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BIO 351 TEST 3
What’s the motor system?
Motor systems control different movements from simple reflexes (knee jerk) to voluntary movements (96mph fast ball)
Motor systems generate a motor output
Motor systems are made up of motor units
Motor Unit
• A single motor neuron innervates a group of muscle fibers - this arrangement is called a motor unit
•When a motor neuron fires, the muscles it innervates contract.
• For controlled movement, many motor units must be synchronized.
Cerebellum
Cerebellar cortex
Cortex that covers surface of cerebellum
Deep cerebellar nucleus
Nuclei located within cerebellar hemispheres
Receive projections from cerebellar cortex and send projections out of cerebellum to other parts of brain
Cerebellar peduncle (pee dun kul)
One of three bundles of axons that attach each cerebellar
hemisphere to the dorsal pons
Damage to cerebellum impairs standing, walking, or performance of coordinated movements
Cerebellum receives visual, auditory, vestibular, and somatosensory information, and it also receives information about individual muscle movements being directed by brain
Cerebellum integrates this information and modifies the motor outflow, exerting a coordinating and smoothing effect on the movements
Cerebellar damage results in jerky, poorly coordinated, exaggerated movements; extensive cerebellar damage makes it impossible even to stand
Basal Ganglia
Basal ganglia: control of voluntary movements, procedural learning, cognition, and emotions
regulates posture, counteracts tremor and maintains muscular contractions.
regulates motor control
Key Structures:
Caudate
Putamen
Globus pallidus
Substanitia nigra
Nucleus accumbens
Subthalamic nucleus
Spinal Cord
Lateral Corticospinal Tract
Ventral Corticospinal Tract
*the ventral and lateral corticospinal tract make up the major pathway from the motor cortex to the spinal cordRubrospinal Tract
Reticulospinal Tract
Tectospinal Tract
Lateral Corticospinal Tract -
originates in the motor and premotor areas of the cortex.
Fibers in pyramidal cells of the cortex pass through the internal capsule, cerebral peduncles to the
medullary pyramids, cross midline and
terminate on motoneurons and interneurons in the lateral gray matter
Ventral Corticospinal tract -
originates in the motor and premotor areas of the cortex.
Fibers in pyramidal cells of the cortex pass through the internal capsule, cerebral peduncles to the medullary pyramids,
**does not cross midline terminate in the cervical and upper thoracic levels.
Control limb posture and position of the head.
Controls trunk muscles on both sides of the body.
Rubrospinal tract -
originate in the red nuclei cross midline at the level of the pons before descending in the spinal cord to terminate on interneurons.
Vestibulospinal tracts -
originates with cells in the lateral vestibular nucleus
Descends uncrossed in the spinal cord to terminate on medial motoneurons that control postural muscles and extensor and flexor muscles.
Reticulospinal tracts -
Cells originating from the pons are excitatory
descends ipsilaterally and ends on segmental interneurons that provide bilateral excitation to medial extensor motor neurons.
Tectospinal tract -
Cells originating from the medulla are inhibitory.
terminate in the cervical and upper thoracic levels.
Control limb posture and position of the head.
Reflexes
limb movement is produced by coordinated muscle action of extensors (muscles open or extend) and flexors (close or flex the joint).
Myotatic reflex is activated by muscle stretch - example: Knee Jerk Reflex
Postural adjustments
Context
Maintain balance--supported v/s unsupported
Feedback
Error correction Response lags stimulus; sometimes too late
Feed-forward
Response anticipates stimulus More timely, but depends on internal models Practice, learning
Voluntary movements
All the connections in the cerebellum allow actual or intended movements to be compared during execution to the plans of the movement in the cortex.
Usually include multiple systems - vestibular, visual, premotor, motor, spinal tracts
Organized around purposeful act
Voluntary movements are organized by motor programs
Translate goal into action
Formation of a movement representation, or motor program
Program
To produce the desired goal, which muscles should contract and when
2 Key movement characteristics
Spatial (hand path; joint angles) - Kinematic plan
Forces/loads - Dynamic plan
All accomplished by contracting muscles
Central Pattern Generators
coordinated, rhythmical movement.
