Is the process that occurs when special receptors in the sense organs are activated allowing various forms of outside stimuli to become neural signals... ✅ [Update]
Thủ Thuật về Is the process that occurs when special receptors in the sense organs are activated allowing various forms of outside stimuli to become neural signals... 2022
Lê Bình Nguyên đang tìm kiếm từ khóa Is the process that occurs when special receptors in the sense organs are activated allowing various forms of outside stimuli to become neural signals... được Cập Nhật vào lúc : 2022-09-29 03:03:03 . Với phương châm chia sẻ Thủ Thuật Hướng dẫn trong nội dung bài viết một cách Chi Tiết 2022. Nếu sau khi Read nội dung bài viết vẫn ko hiểu thì hoàn toàn có thể lại Comment ở cuối bài để Ad lý giải và hướng dẫn lại nha.This chapter describes the general organization of somatosensory pathways and the anatomy of the somatosensory pathways involved in processing discriminative touch and proprioceptive information, and those involved with sharp pain and cool/cold information. Discriminative touch and proprioceptive information allow for the recognition of objects by touch, provide for a sense of our body toàn thân image and is used for maintaining balance and posture. Sharp, pricking pain and cool/cold information allows for the detection and localization of potential tissue-damaging stimuli in a timely manner.
Nội dung chính- What is the process that occurs when special receptors in the sense organs are activated?What is the activation of the sense organs called?What are the receptors for special senses?What activates a sensory receptor?
4.1 General Organization of Somatosensory Pathways
Sensory pathways consist of the chain of neurons, from receptor organ to cerebral cortex, that are responsible for the perception of sensations.
4.2 Common Anatomical Features
Somatosensory stimuli activate a chain of neurons starting with the peripheral first-order (1°) afferent and ending in the cerebral cortex (e.g., Figure 4.1).
Figure 4.1
Common anatomical features of spinal somatosensory pathways
Within each somatosensory pathway,
- The 1° afferent is a pseudounipolar neuron that has its cell body toàn thân located in a peripheral (spinal or cranial) ganglion. It has a peripheral axon that forms or innervates somatosensory receptors and a central process that synapses with 2° afferent neuron(s) in a spinal cord or brain stem nucleus. The 2° afferent may synapse with 3° afferent neurons in the spinal cord or may ascend the neuraxis to synapse with 3° afferent
neurons in the thalamus. There is a decussation (i.e., axons crossing the midline to the opposite side of the spinal cord or brain stem) in each somatosensory pathway below the level of the thalamus. All somatosensory pathways include a thalamic nucleus. The thalamic neurons send their axons in the posterior limb of the internal capsule to end in the cerebral cortex. Most somatosensory pathways terminate in the parietal lobe of the cerebral cortex.
Each somatosensory pathway is named after a major tract or nucleus in the pathway.
In general, conscious perception of sensory stimuli requires the involvement of neurons in the thalamus and cerebral cortex. For example, electrical stimulation of a structure in pathways connecting muscle and joint receptors to the cerebellum (e.g., electrical stimulation of the anterior spinocerebellar tract) will not produce a sensation of limb movement, as these pathways do not include the thalamus or cortex. In contrast, electrical stimulation of a structure in the posterior column-medial lemniscal pathway (e.g., electrical stimulation of the medial lemniscus) may result in a sensation of limb movement, as this pathway includes the thalamus and terminates in the cerebral cortex.
4.3 Peripheral Somatosensory Axons
The morphology of the peripheral somatosensory axon is related to the receptor it innervates or forms and to the sensory information it carries (Figure 4.2).
- The Group I and II 1° afferent axons, which form the muscle/tendon receptors and carry body toàn thân proprioceptive information, have the largest diameter and the thickest myelin of all the somatosensory 1° afferent axons. The Type C 1° afferent axons, which form không lấy phí nerve endings and carry dull pain, deep pain, crude touch or warm/hot information, are the smallest 1° afferent axons and are unmyelinated. The Type Aδ1° afferent axons,
which form không lấy phí nerve endings and carry sharp pain or cool/cold information, are thinly myelinated and larger than the Type C axons. The Type Aβ 1° afferent axons, which form encapsulated endings in skin and joints or hair follicle endings or Merkel disks in skin, are myelinated and have diameter less than Group I afferents and greater than the Type Aδ 1° afferent axons.
Figure 4.2
The relationship between axon diameter, myelin thickness and conduction velocity of somatosensory 1° afferent peripheral processes.
The morphology of the peripheral somatosensory axon is also related to the conduction velocity of the action potentials generated by the axon.
The conduction velocity of an axon is determined by electrically stimulating the axon and recording the time (latency) it takes the electrically elicited action potential to reach a recording electrode (Figure 4.3). The distance traveled from the electrical stimulating site to the recording site divided by the latency provides the conduction velocity of the axon.
