Perfusion

In 1920, August Krogh was awarded the Nobel Prize in Physiology or Medicine for his discovering the mechanism of regulation of capillaries in skeletal muscle.{{Cite journal | last1 = Larsen | first1 = E. H. | title = August Krogh (1874–1949): 1920 Nobel Prize | journal = Ugeskrift for Laeger | volume = 169 | issue = 35 | pages = 2878 | year = 2007 | pmid = 17877986}}{{Cite journal | last1 = Sulek | first1 = K. | title = Nobel prize for August Krogh in 1920 for his discovery of regulative mechanism in the capillaries | journal = Wiadomosci Lekarskie | volume = 20 | issue = 19 | pages = 1829 | year = 1967 | pmid = 4870667}} Krogh was the first to describe the adaptation of blood perfusion in muscle and other organs according to demands through the opening and closing of arterioles and capillaries.{{citation needed|date=January 2014}}

Malperfusion can refer to any type of incorrect perfusion though it usually refers to hypoperfusion. The meaning of the terms "overperfusion" and "underperfusion" is relative to the average level of perfusion that exists across all the tissues in an individual body. Perfusion levels also differ from person to person depending on metabolic demand.{{citation needed|date=March 2021}}

Examples follow:{{citation needed|date=March 2021}}

• Heart tissues are considered overperfused because they normally are receiving more blood than the rest of tissues in the organism; they need this blood because they are constantly working.
• In the case of skin cells, extra blood flow in them is used for thermoregulation of a body. In addition to delivering oxygen, blood flow helps to dissipate heat in a body by redirecting warm blood closer to its surface where it can help to cool a body through sweating and thermal dissipation.
• Many types of tumors, and especially certain types, have been described as "hot and bloody" because of their overperfusion relative to the body overall.

Overperfusion and underperfusion should not be confused with hypoperfusion and hyperperfusion, which relate to the perfusion level relative to a tissue's current need to meet its metabolic needs. For example, hypoperfusion can be caused when an artery or arteriole that supplies blood to a volume of tissue becomes blocked by an embolus, causing either no blood or at least not enough blood to reach the tissue. Hyperperfusion can be caused by inflammation, producing hyperemia of a body part. Malperfusion, also called poor perfusion, is any type of incorrect perfusion. There is no official or formal dividing line between hypoperfusion and ischemia; sometimes the latter term refers to zero perfusion, but often it refers to any hypoperfusion that is bad enough to cause necrosis.{{citation needed|date=March 2021}}

{{main|Perfusion scanning}}

In equations, the symbol Q is sometimes used to represent perfusion when referring to cardiac output. However, this terminology can be a source of confusion since both cardiac output and the symbol Q refer to flow (volume per unit time, for example, L/min), whereas perfusion is measured as flow per unit tissue mass (mL/(min·g)).{{citation needed|date=March 2021}}

{{main|Microspheres}}

Microspheres that are labeled with radioactive isotopes have been widely used to measure perfusion since the 1960s. Radioactively labeled particles are injected into the test subject and a radiation detector measures radioactivity in tissues of interest.Studies of the Circulation with Radioactive Microspheres., Wagner et al, Invest. Radiol., 1969. 4(6): pp. 374–86. Microspheres are used in radionuclide angiography, a method of diagnosing heart problems.

In the 1990s, methods for using fluorescent microspheres became a common substitute for radioactive particles.{{cite web|title=Fluorescent Microspheres|url=http://fmrc.pulmcc.washington.edu/DOCUMENTS/FMRCMAN99.pdf|publisher=Fluorescent Microsphere Resource Center|url-status=dead|archive-url=https://web.archive.org/web/20121002175850/http://fmrc.pulmcc.washington.edu/DOCUMENTS/FMRCMAN99.pdf|archive-date=2012-10-02}}

{{main|Nuclear medicine}}

Perfusion of various tissues can be readily measured in vivo with nuclear medicine methods which are mainly positron emission tomography (PET) and single photon emission computed tomography (SPECT).{{citation needed|date=January 2014}} Various radiopharmaceuticals targeted at specific organs are also available, some of the most common are:{{citation needed|date=March 2021}}

• ^99mTc labelled HMPAO and ECD for brain perfusion (rCBF) studied with SPECT
• ^99mTc labelled Tetrofosmin and Sestamibi for myocardial perfusion imaging with SPECT
• ¹³³Xe-gas for absolute quantification of brain perfusion (rCBF) with SPECT
• ¹⁵O-labeled water for brain perfusion (rCBF) with PET (absolute quantification is possible when measuring arterial radioactivity concentration)
• ⁸²Rb-chloride for measuring myocardial perfusion with PET (absolute quantification is possible)

{{main|Magnetic resonance imaging}}

Two main categories of magnetic resonance imaging (MRI) techniques can be used to measure tissue perfusion in vivo.

• The first is based on the use of an injected contrast agent that changes the magnetic susceptibility of blood and thereby the MR signal which is repeatedly measured during bolus passage.Huettel, S. A.; Song, A. W.; McCarthy, G. (2009), Functional Magnetic Resonance Imaging (2 ed.), Massachusetts: Sinauer, {{ISBN|978-0-87893-286-3}}
• The other category is based on arterial spin labelling (ASL), where arterial blood is magnetically tagged before it enters into the tissue being examined and the amount of labelling that is measured and compared to a control recording obtained without spin labelling.{{Cite journal|title = Applications of arterial spin labeled MRI in the brain|journal = Journal of Magnetic Resonance Imaging|date = 2012-05-01|issn = 1522-2586|pmc = 3326188|pmid = 22246782|pages = 1026–1037|volume = 35|issue = 5|doi = 10.1002/jmri.23581|first1 = John A.|last1 = Detre|first2 = Hengyi|last2 = Rao|first3 = Danny J. J.|last3 = Wang|first4 = Yu Fen|last4 = Chen|first5 = Ze|last5 = Wang}}

{{main|Computed tomography}}

Brain perfusion (more correctly transit times) can be estimated with contrast-enhanced computed tomography.L. Axel. "Cerebral blood flow determination by rapid-sequence computed-tomography: theoretical analysis". Radiology 137: 679–86, December 1980

{{main|Molecular diffusion}}

Perfusion can be determined by measuring the total thermal diffusion and then separating it into thermal conductivity and perfusion components.{{cite journal |vauthors=Vajkoczy P, Roth H, Horn P, et al |title=Continuous monitoring of regional cerebral blood flow: experimental and clinical validation of a novel thermal diffusion microprobe |journal=Journal of Neurosurgery |volume=93 |issue=2 |pages=265–74 | date=August 2000 |pmid=10930012 |doi=10.3171/jns.2000.93.2.0265|s2cid=30375395 }} rCBF is usually measured continuously in time. It is necessary to stop the measurement periodically to cool down and reassess the thermal conductivity.{{citation needed|date=March 2021}}

• {{annotated link|Reperfusion injury}}
• {{annotated link|Machine perfusion}}
• {{annotated link|Perfusionist}}
• {{annotated link|Myocardial perfusion imaging}}
• {{annotated link|Cerebral circulation#Imaging |rCBF}}
• {{annotated link|Cerebral edema}}
• Pressure ulcer — continuous external pressure impairs perfusion
• Cerebral perfusion pressure

{{reflist}}

• [https://iperfusion.org/ International Perfusion Association]
• [https://web.archive.org/web/20150801033810/http://cardiacsurgeryportal.com/ Cardiac Surgery Portal]
• [https://perfusioneducation.com/blog/ Perfusion Education Portal]

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