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HISTOLOGY OF MUSCLE TISSUE 1
What are the major function of muscle tissue There are four characteristics associated with muscle tissue 1. Excitability Tissue can receive and respond to stimulation 2. Contractility Tissue can shorten and thicken 3. Extensibility Tissue can lengthen 4. Elasticity Tissue can return to its resting state 2 INTRODUCTION
The characteristic of muscle tissue enable it to perform some important functions, including: Movement (both voluntaryily and involuntarily) Maintaining posture Supporting soft tissues within body cavities Guarding entrance and exits of the body Maintaining body temperature 3
Types of Muscles Tissue 4 1. Skeletal Muscle Responsible for skeletal movement and organs such as eyeballs. Fibres are cylindrical in shape and Striated due to arrangment of contractile proteins. Multinucleated and eccentrical nucleus Under voluntary control. Account for 40% body weight
2. Cardiac Muscles Found only in the wall of the heart, Striated and involuntary contraction Muscle fibres are cylindrical but branched Intercalated disk is present Single nucleus that is centrally located 5
3. Smooth Muscle Found in walls of hollowed organs Non striated Involuntary contraction Spindled shape cells with centrally located nucleus 6
Their cells are called fibres because they are elongated Contractions depend on myofilaments Actin Myosin Cytoplasm is called sarcoplasm Smooth endoplasmic reticulum is called sarcoplasmic reticulum Plasmamembrane is called sarcolemma Sarcos = flesh Lemma = sheath 7 Similarities between the three types of Muscles
Skeletal Muscle Skeletal muscle is composed of long, cylindrical, multinucleated cells that undergo voluntary contraction to facilitate movement of the body or its parts During embryonic development, several hundred myoblasts, precursors of skeletal muscle fibers, line up end to end, fusing with one another to form long multinucleated cells known as myotubes. These newly formed myotubes manufacture cytoplasmic constituents as well as contractile elements, called myofibrils Myofibrils are composed of specific arrays of myofilaments, the proteins responsible for the contractile capability of the cell 8
9
Endomysium; Reticular fibers surrounding each muscle fibre plus the external (basal) lamina produced by the muscle fiber Perimysium; Dense connective tissue surrounding groups of fibers and dividing the muscle into fascicles Epimysium; Dense connective tissue surrounding the entire muscle, blends with the deep fascia and tendons Connective Tissue Covering Of Skeletal Muscle 10
One of the most important roles of connective tissue is to mechanically transmit the forces generated by contracting muscle cells, because in most instances, individual muscle cells do not extend from one end of a muscle to the other 11
12 Fig; connective tissue covering; endomysium, perimysium and epimysium
Myofilaments; Visible only with the electron microscope; composed primarily of actin, which forms 5-nm wide thin filaments, and myosin, which forms 15-nm wide thick filaments Myofibrils; Visible with the light microscope, 1–2 microns wide, oriented parallel to the long axis of the cell; composed of bundles of overlapping myofilaments that are arranged in register, producing an alternating light-dark, striated banding pattern Hierarchy Of Skeletal Muscle Organization 13
Muscle fiber; Specialized term for a muscle cell, 10–100 microns wide; sarcoplasm is filled with hundreds of myofibrils, which are oriented parallel to each other and to the long axis of the muscle fiber. Muscle fascicle; Collection of muscle fibers surrounded by perimysium; collections of muscle fascicles are surrounded by the epimysium and form a muscle. 14
Individual muscle cells(muscle fibre) are grouped together into elongated bundles – fasciculi Each fibre is separated by a thin layer of connective tissue called endomysium A group of fasciculi are surrounded by a connective tissue sheath called perimysium The epimysium is no difference from the deep fascia 15
16
ACTIN FILAMENT 1. F-actin- double helix filament composed of G-actin monomeres 2. Tropomyosin – double helix peptide chain; runs in the groove of F-actin chains 3. Troponin complex (3 globular proteins - subunits): Troponin C (TnC) – binds calcium ions → contraction Troponin T (TnT) – attachment of troponin to tropomyosin Troponin I (TnI) – inhibits actin-myosin interaction 17
18 myosin
A troponin complex is attached at one specific site on each tropomyosin molecule In thin filaments, each tropomyosin molecule spans seven G-actin molecules and has one troponin complex bound to its surface 19
MYOSIN Myosin, a much larger complex, can be dissociated into two identical heavy chains and two pairs of light chains. Myosin heavy chains are thin, rodlike molecules made up of two heavy chains twisted together. Myosin head (flexible; binds to actin filament) Myosin head has: Actin binding site ATP binding site ATP-ase activity 20
21
22