As discussed in earlier chapters, the larger and more heavily myelinated the axon, the greater its conduction velocity (Figure 4.3). Consequently, the 1° afferent axons carrying information required for fine motor control and rapid reflex responses (i.e., those forming body toàn thân proprioceptors) conduct action potentials rapidly, whereas those carrying information about body toàn thân and object temperature conduct action potentials a much slower rate.
The whole nerve potential or compound action potential (CAP) is recorded extracellularly from an electrically stimulated nerve and is the sum of the signals produced by each of the individual action potentials of the axons forming the nerve. (Figure 4.3) The mixed nerve (afferent and efferent axons) compound action potential has three prominent peaks that are called A, B and C. The conduction velocity of an axon determines the axon's contribution to the compound action potential peaks. Specifically, the faster the axon conduction velocity, the shorter the latency of axon response and the greater the axon's contribution to the shorter latency peaks (e.g., compare columns CAP Peak and Conduction Velocity in Table I). The axons contributing to a given compound action potential peak (e.g., peak A) are named according to the peak name (e.g., Type A axon). When the relative amplitudes of the peaks differ from those generated by "normal" nerves, the types of damaged axons can be assessed by determining which peaks are abnormal. Consequently, the compound action potential is used clinically to detect nerve damage and to monitor the progress of the regeneration of damaged nerves.
Figure 4.3
The whole nerve potential (aka compound action potential or CAP) recorded from a peripheral nerve in response to electrical stimulation of the nerve. (A)The compound action potential is recorded proximal to an electrical stimulus delivered to a peripheral nerve. (B) The fiber type based on the compound action potential peaks. (C) The voltage change (compound action potential) recorded proximal to the stimulating electrode
is plotted as a function of time (in msec) following the electrical stimulus pulse. Also noted along the abscissa ( each arrow) is the axon diameter (in micrometers) of axons contributing to the peaks in the whole nerve potential.
Somatosensory Receptors and their Peripheral Axons Receptor Type Axon3 Group CAP Peak Conduction Velocity Axon Diameter Information Processed Muscle Spindle: Annulospiral endings 1a Aα 70-120 m/sec 1-20 μM Muscle length and velocity
Muscle Spindle:
Flower Spray endings
For historical reasons, the terminology based on axon conduction velocity (Group I, II, III and IV) is used for afferent and efferent axons innervating muscles and tendons. And the terminology based on the compound action potential (Type A, B or C) is used for afferent axons innervating the skin, joints and viscera.
Note that the fastest conducting somatosensory 1° afferents (Group Ia) innervate skeletal muscle and the slowest (C-fibers) form the receptors of the pain systems. While one might expect painful, tissue damaging stimuli to have priority over all other somatosensory stimuli, the afferent information required to control the reaction to the painful stimuli are conveyed by the faster conducting muscle and joint afferents. Even afferents providing more exact information about the location of a cutaneous stimulus, the Aβ axons, conduct a faster rate than the Aδ and C axons carrying information about painful stimuli.
4.4 Somatotopic Organization
Somatosensory neurons are topographically (i.e., spatially) organized so that adjacent neurons represent neighboring regions of the body toàn thân or face (Figure 4.4). This organization is preserved by a precise point-to-point somatotopic pattern of connections from the spinal cord and brain stem to the thalamus and cortex. Consequently, within each somatosensory pathway there is a complete map (spatial representation) of the body toàn thân or face in each of the somatosensory nuclei, tracts, and cortex. Additional information on somatotopic organization is presented in Chapter 5 of Section II.
Figure 4.4
The somatotopic representation of the body toàn thân and face in the primary somatosensory cortex (i.e., the postcentral gyrus and posterior paracentral lobule).
4.5 Somatosensory Pathways
The sensory information processed by the somatosensory systems travels along different anatomical pathways depending on the information carried. For example, the posterior column-medial lemniscal pathway carries discriminative touch and proprioceptive information from the body toàn thân, and the main sensory trigeminal pathway carries this information from the face. Whereas, the spinothalamic pathways carry crude touch, pain and temperature information from the body toàn thân, and the spinal trigeminal pathway carries this information from the face.
4.6 Medial Lemniscal Pathway: Body Discriminative Touch and Proprioception
The posterior (dorsal) column - medial lemniscal pathway (i.e., the medial lemniscal pathway) carries and processes discriminative touch and proprioceptive information from the body toàn thân (Figure 4.5). It is important to keep in mind that within the medial lemniscal pathway, the afferents carrying discriminative touch information are kept separate from those carrying proprioceptive information up to the level of the cerebral cortex.
