Capillary

(Redirected from Sinusoids)

A capillary is a small blood vessel, from 5 to 10 micrometres in diameter, and is part of the microcirculation system. Capillaries are microvessels and the smallest blood vessels in the body. They are composed of only the tunica intima (the innermost layer of an artery or vein), consisting of a thin wall of simple squamous endothelial cells.[2] They are the site of the exchange of many substances from the surrounding interstitial fluid, and they convey blood from the smallest branches of the arteries (arterioles) to those of the veins (venules). Other substances which cross capillaries include water, oxygen, carbon dioxide, urea,[3] glucose, uric acid, lactic acid and creatinine. Lymph capillaries connect with larger lymph vessels to drain lymphatic fluid collected in microcirculation.

Capillary
Diagram of a capillary
A simplified illustration of a capillary network
Details
PronunciationUS: /ˈkæpəlɛri/, UK: /kəˈpɪləri/
SystemCirculatory system
Identifiers
Latinvas capillare[1]
MeSHD002196
TA98A12.0.00.025
TA23901
THH3.09.02.0.02001
FMA63194
Anatomical terminology

Etymology

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Capillary comes from the Latin word capillaris, meaning "of or resembling hair", with use in English beginning in the mid-17th century.[4] The meaning stems from the tiny, hairlike diameter of a capillary.[4] While capillary is usually used as a noun, the word also is used as an adjective, as in "capillary action", in which a liquid flows without influence of external forces, such as gravity.

Structure

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Transmission electron microscope image of a cross-section of a capillary occupied by a red blood cell

Blood flows from the heart through arteries, which branch and narrow into arterioles, and then branch further into capillaries where nutrients and wastes are exchanged. The capillaries then join and widen to become venules, which in turn widen and converge to become veins, which then return blood back to the heart through the venae cavae. In the mesentery, metarterioles form an additional stage between arterioles and capillaries.

Individual capillaries are part of the capillary bed, an interweaving network of capillaries supplying tissues and organs. The more metabolically active a tissue is, the more capillaries are required to supply nutrients and carry away products of metabolism. There are two types of capillaries: true capillaries, which branch from arterioles and provide exchange between tissue and the capillary blood, and sinusoids, a type of open-pore capillary found in the liver, bone marrow, anterior pituitary gland, and brain circumventricular organs. Capillaries and sinusoids are short vessels that directly connect the arterioles and venules at opposite ends of the beds. Metarterioles are found primarily in the mesenteric microcirculation.[5]

Lymphatic capillaries are slightly larger in diameter than blood capillaries, and have closed ends (unlike the blood capillaries open at one end to the arterioles and open at the other end to the venules). This structure permits interstitial fluid to flow into them but not out. Lymph capillaries have a greater internal oncotic pressure than blood capillaries, due to the greater concentration of plasma proteins in the lymph.[6]

Types

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Types of capillaries: (left) continuous with no big gaps, (center) fenestrated with small pores, and (right) sinusoidal (or 'discontinuous') with intercellular gaps

Blood capillaries are categorized into three types: continuous, fenestrated, and sinusoidal (also known as discontinuous).

Continuous

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Continuous capillaries are continuous in the sense that the endothelial cells provide an uninterrupted lining, and they only allow smaller molecules, such as water and ions, to pass through their intercellular clefts.[7][8] Lipid-soluble molecules can passively diffuse through the endothelial cell membranes along concentration gradients.[9] Continuous capillaries can be further divided into two subtypes:

  1. Those with numerous transport vesicles, which are found primarily in skeletal muscles, fingers, gonads, and skin.[10]
  2. Those with few vesicles, which are primarily found in the central nervous system. These capillaries are a constituent of the blood–brain barrier.[8]

Fenestrated

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Fenestrated capillaries have pores known as fenestrae (Latin for "windows") in the endothelial cells that are 60–80 nanometres (nm) in diameter. They are spanned by a diaphragm of radially oriented fibrils that allows small molecules and limited amounts of protein to diffuse.[11][12] In the renal glomerulus the capillaries are wrapped in podocyte foot processes or pedicels, which have slit pores with a function analogous to the diaphragm of the capillaries. Both of these types of blood vessels have continuous basal laminae and are primarily located in the endocrine glands, intestines, pancreas, and the glomeruli of the kidney.

