Line 1: |
Line 1: |
− | <big><center>[[Musculoskeletal System - Anatomy & Physiology|'''BACK TO MUSCULOSKELETAL ANATOMY AND PHYSIOLOGY''']]</center></big>
| |
| | | |
| + | ==Introduction== |
| + | [[Image:Aspinall Slide3.JPG|thumb|right|250px|<small>Image from [http://www.elsevierhealth.co.uk/veterinary-nursing/spe-60136/ Aspinall, The Complete Textbook of Veterinary Nursing], Elsevier Health Sciences, ''All rights reserved''</small>]] |
| + | Muscle mass accounts for a large majority of the carcass weight of domestic animals. Muscular contraction is necessary for voluntary and involuntary movement of limbs, stabilization of joints, maintaining luminal diameter (in the case of arteries, bowel, etc), and to produce heat. The number of muscle fibers an individual possesses is determined by genetics and is set at birth, although muscle size and type (i.e. glycolytic to oxidative and vice versa) can be altered. Further muscle development therefore occurs by hypertrophy, rather than hyperplasia of muscle fibers. Three types of muscle can be described: |
| | | |
− | ===Introduction===
| + | 1. Skeletal (also referred to as Striated, Somatic, Voluntary) |
| | | |
− | *Skeletal muscle includes muscles of:
| + | 2. Smooth (also referred to as Visceral) |
− | **Posture
| |
− | **Movement
| |
− | **Respiration
| |
| | | |
| + | 3. Cardiac |
| | | |
− | *Two basic types of skeletal myofibre:
| + | ==Skeletal Muscle== |
− | **<u>'''Type I'''</u>
| + | [[Image:Striated Muscle 1.jpg|thumb|right|250px|Striated muscle - Copyright RVC 2008]] |
− | ***Grossly '''red'''
| + | [[Image:muscle.jpg|thumb|right|250px|Triad Junction - Copyright RVC 2008]] |
− | ***'''High''' myoglobin level
| |
− | ***'''Slow''' rate of contraction
| |
− | ***High '''oxidative''' activity
| |
− | ***Function - postural
| |
− | **<u>'''Type II'''</u>
| |
− | ***Grossly '''white'''
| |
− | ***'''Low''' myoglobin level
| |
− | ***'''Fast''' rate of contraction
| |
− | ***High '''glycolytic''' activity
| |
− | ***Function - exercise
| |
| | | |
| + | Each muscle '''belly''' is composed of multiple '''fascicles''', each of which consists of a bundle of muscle '''fibers'''. Muscle "fiber" means a single cell, which is multi-nucleate, and known as '''syncitia'''. |
| | | |
− | *Each muscle is composed of multiple '''fascicles'''
| + | '''Parallel''' fibers: Run from origin to insertion, long fibers allow for a faster contraction and a greater range of motion. |
− | **Each fascicle is composed of multiple polygonal '''myofibres'''
| |
| | | |
| + | '''Pennate''' fibers: Run at an angle to the line of pull of an internal tendon or aponeurosis. Short fibers allow for a greater force capacity. |
| | | |
| + | Within each fiber are groups of parallel, longitudinal myofibrils. Myofibrils are arranged as '''sarcomeres''', bound by Z-discs, which are the functional unit of muscle contraction. Each sarcomere contains two separate groups of myofilaments: |
| + | :#Thin filament, containing '''actin''', located centrally |
| + | :#Thick filament, containing '''myosin''', originating from either side of each Z-disc |
| | | |
| + | There are two basic types of skeletal myofibre: |
| + | :'''Primary: Oxidative''' - Grossly red, with high myoglobin level, slow rate of contraction and a high oxidative activity. The function is for postural, sustained activity. |
| + | :'''Secondary: Glycolytic''' - Grossly white, with low myoglobin level, fast rate of contraction and a high glycolytic activity. The function is for exercise and bursts of activity. |
| | | |
− | ===Regeneration=== | + | ===Neurogenic Contraction=== |
− | [[Image:Muscle regeneration.jpg|right|thumb|100px|<small><center>Muscle regeneration (Image sourced from Bristol Biomed Image Archive with permission)</center></small>]]
| |
| | | |
− | *Skeletal muscle myofibres have substantial regenerative ability