Sensory feedback is not necessary (and not ignored)
Two key examples - respiration and walking
Overview of Muscle Tissue
Nearly half of body’s mass
Can transform chemical energy (ATP) into directed mechanical energy, which is capable of exerting force
To investigate muscle, we look at:
– Types of muscle tissue
– Characteristics of muscle tissue
– Muscle functions
Types of Muscle Tissue
Terminologies: Myo, mys, and sarco are prefixes for muscle
– Example: sarcoplasm: muscle cell cytoplasm
Three types of muscle tissue
– Skeletal – Cardiac – Smooth
Only skeletal and smooth muscle cells are elongated and referred to as muscle fibers
Characteristics of Muscle Tissue
All muscles share four main characteristics:
Excitability (responsiveness): ability to receive and respond to stimuli
Contractility: ability to shorten forcibly when stimulated
Extensibility: ability to be stretched
Elasticity:abilitytorecoilto resting length
Muscle Functions
• Four important functions
Produce movement: responsible for all locomotion and manipulation
Example: walking, digesting, pumping blood
Maintain posture and body position
Stabilize joints
Generate heat as they contract
Skeletal Muscle Anatomy
• Skeletal muscle is an organ made up of different tissues with three features: nerve and blood supply, connective tissue sheaths, and attachments
Muscle Fiber Microanatomy and Sliding Filament Model
Skeletal muscle fibers are long, cylindrical cells that contain multiple nuclei
Sarcolemma: muscle fiber plasma membrane
Sarcoplasm: muscle fiber cytoplasm
Contains many glycosomes for glycogen storage, as well as myoglobin for O2 storage
Modified organelles – Myofibrils
– Sarcoplasmic reticulum
– T tubules
Myofibrils
Myofibrils are densely packed, rodlike elements
– Single muscle fiber can contain 1000s
– Accounts for ~80% of muscle cell volume
Myofibril features
– Striations
– Sarcomeres
– Myofilaments
– Molecular composition of myofilaments
Myofibrils: Straitions
• Striations: stripes formed from repeating series of dark and light bands along length of each myofibril
– A bands: dark regions
▪ H zone: lighter region in middle
of dark A band
– M line: line of protein (myomesin) that bisects H zone vertically
– I bands: lighter regions
▪ Z disc (line): coin-shaped sheet of proteins on midline of light I band
Myofibrils: Sarcomere
• Sarcomere
Smallest contractile unit (functional unit) of muscle fiber
Contains A band with half of an I band at each end
Consists of area between Z discs
Individual sarcomeres align end to end along myofibril, like boxcars of train
Myofibrils: Myofilaments
• Myofilaments
Orderly arrangement of actin and myosin myofilaments within sarcomere
Actin myofilaments: thin filaments
Extend across I band and partway in A band
Anchored to Z discs
Myosin myofilaments: thick filaments
Extend length of A band
Connected at M line
Sarcomere cross section shows hexagonal arrangement of one thick filament surrounded by six thin filaments
Myofibrils: Molecular
• Molecular composition of myofilaments
– Thick filaments: composed of protein myosin that contains two heavy and four light polypeptide chains
Heavy chains intertwine to form myosin tail
Light chains form myosin globular head
During contraction, heads link thick and thin filaments together, forming cross bridges
▪ Myosins are offset from each other, resulting in staggered array of heads at different points along thick filament
Myofibrils: Molecular
• Molecular composition of myofilaments (cont.)
Thin filaments: composed of fibrous protein actin
Actin is polypeptide made up of kidney-shaped G actin (globular) subunits
G actin subunits bears active sites for myosin head attachment during contraction
G actin subunits link together to form long, fibrous F actin (filamentous)
Two F actin strands twist together to form a thin filament
– Tropomyosin and troponin: regulatory proteins bound to actin
Myofibril: Molecular
Molecular composition of myofilaments (cont.)