Figure 4.5
The medial lemniscal pathway. Press PLAY to view the course of the pathway. Click on the structure labels to view their locations in the sections. Click on the label "Cuneate fasciculus" or "Gracile fasciculus" to view the somatotopic organization of the posterior funiculus and the blood supply provided by the posterior spinal artery. Click on the label "Medial lemniscus" to view its somatotopic organization and the blood supply
provided by the paramedian branches of the basilar artery.
The peripheral axons of the 1° afferents are myelinated, large or medium diameter axons. Each axon travels via a posterior root, spinal nerve and peripheral nerve to skin, muscle or joint- where it forms or innervates a somatosensory receptor.
The 1° medial lemniscal afferent peripheral process that end in the
- skin, are Aβ axons that branch to innervate hair follicles or Merkel’s cells or form Meissner, Pacinian or Ruffini corpuscles. joints,
are Aβ axons that branch to form encapsulated endings similar to the Ruffini and Pacinian corpuscles and Golgi tendon organs. muscle, are Group I and II axons that branch to terminate in muscle spindles (Ia and II axons) or Golgi tendon organs (Ib axons).
The 1° medial lemniscal afferent central axons
- join a posterior root, enters the spinal cord, and ascends to the brain stem in the posterior column of the spinal cord (Figure 4.5). of
coccygeal to mid-thoracic posterior roots (i.e., up to T7) ascend the spinal cord in the ipsilateral gracile fasciculus. of the upper thoracic (level T6 and above) and cervical roots collect in the ipsilateral cuneate fasciculus. of the gracile and cuneate fasciculi are collectively called the posterior funiculus or posterior column. ascends the spinal cord in the posterior funiculus up to the medulla without synapsing or decussating (i.e., without crossing the midline
to the contralateral half of the spinal cord).
In the medulla,
- the 1° afferents in the gracile fasciculus synapse in the gracile nucleus the 1° afferents in the cuneate fasciculus synapse in the cuneate nucleus. the axons of the gracile and cuneate nuclei (2° afferents) pass anteriorly and decussate to form the medial lemniscus, contralateral to their cells of origin. above the level of the gracile and cuneate nuclei, each half of the body toàn thân
is represented contralaterally (e.g., left half of body toàn thân in right medial lemniscus) within the medial lemniscal pathway.
The 2° medial lemniscal afferents
- ascend the brain stem in the medial lemniscus to the diencephalon.terminate in the ventral posterolateral (VPL) nucleus of the thalamus.carrying cutaneous information terminate in the core of the VPL.carrying proprioceptive information terminate in the surrounding shell of the VPL.
The axons of the VPL 3° afferent neurons
- travel in the posterior limb of the internal capsule.terminate in the postcentral gyrus and posterior paracentral lobule of the parietal lobe.
The postcentral gyrus and posterior paracentral lobule
- are called the primary somatosensory cortex.are the primary cortical receiving areas of the somatosensory system.
The lower part of the body toàn thân (foot and leg) are represented in the posterior paracentral lobule, whereas the upper body toàn thân (chest, arm, and hand) are represented in the upper postcentral gyrus (See Figure 4.4).
Figure 4.6
Afferent neurons in the medial lemniscal pathway activated by touching the left foot with a wisp of cotton. Press PLAY to animate. The flash of light each synapse represents the release of neurotransmitter by the presynaptic axon terminal.
The action potentials ascend the spinal cord via the central process of the 1° afferent in the fasciculus gracilis of the posterior column until they reach the medulla. In the medulla, the action potentials initiate the release of neurotransmitter from the 1° afferent axon terminals onto 2° afferents within the gracile nucleus. The 2° afferent generates action potentials that are conducted by its axons, which decussate to form the medial lemniscus. These action potentials are conducted by the 2° afferent axon contralateral to their site of origin and contralateral to the foot where the stimulus was applied. The action potentials ascend to the thalamus where they initiate the release of neurotransmitter from the 2° afferent axon terminals. They release neurotransmitters onto the 3° afferents in the core of the VPL of the thalamus. The action potentials generated by the 3° VPL afferents are conducted by their axons, which travel in the posterior limb of the internal capsule, to the posterior paracentral lobule of the parietal cortex. These action potentials initiate the release of neurotransmitter from the 3° afferent axon terminals onto cortical neurons and initiate the higher-order processing of the stimulus information generated by the Meissner corpuscle. The point-to-point connections within the pathway provide the basis for a somatotopic map that is used to locate the area of contact with the stimulus and for modality specific information used to identify the stimulus as tactile and from a Meissner corpuscle.
4.7 Main Sensory Trigeminal Pathway: Face Discriminative Touch and Proprioception
The main sensory trigeminal pathway carries and processes discriminative touch and proprioceptive information from the face (Figure 4.7). Consequently, it is the cranial homologue of the medial lemniscal pathway.