Sinusoidal

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Scanning electron micrograph of a liver sinusoid with fenestrated endothelial cells. Fenestrae are approximately 100 nm in diameter.

Sinusoidal capillaries or discontinuous capillaries are a special type of open-pore capillary, also known as a sinusoid,[13] that have wider fenestrations that are 30–40 micrometres (μm) in diameter, with wider openings in the endothelium.[14] Fenestrated capillaries have diaphragms that cover the pores whereas sinusoids lack a diaphragm and just have an open pore. These types of blood vessels allow red and white blood cells (7.5 μm – 25 μm diameter) and various serum proteins to pass, aided by a discontinuous basal lamina. These capillaries lack pinocytotic vesicles, and therefore use gaps present in cell junctions to permit transfer between endothelial cells, and hence across the membrane. Sinusoids are irregular spaces filled with blood and are mainly found in the liver, bone marrow, spleen, and brain circumventricular organs.[14][15]

Development

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During early embryonic development, new capillaries are formed through vasculogenesis, the process of blood vessel formation that occurs through a novel production of endothelial cells that then form vascular tubes.[16] The term angiogenesis denotes the formation of new capillaries from pre-existing blood vessels and already-present endothelium which divides.[17] The small capillaries lengthen and interconnect to establish a network of vessels, a primitive vascular network that vascularises the entire yolk sac, connecting stalk, and chorionic villi.[18]

Function

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Annotated diagram of the exchange between capillary and body tissue through the exchange of materials between cells and fluid

The capillary wall performs an important function by allowing nutrients and waste substances to pass across it. Molecules larger than 3 nm such as albumin and other large proteins pass through transcellular transport carried inside vesicles, a process which requires them to go through the cells that form the wall. Molecules smaller than 3 nm such as water and gases cross the capillary wall through the space between cells in a process known as paracellular transport.[19] These transport mechanisms allow bidirectional exchange of substances depending on osmotic gradients.[20] Capillaries that form part of the blood–brain barrier only allow for transcellular transport as tight junctions between endothelial cells seal the paracellular space.[21]

Capillary beds may control their blood flow via autoregulation. This allows an organ to maintain constant flow despite a change in central blood pressure. This is achieved by myogenic response, and in the kidney by tubuloglomerular feedback. When blood pressure increases, arterioles are stretched and subsequently constrict (a phenomenon known as the Bayliss effect) to counteract the increased tendency for high pressure to increase blood flow.[22]

In the lungs, special mechanisms have been adapted to meet the needs of increased necessity of blood flow during exercise. When the heart rate increases and more blood must flow through the lungs, capillaries are recruited and are also distended to make room for increased blood flow. This allows blood flow to increase while resistance decreases.[citation needed] Extreme exercise can make capillaries vulnerable, with a breaking point similar to that of collagen.[23]

Capillary permeability can be increased by the release of certain cytokines, anaphylatoxins, or other mediators (such as leukotrienes, prostaglandins, histamine, bradykinin, etc.) highly influenced by the immune system.[24]

Starling equation

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Diagram of the filtration and reabsorption in capillaries

The transport mechanisms can be further quantified by the Starling equation.[20] The Starling equation defines the forces across a semipermeable membrane and allows calculation of the net flux:

 

where:

  is the net driving force,
  is the proportionality constant, and
  is the net fluid movement between compartments.

