Anrep effect: Difference between revisions

Latest revision as of 05:11, 19 March 2025

Anrep Effect is an intrinsic autoregulatory mechanism of the heart, in which an increase in afterload leads to an increase in myocardial contractility. This physiological response helps the ventricles compensate for increased resistance to blood ejection, ensuring stable stroke volume and cardiac output despite variations in aortic pressure.

The effect was first described in 1912 by Russian physiologist Gleb von Anrep, who experimentally demonstrated that increasing afterload results in a proportional and linear increase in ventricular contractility, independent of neural or hormonal influences. This phenomenon has since been recognized as an important component of cardiac autoregulation.

Mechanism[edit]

The Anrep effect is primarily mediated by mechanosensitive ion exchange mechanisms in cardiac myocytes, which enable the heart to adjust contractility in response to changes in arterial pressure. The process involves the following steps:

Increased afterload: A sudden rise in aortic blood pressure leads to an increased end-systolic volume and reduced stroke volume due to the greater resistance encountered by the ventricles.
Myocardial stretch: The sustained increase in ventricular wall tension due to the higher end-diastolic volume activates stretch-sensitive Na⁺/H⁺ exchangers in the sarcolemma.
Sodium accumulation: Activation of the Na⁺/H⁺ exchanger leads to an influx of Na⁺ ions, altering the intracellular sodium gradient.
Calcium retention: The increased intracellular Na⁺ levels reduce the driving force for the sodium-calcium exchanger (NCX), impairing the normal extrusion of Ca²⁺ from the cell.
Enhanced calcium cycling: The sarco/endoplasmic reticulum Ca²⁺-ATPase (SERCA) actively uptakes the excess intracellular calcium, leading to:

Increased calcium-induced calcium release (CICR) from the sarcoplasmic reticulum.
Increased contractile force during subsequent cardiac cycles.

Compensation: The stronger contractions help restore stroke volume and maintain perfusion pressure to vital organs.

This adaptation is particularly crucial for preventing circulation failure when systemic vascular resistance increases, such as during hypertension or exercise.

Physiological Significance[edit]

The Anrep effect plays an essential role in cardiac physiology by:

Allowing the heart to maintain adequate stroke volume despite fluctuations in arterial pressure.
Preventing a decline in cardiac output when afterload increases.
Acting as an intrinsic mechanism of cardiac adaptation, independent of autonomic regulation.
Helping compensate for transient fluctuations in blood pressure, ensuring stable perfusion to vital organs.

Without the Anrep effect, an acute rise in aortic blood pressure would result in a persistent reduction in stroke volume, compromising circulation and leading to inadequate tissue perfusion.

Experimental Observations[edit]

The Anrep effect has been confirmed through experiments in denervated heart preparations, such as the Starling Preparation, which eliminates the influence of autonomic nervous system regulation. This confirms that the effect is an intrinsic myocardial response, rather than a reflexive adaptation involving neural or hormonal pathways.

Clinical Implications[edit]

While the Anrep effect is generally a beneficial physiological response, its dysfunction or exaggeration can contribute to certain cardiovascular conditions:

Heart Failure with Preserved Ejection Fraction (HFpEF): Chronic elevation of afterload (e.g., due to hypertension) can lead to pathological myocardial hypertrophy, impairing ventricular compliance.
Hypertension: Sustained activation of the Anrep effect may contribute to left ventricular hypertrophy, a risk factor for heart failure and arrhythmias.
Ischemic Heart Disease: Some studies suggest that the Anrep effect may arise as a transient compensatory response to myocardial ischemia, particularly in the setting of acute hypertensive episodes.

Controversies and Alternative Theories[edit]

There has been some debate regarding whether the Anrep effect is a distinct physiological process or a secondary effect of myocardial recovery from ischemia. Some researchers have proposed that:

The observed increase in contractility following an abrupt rise in afterload may be due to reperfusion recovery from transient ischemia.
The role of autocrine and paracrine factors in myocardial stretch response remains under investigation.

Despite these debates, the Anrep effect remains a well-established concept in cardiac physiology, with significant implications for hemodynamic regulation.

Historical Perspective[edit]

The Anrep effect is named after Gleb von Anrep, a Russian physiologist who first described this phenomenon in 1912. His research on cardiovascular autoregulation provided foundational insights into how the heart adapts to changes in arterial resistance. His discoveries complemented earlier work on cardiac function, including Starling’s law of the heart.