Figure 4.7
The main sensory trigeminal pathway. Press PLAY to view the course of the pathway. Click on the structure labels to view their locations in the sections.
The cranial 1° main sensory trigeminal afferent neurons
- peripheral processes are located in the trigeminal (predominantly), facial, glossopharyngeal and vagus nerves. form mechanoreceptors in the skin, mucous membranes, muscles and joints of the face. The relationship between receptor type formed and the axon Type/Group are similar to those of the medial lemniscal 1° afferents. have pseudounipolar cell bodies in the cranial ganglia of the
trigeminal, facial, glossopharyngeal and vagus nerves (Table II). send their central axons to the brain stem. synapse in the main sensory trigeminal nucleus (2° afferents).
The main sensory trigeminal 2° afferent axons
- decussate immediately on leaving the main sensory trigeminal nucleus. join the contralateral ventral trigeminal lemniscus.
above the level of the main sensory trigeminal nucleus (i.e., the mid pons), carries information about the contralateral face (i.e., the right ventral trigeminal lemniscus carries information about the left side of the face).
The 2° main sensory trigeminal afferents in the ventral trigeminal lemniscus
- ascend to the diencephalon. terminate in the ventral posteromedial (VPM) nucleus of the thalamus.
The axons of the 3° main sensory trigeminal afferents (VPM neurons)
- travel in the posterior limb of the internal capsule. end in the postcentral gyrus of the parietal lobe.
The postcentral gyrus
- is part of the primary cortical receiving area of the somatosensory system.
The face is represented in the lower half of the postcentral gyrus (See Figure 4.4).
Figure 4.8 illustrates the course of action potentials generated in response to touching the left cheek with a wisp of cotton. A Merkel receptor in the left cheek is stimulated, and its 1° afferent generates action potentials that are conducted by the 1° afferent Ab axon, past its pseudounipolar soma, into the brain stem.
Figure 4.8
Afferent neurons in the main sensory trigeminal pathway activated by touching the left cheek with a wisp of cotton. Press to animate. The flash of light each synapse represents the release of neurotransmitter by the presynaptic axon terminal.
The 1° afferent central process conducts the action potentials into the pons where they initiate the release neurotransmitter from the 1° afferent axon terminals. The neurotransmitter is released onto 2° afferents within the main sensory trigeminal nucleus. The 2° afferent generates action potentials that are conducted along its axon, which decussates in the pons to join the ventral trigeminal lemniscus. These action potentials are conducted by the 2° afferent axon contralateral to their site of origin and contralateral to the site where the stimulus was applied. The action potentials ascend to the thalamus where they initiate the release of neurotransmitter from the 2° afferent axon terminals. They release neurotransmitters onto the 3° afferents in the core of the VPM of the thalamus. The action potentials generated by the 3° VPM afferents are conducted by their axons, which travel in the posterior limb of the internal capsule, to the postcentral gyrus of the parietal cortex. These action potentials initiate the release of neurotransmitter from the 3° afferent axon terminals onto cortical neurons and initiate the higher-order processing of the stimulus information generated by the Merkel cell. The point-to-point connections within the pathway provide the basis for a somatotopic map that is used to locate the area of contact with the stimulus and for modality specific information used to identify the stimulus as tactile and from a Merkel cell.
There is a minor proprioceptive component for the jaw in cranial nerve V that has 1° afferent cell bodies located in the mesencephalic trigeminal nucleus. The peripheral axons of these afferents travel in the mandibular branch of the trigeminal nerve and end in the jaw muscles and joint. The central processes of most of these afferents end in the trigeminal motor nucleus that controls the muscles of the jaw. Few synapse in the main sensory trigeminal nucleus.
4.8 Neospinothalamic Pathway: Body - Sharp Prickling Pain and Cool/Cold
The neospinothalamic pathway carries and processes sharp, pricking pain and dropping temperature (cool/cold) information from the body toàn thân (Figure 4.9). The pain information carried by the neospinothalamic pathway is well localized and the sensations are the short lasting “fast” or “first” pain elicited by tissue-damaging cutaneous stimuli. The neospinothalamic pathway is also characterized by somatotopic representation, which allows for accurate localization of the painful stimulus.
Recall that there are multiple spinal pathways processing pain information (see Somatosensory Systems Table I). Most of the ascending afferents of the spinal pain pathways travel with the neospinothalamic afferents in a fiber tract called the "spinothalamic tract" or "anterolateral spinothalamic tract". Elements of these other pain pathways will be mentioned below to help you understand how pain sensations may remain after damage to the neospinothalamic pathway. The pain pathways will be covered in greater detail in later chapters.