Other proteins help form the structure of the myofibril ▪
Elastic filament: composed of protein titin
Holds thick filaments in place; helps recoil after stretch; resists excessive stretching
Dystrophin
Links thin filaments to proteins of sarcolemma
Nebulin, myomesin, C proteins bind filaments or sarcomeres together
Maintain alignment of sarcomere
Sarcoplasmic Reticulum and T Tubules
Sarcoplasmic reticulum: network of smooth endoplasmic reticulum tubules surrounding each myofibril
Most run longitudinally
Terminal cisterns form perpendicular cross channels at the A–I band junction
SR functions in regulation of intracellular Ca2+ levels
Stores and releases Ca2+
Sarcoplasmic Reticulum and T Tubules
T tubules
Tube formed by protrusion of sarcolemma deep into cell interior
Increase muscle fiber’s surface area greatly
Lumen continuous with extracellular space
Allow electrical nerve transmissions to reach deep into interior of each muscle fiber
Tubules penetrate cell’s interior at each A–I band junction between terminal cisterns
Triad: area formed from terminal cistern of one sarcomere, T tubule, and terminal cistern of neighboring sarcomere
Triad relationship
T tubule contains integral membrane proteins that protrude into intermembrane space (space between tubule and muscle fiber sarcolemma)
Tubule proteins act as voltage sensors that change shape in response to an electrical current
SR cistern membranes also have integral membrane proteins that protrude into intermembrane space
SR integral proteins control opening of calcium channels in SR cisterns
Triad relationships (cont.)
When an electrical impulse passes by, T tubule proteins change shape, causing SR proteins to change shape, causing release of calcium into cytoplasm
Sliding Filament Model of Contraction
Contraction: the activation of cross bridges to generate force
Shortening occurs when tension generated by cross bridges on thin filaments exceeds forces
opposing shortening
Contraction ends when cross bridges become inactive
In the relaxed state, thin and thick filaments overlap only slightly at ends of A band
Sliding filament model of contraction states that during contraction, thin filaments slide past thick filaments, causing actin and myosin to overlap more
Neither thick nor thin filaments change length, just overlap more
When nervous system stimulates muscle fiber, myosin heads are allowed to bind to actin, forming cross bridges, which cause sliding (contraction) process to begin
Cross bridge attachments form and break several times, each time pulling thin filaments a little closer toward center of sarcome in a ratcheting action
Causes shortening of muscle fiber
Z discs are pulled toward M line
I bands shorten
Z discs become closer
H zones disappear
A bands move closer to each other
Muscle Fiber Contraction
Background and Overview
Decision to move is activated by brain, signal is transmitted down spinal cord to motor neurons which then activate muscle fibers
Neurons and muscle cells are excitable cells capable of action potentials
Excitable cells are capable of changing resting membrane potential voltages
AP crosses from neuron to muscle cell via the neurotransmitter acetylcholine (ACh)
Ion Channels
Play the major role in changing of membrane potentials
Two classes of ion channels:
Chemically gated ion channels – opened by chemical messengers such as neurotransmitters
– Example: ACh receptors on muscle cells
Voltage-gated ion channels – open or close in response to voltage changes in membrane potential
The Motor Unit
Motor unit consists of the motor neuron and all muscle fibers (four to several hundred) it supplies
Smaller the fiber number, the greater the fine control
Muscle fibers from a motor unit are spread throughout the whole muscle, so stimulation of a single motor unit causes only weak contraction of entire muscle
Background and Overview
Anatomy of Motor Neurons and the Neuromuscular Junction
Skeletal muscles are stimulated by somatic motor neurons
Axons (long, threadlike extensions of motor neurons) travel from central nervous system to skeletal muscle
Each axon divides into many branches as it enters muscle
Axon branches end on muscle fiber, forming neuromuscular junction or motor end plate
Each muscle fiber has one neuromuscular junction with one motor neuron
Axon terminal (end of axon) and muscle fiber are separated by gel- filled space called synaptic cleft
Stored within axon terminals are membrane-bound synaptic vesicles
Synaptic vesicles contain neurotransmitter acetylcholine (ACh)
Infoldings of sarcolemma, called junctional folds, contain millions of ACh receptors
NMJ consists of axon terminals, synaptic cleft, and junctional folds
Generation of an Action Potential Across the Sarcolemma
Resting sarcolemma is polarized, meaning a voltage exists across membrane
Inside of cell is negative compared to outside
Action potential is caused by changes in electrical charges
Occurs in three steps
Generation of end plate potential (EPP)
Depolarization
Repolarization
Generation of an Action Potential Across the Sarcolemma
1.End plate potential
