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Muscular System
Locomotion
( movement of the parts or the whole body).
Types of muscles
• According to the histological structure
1- Striated muscles, contain striations.
2- Unstriated muscles, no striations (smooth).
• According to the position :
1- Skeletal muscles, present around the skeleton.
2- Cardiac muscles, present in the heart.
3- Visceral muscles, present in the viscera and urinary bladder.
• According to the ability of controlling the contraction:
1- Voluntary muscles, contract under our control.
2- Unvoluntary muscles, contract without control of us.
Skeletal muscle
• according to protein in myosin: two types:
a) Slow unit
* red - dark- respond slowly- long twitch duration (up to
100 ms) - low mitochondrial ATP ase activity ,
* Produce ATP slowly
* In large limp muscle
* Ex. marathon runners (more red fibers)
b) Fast unit
* Pale(white) - short twitch duration ( 7 ms) - * produce
ATP quickly – more powerful contractions – fine ,skilled
movement
* Ex. Weighlifters
Skeletal (voluntary; striated) muscle
• Attach to skeleton
• Function in movement (bone)
• Contract voluntary
C.N.S. neuromuscular junction
• Connect to the bone through the beginning
(origin) other end (insertion)
• If the origin formed of 2 parts(Biceps) or 3
(Triceps)
• Ends with tendons
Structure
Each muscle composed of many myofibrils(muscle
fibers).
Cylindrical shape, multinucleated.
Each myofibril composed of many myofibrils .
Each myofibril composed of many repeated sarcomeres.
Myofibrile appear as alternated dark and light bands.
Light band is called Isotropic band (I),
Dark band is called Anisotropic band (A).
Each sarcomere composed of many myofilaments.
( thin ) actin , troponin , tropomysin
( thick ) myosin .
Molecular structure:
Myosin:
• Thick helical protein filament.
• Consists of heads and tails.
• By proteiolytic enzyme(trypsin) broken into:
** light meromyosin (LMM) : H-zone
No ATPase activity and can’t combine with actin.
No heads at the H-zone.
** Heavy meromyosin (HMM) contain ATP ase activity , can
combine with actin.
• Release the heads from the tails if treated with pepsin enzyme.
• The head of the myosin molecule forms cross bridge with the
adjacent actin filament.
Actin:
•Thin filaments actin with small amount of tropomyosin and
troponin.
•In ionic environment of the cell, actin exist in the fibrous
form (F-actin) containing 2 chains of actin monomer coiled
around each other.
•In the absence of salts, actin becomes globular (G-actin).
•The change from F- actin to G- actin is reversible and is
called ( G F ) transformation;
• Troponin and tropomyosin
(Regulatory agent in muscle contraction)
At rest ,tropomyosin block the binding of actin to myosin.
• Troponin is formed of 3 subunits:
Troponin (I) inhibit the interaction of myosin to actin.
Troponin (C) which contain the binding sites of Ca++ that
initiate the contraction of the myofilaments.
Troponin (T) binds the other troponin component to
tropomyosin.
Classification according to the movement
:
• 1- a) Flexor; bends one part upon another.
• b) Extensor; straightens or extends part.
• 2- a) Adductor; draws a part towards the axis
• b) Abductor; draws a part away of the axis
• 3- a) Depressor; lowers a part.
• b) Elevator; elevate or raise a part.
• 4- a) Constrictor; constricts or close an organ.
• b) Dilator; cause dilation of the same organ.
• 5- Rotator Muscle; rotates on part on another
CARDIAC MUSCLES:
 They contract involuntary, and rythimitically.
 They obey all or non law.
They are auto stimulated (pace maker).
Striated muscle
 Pump blood
 Adapted for resistant to fatigue
**A lot mitochondria (aerobic respiration)
**Numerous myoglobins (O2 storing pigment)
**Good blood supply
Intercalated discs (support contration) double membrane separating
adjacent cells.
Cell junctions fuse together the plasma membranes of cardiac muscle cells,
allow the cells to contract as a unit.