Several hundred myosin molecules are arranged within each thick filament with their rodlike portions overlapping and their globular heads directed toward either end Analysis of thin sections of striated muscle shows the presence of cross-bridges between thin and thick filaments. These bridges, which are known to be formed by the head of the myosin molecule plus a short part of its rodlike portion, are involved in the conversion of chemical energy into mechanical energy 23
Arrangement of myofilaments within a myofibril in register result in the banding pattern seen at microscopic levels. • A band appears dark and contains actin and myosin. • I band appears light and contains actin only. 24
• Z-line, composed of alpha-actinin, is located in the center of the I band. • H band is located in the center of the A band and represents the area where actin is not present. • M band is located in the center of the H band and represents areas of cross-connections between myosin filaments. 25
26
27
Contractile unit of striated muscle fibers, seen in both skeletal and cardiac muscle fibers It extend from Z-line to Z-line Contains α-actinin, protein that binds actin filaments to Z-line Sarcomeres are repeated in series along the length of each myofibril. Adjacent myofibrils maintain the alignment of sarcomeres. 28 SARCOMERE
29
No changes in lenght of : 1. A-band 2. actin and myosin filaments. 30 Alterations In Sarcomeres During Contraction During contraction occurs shortening of 1. Sarcomeres shorten. 2. Z-line interval narrows. 3. I-band 4. H-band (in maximal contraction could disapear
MECHANISM OF CONTRACTION Resting sarcomeres consist of partially overlapping thick and thin filaments. During contraction, both the thick and thin filaments retain their original length. Because contraction is not caused by a shortening of individual filaments, it must be the result of an increase in the amount of overlap between the filaments. The sliding filament hypothesis of muscle contraction has received the most widespread acceptance 31
The following is a brief description of how actin and myosin interact during a contraction cycle. At rest, ATP binds to the ATPase site on the myosin heads, but the rate of hydrolysis is very slow. Myosin requires actin as a cofactor to break down ATP rapidly and release energy. In a resting muscle, myosin cannot associate with actin, because the binding sites for myosin heads on actin molecules are covered by the troponin, tropomyosin complex on the F-actin filament 32
When sufficiently high concentrations of calcium ions are available, however, they bind to the TnC subunit of troponin. The spatial configuration of the three troponin subunits changes and drives the tropomyosin molecule deeper into the groove of the actin helix This exposes the myosin-binding site on the globular actin components, so that actin is free to interact with the head of the myosin molecule 33
The binding of calcium ions to the TnC unit corresponds to the stage at which myosin ATP is converted into the active complex. As a result of bridging between the myosin head and the G-actin subunit of the thin filament, the ATP is split into ADP and Pi (phosphate ion), and energy is released. This activity leads to a deformation, or bending, of the head and a part of the rodlike portion (hinge region) of the myosin Because the actin is bound to the myosin, movement of the myosin head pulls the actin past the myosin filament. The result is that the thin filament is drawn farther into the A band. 34
Although a large number of myosin heads extends from the thick filament, at any one time during the contraction only a small number of heads aligns with available actin-binding sites. As the bound myosin heads move the actin, however, they provide for alignment of new actin myosin bridges. The old actin myosin bridges detach only after the myosin binds a new ATP molecule; This action also resets the myosin head and prepares it for another contraction cycle. If no ATP is available, the actin myosin complex becomes stable; This accounts for the extreme muscular rigidity (rigor mortis) that occurs after death. 35
A single muscle contraction is the result of hundreds of bridge-forming and bridge-breaking cycles. The contraction activity that leads to a complete overlap between thin and thick filaments continues until Ca2+ ions are removed and the troponin “tropomyosin complex again covers the myosin-binding site 36
During contraction, the I band decreases in size as thin filaments penetrate the A band. The H band ”the part of the A band with only thick filaments” diminishes in width as the thin filaments completely overlap the thick filaments. A net result is that each sarcomere, and consequently the whole cell (fiber), is greatly shortened 37
Skeletal Muscle Innervation Skeletal muscle cells and the single motor neuron that innervates them constitute a motor unit. Each skeletal muscle receives at least two types of nerve fibers: motor and sensory. The motor nerve functions in eliciting contraction, whereas the sensory fibers pass to muscle spindles Additionally, autonomic fibers supply the vascular elements of skeletal muscle. The specificity of motor innervation is a function of the muscle innervated 38
Muscle fatigue For a single muscle fiber, fatigue indicates an inability to develop tension when it is stimulated Causes: reduction in the rate of intracellular calcium release and uptake by sacroplasmic reticulum It dependent on muscle itself, exercise duration, fiber type composition, and/or pattern of motor unit activation 39