ACh released from motor neuron binds to ACh receptors on sarcolemma
Causes chemically gated ion channels (ligands) on sarcolemma to open
Na+ diffuses into muscle fiber
Some K+ diffuses outward,but not much
Because Na+ diffuses in, interior of sarcolemma becomes less negative (more positive)
Results in local depolarization called end plate potential
2.Depolarization: generation and propagation of an action potential (AP)
If end plate potential causes enough change in membrane voltage to reach critical level called threshold, voltage-gated Na+ channels in membrane will open
Large influx of Na+ through channels into cell triggers AP that is unstoppable and will lead to muscle fiber contraction
AP spreads across sarcolemma from one voltage-gated Na+ channel to next one in adjacent areas, causing that area to depolarize
3.Repolarization: restoration of resting conditions
Na+ voltage-gated channels close, and voltage-gated K+ channels open
K+ efflux out of cell rapidly brings cell back to initial resting membrane voltage
Refractory period: muscle fiber cannot be stimulated for a specific amount of time, until repolarization is complete
Ionic conditions of resting state are restored by Na+-K+ pump
Na+ that came into cell is pumped back out, and K+ that flowed outside is pumped back into cell
Excitation-Contraction (E-C) Coupling
Excitation-contraction (E-C) coupling: events that transmit AP along sarcolemma (excitation) are coupled to sliding of myofilaments (contraction)
AP is propagated along sarcolemma and down into T tubules, where voltage-sensitive proteins in tubules stimulate Ca2+ release from SR
Ca2+ release leads to contraction
AP is brief and ends before contraction is seen
The Muscle Twitch
Muscle twitch: simplest contraction resulting from a muscle fiber’s response to a single action potential from motor neuron
Muscle fiber contracts quickly, then relaxes
Twitch can be observed and recorded as a myogram
Tracing: line recording contraction activity
Three phases of muscle twitch
Latent period: events of excitation-contraction
coupling
No muscle tension seenng
Period of contraction: cross bridge formation
Tension increases
Period of relaxation: Ca2+ reentry into SR
Tension declines to zero
Muscle contracts faster than it relaxes
Graded Muscle Responses
Normal muscle contraction is relatively smooth, and strength varies with needs
A muscle twitch is seen only in lab setting or with neuromuscular problems, but not in normal muscle
Graded muscle responses vary strength of contraction for different demands
Required for proper control of skeletal movement
Responses are graded by:
Changing frequency of stimulation
Changing strength of stimulation
Wave (temporal) summation results if two stimuli are received by a muscle in rapid succession
Muscle fibers do not have time to completely relax between stimuli, so twitches increase in force with each stimulus
Additional Ca2+ that is released with second stimulus stimulates more shortening
If stimuli frequency increases, muscle tension reaches near maximum
Produces smooth, continuous contractions that add up (summation)
Further increase in stimulus frequency causes muscle to progress to sustained, quivering contraction referred to as unfused (incomplete) tetanus
If stimuli frequency further increase, muscle tension reaches maximum
Referred to as fused (complete) tetanus because contractions “fuse” into one smooth sustained contraction plateau
Prolonged muscle contractions lead to muscle fatigue
Isotonic and Isometric Contractions
Isotonic contractions: muscle changes in length and moves load
Isotonic contractions can be either concentric or eccentric:
Concentric contractions: muscle shortens and does work
Example: biceps contract to pick up a book
Eccentric contractions: muscle lengthens and generates force
Example: laying a book down causes biceps to lengthen while generating a force
Isometric contractions
Load is greater than the maximum tension muscle can generate, so muscle neither shortens nor lengthens
Electrochemical and mechanical events are same in sotonic or isometric contractions, but results are different
In isotonic contractions, actin filaments shorten and cause movement
In isometric contractions, cross bridges generate force, but actin filaments do not shorten
Myosin heads “spin their wheels” on same actin- binding site
Differences between Smooth and Skeletal Muscle Fibers
Smooth muscle fibers are spindle-shaped fibers
thin and short compared with
skeletal muscle fibers which are wider and much longer
Only one nucleus, no striations
Lacks connective tissue sheaths
Contains endomysium only
Contain varicosities (bulbous swellings) of nerve fibers instead of neuromuscular junctions
Varicosities store and release neurotransmitters into a wide synaptic cleft referred to as a diffuse junction
Innervated by the autonomic nervous system
Smooth muscle has less elaborate SR, and no T tubules
SR is less developed than in skeletal muscle
SR does store intracellular Ca2+, but most calcium used for contraction has extracellular origins