Figure 4.9
The neospinothalamic pathway.
Press PLAY to view the course of the pathway. Click on the structure labels to view their locations in the sections. Click on the label "Spinothalamic tract" to view the somatotopic organization of the tract fibers and the blood supply provided by the anterior spinal artery. Click on the label "Medial lemniscus" to view the blood supply provided by the posterior inferior cerebellar artery.
The 1° neospinothalamic afferents
- have Type Aδ peripheral axons that form không lấy phí nerve endings in skin, muscles and joints. have central processes that enter the spinal cord. synapse in the posterior marginal nucleus (2° afferents) of the posterior horn.
The 2° neospinothalamic afferent axons
- decussate in the spinal cord anterior white commissure. form the lateral part of the spinothalamic tract in
the lateral funiculus.
Note that the fibers in the lateral spinothalamic tract are contralateral to their cells of origin and contralateral to the body toàn thân area they represent.
The crossed 2° neospinothalamic afferent axons
- ascend the spinal cord and brain stem as part of the spinothalamic tract. travel with other pain (archispinothalamic) afferents that leave the spinothalamic tract and terminate in the brain stem as:
- spinoreticular fibers that end in the reticular formation of the brain stem. spinomesencephalic fibers that end near the periaqueductal gray of the midbrain.
- the neospinothalamic afferents terminate in the ventral posterolateral (VPL) nucleus of the thalamus. the paleospinothalamic afferents terminate in the intralaminar nuclei of the thalamus.
The spinothalamic afferent axons from the thalamus
- travel in the posterior limb of the internal capsule. VPL (i.e., the 3° neospinothalamics) end in the postcentral gyrus and posterior paracentral lobule of the parietal lobe. Intralaminar nuclei (i.e., paleospinothalamics) end in the insula and rostral cingulate gyrus.
The postcentral gyrus and posterior paracentral lobule are
- the neospinothalamic pathway termination sites. the
primary cortical receiving areas for sharp, cutting pain information. not the exclusive cortical receiving area for pain information.
The insula and rostral cingulate gyrus
- are the archispinothalamic and paleospinothalamic pathways' termination sites. receive dull and deep pain information. are responsible for poorly localized, longer lasting pain sensations and add the emotional (i.e., unpleasant) features to these sensations.
Figure 4.10
Afferent neurons in the neospinothalamic pathway activated by a pin prick to the left foot.
Press PLAY to animate. The flash of light each synapse represents the release of neurotransmitter by the presynaptic axon terminal.
Figure 4.10 illustrates the course of action potentials generated in response to a pin prick into the left foot. Free nerve endings in the left foot are stimulated by the pin prick. Action potentials are generated and conducted by the 1° afferent Aδ axon, past the pseudounipolar soma, and into the spinal cord (Figure 4.10).
The action potentials enter the spinal cord via the central process of the 1° afferents to initiate the release neurotransmitter from the 1° afferent axon terminals onto 2° afferents within the posterior marginal nucleus. The 2° afferent generates action potentials that are conducted by its axon, which decussates in the anterior white commissure of the spinal cord. The crossed 2° neospinothalamic afferent axons form the lateral component of the spinothalamic tract. The action potentials conducted by the crossed 2° afferent axon are contralateral to their site of origin and contralateral to the foot where the stimulus was applied. The action potentials ascend to the thalamus where they initiate the release of neurotransmitter from the 2° afferent axon terminals. They release neurotransmitters onto the 3° afferents in the VPL of the thalamus. The action potentials generated by the 3° VPL afferents are conducted by their axons, which travel in the posterior limb of the internal capsule, to the posterior paracentral lobule of the parietal cortex. These action potentials initiate the release of neurotransmitter from the 3° afferent axon terminals onto cortical neurons and initiate the higher-order processing of the stimulus information generated by the không lấy phí nerve ending. The point-to-point connections within the pathway provide the basis for a somatotopic map that is used to locate the area of contact with the stimulus and for modality specific information used to identify the stimulus as a sharp pinprick.
4.9 Spinal Trigeminal Pathway: Face Pain, Temperature and Crude Touch
The spinal trigeminal pathway carries and processes crude touch, pain and temperature information from the face (Figure 4.11) Consequently, it is the cranial homologue of the spinothalamic pathways i.e., homologous to all the spinothalamic pathways, the archi-, paleo- and neospinothalamic pathways. As in the spinothalamic pathways, the afferents carrying crude touch information are kept separate from those carrying temperature information and from others carrying pain information. Also the trigeminal afferents carrying sharp, cutting pain information are segregated from those carrying dull, burning pain and deep aching pain information.
Figure 4.11
The spinal trigeminal pathway.