References[edit]

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-The '''Anrep effect''' is an autoregulation method in which [[myocardial]] [[contractility]] increases with [[afterload]]. It was experimentally determined that increasing afterload caused a proportional linear increase in [[Ventricle (heart)|ventricular]] inotropy.<ref>{{Cite journal | last1 = Von Anrep | first1 = G. | title = On the part played by the suprarenals in the normal vascular reactions of the body | journal = The Journal of Physiology | volume = 45 | issue = 5 | pages = 307–317 | year = 1912 | pmid = 16993158 | pmc = 1512890 | doi=10.1113/jphysiol.1912.sp001553}}</ref>
+'''Anrep Effect''' is an intrinsic autoregulatory mechanism of the [[heart]], in which an increase in [[afterload]] leads to an increase in [[myocardial]] [[contractility]]. This physiological response helps the [[ventricle (heart)|ventricles]] compensate for increased resistance to blood ejection, ensuring stable [[stroke volume]] and [[cardiac output]] despite variations in [[aortic pressure]].
-This effect is found in denervated [[heart]] preparations, such as the '''Starling Preparation''', and as such, represents an intrinsic autoregulation mechanism.
+The effect was first described in 1912 by Russian physiologist '''[[Gleb von Anrep]]''', who experimentally demonstrated that increasing [[afterload]] results in a proportional and linear increase in [[ventricular]] contractility, independent of [[neural]] or [[hormonal]] influences. This phenomenon has since been recognized as an important component of [[cardiac autoregulation]].
-The Anrep effect is named after Russian physiologist Gleb von Anrep,<ref name="gleb">{{Cite journal | last1 = Gaddum | first1 = J. H. | doi = 10.1098/rsbm.1956.0002 | title = Gleb Anrep. 1891-1955 | journal = Biographical Memoirs of Fellows of the Royal Society | volume = 2 | pages = 19–42 | year = 1956 | jstor = 769473| pmid =  | pmc = }}</ref> who described it in 1912.
+== Mechanism ==
+The Anrep effect is primarily mediated by '''mechanosensitive ion exchange mechanisms''' in [[cardiac myocytes]], which enable the heart to adjust contractility in response to changes in [[arterial pressure]]. The process involves the following steps:
-Functionally, the Anrep effect allows the heart to compensate for an increased end-systolic volume present and the decreased stroke volume that occurs when aortic blood pressure increases. Without the Anrep effect, an increase in aortic [[blood pressure]] would create a decrease in stroke volume that would compromise circulation to peripheral and visceral tissues.
+# '''Increased [[afterload]]:''' A sudden rise in [[aortic blood pressure]] leads to an increased '''end-systolic volume''' and reduced '''stroke volume''' due to the greater resistance encountered by the ventricles.
+# '''Myocardial stretch:''' The sustained increase in ventricular wall tension due to the higher '''end-diastolic volume''' activates stretch-sensitive Na<sup>+</sup>/H<sup>+</sup> exchangers in the '''sarcolemma'''.
+# '''Sodium accumulation:''' Activation of the '''Na<sup>+</sup>/H<sup>+</sup> exchanger''' leads to an influx of '''Na<sup>+</sup> ions''', altering the intracellular '''sodium gradient'''.
+# '''Calcium retention:''' The increased '''intracellular Na<sup>+</sup> levels''' reduce the driving force for the '''sodium-calcium exchanger (NCX)''', impairing the normal extrusion of '''Ca<sup>2+</sup>''' from the cell.
+# '''Enhanced calcium cycling:''' The '''sarco/endoplasmic reticulum Ca<sup>2+</sup>-ATPase (SERCA)''' actively uptakes the excess intracellular calcium, leading to:
+* Increased '''calcium-induced calcium release (CICR)''' from the '''sarcoplasmic reticulum'''.
+* Increased '''contractile force''' during subsequent cardiac cycles.
+# '''Compensation:''' The stronger contractions help restore '''stroke volume''' and maintain '''perfusion pressure''' to vital organs.
-Sustained myocardial stretch activates tension dependent Na<sup>+</sup>/H<sup>+</sup> exchangers, bringing Na<sup>+</sup> ions into the sarcolemma.
+This adaptation is particularly crucial for preventing circulation failure when '''systemic vascular resistance''' increases, such as during '''hypertension''' or '''exercise'''.
-This increase in Na<sup>+</sup> in the sarcolemma reduces the Na<sup>+</sup> gradient exploited by [[sodium-calcium exchanger]] (NCX) and stops them from working effectively.
-Ca<sup>2+</sup> ions accumulate inside the sarcolemma as a result and are uptaken by sarco/endoplasmic reticulum Ca2+-ATPase ([[SERCA]]) pumps.