By convention, outward force is defined as positive, and inward force is defined as negative. The solution to the equation is known as the net filtration or net fluid movement (Jv). If positive, fluid will tend to leave the capillary (filtration). If negative, fluid will tend to enter the capillary (absorption). This equation has a number of important physiologic implications, especially when pathologic processes grossly alter one or more of the variables.[citation needed]

According to Starling's equation, the movement of fluid depends on six variables:

  1. Capillary hydrostatic pressure (Pc)
  2. Interstitial hydrostatic pressure (Pi)
  3. Capillary oncotic pressure (πc)
  4. Interstitial oncotic pressure (πi)
  5. Filtration coefficient (Kf)
  6. Reflection coefficient (σ)

Clinical significance

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Disorders of capillary formation as a developmental defect or acquired disorder are a feature in many common and serious disorders. Within a wide range of cellular factors and cytokines, issues with normal genetic expression and bioactivity of the vascular growth and permeability factor vascular endothelial growth factor (VEGF) appear to play a major role in many of the disorders. Cellular factors include reduced number and function of bone-marrow derived endothelial progenitor cells.[25] and reduced ability of those cells to form blood vessels.[26]

  • Formation of additional capillaries and larger blood vessels (angiogenesis) is a major mechanism by which a cancer may help to enhance its own growth. Disorders of retinal capillaries contribute to the pathogenesis of age-related macular degeneration.
  • Reduced capillary density (capillary rarefaction) occurs in association with cardiovascular risk factors[27] and in patients with coronary heart disease.[26]

Therapeutics

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Major diseases where altering capillary formation could be helpful include conditions where there is excessive or abnormal capillary formation such as cancer and disorders harming eyesight; and medical conditions in which there is reduced capillary formation either for familial or genetic reasons, or as an acquired problem.

Blood sampling

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Capillary blood sampling can be used to test for blood glucose (such as in blood glucose monitoring), hemoglobin, pH and lactate.[30][31] It is generally performed by creating a small cut using a blood lancet, followed by sampling by capillary action on the cut with a test strip or small pipette.[32] It is also used to test for sexually transmitted infections that are present in the blood stream, such as HIV, syphilis, and hepatitis B and C, where a finger is lanced and a small amount of blood is sampled into a test tube.[33]

History

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William Harvey did not explicitly predict the existence of capillaries, but he saw the need for some sort of connection between the arterial and venous systems. In 1653, he wrote, "...the blood doth enter into every member through the arteries, and does return by the veins, and that the veins are the vessels and ways by which the blood is returned to the heart itself; and that the blood in the members and extremities does pass from the arteries into the veins (either mediately by an anastomosis, or immediately through the porosities of the flesh, or both ways) as before it did in the heart and thorax out of the veins, into the arteries..."[34]

Marcello Malpighi was the first to observe directly and correctly describe capillaries, discovering them in a frog's lung 8 years later, in 1661.[35]

August Krogh discovered how capillaries provide nutrients to animal tissue. For his work he was awarded the 1920 Nobel Prize in Physiology or Medicine.[36] His 1922 estimate that total length of capillaries in a human body is as long as 100,000 km, had been widely adopted by textbooks and other secondary sources. This estimate was based on figures he gathered from "an extraordinarily large person".[37] More recent estimates give a number between 9,000 and 19,000 km.[38][37]