When muscles cause a limb to move through the joint's range of motion, They usually act and are further classified into the following cooperating groups: AGONIST MUSCLES In a desired movement, the muscle mostly involved with that movement is the agonist or commonly referred to as prime movers. Agonist or prime movers may contract concentrically to lift a weight, or eccentrically to lower that weight. 40
ANTAGONISTIC MUSCLES The muscle that lies directly opposite to the agonist or prime mover and is responsible for the opposing action of that movement is the antagonistic muscle. The triceps are the antagonist muscle to the biceps curl for instance, and the biceps would be the antagonist in a triceps extension. They are responsible for returning a limb to its initial position. 41
SYNERGISTS These muscles perform, or assist in performing, the same set of joint motion as the agonists. Synergists are sometimes referred to as neutralizers because they help cancel out, or neutralize, extra motion from the agonists to make sure that the force generated works within the desired plane of motion. 42
43 Bundles form thick myocardium Cells are branch Cells join at intercalated discs 1-2 nuclei in center Inherent rhythmicity: each cell! (muscle cells beat separately without any stimulation) Myofilament organisation is similar to skeletal muscles’s hence the striations CARDIAC MUSCLES
Smooth Muscles Muscles are spindle-shaped cells One central nucleus Grouped into sheets: often running perpendicular to each other Peristalsis No striations (no sarcomeres) Contractions are slow, sustained and resistant to fatigue Does not always require a nervous signal: can be stimulated by stretching or hormones 44
Major Locations Inside the eye Walls of vessels Respiratory tubes Digestive tubes Urinary organs Reproductive organs 45
Actin and myosin myofilaments are present, but they are not organized into a regular pattern, they are randomly arranged. Electron Dense bodies containing alpha actin are present in the cytoplasm of smooth muscle cells These dense bodies Serve as insertion points for myofilaments to transmit the force of filament sliding Thus, resemble Z-lines of striated muscle 46 Organization of the Contractile Proteins in Smooth Muscles
47

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  • 2. What are the major function of muscle tissue There are four characteristics associated with muscle tissue 1. Excitability Tissue can receive and respond to stimulation 2. Contractility Tissue can shorten and thicken 3. Extensibility Tissue can lengthen 4. Elasticity Tissue can return to its resting state 2 INTRODUCTION
  • 3. The characteristic of muscle tissue enable it to perform some important functions, including: Movement (both voluntaryily and involuntarily) Maintaining posture Supporting soft tissues within body cavities Guarding entrance and exits of the body Maintaining body temperature 3
  • 4. Types of Muscles Tissue 4 1. Skeletal Muscle Responsible for skeletal movement and organs such as eyeballs. Fibres are cylindrical in shape and Striated due to arrangment of contractile proteins. Multinucleated and eccentrical nucleus Under voluntary control. Account for 40% body weight
  • 5. 2. Cardiac Muscles Found only in the wall of the heart, Striated and involuntary contraction Muscle fibres are cylindrical but branched Intercalated disk is present Single nucleus that is centrally located 5
  • 6. 3. Smooth Muscle Found in walls of hollowed organs Non striated Involuntary contraction Spindled shape cells with centrally located nucleus 6
  • 7. Their cells are called fibres because they are elongated Contractions depend on myofilaments Actin Myosin Cytoplasm is called sarcoplasm Smooth endoplasmic reticulum is called sarcoplasmic reticulum Plasmamembrane is called sarcolemma Sarcos = flesh Lemma = sheath 7 Similarities between the three types of Muscles
  • 8. Skeletal Muscle Skeletal muscle is composed of long, cylindrical, multinucleated cells that undergo voluntary contraction to facilitate movement of the body or its parts During embryonic development, several hundred myoblasts, precursors of skeletal muscle fibers, line up end to end, fusing with one another to form long multinucleated cells known as myotubes. These newly formed myotubes manufacture cytoplasmic constituents as well as contractile elements, called myofibrils Myofibrils are composed of specific arrays of myofilaments, the proteins responsible for the contractile capability of the cell 8
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  • 10. Endomysium; Reticular fibers surrounding each muscle fibre plus the external (basal) lamina produced by the muscle fiber Perimysium; Dense connective tissue surrounding groups of fibers and dividing the muscle into fascicles Epimysium; Dense connective tissue surrounding the entire muscle, blends with the deep fascia and tendons Connective Tissue Covering Of Skeletal Muscle 10
  • 11. One of the most important roles of connective tissue is to mechanically transmit the forces generated by contracting muscle cells, because in most instances, individual muscle cells do not extend from one end of a muscle to the other 11