Smooth muscle
Unstriated
 Walls of hollow organs
( gastrointestinal tube & respiratory system )
 Two types
 multi-unit: without interconnection,iris
 single-unit :(walls of viscera)
Spindle shape –single nucleus
 Arranged in sheets
 Few mitochondria(depend on anaerobic glycolysis)
 Contain myosin & actin (not arranged into
sarcomeres)
 Stimulated by
Autonomic nervous system ( involuntary)
Hormons ( vasoconstriction & vasodilators)
adrenalin
EFFECT OF STIMULUS:
a- In skeletal Muscle:
• Threshold Stimulus:
no responds occur.
• Minimal Stimulus:
responds by minimal observed line.
• Submaximal Stimulus:
increasing the stimulus, the number of
responding fibers increase
• Maximum Stimulus:
all muscle fibers contract.
• Supra-maximum Stimulus:
increasing the stimulus, no more effect.
B- In cardiac Muscle:
• Sub-minimal stimulus;
no responds occur.
• Threshold value;
all muscle fibers
respond,increasing
stimulus no more effect
will resulted.
Steps of Contraction:
• Release of transmitter at motor end
plate.
• Generation of action potential.
• Inward spread of depolarization
along T-tubules.
• Release of Ca++ ions.
• Binding of Ca++ ions to troponin C.
• Uncovering myosin binding sites on
actin.
• Formation of cross-Linkage between
actin and myosin
• Sliding of actin over myosin,
producing shortening.
Steps Of Relaxation:
•Ca++ ions pumped back
into sarcoplasmic
reticulum.
•Release of Ca++ ions from
troponin.
•Cessation of interaction
between actin and
myosin.
Changes accompanying muscle contraction:
Thermal Change:
Heat of contraction and relaxation.
PH Changes:
Accompanied the chemical changes, acid by
splitting ATP or base by breakdown of CP.
Electrical change:
Direct or indirect depolarization through the
connected nerve.
Chemical change:
(Aerobic or anaerobic) oxidative respiration,
CP is an immediate source of ATP ( phosphrelate
ADP).
Mechanical
changes:
Sliding of actin
filament over the
myosin filaments,
( cross bridge).
physiology : muscular system
physiology : muscular system

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physiology : muscular system

  • 1.
  • 2. Muscular System Locomotion ( movement of the parts or the whole body).
  • 3. Types of muscles • According to the histological structure 1- Striated muscles, contain striations. 2- Unstriated muscles, no striations (smooth). • According to the position : 1- Skeletal muscles, present around the skeleton. 2- Cardiac muscles, present in the heart. 3- Visceral muscles, present in the viscera and urinary bladder. • According to the ability of controlling the contraction: 1- Voluntary muscles, contract under our control. 2- Unvoluntary muscles, contract without control of us.
  • 5.
  • 6.
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  • 8.
  • 9. • according to protein in myosin: two types: a) Slow unit * red - dark- respond slowly- long twitch duration (up to 100 ms) - low mitochondrial ATP ase activity , * Produce ATP slowly * In large limp muscle * Ex. marathon runners (more red fibers) b) Fast unit * Pale(white) - short twitch duration ( 7 ms) - * produce ATP quickly – more powerful contractions – fine ,skilled movement * Ex. Weighlifters
  • 10. Skeletal (voluntary; striated) muscle • Attach to skeleton • Function in movement (bone) • Contract voluntary C.N.S. neuromuscular junction • Connect to the bone through the beginning (origin) other end (insertion) • If the origin formed of 2 parts(Biceps) or 3 (Triceps) • Ends with tendons
  • 11. Structure Each muscle composed of many myofibrils(muscle fibers). Cylindrical shape, multinucleated. Each myofibril composed of many myofibrils . Each myofibril composed of many repeated sarcomeres. Myofibrile appear as alternated dark and light bands. Light band is called Isotropic band (I), Dark band is called Anisotropic band (A). Each sarcomere composed of many myofilaments. ( thin ) actin , troponin , tropomysin ( thick ) myosin .
  • 12.
  • 13.
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  • 15.
  • 16.
  • 17.