See also

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References

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  1. ^ Federative International Committee on Anatomical Terminology (2008). Terminologia Histologica: International Terms for Human Cytology and Histology. Baltimore: Lippincott Williams & Wilkins. p. 87. ISBN 9780781766104.
  2. ^ "Structure and Function of Blood Vessels | Anatomy and Physiology II". courses.lumenlearning.com. Retrieved 19 November 2021.
  3. ^ Maton, Anthea (1993). Human Biology and Health. Englewood Cliffs, New Jersey: Prentice Hall. pp. 87, 114, 120. ISBN 978-0-13-981176-0.
  4. ^ a b "Capillary". Online Etymology Dictionary. 2021. Retrieved 14 July 2021.
  5. ^ Sakai, T; Hosoyamada, Y (2013). "Are the precapillary sphincters and metarterioles universal components of the microcirculation? An historical review". The Journal of Physiological Sciences. 63 (5): 319–31. doi:10.1007/s12576-013-0274-7. PMC 3751330. PMID 23824465.
  6. ^ Guyton, Arthur C.; Hall, John Edward (2006). "The Microcirculation and the Lymphatic System". Textbook of Medical Physiology (11th ed.). Philadelphia: Elsevier Saunders. pp. 187–188. ISBN 9780808923176.
  7. ^ Stamatovic, S. M.; Johnson, A. M.; Keep, R. F.; Andjelkovic, A. V. (2016). "Junctional proteins of the blood-brain barrier: New insights into function and dysfunction". Tissue Barriers. 4 (1): e1154641. doi:10.1080/21688370.2016.1154641. PMC 4836471. PMID 27141427.
  8. ^ a b Wilhelm, I.; Suciu, M.; Hermenean, A.; Krizbai, I. A. (2016). "Heterogeneity of the blood-brain barrier". Tissue Barriers. 4 (1): e1143544. doi:10.1080/21688370.2016.1143544. PMC 4836475. PMID 27141424.
  9. ^ Sarin, H. (2010). "Overcoming the challenges in the effective delivery of chemotherapies to CNS solid tumors". Therapeutic Delivery. 1 (2): 289–305. doi:10.4155/tde.10.22. PMC 3234205. PMID 22163071.
  10. ^ Michel, C. C. (2012). "Electron tomography of vesicles". Microcirculation. 19 (6): 473–6. doi:10.1111/j.1549-8719.2012.00191.x. PMID 22574942. S2CID 205759387.
  11. ^ Histology image:22401lba from Vaughan, Deborah (2002). A Learning System in Histology: CD-ROM and Guide. Oxford University Press. ISBN 978-0195151732.
  12. ^ Pavelka, Margit; Roth, Jürgen (2005). "Fenestrated Capillary". Functional Ultrastructure: An Atlas of Tissue Biology and Pathology. Vienna: Springer. p. 232. doi:10.1007/3-211-26392-6_120. ISBN 978-3-211-26392-1.
  13. ^ "Histology Laboratory Manual". www.columbia.edu.
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  15. ^ Gross, P. M (1992). "Chapter 31: Circumventricular organ capillaries". Circumventricular Organs and Brain Fluid Environment - Molecular and Functional Aspects. Progress in Brain Research. Vol. 91. pp. 219–33. doi:10.1016/S0079-6123(08)62338-9. ISBN 9780444814197. PMID 1410407.
  16. ^ John S. Penn (11 March 2008). Retinal and Choroidal Angiogenesis. Springer. pp. 119–. ISBN 978-1-4020-6779-2. Retrieved 26 June 2010.
  17. ^ Gilbert, Scott F. (2000). "Endoderm". Developmental Biology (6th ed.). Sunderland, Mass.: Sinauer Associates. ISBN 0-87893-243-7. Retrieved 1 February 2021.
  18. ^ Schoenwolf, Gary C. (2015). Larsen's human embryology (Fifth ed.). Philadelphia, PA. p. 306. ISBN 9781455706846.{{cite book}}: CS1 maint: location missing publisher (link)
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  20. ^ a b Nagy, JA; Benjamin, L; Zeng, H; Dvorak, AM; Dvorak, HF (2008). "Vascular permeability, vascular hyperpermeability and angiogenesis". Angiogenesis. 11 (2): 109–119. doi:10.1007/s10456-008-9099-z. PMC 2480489. PMID 18293091.
