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Structural Support and Movement Chapter 36 Part 2 36.7 How Does Skeletal Muscle Contract? Myofibrils (bundles of contractile filaments) run the length of the muscle fiber Myofibrils are divided into bands (striations) that define units of contraction (sarcomeres) • Z-bands attach sarcomeres to each other Sarcomeres contain two types of filaments • Thin, globular protein filaments (actin) • Thick, motor protein filaments (myosin) Fine Structure of Skeletal Muscle Fig. 36-17a, p. 628 outer sheath of one skeletal muscle one bundle of many muscle fibers in parallel inside the sheath one myofibril in one fiber Fig. 36-17a, p. 628 Fig. 36-17b, p. 628 one myofibril inside fiber b Skeletal muscle fiber, longitudinal section. All bands of its myofibrils line up in rows and give the fiber a striped appearance. sarcomere Z band sarcomere Z band H zone Z band Fig. 36-17b, p. 628 Fig. 36-17c, p. 628 Z band H zone Z band c Sarcomeres. Many thick and thin filaments overlap in an A band. Only thick filaments extend across the H zone. Only thin filaments extend across I bands to the Z bands. Different proteins organize and stabilize the array. I band A band I band Fig. 36-17c, p. 628 Fig. 36-17 (d-e), p. 628 one actin molecule d Arrangement of actin molecules in the thin filaments part of a myosin molecule e part of a thin filament part of a thick filament Arrangement of myosin molecules in the thick filaments Fig. 36-17 (d-e), p. 628 Animation: Structure of skeletal muscle The Sliding Filament Model Sliding filament model • Interactions among protein filaments within a muscle fiber’s individual contractile units (sarcomeres) bring about muscle contraction • A sarcomere shortens when actin filaments are pulled toward the center of the sarcomere by ATP-fueled interactions with myosin filaments The Sliding Filament Model Fig. 36-18a, p. 629 A Relative positions of actin and myosin filaments inside a sarcomere between contractions actin Z band myosin actin Z band Fig. 36-18a, p. 629 Fig. 36-18b, p. 629 B Relative positions of actin and myosin filaments in the same sarcomere, contracted Fig. 36-18b, p. 629 Fig. 36-18c, p. 629 myosin head one of many myosin-binding sites on actin C Myosin in a muscle at rest. Earlier, all myosin heads were energized by binding ATP, which they hydrolyzed to ADP and inorganic phosphate. Fig. 36-18c, p. 629 Fig. 36-18d, p. 629 cross-bridge cross-bridge D A rise in the local concentration of calcium exposes binding sites for myosin on actin filaments, so cross-bridges form. Fig. 36-18d, p. 629 Fig. 36-18e, p. 629 E Binding makes each myosin head tilt toward the sarcomere’s center and slide the bound actin along with it. ADP and phosphate are released as the myosin heads drag the actin filaments inward, which pulls the Z bands closer. Fig. 36-18e, p. 629 Fig. 36-18f, p. 629 F New ATP binds to myosin heads, which detach from actin. ATP is hydrolyzed, which returns myosin heads to their original positions. Fig. 36-18f, p. 629 A Relative positions of actin and myosin filaments inside a sarcomere between contractions actin myosin actin Z band Z band B Relative positions of actin and myosin filaments in the same sarcomere, contracted myosin head one of many myosin-binding sites on actin cross-bridge cross-bridge C Myosin in a muscle at rest. Earlier, all myosin heads were energized by binding ATP, which they hydrolyzed to ADP and inorganic phosphate. D A rise in the local concentration of calcium exposes binding sites for myosin on actin filaments, so crossbridges form. E Binding makes each myosin head tilt toward the sarcomere’s center and slide the bound actin along with it. ADP and phosphate are released as the myosin heads drag the actin filaments inward, which pulls the Z bands closer. F New ATP binds to myosin heads, which detach from actin. ATP is hydrolyzed, which returns myosin heads to their original positions. Stepped Art Fig. 36-18, p. 629 Animation: Sliding filament model 36.8 From Signal to Response: A Closer Look at Contraction Like neurons, muscle cells are excitable • Skeletal muscle contracts in response to a signal from a motor neuron • Release of ACh at a neuromuscular junction causes an action potential in the muscle cell Nervous Control of Contraction Action potentials travel along muscle plasma membrane, down T tubules, to the sarcoplasmic reticulum (a smooth endoplasmic reticulum) Action potentials open voltage-gated channels in sarcoplasmic reticulum, triggering calcium release that allows contraction in myofibrils Nervous Control of Contraction Fig. 36-19a, p. 630 motor neuron A A signal travels along the axon of a motor neuron, from the spinal cord to a skeletal muscle. section from spinal cord Fig. 36-19a, p. 630 Fig. 36-19b, p. 630 B The signal is transferred from the motor neuron to the muscle at neuromuscular junctions. Here, ACh released by the neuron’s axon terminals diffuses into the muscle fiber and causes action potentials. neuromuscular junction section from skeletal muscle Fig. 36-19b, p. 630 Fig. 36-19c, p. 630 C Action potentials propagate along a muscle