The Heart As A Pump - physiological processes involved in cardiac pump function Flashcards
How many chambers does the mammalian heart have?
Colours?
4
RA (blood from body)
RV (pumps the o2-poor blood to the lungs)
LA (blood from the lungs)
LV (pumps the o2-rich blood to the body)
Right = blue Left = red
The heart has a thick muscular wall, particularly in the LV
The structure of Heart muscle?
Vena cava
RA > Tricuspid valve > RV > Pulmonary valve >
Pulmonary Artery
Pulmonary vein
LA > mitral valve > LV > aortic valve >
Aorta
Cardiac cycle graph..
Reasoning for the dichortic notches in aortic pressure and atrial pressure
Why LAP continues dropping for a while even after the mitral valve has opened.
Aortic pressure
Atrial pressure
Ventricular pressure
Ventricular volume
ECG…
Systole: increase ventricular pressure, decrease in ventricular volume
Diastole: heart relaxing
What is the muscular myocardium mainly made up of?
Mainly made up of cardiomyocytes. - has a v.limited capacity to regenerate (‘terminally differentiated’)
Describe the process of regulating excitation-contraction coupling.
Depolarization of muscle cells activates the L-type Ca channel…
That Inflow of Ca activates another Ca channel (ryr-receptor)…
>Calcium-induced Calcium-release
This amount of Ca that’s available for contraction can be regulated in both directions: increase Ca = stronger contractile force
Note: This Ca oscillates bw the SR and cytosol on a beat-to-beat basis.
Back into SR thru protein SERCA2 - a key regulator of cardiac diastolic function
How can the Excitation-Contraction coupling process be regulated?
(B-adrenergic stimulation = increase HR, increase in the strength of contraction, and increase in the rate of myocyte contraction + relaxation).
PKA - the common modulator - targets the proteins that are key regulators of each of these processes.
PLN inhibits the cardiac muscle SR Ca ATPase = decrease contractility and the rate of muscle relaxation.
However, when phosphorylated (by PKA), the protein is disinhibited = faster Ca uptake into the SR.
PKA activators: beta-adrenergic agonist Epinephrine. May enhance the rate of cardiac myocyte relaxation. In addition, since the protein is more active, increased contractility
> Adrenaline: increase HR + force of contraction via B1-receptors - due to phosphorylation, by PKA
Epinephrine: increase HR + force of contraction via B1-receptors (results in increase in cardiac output)
ACh: decrease HR + cardiac output etc via cholinergic (M2) receptors.
3 ways how Heart rate & force of contraction can be regulated
> Adrenaline (hormone)
Sympathetic neural activation
ACh (parasympathetic)
How can Excitation-contraction mechanism go wrong in diseases?
Eg: Ischemia. Decrease in ATP = Ca overload = cell death
Ischemia happens during heart attack or myocardial infarction (supply to myocardium is interrupted)
Cardiac diastolic function reduced, weak/ prevent next AP for next contractility
Length-tension relationship
Because of the structure of the myofilaments of the muscle (where you have the thick + thin filaments sliding over each other) there’s a relationship bw the development of contractile force and the length of the sarcomere - and the repeating units of the thick + thin filaments where they overlap.
There’s an optimal sarcomere length in order to generate force of contraction, where you have maximum overlap of thick + thin filaments (myosin heads interacting w actin myosin in thin filament)
What is the optimal sarcomere length in cardiac muscle?
~2.2 micrometer
Each sarcomere = contractile unit.
It is repeated many times in muscle cells
The filament overlap explanation is unlikely to be the full story. What are the Other possible explanations?
> stretch-dependent sensitivity of Troponin C to Ca
> decreasing inter-filament spacing facilitating cross-bridge formation when myocytes are stretched.
Preload?
If the muscle is sensitive to stretch, it means it’s responsible to these concepts…
Preload - LV wall stress/tension at End Diastole.
Therefore can apply LaPlace’s law!
Higher preload means there’s a higher diastolic volume in ventricle (so also a higher ED ventricular pressure)
LaPlace’s law?
Apply this to Preload..
Wall stress (T) = (P * r) / 2w
r = r(in) + w
Pressure = mmHg 1mL = 1cm^3
V=P/Elastane (constant for a while, but goes up very quickly after a certain point
When the wall thickness of LV and Elastance are constant, people don’t need to use equation to know preload. They’ll know if it’s changed just by looking at change in pressure.
Impact of stretching out heart cells?
Effect of (ED) preload on LV pressure during systole?
Increase stretching of heart cells essentially allows more myosin burning ATP and turning it into mechanical energy (how?).
>larger LV force of contraction
Via 2 mechanisms: Frank-starling & Inotropic
Force - pushing blood out against a certain area. Force/area=pressure
So larger force of contraction = large LV pressure (during systole)
Therefore a higher preload (set up the stretching of heart cells) = (as a result of 2 mechanisms) larger LV pressure during systole.
Frank-starling mechanism
>idea of stretch relating to force.
Goal is to pull the Z-disks in closer to each other -myosin holding onto actin to bring Z-disks in.
Very low preload:
Titin has almost no space, myosin (crowded) almost touching the Z-disk = almost no force.
A lot of Myosin not grabbing the correct Actin (polarity). They’re blocked by the other Actin segment
High preload:
Z-disks have a lot of room
There is no actin overlap. = lots of force!
Too stretched:
No crowding issue
However, actin is out of reach. = no force
