neuromuscular junctions Flashcards

1
Q

what are the three types of muscle tissue ?

A

cardiac, smooth, skeletal

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2
Q

which muscle tissue is multinucleated ?

A

Skeletal

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3
Q

Name a function of skeletal muscle

A

causes movement
stops movement
prevent excess movement
of the bones and joints, maintaining skeletal stability and preventing skeletal structure damage or deformation.

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4
Q

what is the connective tissue that each muscle is wrapped in called ?

A

epimysium,

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5
Q

what are the functions of epimysium

A

epimysium,
which allows a muscle to contract and move powerfully while maintaining its structural integrity. The epimysium also
separates muscle from other tissues and organs in the area, allowing the muscle to move independently

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6
Q

what are the three types of connective tissues that help support muscles called ?

A

epimysium, perimysium,endomysium

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7
Q

what is the purpose of endomysium ?

A

The endomysium contains the extracellular fluid and nutrients to support the muscle
fiber. These nutrients are supplied via blood to the muscle tissue.

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8
Q

What is the sarcolemma

A

The plasma

membrane of muscle fibers

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9
Q

what is the sarcoplasm

A

the cytoplasm of muscle fibers

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10
Q

what is the sarcoplasmic reticulum

A

the specialized

smooth endoplasmic reticulum, which stores, releases, and retrieves calcium ions (Ca++)

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11
Q

What is the sarcomere ?

A

Each packet of these microfilaments(actin and myosin ) and their regulatory
proteins, troponin and tropomyosin (along with other proteins)
or
the smallest contractile unit of a muscle cell

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12
Q

what is a summary of excitation-contraction coupling ?

A

for a skeletal
muscle fiber to contract, its membrane must first be “excited”—in other words, it must be stimulated to fire an action
potential. The muscle fiber action potential, which sweeps along the sarcolemma as a wave, is “coupled” to the actual
contraction through the release of calcium ions (Ca++) from the SR. Once released, the Ca++ interacts with the shielding
proteins, forcing them to move aside so that the actin-binding sites are available for attachment by myosin heads. The
myosin then pulls the actin filaments toward the center, shortening the muscle fiber.

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13
Q

which neurotransmitter is present at neuromuscular junctions ?

A

acetyl choline

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14
Q

what happens before excitation-contraction coupling ?

A

Signaling begins when a neuronal action potential travels along the axon of a motor neuron, and then along the individual
branches to terminate at the NMJ. At the NMJ, the axon terminal releases a chemical messenger, or neurotransmitter,
called acetylcholine (ACh). The ACh molecules diffuse across a minute space called the synaptic cleft and bind to
ACh receptors located within the motor end-plate of the sarcolemma on the other side of the synapse. Once ACh binds,
a channel in the ACh receptor opens and positively charged ions can pass through into the muscle fiber, causing it to
depolarize, meaning that the membrane potential of the muscle fiber becomes less negative (closer to zero.)
Muscle Tissue

As the membrane depolarizes, another set of ion channels called voltage-gated sodium channels are triggered to open.
Sodium ions enter the muscle fiber, and an action potential rapidly spreads (or “fires”) along the entire membrane to initiate
excitation-contraction coupling.

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15
Q

The receptors on the motor end plate are nicotinic acetylcholine receptors. How can these best be described and what type of ion passes through when acetylcholine binds to them?

A

ligand gated ion channels and sodium is the ion that passes through

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16
Q

What is responsible for the high concentration of calcium ions in the sarcoplasmic reticulum, and what allows its release?

A

the calcium pump pumps calcium against its concentration gradient into the sarcoplasmic reticulum which is released by voltage-gated calcium channels

17
Q

What must happen to the calcium ions surrounding the muscle fibers to allow muscle relaxation?

A

it needs to be sequestered back into the sarcoplasmic reticulum

18
Q

What is an agonist?

A

A ligand that binds to a receptor mediating its activity (i.e. mimicking the original ligand/molecule/neurotransmitter)

19
Q

What is an antagonist?

A

A ligand that binds to a receptor blocking its activity

20
Q

How can both agonists and antagonists to nicotinic acetylcholine receptors both result in muscle relaxation.

A

an antagonist blocks the receptor, not allowing depolarization of the motor end plate. In this case there is no depolarization to cause calcium release from the sarcoplasmic reticulum so no muscle contraction is initiated. In contrast, whilst an agonist activates the receptor causing an initial depolarization it also stays bound to the receptor stopping further depolarisations causing the released calcium ions to be sequestered and muscle relaxation to occur.

21
Q

Why are drugs that cause non-reversible inhibition of enzymes (such as acetylcholinesterase) a bad starting point for developing therapeutics?

A

their action cannot be reversed causing permanent effect and therefore modulation and fidelity is completely lost and will most likely result in severe (life threatening) side effects. Sarin nerve gas being a case in point

22
Q

describe in terms of a sarcomere, why, for the majority of our skeletal muscles, the tension or force is maximum approximately halfway through the range of contraction.

A

The contraction of our muscles is mediated by the cross-bridge cycling between myosin and actin. When the muscle (and therefore the sarcomere) is at its most stretched the h-zone is at its largest. At this point not all the thick filament (composed of myosin molecules) are overlapping the thin filaments (actin, tropomyosin, and troponin) which means that less force can be developed through the cross bridge cycling. At the mid point of the contraction range, the h-zone is smaller, and all the myosin heads are overlapping actin molecules – allowing for maximum tension to be developed. At the final point of the contraction range, there is no more h-zone, there is no further room for the thick filaments to move (i.e. at the z-line) and even some of the thin filaments overlap, losing some of the capacity for cross-bridge cycling hence no more tension can be developed.