage results in AP sent along nociceptor into dorsal horn.
If provide mechanical stimulation to same area, will travel through A-beta fibers, and will therefore transmit APs faster than A-delta fibers, so travel along the fiber and stimulate inhibitory neurons, resulting in presynaptic inhibition of pain information, so mechanoreceptors will stimulate target cell as opposed to the nociceptor.