Press PLAY to view the course of the pathway. Click on the structure labels to view their locations in the sections. Click on the label "Spinothalamic tract" to view the vascular supply to the spinal trigeminal tract and nucleus, which is provided by the posterior inferior cerebellar artery.
The 1° spinal trigeminal afferents
- are located in the same nerves and ganglia as those of the main sensory trigeminal pathway (Table II). have Aδ and C peripheral axons that form không lấy phí nerve endings in the dura and face. on entering the brain stem, form the spinal trigeminal tract.
The spinal trigeminal tract
- extends
from mid pontine levels (the level of entry of trigeminal nerve) down to C1 of the spinal cord. consists of spinal trigeminal 1° afferent axons (predominantly of the trigeminal nerve). 1° afferents synapse in the spinal trigeminal nucleus (2° spinal trigeminal afferents).
The 2° spinal trigeminal afferent axons
- decussate and form the ventral trigeminal lemniscus contralateral to their cells of origin. ascend in the ventral trigeminal
lemniscus as crossed 2° spinal trigeminal afferents. travel with afferents that leave the ventral trigeminal lemniscus as trigeminoreticular fibers, which terminate in the brain stem reticular formation. are joined by the crossed 2° main sensory trigeminal afferents mid-pons. travel with afferents that leave the ventral trigeminal lemniscus as trigeminomesencephalic fibers, which terminate near the midbrain periaqueductal gray. terminate in the VPM and in
the intralaminar nuclei of the thalamus.
Multiple thalamic nuclei process information in this pathway
- the VPM processes sharp pricking pain. the intralaminar nuclei processes other poorly localized sensations of dull, burning pain, deep, aching pain, temperature and crude touch.
The 3° spinal trigeminal afferent axons from the thalamus:
- travel in the posterior limb of the internal capsule. end in multiple areas of the
cerebral cortex.
The spinal trigeminal pathway terminates in multiple cortical areas:
- the 3° VPM axons end in the primary somatosensory cortex (See Figure 4.4), which provides for accurate localization in the face area of the source of the sharp, pricking pain. the intralaminar nuclei axons terminate in the cingulate gyrus and insula of the cerebral cortex, which
provide for poorly localized sensations of dull and aching pain, temperature and crude touch.
Figure 4.12
Afferent neurons in the spinal trigeminal pathway activated by a pin prick applied to the left cheek. Press to animate. The flash of light each synapse represents the release of neurotransmitter by the presynaptic axon terminal.
Figure 4.12 illustrates the course of action potential generated in response to a pin prick to the left cheek. Free nerve endings in the left cheek are stimulated by the pin prick. Action potentials are generated and conducted by the 1° afferent Aδ axon, past the pseudounipolar soma, and into the brain stem
The 1° afferent central process bypasses the main sensory trigeminal nucleus and descends the brain stem in the spinal trigeminal tract. The action potentials are conducted in this descending tract to the spinal trigeminal nucleus, where they initiate the release neurotransmitter from the 1° afferent axon terminals. The neurotransmitter is released onto 2° afferents within the spinal trigeminal nucleus. The 2° afferent generates action potentials that are conducted along its axon, which decussates to form the ventral trigeminal lemniscus. These action potentials are conducted by the 2° afferent axon contralateral to their site of origin and contralateral to the cheek where the stimulus was applied. The action potentials ascend to the thalamus where they initiate the release of neurotransmitter from the 2° afferent axon terminals. They release neurotransmitters onto the 3° afferents in the VPM. The action potentials generated by the 3° VPM afferents are conducted by their axons, which travel in the posterior limb of the internal capsule, to the postcentral gyrus of the parietal cortex. These action potentials initiate the release of neurotransmitter from the 3° afferent axon terminals onto cortical neurons and initiate the higher-order processing of the stimulus information generated by the không lấy phí nerve ending. The point-to-point connections within the pathway provide the basis for a somatotopic map that is used to locate the area of contact with the stimulus and for modality specific information used to identify the stimulus as a sharp pinprick.
4.10 Concluding Remarks
Clinically, it
is important to remember what information is carried by a particular pathway and the level of the pathway which decussation occurs (Figure 4.13).
Figure 4.13
The pathways involved with processing discriminative touch and proprioception from the body toàn thân and face and the pathways involved with processing sharp pain and temperature from the body toàn thân and face.