| + | Muscle activation is initiated by a nervous impulse crossing the '''neuromuscular junction'''. Each muscle fiber is controlled by a single motor neuron. The neurotransmitter, '''acetylcholine (Ach)''', binds receptors in the muscle fiber to open Na<sup>+</sup> channels. This causes a wave of depolarization along the sarcoplasmic membrane, further opening voltage-gated Na<sup>+</sup> channels, which propagates the signal along the sarcolemma. Depolarization of the sarcoplasmic reticulum causes [[Calcium|calcium]] to be released, which activates muscle contraction. |
− | *Success depends on:
| |
− | **An intact '''sarcolemmal tube''' - to act as a support and guide
| |
− | **Availability of '''satellite cells''' - to act as progenitor cells for new sarcoplasm production
| |
− | **Macrophages to clear up cell debris
| |
− | **If these conditions are not met (e.g. severe thermal damage) '''fibrosis''' will occur
| |
− | *Stages:
| |
− | #Nuclei in [[Muscles - degenerative#Necrosis|necrotic segement]] disappear, hyalinased sarcoplasm due to loss of normal myofibrillar structure, may separate from adjacent normal myofibrils and/or [[Muscles - degenerative#Calcification|mineralise]]
| |
− | #Monocytes from capillaries -> macrophages in necrotic portion, satellite cells swell -> vesicular with prominent nucleoli -> mitosis (within 1-4 days after initial injury)
| |
− | #Satellite cells move to centre
| |
− | #Macrophages clear the sacrolemmal tube, plasmalemma disappears, shape maintained by basal lamina
| |
− | #Satellite cells -> myoblasts (contain myosin) -> fuse forming myotubes with row of central nuclei; cytoplasmic processes fusing
| |
− | #Growing and differentiating fibre, striations appear - formation of sarcomeres
| |
− | #Nuclei move to peripheral position (2-3 weeks after initial injury)
| |
− | *Regeneration by '''budding'''
| |
− | **When conditions are not optimal, disrupted sacrolemma
| |
− | **E.g. injection of irritating substance, trauma, [[Muscles - degenerative#Ischaemia|infarction]]
| |
− | **Myoblasts proliferate -> sacrolamma bulges from cut part -> club-shaped with numerous central nuclei = muscle giant cells
| |
− | *Monophasic lesions - all at same phase above
| |
− | **Damage occured at one time, e.g. trauma or one toxin exposure
| |
− | *Multiphasic lesions - different stages as described above
| |
− | **Ongoing damage, e.g. vitamin E - selenium deficiency, continuous exposure to toxin
| |
| | | |
| + | Muscle contraction occurs when (thin) actin filaments slide past (thick) myosin filaments. The myosin heads bind actin subunits, forming cross-bridges, hydrolyzing ATP and providing energy for contraction. Myosin heads undergo power stroke, displacing actin and releasing ADP and Pi. In the off state, tropomyosin coiled-coils block the helical grooves of the actin filament. Tropomyosin movement relieves the steric block, allowing access to myosin binding sites. Calcium regulates muscle contraction by binding troponin-C, which is attached to the thin filament. This causes inhibition of the steric block keeping actin and myosin from interacting. Increased calcium causes a negative feedback inhibition of Ca release, and it is pumped back into the sarcoplasmic reticulum by the Ca/ATPase pump. |
| | | |
− | ===Rigor Mortis===
| + | Types of Muscle Contraction: |
| + | :'''Concentric''': muscle shortens and bones are brought closer together. |
| + | :'''Isometric''': muscle is active but does not change in length (force without motion). |
| + | :'''Eccentric''': muscle is active while lengthening. |
| | | |
− | *Muscles remain biochemically active after the death of an animal
| + | ==Smooth Muscle== |
− | *Following a period of relaxation, contraction and stiffening occurs
| + | [[Image:Smooth Muscle 1.jpg|thumb|right|250px|Smooth muscle - Copyright RVC 2008]] |
− | *Due to deficiency of ATP releasing myosin heads from their binding sites at end of power stroke
| |
− | *Onset faster in ATP deprived animals (starvation, hunting, tetanus...)