  • 18. Molecular structure: Myosin: • Thick helical protein filament. • Consists of heads and tails. • By proteiolytic enzyme(trypsin) broken into: ** light meromyosin (LMM) : H-zone No ATPase activity and can’t combine with actin. No heads at the H-zone. ** Heavy meromyosin (HMM) contain ATP ase activity , can combine with actin. • Release the heads from the tails if treated with pepsin enzyme. • The head of the myosin molecule forms cross bridge with the adjacent actin filament.
  • 19. Actin: •Thin filaments actin with small amount of tropomyosin and troponin. •In ionic environment of the cell, actin exist in the fibrous form (F-actin) containing 2 chains of actin monomer coiled around each other. •In the absence of salts, actin becomes globular (G-actin). •The change from F- actin to G- actin is reversible and is called ( G F ) transformation;
  • 20. • Troponin and tropomyosin (Regulatory agent in muscle contraction) At rest ,tropomyosin block the binding of actin to myosin. • Troponin is formed of 3 subunits: Troponin (I) inhibit the interaction of myosin to actin. Troponin (C) which contain the binding sites of Ca++ that initiate the contraction of the myofilaments. Troponin (T) binds the other troponin component to tropomyosin.
  • 21.
  • 22.
  • 23. Classification according to the movement : • 1- a) Flexor; bends one part upon another. • b) Extensor; straightens or extends part. • 2- a) Adductor; draws a part towards the axis • b) Abductor; draws a part away of the axis • 3- a) Depressor; lowers a part. • b) Elevator; elevate or raise a part. • 4- a) Constrictor; constricts or close an organ. • b) Dilator; cause dilation of the same organ. • 5- Rotator Muscle; rotates on part on another
  • 24. CARDIAC MUSCLES:  They contract involuntary, and rythimitically.  They obey all or non law. They are auto stimulated (pace maker). Striated muscle  Pump blood  Adapted for resistant to fatigue **A lot mitochondria (aerobic respiration) **Numerous myoglobins (O2 storing pigment) **Good blood supply
  • 25. Intercalated discs (support contration) double membrane separating adjacent cells. Cell junctions fuse together the plasma membranes of cardiac muscle cells, allow the cells to contract as a unit.
  • 26. Smooth muscle Unstriated  Walls of hollow organs ( gastrointestinal tube & respiratory system )  Two types  multi-unit: without interconnection,iris  single-unit :(walls of viscera)
  • 27. Spindle shape –single nucleus  Arranged in sheets  Few mitochondria(depend on anaerobic glycolysis)  Contain myosin & actin (not arranged into sarcomeres)  Stimulated by Autonomic nervous system ( involuntary) Hormons ( vasoconstriction & vasodilators) adrenalin
  • 28. EFFECT OF STIMULUS: a- In skeletal Muscle: • Threshold Stimulus: no responds occur. • Minimal Stimulus: responds by minimal observed line. • Submaximal Stimulus: increasing the stimulus, the number of responding fibers increase • Maximum Stimulus: all muscle fibers contract. • Supra-maximum Stimulus: increasing the stimulus, no more effect. B- In cardiac Muscle: • Sub-minimal stimulus; no responds occur. • Threshold value; all muscle fibers respond,increasing stimulus no more effect will resulted.
  • 29.
  • 30.
  • 31. Steps of Contraction: • Release of transmitter at motor end plate. • Generation of action potential. • Inward spread of depolarization along T-tubules. • Release of Ca++ ions. • Binding of Ca++ ions to troponin C. • Uncovering myosin binding sites on actin. • Formation of cross-Linkage between actin and myosin • Sliding of actin over myosin, producing shortening.
  • 32.
  • 33. Steps Of Relaxation: •Ca++ ions pumped back into sarcoplasmic reticulum. •Release of Ca++ ions from troponin. •Cessation of interaction between actin and myosin.
  • 34. Changes accompanying muscle contraction: Thermal Change: Heat of contraction and relaxation. PH Changes: Accompanied the chemical changes, acid by splitting ATP or base by breakdown of CP. Electrical change: Direct or indirect depolarization through the connected nerve. Chemical change: (Aerobic or anaerobic) oxidative respiration, CP is an immediate source of ATP ( phosphrelate ADP).
  • 35. Mechanical changes: Sliding of actin filament over the myosin filaments, ( cross bridge).