For example, if the posterior funiculus were sectioned, sparing the rest of the spinal cord, discriminative touch and proprioception would be affected but not pain, temperature, or crude touch. Also, the loss of discriminative touch and proprioception would be ipsilesional (e.g., on the right side of the body toàn thân with section of the right posterior column) because the 1° afferent axons in the posterior columns do not decussate. Consequently, damage to the posterior column in the spinal cord would be suspected if a patient presented with a loss of discriminative touch and proprioception in the right leg and foot, with no change in pain or temperature sense in the body toàn thân or face. This area of loss resulted because the ascending medial lemniscal 1° afferent axons from coccygeal to lower thoracic levels were cut off from the brain stem, and the information they carried could not be sent on to the thalamus and cortex. In contrast, a stroke affecting the posterior paracentral lobule would produce sensory deficits in discriminative touch, proprioception and sharp pricking pain contralateral to the site of stroke. However such a stroke would affect other pain, temperature and crude touch sensations less than a large spinal cord lesion because these somatic sensations are represented in diffuse areas of the cortex.
Table IIThe Nerve Roots and Ganglia Associated with the Somatic and Visceral Afferent Pathways Nerve Root Ganglia Somatic Innervation Visceral Innervation Spinal Cord: Sacral posterior root: S5 to S1 buttocks, back of leg and foot, genitals lower pelvic region, e.g., Rectum Spinal Cord: Lumbar posterior root: L5 to L1 lower back, hip, pelvic area, side and front of leg and foot leg and pelvic region, e.g., bladder Spinal Cord: Thoracic posterior root: T12 to T1 trunk (abdomen, back, and chest), part of arm
lower roots: Lower abdomen (e.g., kidney, colon, appendix)
middle roots: Upper abdomen (e.g., stomach, liver, gall bladder)
upper roots: Chest (e.g., diaphragm, esophagus, lung, heart)
Spinal Cord: Cervical posterior root: C8 to C2 shoulder, arm, hand, fingers, neck and back of head minor to blood vessels and sweat glands of upper body toàn thân and extremities Cranial Nerve: Vagus Nervejugular (superior)
nodose (inferior)
back of ear, external auditory canal and duranone
throat, thoracic and abdominal viscera
Cranial Nerve: Glossopharyngealsuperior (jugular)
petrosal (inferior)
back of ear (minor), ear drum, middle ear
ear drum, middle ear, Eustachian tube, tonsil, pharynx, soft palate and posterior tongue
none
carotid body toàn thân and sinus
Cranial Nerve: Facial geniculate skin of ear minor - Parotid gland Cranial Nerve: Trigeminal semilunar face, eye, oral and nasal cavities, and meninges noneTest Your Knowledge
Make the best match between the 1° somatosensory axon type and the sensations carried by the axon.
- Match: C FibersABCDEF
A. Vibration
B. Static muscle stretch
C. Dull, burning pain
D. Isotonic muscle contraction
E. Sharp "fast" pain
F. Dynamic muscle stretch
A. Vibration This is an INCORRECT match.
B. Static muscle stretch
C. Dull, burning pain
D. Isotonic muscle contraction
E. Sharp "fast" pain
F. Dynamic muscle stretch
A. Vibration
B. Static muscle stretch This is an INCORRECT match.
C. Dull, burning pain
D. Isotonic muscle contraction
E. Sharp "fast" pain
F. Dynamic muscle stretch
A. Vibration
B. Static muscle stretch
C. Dull, burning pain This is the CORRECT match!
The C fibers carry information about dull and deep pain and warm/hot from somatic structures. They do not carry sharp "fast" pain information.
D. Isotonic muscle contraction
E. Sharp "fast" pain
F. Dynamic muscle stretch
A. Vibration
B. Static muscle stretch
C. Dull, burning pain
D. Isotonic muscle contraction This is an INCORRECT match.
E. Sharp "fast" pain
F. Dynamic muscle stretch
A. Vibration
B. Static muscle stretch
C. Dull, burning pain
D. Isotonic muscle contraction
E. Sharp "fast" pain This is an INCORRECT match.
F. Dynamic muscle stretch
A. Vibration
B. Static muscle stretch
C. Dull, burning pain
D. Isotonic muscle contraction
E. Sharp "fast" pain
F. Dynamic muscle stretch This is an INCORRECT match.
- Match: A delta fibersABCDEF
A. Vibration
B. Static muscle stretch
C. Dull, burning pain
D. Isotonic muscle contraction
E. Sharp "fast" pain
F. Dynamic muscle stretch
A. Vibration This is an INCORRECT match.
B. Static muscle stretch
C. Dull, burning pain
D. Isotonic muscle contraction
E. Sharp "fast" pain
F. Dynamic muscle stretch
A. Vibration
B. Static muscle stretch This is an INCORRECT match.
C. Dull, burning pain
D. Isotonic muscle contraction
E. Sharp "fast" pain
F. Dynamic muscle stretch
A. Vibration
B. Static muscle stretch
C. Dull, burning pain This is an INCORRECT match.
D. Isotonic muscle contraction
E. Sharp "fast" pain
F. Dynamic muscle stretch
A. Vibration
B. Static muscle stretch
C. Dull, burning pain
D. Isotonic muscle contraction This is an INCORRECT match.
E. Sharp "fast" pain
F. Dynamic muscle stretch
A. Vibration
B. Static muscle stretch
C. Dull, burning pain
D. Isotonic muscle contraction
E. Sharp "fast" pain This is the CORRECT match!
The A delta fibers carry information about sharp "fast" pain, cold/cool. The C fibers carry dull and deep pain and warm/hot information from somatic structures.