| |
− | *May be absent in cachetic animals
| |
− | *Disappears due to autolysis or putrefaction
| |
− | *See [[General Pathology - Post-Mortem Change#Rigor Mortis|general pathology]]
| |
| | | |
| + | Smooth muscles have slower contraction and relaxation. An undeveloped sarcoplasmic reticulum means that smooth muscle depends on the plasmalemma release of Ca. Smooth muscle lacks troponin. The control of smooth muscle contraction involves thin and thick filament regulation. Thin filament regulation is carried out by the actin binding protein, '''caldesmon''', which binds the thin filament and blocks myosin access. '''Calmodulin''' (activated by binding Ca) binds caldesmon and causes its dissociation from actin, enabling contraction. Thick filament regulation occurs by the '''phosphorylation''' of the '''regulatory light chain (RLC)'''. Calmodulin-Ca binds and activates myosin light chain kinase (MLCK), MLCK then phosphorylates RLC, turning myosin on. Myosin light chain phosphatase (MLCP) switches myosin off. |
| | | |
| + | ==Cardiac Muscle== |
| | | |
− | <big><center>[[Musculoskeletal System - Anatomy & Physiology|'''BACK TO MUSCULOSKELETAL ANATOMY AND PHYSIOLOGY''']]</center></big> | + | Cardiac muscle is striated but uninucleate and highly vascularized. There are gap junctions concentrated at intercalated discs. |
| + | |
| + | '''Myogenic Contraction''' spreads cell to cell and does not depend on nervous input to individual cells. Areas of low electrical resistance allow rapid spread of action potentials. Contraction is regulated by autonomic neurons and circulating hormones. The contractile mechanism is similar to skeletal muscle, an increase in cytosolic Ca. There is a Ca influx across the plasma membrane AND the sarcoplasmic reticulum. The action potential has a prolonged plateau phase. |
| + | |
| + | ==Tendon== |
| + | [[Image:Tendon micro structure.jpg|right|thumb|250px|Histology of tendon Copyright RVC 2008]] |
| + | |
| + | A tendon is a connective tissue point of attachment between muscle and bone. It consists of dense collagen type 1 fibres and fibroblasts (tenocytes). They possess great tensile strength and are highly elastic. This is important in absorbing and storing energy. An elastic recoil provides a crucial role in locomotion. Tendons can be protected by sesamoid bones at a point of angulation over a bony surface. Fluid-filled bursae provide cushioning and protection where necessary. Walls and sheaths resemble synovial joint components. |
| + | |
| + | ==Links== |
| + | |
| + | Click here for information on [[:Category:Muscles - Pathology|muscle pathology]]. |
| + | |
| + | Click here for information on [[:Category:Bursae and Tendons - Pathology|bursae and tendons pathology]]. |
| + | |
| + | {{Template:Learning |
| + | |powerpoints = [[Muscle Tissue Histology resource|Muscle tissue histology tutorial which looks at different types of muscle in different tissues]] |
| + | |dragster = [[Muscle Histology Resource]] |
| + | }} |
| + | |
| + | |
| + | ==Webinars== |
| + | <rss max="10" highlight="none">https://www.thewebinarvet.com/orthopaedics/webinars/feed</rss> |
| + | [[Category:Musculoskeletal System - Anatomy & Physiology]] |
| + | [[Category:A&P Done]] |