Describe the smooth muscle distribution of pre and post capillary vessels:
Pre capillary vessels have far more smooth muscle that post.
Describe the ANS innervation of the vascular beds:
Innervation: Post ganglion nerve processes characterised by regular swellings (Sympathetic adrenergic nerve terminals)
- Arteries and arterioles densely innervated
- Caps not.
- Veins sparsely innervated (but increases with size)
NB: Some organs have PSNS cholingergic innervation of precap. vessels. (gut?)
Describe the pressure drop across the network:
- Large conduit art. have little drop
- Gradient drop across the small arteries and arterioles (a.k.a pre-cap resistance vessels) These create the variable resistance
- Cap, venules, and small veins contribute to SOME resistance
What regulates the blood flow to vascular networks? in the physical sense? How does this change pressure dynamics?
Reference:
- Resistance
- Pressure gradient
- Hydrostatic pressure
- Coordinated alteration of the lumen of pre-cap resistance vessels
-[Vasodilation drops resistance and increases blood flow. Vasoconstriction increases resistance and reduces blood flow.]
= Changed pressure across a network
= Increased pressure gradient across vessels with higher resistance
= Increased resistance upstream causes reduces hydrostatic pressure in caps b/c the energy is dissipated prev.
Conversely:
- Dilation of preacps, drops pressure gradient in them but increases blood flow and increase cap hydrostatic pressure.
Where is most of the circulatory blood stored?
Small veins and venules
What happens with venoconstriction?
- Pressure (VR and Cap)
Reduced capacity to store blood and increases effective driving pressure back to the heart. (Venous return)
Such changes influence post cap. resistance and thus cap. hydrostatic pressure.
How does intravascular pressure also impact the fluid compartments?
Intravascular pressure distribution affects the movement between fluid compartments i.e
Cap pressure magnitude and direction of fluid movement is determined by balance of:
- Transmural gradients of hydrostatic and colloid osmotic pressure.
What typically happens with fluid movement in the capillaries? When might this change?
- Fluid filtered at arterial end is normally absorbed at venous end.
= Net fluid movement is little.
BUT constriction of pre-cap = inc. resistance, decreased flow and hydrostatic pressure = favours movement from interstital space to vascular compartment. Vasodilation does vice versa.
Does vascular SM contain basal tone? Does it have pacemaker activity?
Yes, it has spontaneous activity.
Yes it has pacemaker activity and because cells are coupled this spreads.
What does the small dimension of vascular smooth muscle mean?
They are effected significantly by the external environment i.e
- Metabolism
- Paracrine factors
- Hormones
- Autonomic nerves
- The endothelial layer also influences their activity
What are the things that affect vascular smooth muscle?
Autoregulation:
- Myogenic control
- Metabolic control
- Endothelial control
- Flow induce vasodilation
- Neurohormonal control
What is VSM autoregulation?
- Intrinsic tendency of an organ to maintain a constant blood flow despite changes in the perfusion pressure.
(perfusion pressure being arterio-venous delta)
i.e Even if venous pressure increase, there may be an increase of flow but it returns to steady state.(and vice versa)
The level of blood that is maintained is determined by its metabolic needs.
Describe how the effectiveness of autoregulation varies between vascular beds:
- Cutaneous blood flow exhibits nearly not autoregulation
- Cerebral is tightly regulated, but this is limited to between 50-180mmHg. (true for all vascular beds but varies)
What does reactive hyperaemia demonstrate?
- Links metabolism to blood flow
- If you occlude blood vessels for short periods of time, post release BF is elevated above pre-occlusion levels and this hyperaemia is maintained for for a period roughly proportional to the occlusion time.
What do autoregulation and reactive hyperaemia reflect?
- Operation of local control
- Occurs in deinnervated vascular beds.
What is myogenic control?
- An increase in transmural pressure acting in a BV = increased vascular contraction. (vice versa)
- Most potent in medium arterioles, small and medium veins.