F. Dynamic muscle stretch
A. Vibration
B. Static muscle stretch
C. Dull, burning pain
D. Isotonic muscle contraction
E. Sharp "fast" pain
F. Dynamic muscle stretch This is an INCORRECT match.
- Match: A beta fibersABCDEF
A. Vibration
B. Static muscle stretch
C. Dull, burning pain
D. Isotonic muscle contraction
E. Sharp "fast" pain
F. Dynamic muscle stretch
A. Vibration This is the CORRECT match!
B. Static muscle stretch
C. Dull, burning pain
D. Isotonic muscle contraction
E. Sharp "fast" pain
F. Dynamic muscle stretch
A. Vibration
B. Static muscle stretch This is an INCORRECT match.
C. Dull, burning pain
D. Isotonic muscle contraction
E. Sharp "fast" pain
F. Dynamic muscle stretch
A. Vibration
B. Static muscle stretch
C. Dull, burning pain This is an INCORRECT match.
D. Isotonic muscle contraction
E. Sharp "fast" pain
F. Dynamic muscle stretch
A. Vibration
B. Static muscle stretch
C. Dull, burning pain
D. Isotonic muscle contraction This is an INCORRECT match.
E. Sharp "fast" pain
F. Dynamic muscle stretch
A. Vibration
B. Static muscle stretch
C. Dull, burning pain
D. Isotonic muscle contraction
E. Sharp "fast" pain This is an INCORRECT match.
F. Dynamic muscle stretch
A. Vibration
B. Static muscle stretch
C. Dull, burning pain
D. Isotonic muscle contraction
E. Sharp "fast" pain
F. Dynamic muscle stretch This is an INCORRECT match.
- Question 1ABCDE
The neospinothalamic tract crosses the midline in which of the following structures?
A. Anterior white commissure
B. Internal arcuate fibers
C. Spinal trigeminal tract
D. Dorsal columns
E. Medial lemniscus
The neospinothalamic tract crosses the midline in which of the following structures?
A. Anterior white commissure This answer is CORRECT!
B. Internal arcuate fibers
C. Spinal trigeminal tract
D. Dorsal columns
E. Medial lemniscus
The neospinothalamic tract crosses the midline in which of the following structures?
A. Anterior white commissure
B. Internal arcuate fibers This answer is INCORRECT.
C. Spinal trigeminal tract
D. Dorsal columns
E. Medial lemniscus
The neospinothalamic tract crosses the midline in which of the following structures?
A. Anterior white commissure
B. Internal arcuate fibers
C. Spinal trigeminal tract This answer is INCORRECT.
D. Dorsal columns
E. Medial lemniscus
The neospinothalamic tract crosses the midline in which of the following structures?
A. Anterior white commissure
B. Internal arcuate fibers
C. Spinal trigeminal tract
D. Dorsal columns This answer is INCORRECT.
E. Medial lemniscus
The neospinothalamic tract crosses the midline in which of the following structures?
A. Anterior white commissure
B. Internal arcuate fibers
C. Spinal trigeminal tract
D. Dorsal columns
E. Medial lemniscus This answer is INCORRECT.
- Question 2A
BCDE
The medial lemniscus crosses the midline which level of the nervous system?
A. Spinal cord
B. Medulla
C. Pons
D. Mesencephalon
E. Diencephalon
The medial lemniscus crosses the midline which level of the nervous system?
A. Spinal cord This answer is INCORRECT.
B. Medulla
C. Pons
D. Mesencephalon
E. Diencephalon
The medial lemniscus crosses the midline which level of the nervous system?
A. Spinal cord
B. Medulla This answer is CORRECT!
C. Pons
D. Mesencephalon
E. Diencephalon
The medial lemniscus crosses the midline which level of the nervous system?
A. Spinal cord
B. Medulla
C. Pons This answer is INCORRECT.
D. Mesencephalon
E. Diencephalon
The medial lemniscus crosses the midline which level of the nervous system?
A. Spinal cord
B. Medulla
C. Pons
D. Mesencephalon This answer is INCORRECT.
E. Diencephalon
The medial lemniscus crosses the midline which level of the nervous system?
A. Spinal cord
B. Medulla
C. Pons
D. Mesencephalon
E. Diencephalon This answer is INCORRECT.
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