Sarcolemma contains pouchlike infoldings called caveolae
Caveolae contain numerous Ca2+ channels that open to allow rapid influx of extracellular Ca2+
Smooth muscle fibers are usually electrically connected via gap junctions whereas skeletal muscle fibers are electrically isolated
Gap junctions are specialized cell connections that allow depolarization to spread from cell to cell
There are no striations and no sarcomeres, but they do contain overlapping thick and thin filaments
Smooth muscle also differs from skeletal muscle in following ways:
Thick filaments are fewer and have myosin heads along entire length
Ratio of thick to thin filaments (1:13) is much lower than in skeletal muscle (1:2)
Thick filaments have heads along entire length, making smooth muscle as powerful as skeletal muscle
No troponin complex
Does contain tropomyosin, but not troponin
Protein calmodulin binds Ca2+
Thick and thin filaments arranged diagonally
Myofilaments are spirally arranged, causing smooth muscle to contract in corkscrew manner
Intermediate filament–dense body network
Contain lattice-like arrangement of non contractile intermediate filaments that resist tension
Dense bodies: proteins that anchor filaments to sarcolemma at regular intervals
Correspond to Z discs of skeletal muscle
During contraction, areas of sarcolemma between dense bodies bulge outward
Make muscle cell look puffy
Contraction of Smooth Muscle
Mechanism of contraction
Slow, synchronized contractions
Cells electrically coupled by gap junctions
Action potentials transmitted from fiber to fiber
Some cells are self-excitatory (depolarize without external stimuli)
Act as pacemakers for sheets of muscle
Rate and intensity of contraction may be modified by neural and chemical stimuli
Contraction in smooth muscle is similar to skeletal muscle contraction in following ways:
Actin and myosin interact by sliding filament mechanism
Final trigger is increased intracellular Ca2+ level
ATP energizes sliding process
Contraction stops when Ca2+ is no longer available
Contraction of Smooth Muscle
Contraction in smooth muscle is different from skeletal muscle in following ways:
Some Ca2+ still obtained from SR, but mostly comes from extracellular space
Ca2+ binds to calmodulin, not troponin
Activated calmodulin then activates myosin kinase (myosin light chain kinase)
Activated myosin kinase phosphorylates myosin head, activating it
Leads to crossbridge formation with actin
Stopping smooth muscle contraction requires more steps than skeletal muscle
Relaxation requires:
Ca2+ detachment from calmodulin
Active transport of Ca2+ into SR and intracellularly
Dephosphorylation of myosin to inactive myosin
Contraction of Smooth Muscle
Energy efficiency of smooth muscle contraction
Slower to contract and relax but maintains contraction for prolonged periods with little energy cost
Slower ATPases
Myofilaments may latch together to save energy
Most smooth muscle maintain moderate degree of contraction constantly without fatiguing
Referred to as smooth muscle tone
Makes ATP via aerobic respiration pathways
Contraction of Smooth Muscle
Regulation of contraction
Controlled by nerves, hormones, or local chemical changes
Neural regulation
Neurotransmitter binding causes either graded (local) potential or action potential
Results in increases in Ca2+ concentration in sarcoplasm
Response depends on neurotransmitter released and type of receptor molecules
One neurotransmitter can have a stimulatory effect on smooth muscle in one organ, but an inhibitory effect in a different organ
Hormones and local chemicals
Some smooth muscle cells have no nerve supply
Depolarize spontaneously or in response to chemical stimuli that bind to G protein–linked receptors
Chemical factors can include hormones, high CO2, pH, low oxygen
Some smooth muscles respond to both neural and chemical stimuli
Contraction of Smooth Muscle
Special features of smooth muscle contraction
Response to stretch
Stress-relaxation response: responds to stretch only briefly, then adapts to new length
Retains ability to contract on demand
Enables organs such as stomach and bladder to temporarily store contents
Length and tension changes
Can contract when between half and twice its resting length
Allows organ to have huge volume changes without becoming flabby when relaxed
Spinal nerve
Peripheral nerve attached to the spinal cord
Afferent axon
Axon directed toward central nervous system, conveying sensory information
Dorsal root ganglion
Nodule on a dorsal root that contains cell bodies of afferent spinal nerve neurons
Efferent axon (eff ur ent)
Axon directed away from central nervous system, conveying motor commands to muscles and glands
Extrapyramidal System
Part of the Motor System
Named “extrapyramidal” to separate it from the tracts that originate in the cortex
Originates in the brainstem
Carries motor fibers to the spinal cord
Responsible for involuntary movement
Amyotrophic Lateral Sclerosis (ALS)
ALS is characterized for the degeneration of Lower motor neurons in the ventral horn of the spinal cord and brainstem (lower motor neurons).