How is myogenic control hypothesised to work?
- Distension triggers depolarisation and contraction of VSM.
- Stretch sensitive ion channels.
What is metabolic control when it comes to VSM? Where is it most potent?
- Metabolism produces vasoactive substances i.e Adenosine, osmolarity, CO2, K. (Varying mechanisms)
- They can induce vascular vasodilation.
- Their concentrations depend on rate of production and wash out. Thus varying effect)
- Most potent in pre-cap vessels.
Describe the endothelial control of blood vessels: What are two examples:
- Produce a number of vasoactive substances in response to blood flow and likely endothelial deformation
i.e
NO = cGMP = Dec. Ca, Hyperpolarisation = Vasodilation
Endothelin: Ca channel agonist, alters ANS of VSM = vasoconstrictor
What does the myogenic, metabolic and endothelial mechanisms fail to explain?
They dont explain the vasodilation that occurs rapidly in proximal pre-capillary blood vessels, when tissue metabolism is increased. (i.e metabolic explains distal microcirculation dilations etc but not upstream)
Thus there must be additional pathways that signal upstream.
Describe the proposed integrated model of local control:
- Metabolites dilate the microcirculation beds
- This increases flow and the increased flow signals upstream to dilate these precapillary vessels.
- Furthermore, ATP release from Hb when they are reduced is posited to release a ‘wave of endothelial electrical activity that causes vasodilation’. Hypothesis of course.
What are the vascular mechanisms of the venous vessels?
- Vasodilator metabolites have little effect
- Vascular pressure and thus myogenic response facilitates constriction and enhanced venous return.
Overview of the neurohormonal control of vascular function:
- Neurotransmitters act on vessels of circulating hormones bind to receptors on vascular smooth muscle of endothelium and induce an effect
Describe how sympathetic adrenergic nerves cause vasoconstriction:
- NE main neurotransmitter, but co-transmitters i.e ATP and NPY are stored in vesicles and released.
- NE -> Gprotein (a1) or a2 = Vasoconstriction
NB: Increased cAMP = Vasodilation because it activates PKA which sequesters Ca.
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Lecture 5: Nephron function 133
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Lecture 6: Nephron function 222
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Lecture 2: Renal Histology31
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Lecture 14: Water and salt balance Part 121
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Lecture 15: Renal disease34
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Lecture 18: Clinical problem solving: Hyponatraemia36
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Lecture 21: Clinical problem solving - Renal failure23
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Lecture 25: Water and salt balance 215
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Lecture 1: CV function10
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Lecture 2: Cardiac electrophysiology and arrhythmia25
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Lecture 3: Pathophysiology of resp. failure28
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Lecture 4: Treatment of cardiac rhythm disturbances32
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Lecture 5: Pathophysiology of resp. failure part 215
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Lecture 6: Anticoagulant drugs33
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Lecture 7: Regulation of cardiac function21
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Lecture 8: ACE inhibitors29
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Lecture 9: Alpha blockers and Ca channel blockers22
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Lecture 10: Vascular function 129
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Lecture 11: Beta blockers22
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Lecture 12: Antihypertensives26
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Lecture 13: Vascular function part 211
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Lecture 14: Aspirin21
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Lecture 15: Clinical endocrinology0
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Lecture 16: CV Control 115
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Lecture 17: Statins20
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Lecture 18: CV control 221
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Lecture 19: Clinical renal failure50
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Lecture 20: Salt and water45
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Lecture 21: Mg and K33
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Lecture 22-24: Acid:Base Part One39
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Lecture 22-24: Acid:Base Part Two44
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Drug essentials1
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GI Problems One: Luminal pathology30
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GI Problems Two: Jaundice38
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GI problems Three: The liver39
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GI Problems Four: Viral hepatitis13
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Cardiac rhythm problems38
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Ischeamic heart disease problems30
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Cardiac function problems16