fiber’s plasma membrane down to T tubules, then to the sarcoplasmic reticulum, which releases calcium ions. The ions promote interactions of myosin and actin that result in contraction. sarcoplasmic T reticulum tubule one myofibril in muscle fiber muscle fiber’s plasma membrane Fig. 36-19c, p. 630 Animation: Nervous system and muscle contraction The Roles of Troponin and Tropomyosin Two proteins regulate bonding of actin to myosin • Tropomyosin prevents actin from binding to myosin • Troponin has calcium binding sites Calcium binds to troponin, which pulls tropomyosin away from myosin-binding sites on actin Cross-bridges form, sarcomeres shorten, and muscle contracts Interactions of Actin, Tropomyosin, and Troponin A Actin (tan) with troponin (teal) and tropomyosin (green) in a thin filament myosin-binding of muscle at rest. site blocked by B View of a section through the filament tropomyosin shown above. C Some calcium ions (orange) released by the sarcoplasmic reticulum bind to troponin. D Troponin changes shape and pulls tropomyosin away from the myosin-binding site. myosin head E The myosin head binds to the nowexposed binding site. F A cross-bridge forms between actin and myosin. Fig. 36-20, p. 631 Animation: Troponin and tropomyosin 36.9 Energy for Contraction Multiple metabolic pathways can supply the ATP required for muscle contraction Muscles use any stored ATP, then transfer phosphate from creatine phosphate to ADP to form ATP With ongoing exercise, aerobic respiration and lactic acid fermentation supply ATP Three Metabolic Pathways Supply ATP pathway 1 dephosphorylation of creatine phosphate ADP + Pi creatine pathway 2 aerobic respiration oxygen pathway 3 lactate fermentation glucose from bloodstream and from glycogen breakdown in cells Fig. 36-21, p. 631 pathway 1 dephosphorylation of creatine phosphate ADP + Pi creatine pathway 2 aerobic respiration oxygen pathway 3 lactate fermentation glucose from bloodstream and from glycogen breakdown in cells Stepped Art Fig. 36-21, p. 631 Animation: Energy sources for contraction 36.10 Properties of Whole Muscles Motor unit • One motor neuron and all of the muscle fibers its axons synapse with Muscle twitch • Contraction produced by brief stimulation of a motor unit Tetanus • A sustained contraction caused by repeated stimulation of a motor unit in a short interval Muscle Twitch and Tetanus B Repeated stimuli over a short time have an additive effect; they increase the force of contraction. Force relaxation starts stimulus contraction Force A A single, brief stimulus causes a twitch, a rapid contraction followed by immediate relaxation. C Sustained stimulation causes tetanus, a sustained contraction with several times the force of a twitch. Force six stimulations per second twitch tetanic contraction repeated stimulation Time Fig. 36-22, p. 632 B Repeated stimuli over a short time have an additive effect; they increase the force of contraction. Force relaxation starts stimulus contraction Force A A single, brief stimulus causes a twitch, a rapid contraction followed by immediate relaxation. C Sustained stimulation causes tetanus, a sustained contraction with several times the force of a twitch. Force six stimulations per second twitch tetanic contraction repeated stimulation Time Stepped Art Fig. 36-22, p. 632 Animation: Types of contractions Motor Units and Muscle Tension Muscle tension • The mechanical force exerted by a muscle • The more motor units stimulated, the greater the muscle tension A load opposes muscle tension • Isotonic contraction: muscle shorten and move the load • Isometric contraction: muscles tense but do not shorten or move the load Isotonic and Isometric Contraction contracted muscle can shorten contracted muscle can’t shorten Fig. 36-23, p. 632 Fatigue, Exercise, and Aging Muscle fatigue • Decrease in capacity to generate force; muscle tension declines despite repeated stimulation • Aerobic exercise makes muscles more resistant to fatigue (increases blood supply, mitochondria) • Intense exercise increases actin and myosin All muscle fibers form before birth; number and size of muscle fibers decline as people age 36.11 Disruption of Muscle Contraction Some genetic disorders, diseases, or toxins can cause muscles to contract too little or too much • Muscular dystrophy (X-linked disorder) • Motor neuron disorders (polio, ALS) • Botulism (Clostridium botulinum toxin) and tetanus (C. tetani toxin) Muscular Dystrophy Muscle fibers break down, muscles fail – death results from respiratory failure Fig. 36-24a, p. 633 Fig. 36-24b, p. 633 Tetanus C. tetani infection, preventable by tetanus vaccine 36.7-36.11 Key Concepts Skeletal Muscle Function Muscle fibers contract in response to signals from a motor neuron A muscle fiber contains many myofibrils, each divided crosswise into sarcomeres ATP-driven interactions between protein filaments shorten sarcomeres, causing muscle contraction Animation: Muscle contraction overview ABC video: Taller and Taller ABC video: Dolphin receives artificial fin Video: Pumping up muscles Video: Hummingbird at nest Animation: Structure of a sarcomere