There is also degeneration of pyramidal neurons in the motor cortex (upper motor neurons).
ALS has an incidence of 1-3 people per 100,000 population
ALS has a prevalence of 5-9 per 100,000 population (20,000 people with ALS at any
time in USA)
The onset of symptoms is assumed to occur when approximately an 80% loss of
motor neurons has been achieved
There is not treatment for ALS, and the survival rate is 1-10 year with onset at 40-50
years of age.
The causes of ALS remain unknown, 10% of cases are familial
NMJ disorders: Genetic defects in myelin
A. Myelin production and function in the Schwann cell are adversely affected by multiple genetic defects including abnormalities in transcription factors, ABC (ATP-binding cassette) transporters in peroxisomes, and multiple proteins implicated in organizing myelin. In compact myelin thin processes of Schwann cells are tightly wrapped around an axon. Viewed microscopically at high power, the site of apposition of the intracellular races of the Schwann cell membrane appears as a dense line, whereas the apposed extracellular faces are described as the intraperiod line (see definition in part C).
B. Peripheral axons are wrapped in myelin, which is compact and tight except near the nodes of Ranvier and at focal sites described as "incisures"
C. The rim of cytoplasm, in which myelin basic protein (MBP) is located, defines the major dense line, whereas the thin layer of residual extracellular space defines the intraperiod line. Three myelin-associated proteins are defective in three different demyelinating neuropathies
NMJ disorders: Morphological abnormalities in MG
Morphological abnormalities of the neuromuscular junction in myasthenia gravis. At the neuromuscular junction ACh is released by exocytosis of synaptic vesicles at active zones in the nerve terminal. Acetylcholine flows across the synaptic cleft to reach receptors that are concentrated at the peaks of junctional folds. Acetylcholinesterase in the cleft rapidly terminates transmission by hydrolyzing ACh. The myasthenic neuromuscular junction has a reduced number of ACh receptors, simplified synaptic folds, and a widened synaptic space, but a normal nerve terminal.
Turnover of ACh receptors increases in myasthenia.
Normal turnover of randomly spaced ACh receptors takes places every 5 to 7 days.
In myasthenia gravis and experimental myasthenia gravis, the cross-linking of ACh receptors by antibodies facilitates endocytosis and the phagocytic destruction of the receptors, which leads to a two- to threefold increase in the rate of receptor turnover. Binding of antireceptor antibody activates the complement cascade, which is involved in focal lysis of the postsynaptic membrane. This focal lysis is probably primarily responsible for the characteristic morphological alterations of postsynaptic membranes in myasthenia
The vestibular apparatus of the inner ear.
The orientations of the vestibular and cochlear divisions of the inner ear are shown with respect to the head.
The inner ear is divided into bony and membranous labyrinths. The bony labyrinth is bounded by the petrous portion of the temporal bone. Lying within this structure is the membranous labyrinth, which contains the receptor organs for hearing (the cochlea) and equilibrium (the utricle, saccule, and semicircular canals). The space between bone and membrane is filled with perilymph, whereas the membranous labyrinth is filled with endolymph. Sensory cells in the utricle, saccule, and ampullae of the semicircular canals respond to motion of the head. Adapted, with permission, from lurato 1967)
The left and right horizontal semicircular canals work together to signal head movement.
Because of inertia, rotation of the head in a counterclockwise direction causes endolymph to move clockwise with respect to the canals. This deflects the stereocilia in the left canal in the excitatory direction, thereby exciting the afferent fibers on this side. In the right canal the afferent fibers are hyperpolarized so that firing decreases.