Cardiac muscle cell

Cardiac muscle cells

Illustration of a myocardiocyte, including organelles and cell membrane functions
Details
Precursor Mesoderm
System Cardiovascular system
Identifiers
Latin cardiomyocytus; myocytus cardiacus
Code TH H2.00.05.2.02004

Anatomical terminology

Cardiac muscle cells or cardiomyocytes (also known as myocardiocytes[1] or cardiac myocytes[2]) are the muscle cells (myocytes) that make up the cardiac muscle. Each myocardial cell contains myofibrils, which are specialized organelles consisting of long chains of sarcomeres, the fundamental contractile units of muscle cells. Cardiomyocytes show striations similar to those on skeletal muscle cells. Unlike multinucleated skeletal cells, the majority of cardiomyocytes contain only one nucleus, although they may have as many as four.[3] Cardiomyocytes have a high mitochondrial density, which allows them to produce adenosine triphosphate (ATP) quickly, making them highly resistant to fatigue.

Structure

There are two types of cells within the heart: the cardiomyocytes and the cardiac pacemaker cells. Cardiomyocytes make up the atria (the chambers in which blood enters the heart) and the ventricles (the chambers where blood is collected and pumped out of the heart). These cells must be able to shorten and lengthen their fibers and the fibers must be flexible enough to stretch. These functions are critical to the proper form during the beating of the heart.[4]

Cardiac pacemaker cells carry the impulses that are responsible for the beating of the heart. They are distributed throughout the heart and are responsible for several functions. First, they are responsible for being able to spontaneously generate and send out electrical impulses. They also must be able to receive and respond to electrical impulses from the brain. Lastly, they must be able to transfer electrical impulses from cell to cell.[5]

All of these cells are connected by cellular bridges. Porous junctions called intercalated discs form junctions between the cells. They permit sodium, potassium and calcium to easily diffuse from cell to cell. This makes it easier for depolarization and repolarization in the myocardium. Because of these junctions and bridges the heart muscle is able to act as a single coordinated unit.[6][7]

The cardiomyocytes are about 100 to 150 micrometers long and 15 to 20 micrometers in diameter.

Development

Humans are born with a set number of heart muscle cells, or cardiomyocytes, which increase in size as our heart grows larger during childhood development. Recent evidence suggests that cardiomyocytes are actually slowly turned over as we age, but that less than 50% of the cardiomyocytes we are born with are replaced during a normal life span.[8] The growth of individual cardiomyocytes not only occurs during normal heart development, it also occurs in response to extensive exercise (athletic heart syndrome), heart disease, or heart muscle injury such as after a myocardial infarction. A healthy adult cardiomyocyte has a cylindrical shape that is approximately 100μm long and 10-25μm in diameter. Cardiomyocyte hypertrophy occurs through sarcomerogenesis, the creation of new sarcomere units in the cell. During heart volume overload, cardiomyocytes grow through eccentric hypertrophy.[9] The cardiomyocytes extend lengthwise but have the same diameter, resulting in ventricular dilation. During heart pressure overload, cardiomyocytes grow through concentric hypertrophy.[9] The cardiomyocytes grow larger in diameter but have the same length, resulting in heart wall thickening.

Function

Depolarization/repolarization cycle

Cardiac action potential consists of two cycles, a rest phase and an active phase. These two phases are commonly understood as systole and diastole. The rest phase is considered polarized. The resting potential during this phase of the beat separates the ions such as sodium, potassium and calcium. Myocardial cells possess the property of automaticity or spontaneous depolarization. This is the direct result of a membrane which allows sodium ions to slowly enter the cell until the threshold is reached for depolarization. Calcium ions follow and extend the depolarization even further. Once calcium stops moving inward, potassium ions move out slowly to produce repolarization. The very slow repolarization of the CMC membrane is responsible for the long refractory period.[10][11]

Clinical significance

Myocardial infarction

Myocardial infarction, commonly known as a heart attack, occurs when the heart's supplementary blood vessels are obstructed by an unstable build-up of white blood cells, cholesterol, and fat. With no blood flow, the cells die, causing whole portions of cardiac tissue to die. Once these tissues are lost, they cannot be replaced, thus causing permanent damage. Current research indicates, however, that it may be possible to repair damaged cardiac tissue with stem cells,[12] as human embryonic stem cells can differentiate into cardiomyocytes under appropriate conditions.[13]

Cardiomyopathy

The cardiomyopathies are a group of diseases characterized by disruptions to cardiac muscle cell growth and / or organization. Presentation can range from asymptomatic to sudden cardiac death.

Cardiomyopathy can be caused by genetic, endocrine, environmental, or other factors.

See also

References

  1. Wolfgang Kühnel (1 January 2003). Color atlas of cytology, histology, and microscopic anatomy. Thieme. pp. 172–. ISBN 978-3-13-562404-4. Retrieved 18 April 2010.
  2. Julian Seifter; Austin Ratner; David Sloane (1 October 2005). Concepts in medical physiology. Lippincott Williams & Wilkins. pp. 201–. ISBN 978-0-7817-4489-8. Retrieved 18 April 2010.
  3. Olivetti G, Cigola E, Maestri R, et al. (July 1996). "Aging, cardiac hypertrophy and ischemic cardiomyopathy do not affect the proportion of mononucleated and multinucleated myocytes in the human heart". Journal of Molecular and Cellular Cardiology. 28 (7): 1463–77. doi:10.1006/jmcc.1996.0137. PMID 8841934.
  4. Severs, Nicholas. "The Cardiac Muscle Cell" (PDF). Archived from the original (PDF) on 2016-03-09. Retrieved 2012. Check date values in: |access-date= (help)
  5. "Anatomy and Physiology of the Heart". Retrieved 2012. Check date values in: |access-date= (help)
  6. "American Heart Association: How the Heart Works". Retrieved 2012. Check date values in: |access-date= (help)
  7. Martini, Frederic. "The Fundamentals of Anatomy and Physiology: Chapter 10 Cardiac Muscle Tissue". Archived from the original on 2011-01-01.
  8. Bergmann, O.; Bhardwaj, R. D.; Bernard, S.; Zdunek, S.; Barnabe-Heider, F.; Walsh, S.; Zupicich, J.; Alkass, K.; Buchholz, B. A.; Druid, H.; Jovinge, S.; Frisen, J. (3 April 2009). "Evidence for cardiomyocyte renewal in humans". Science. 324 (5923): 98–102. doi:10.1126/science.1164680. PMC 2991140Freely accessible. PMID 19342590.
  9. 1 2 Göktepe, S; Abilez, OJ; Parker, KK; Kuhl, E (2010-08-07). "A multiscale model for eccentric and concentric cardiac growth through sarcomerogenesis". Journal of Theoretical Biology. 265 (3): 433–42. doi:10.1016/j.jtbi.2010.04.023. PMID 20447409.
  10. Klabunde, Richard. "Cardiovascular Physiology= Cardiac muscle Concept". Retrieved 2012. Check date values in: |access-date= (help)
  11. "Cells Alive: Pumping Myocytes". Retrieved 2012. Check date values in: |access-date= (help)
  12. "Stem Cell Research News". Retrieved 2012. Check date values in: |access-date= (help)
  13. Vidarsson, Hilmar; Hyllner, Johan; Sartipy, Peter (2010-03-01). "Differentiation of human embryonic stem cells to cardiomyocytes for in vitro and in vivo applications". Stem Cell Reviews. 6 (1): 108–20. doi:10.1007/s12015-010-9113-x. ISSN 1558-6804. PMID 20091143.
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