  • 12. 12 Fig; connective tissue covering; endomysium, perimysium and epimysium
  • 13. Myofilaments; Visible only with the electron microscope; composed primarily of actin, which forms 5-nm wide thin filaments, and myosin, which forms 15-nm wide thick filaments Myofibrils; Visible with the light microscope, 1–2 microns wide, oriented parallel to the long axis of the cell; composed of bundles of overlapping myofilaments that are arranged in register, producing an alternating light-dark, striated banding pattern Hierarchy Of Skeletal Muscle Organization 13
  • 14. Muscle fiber; Specialized term for a muscle cell, 10–100 microns wide; sarcoplasm is filled with hundreds of myofibrils, which are oriented parallel to each other and to the long axis of the muscle fiber. Muscle fascicle; Collection of muscle fibers surrounded by perimysium; collections of muscle fascicles are surrounded by the epimysium and form a muscle. 14
  • 15. Individual muscle cells(muscle fibre) are grouped together into elongated bundles – fasciculi Each fibre is separated by a thin layer of connective tissue called endomysium A group of fasciculi are surrounded by a connective tissue sheath called perimysium The epimysium is no difference from the deep fascia 15
  • 16. 16
  • 17. ACTIN FILAMENT 1. F-actin- double helix filament composed of G-actin monomeres 2. Tropomyosin – double helix peptide chain; runs in the groove of F-actin chains 3. Troponin complex (3 globular proteins - subunits): Troponin C (TnC) – binds calcium ions → contraction Troponin T (TnT) – attachment of troponin to tropomyosin Troponin I (TnI) – inhibits actin-myosin interaction 17
  • 19. A troponin complex is attached at one specific site on each tropomyosin molecule In thin filaments, each tropomyosin molecule spans seven G-actin molecules and has one troponin complex bound to its surface 19
  • 20. MYOSIN Myosin, a much larger complex, can be dissociated into two identical heavy chains and two pairs of light chains. Myosin heavy chains are thin, rodlike molecules made up of two heavy chains twisted together. Myosin head (flexible; binds to actin filament) Myosin head has: Actin binding site ATP binding site ATP-ase activity 20
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  • 23. Several hundred myosin molecules are arranged within each thick filament with their rodlike portions overlapping and their globular heads directed toward either end Analysis of thin sections of striated muscle shows the presence of cross-bridges between thin and thick filaments. These bridges, which are known to be formed by the head of the myosin molecule plus a short part of its rodlike portion, are involved in the conversion of chemical energy into mechanical energy 23
  • 24. Arrangement of myofilaments within a myofibril in register result in the banding pattern seen at microscopic levels. • A band appears dark and contains actin and myosin. • I band appears light and contains actin only. 24
  • 25. • Z-line, composed of alpha-actinin, is located in the center of the I band. • H band is located in the center of the A band and represents the area where actin is not present. • M band is located in the center of the H band and represents areas of cross-connections between myosin filaments. 25
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  • 28. Contractile unit of striated muscle fibers, seen in both skeletal and cardiac muscle fibers It extend from Z-line to Z-line Contains α-actinin, protein that binds actin filaments to Z-line Sarcomeres are repeated in series along the length of each myofibril. Adjacent myofibrils maintain the alignment of sarcomeres. 28 SARCOMERE
  • 29. 29
  • 30. No changes in lenght of : 1. A-band 2. actin and myosin filaments. 30 Alterations In Sarcomeres During Contraction During contraction occurs shortening of 1. Sarcomeres shorten. 2. Z-line interval narrows. 3. I-band 4. H-band (in maximal contraction could disapear
  • 31. MECHANISM OF CONTRACTION Resting sarcomeres consist of partially overlapping thick and thin filaments. During contraction, both the thick and thin filaments retain their original length. Because contraction is not caused by a shortening of individual filaments, it must be the result of an increase in the amount of overlap between the filaments. The sliding filament hypothesis of muscle contraction has received the most widespread acceptance 31
  • 32. The following is a brief description of how actin and myosin interact during a contraction cycle. At rest, ATP binds to the ATPase site on the myosin heads, but the rate of hydrolysis is very slow. Myosin requires actin as a cofactor to break down ATP rapidly and release energy. In a resting muscle, myosin cannot associate with actin, because the binding sites for myosin heads on actin molecules are covered by the troponin, tropomyosin complex on the F-actin filament 32
  • 33. When sufficiently high concentrations of calcium ions are available, however, they bind to the TnC subunit of troponin. The spatial configuration of the three troponin subunits changes and drives the tropomyosin molecule deeper into the groove of the actin helix This exposes the myosin-binding site on the globular actin components, so that actin is free to interact with the head of the myosin molecule 33