-Calcium induced calcium release (CICR) from the sarcoplasmic reticulum is increased upon stimulation of the cardiac myocyte by an action potential.
-This leads to an increase in the force of contraction of the cardiac muscle to try and increase stroke volume and cardiac output to maintain tissue perfusion.
-On the other hand, it has been proposed that the Anrep effect may be a spurious effect resulting from the recovery of the myocardium from a transient ischemia arising from the abrupt increase in blood pressure.<ref>{{Cite journal | last1 = Monroe | first1 = R. G. | doi = 10.1172/JCI107074 | title = The Anrep Effect Reconsidered | journal = The Journal of Clinical Investigation | volume = 51 | pages = 2573–2583 | year = 1972 | pmc = 332955 | pmid=5056656}}</ref>
+== Physiological Significance ==
+The Anrep effect plays an essential role in cardiac physiology by:
+* Allowing the heart to maintain '''adequate stroke volume''' despite fluctuations in '''arterial pressure'''.
+* Preventing a '''decline in cardiac output''' when '''afterload increases'''.
+* Acting as an '''intrinsic mechanism''' of cardiac adaptation, independent of '''autonomic regulation'''.
+* Helping compensate for transient '''fluctuations in blood pressure''', ensuring stable perfusion to vital organs.
-==References==
+Without the Anrep effect, an acute rise in '''aortic blood pressure''' would result in a '''persistent reduction in stroke volume''', compromising circulation and leading to inadequate '''tissue perfusion'''.
+== Experimental Observations ==
+The Anrep effect has been confirmed through experiments in denervated '''heart preparations''', such as the '''[[Starling Preparation]]''', which eliminates the influence of '''autonomic nervous system regulation'''. This confirms that the effect is an '''intrinsic myocardial response''', rather than a reflexive adaptation involving '''neural or hormonal pathways'''.
+== Clinical Implications ==
+While the Anrep effect is generally a '''beneficial physiological response''', its dysfunction or '''exaggeration''' can contribute to certain cardiovascular conditions:
+* '''Heart Failure with Preserved Ejection Fraction (HFpEF):''' Chronic elevation of '''[[afterload]]''' (e.g., due to '''hypertension''') can lead to '''pathological myocardial hypertrophy''', impairing ventricular compliance.
+* '''Hypertension:''' Sustained activation of the '''Anrep effect''' may contribute to '''left ventricular hypertrophy''', a risk factor for '''heart failure''' and '''arrhythmias'''.
+* '''Ischemic Heart Disease:''' Some studies suggest that the Anrep effect may arise as a '''transient compensatory response''' to '''myocardial ischemia''', particularly in the setting of acute '''hypertensive episodes'''.
+== Controversies and Alternative Theories ==
+There has been some debate regarding whether the '''Anrep effect''' is a distinct physiological process or a secondary effect of '''myocardial recovery from ischemia'''. Some researchers have proposed that:
+* The observed increase in '''contractility''' following an abrupt rise in '''afterload''' may be due to '''reperfusion recovery''' from transient ischemia.
+* The role of '''autocrine and paracrine factors''' in myocardial stretch response remains under investigation.
+Despite these debates, the '''Anrep effect''' remains a well-established concept in '''[[cardiac physiology]]''', with significant implications for '''hemodynamic regulation'''.
+== Historical Perspective ==
+The '''Anrep effect''' is named after '''[[Gleb von Anrep]]''', a Russian physiologist who first described this phenomenon in '''1912'''. His research on '''cardiovascular autoregulation''' provided foundational insights into how the heart adapts to changes in '''arterial resistance'''. His discoveries complemented earlier work on '''cardiac function''', including '''Starling’s law of the heart'''.
+== See Also ==
+* '''[[Frank-Starling mechanism]]''' – The relationship between ventricular filling and contraction strength.
+* '''[[Bowditch effect]]''' – The increase in myocardial contractility with increasing heart rate.
+* '''[[Laplace's law (heart)]]''' – The relationship between wall tension, pressure, and ventricular radius.
+* '''[[Hypertensive heart disease]]''' – The pathological effects of chronic hypertension on the heart.
+== References ==
 {{reflist}}
 [[Category:Cardiology]]
+[[Category:Cardiac physiology]]
+[[Category:Circulatory system]]
 {{circulatory-stub}}
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