  21. ^ Bauer, HC; Krizbai, IA; Bauer, H; Traweger, A (2014). ""You Shall Not Pass"-tight junctions of the blood brain barrier". Frontiers in Neuroscience. 8: 392. doi:10.3389/fnins.2014.00392. PMC 4253952. PMID 25520612.
  22. ^ Boulpaep, Emile L. (2017). "The Microcirculation". In Boron, Walter F.; Boulpaep, Emile L. (eds.). Medical Physiology (3rd ed.). Philadelphia, PA: Elsevier. p. 481. ISBN 978-1-4557-4377-3.
  23. ^ West, J. B. (2006). "Vulnerability of pulmonary capillaries during severe exercise". British Journal of Sports Medicine. 40 (10): 821. doi:10.1136/bjsm.2006.028886. ISSN 1473-0480. PMC 2465077. PMID 17021008.
  24. ^ Yunfei, Chi; Xiangyu, Liu (9 April 2021), Jiake, Chai (ed.), "A narrative review of changes in microvascular permeability after burn", Annals of Translational Medicine, 9 (8): 719, doi:10.21037/atm-21-1267, PMC 8106041, PMID 33987417
  25. ^ Gittenberger-De Groot, Adriana C.; Winter, Elizabeth M.; Poelmann, Robert E. (2010). "Epicardium derived cells (EPDCs) in development, cardiac disease and repair of ischemia". Journal of Cellular and Molecular Medicine. 14 (5): 1056–60. doi:10.1111/j.1582-4934.2010.01077.x. PMC 3822740. PMID 20646126.
  26. ^ a b Lambiase, P. D.; Edwards, RJ; Anthopoulos, P; Rahman, S; Meng, YG; Bucknall, CA; Redwood, SR; Pearson, JD; Marber, MS (2004). "Circulating Humoral Factors and Endothelial Progenitor Cells in Patients with Differing Coronary Collateral Support" (PDF). Circulation. 109 (24): 2986–92. doi:10.1161/01.CIR.0000130639.97284.EC. PMID 15184289. S2CID 12041051.
  27. ^ Noon, J P; Walker, B R; Webb, D J; Shore, A C; Holton, D W; Edwards, H V; Watt, G C (1997). "Impaired microvascular dilatation and capillary rarefaction in young adults with a predisposition to high blood pressure". Journal of Clinical Investigation. 99 (8): 1873–9. doi:10.1172/JCI119354. PMC 508011. PMID 9109431.
  28. ^ Bird, Alan C. (2010). "Therapeutic targets in age-related macular disease". Journal of Clinical Investigation. 120 (9): 3033–41. doi:10.1172/JCI42437. PMC 2929720. PMID 20811159.
  29. ^ Cao, Yihai (2009). "Tumor angiogenesis and molecular targets for therapy". Frontiers in Bioscience. 14 (14): 3962–73. doi:10.2741/3504. PMID 19273326.
  30. ^ Krleza, Jasna Lenicek; Dorotic, Adrijana; Grzunov, Ana; Maradin, Miljenka (15 October 2015). "Capillary blood sampling: national recommendations on behalf of the Croatian Society of Medical Biochemistry and Laboratory Medicine". Biochemia Medica. 25 (3): 335–358. doi:10.11613/BM.2015.034. ISSN 1330-0962. PMC 4622200. PMID 26524965.
  31. ^ Moro, Christian; Bass, Jessica; Scott, Anna Mae; Canetti, Elisa F.D. (19 January 2017). "Enhancing capillary blood collection: The influence of nicotinic acid and nonivamide". Journal of Clinical Laboratory Analysis. 31 (6): e22142. doi:10.1002/jcla.22142. ISSN 0887-8013. PMC 6817299. PMID 28102549.
  32. ^ "Managing diabetes:Check your blood glucose levels". National Institute of Diabetes and Digestive and Kidney Diseases,US National Institutes of Health. 2021. Retrieved 9 September 2021.
  33. ^ "Fettle - How to take a blood sample". Archived from the original on 16 March 2023. Retrieved 16 March 2023.
  34. ^ Harvey, William (1653). On the motion of the Heart and Blood in Animals. pp. 59–60. Archived from the original on 1 December 2011.
  35. ^ Cliff, Walter John (1976). Blood Vessels. Cambridge University Press. p. 14. ISBN 9780835773287.
  36. ^ "August Krogh". July 2023.
  37. ^ a b Poole, David C; Kano, Yutaka; Shunsaku, Koga; Musch, Timothy I. "August Krogh: Muscle capillary function and oxygen delivery". p. 8. Retrieved 30 October 2024.
  38. ^ Kurzgesagt. "Sources - 100K Blood Vessels". sites.google.com. Retrieved 29 October 2024.
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