  • 34. The binding of calcium ions to the TnC unit corresponds to the stage at which myosin ATP is converted into the active complex. As a result of bridging between the myosin head and the G-actin subunit of the thin filament, the ATP is split into ADP and Pi (phosphate ion), and energy is released. This activity leads to a deformation, or bending, of the head and a part of the rodlike portion (hinge region) of the myosin Because the actin is bound to the myosin, movement of the myosin head pulls the actin past the myosin filament. The result is that the thin filament is drawn farther into the A band. 34
  • 35. Although a large number of myosin heads extends from the thick filament, at any one time during the contraction only a small number of heads aligns with available actin-binding sites. As the bound myosin heads move the actin, however, they provide for alignment of new actin myosin bridges. The old actin myosin bridges detach only after the myosin binds a new ATP molecule; This action also resets the myosin head and prepares it for another contraction cycle. If no ATP is available, the actin myosin complex becomes stable; This accounts for the extreme muscular rigidity (rigor mortis) that occurs after death. 35
  • 36. A single muscle contraction is the result of hundreds of bridge-forming and bridge-breaking cycles. The contraction activity that leads to a complete overlap between thin and thick filaments continues until Ca2+ ions are removed and the troponin “tropomyosin complex again covers the myosin-binding site 36
  • 37. During contraction, the I band decreases in size as thin filaments penetrate the A band. The H band ”the part of the A band with only thick filaments” diminishes in width as the thin filaments completely overlap the thick filaments. A net result is that each sarcomere, and consequently the whole cell (fiber), is greatly shortened 37
  • 38. Skeletal Muscle Innervation Skeletal muscle cells and the single motor neuron that innervates them constitute a motor unit. Each skeletal muscle receives at least two types of nerve fibers: motor and sensory. The motor nerve functions in eliciting contraction, whereas the sensory fibers pass to muscle spindles Additionally, autonomic fibers supply the vascular elements of skeletal muscle. The specificity of motor innervation is a function of the muscle innervated 38
  • 39. Muscle fatigue For a single muscle fiber, fatigue indicates an inability to develop tension when it is stimulated Causes: reduction in the rate of intracellular calcium release and uptake by sacroplasmic reticulum It dependent on muscle itself, exercise duration, fiber type composition, and/or pattern of motor unit activation 39
  • 40. When muscles cause a limb to move through the joint's range of motion, They usually act and are further classified into the following cooperating groups: AGONIST MUSCLES In a desired movement, the muscle mostly involved with that movement is the agonist or commonly referred to as prime movers. Agonist or prime movers may contract concentrically to lift a weight, or eccentrically to lower that weight. 40
  • 41. ANTAGONISTIC MUSCLES The muscle that lies directly opposite to the agonist or prime mover and is responsible for the opposing action of that movement is the antagonistic muscle. The triceps are the antagonist muscle to the biceps curl for instance, and the biceps would be the antagonist in a triceps extension. They are responsible for returning a limb to its initial position. 41
  • 42. SYNERGISTS These muscles perform, or assist in performing, the same set of joint motion as the agonists. Synergists are sometimes referred to as neutralizers because they help cancel out, or neutralize, extra motion from the agonists to make sure that the force generated works within the desired plane of motion. 42
  • 43. 43 Bundles form thick myocardium Cells are branch Cells join at intercalated discs 1-2 nuclei in center Inherent rhythmicity: each cell! (muscle cells beat separately without any stimulation) Myofilament organisation is similar to skeletal muscles’s hence the striations CARDIAC MUSCLES
  • 44. Smooth Muscles Muscles are spindle-shaped cells One central nucleus Grouped into sheets: often running perpendicular to each other Peristalsis No striations (no sarcomeres) Contractions are slow, sustained and resistant to fatigue Does not always require a nervous signal: can be stimulated by stretching or hormones 44
  • 45. Major Locations Inside the eye Walls of vessels Respiratory tubes Digestive tubes Urinary organs Reproductive organs 45
  • 46. Actin and myosin myofilaments are present, but they are not organized into a regular pattern, they are randomly arranged. Electron Dense bodies containing alpha actin are present in the cytoplasm of smooth muscle cells These dense bodies Serve as insertion points for myofilaments to transmit the force of filament sliding Thus, resemble Z-lines of striated muscle 46 Organization of the Contractile Proteins in Smooth Muscles
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