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'''Mitochondria''' (singular '''mitochondrion''') are the source of energy production within a cell. They are semiautonomous and self producing [[organelle]]s, residing in the [[cytoplasm ]]of [[Eukaryote|eukaryotic cells]]. Converting cellular energy [[metabolite]]s in the [[Kreb’s Cycle]], through the process of [[oxidative phosphorylation]] they produce [[adenosine triphosphate]] (ATP) which is used to power other processes in the cell.<ref>[http://mips.gsf.de/genre/proj/mfungd/About/glossary.html] Munich Information Center for Protein Synthesis</ref><ref name=NCBICell>[http://www.ncbi.nlm.nih.gov/About/primer/genetics_cell.html What is a cell?] National Center for Biotechnology Information, National Library of Medicine, National Insitutes of Health</ref><ref name=UTMedMitoStrx>[http://cellbio.utmb.edu/cellbio/mitochondria_1.htm#Substructure Mitochondrial substructure] Cell Biology Graduate Program, University of Texas Medical Branch</ref><ref name=JakubowskiATP>[http://employees.csbsju.edu/hjakubowski/classes/ch331/oxphos/olcouplingoxphos.html ATP and oxidative phosphorylation reactions] Jakubowski, Henry (2006) College of Saint Benedict, Saint John’s University</ref>
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[[Image:MitochondriaSMALL2.jpg|left|frame|Mitochondria are the 'power plants' of cells that convert organic materials into energy. Mitochondria have their own DNA]]
'''Mitochondria''' (singular '''mitochondrion''') are the source of energy production within [[Eukaryote|eukaryotic cells]]. They are semiautonomous and self reproducing [[organelle]]s, residing in the [[cytoplasm]]. Converting cellular energy [[metabolite]]s in the [[Citric acid cycle|Krebs Cycle]], through the process of [[oxidative phosphorylation]] they produce [[adenosine triphosphate]] (ATP), which is used to power other processes in the cell.<ref>[http://mips.gsf.de/genre/proj/mfungd/About/glossary.html] Munich Information Center for Protein Synthesis</ref><ref name=NCBICell>[http://www.ncbi.nlm.nih.gov/About/primer/genetics_cell.html What is a cell?] National Center for Biotechnology Information, National Library of Medicine, National Institutes of Health</ref><ref name=UTMedMitoStrx>[http://cellbio.utmb.edu/cellbio/mitochondria_1.htm#Substructure Mitochondrial substructure] Cell Biology Graduate Program, University of Texas Medical Branch</ref><ref name=JakubowskiATP>[http://employees.csbsju.edu/hjakubowski/classes/ch331/oxphos/olcouplingoxphos.html ATP and oxidative phosphorylation reactions] Jakubowski, Henry (2006) College of Saint Benedict, Saint John’s University</ref>
 
[[Image:MitochondriaSMALL2.jpg|right|frame|Mitochondria are the 'power plants' of cells that convert organic materials into energy. Mitochondria have their own DNA]]
 
Their function is essential to efficient energy production. Without them eukaryotic cells would be dependent on anaerobic [[glycolysis]] for their ATP. Glycolysis releases very little free energy but in the mitochondria the metabolism of sugars is much more efficient and provides 15 times more ATP than is produced through glycolysis.<ref name=AlbertTheMito>[http://www.ncbi.nlm.nih.gov/books/bv.fcgi?highlight=mitochondria&rid=mboc4.section.2495 The mitochondrion] Alberts, B., Johnson, A., Lewis, J., Raff, M., Roberts, K., Walter, P. (2002) ''Molecular Biology of the Cell''. NY:Taylor & Francis Group, Garland Science</ref>
Their function is essential to efficient energy production. Without them eukaryotic cells would be dependent on anaerobic [[glycolysis]] for their ATP. Glycolysis releases very little free energy but in the mitochondria the metabolism of sugars is much more efficient and provides 15 times more ATP than is produced through glycolysis.<ref name=AlbertTheMito>[http://www.ncbi.nlm.nih.gov/books/bv.fcgi?highlight=mitochondria&rid=mboc4.section.2495 The mitochondrion] Alberts, B., Johnson, A., Lewis, J., Raff, M., Roberts, K., Walter, P. (2002) ''Molecular Biology of the Cell''. NY:Taylor & Francis Group, Garland Science</ref>


Mitochondria take up a large portion of the cytoplasmic volume of eukaryotic cells. They are rod shaped<ref>Usually rod shaped. they may also be round.</ref>organelles<ref> a word derived from Greek meaning ''Little organ''</ref> with an inner and an outer membrane. The [[outer membrane]] limits the organelle. The [[inner membrane]] folds in on itself forming the [[cristae mitochondriales]], giving the appearance of partitions and chambers within the organelle in cross section.<ref>[http://cellbio.utmb.edu/cellbio/mitoch1.htm  Mitochondria: Architecture dictates function] Cell Biology Graduate Program, University of Texas Medical Branch</ref>  The cristae number and shape vary according to the type of tissue and organism. Cristae serve to increase the surface area of the inner membrane.<ref name=NCBICell/>.
Mitochondria take up a large portion of the cytoplasmic volume of eukaryotic cells. They are rod shaped<ref>Usually rod shaped. they may also be round.</ref>organelles<ref> a word derived from Greek meaning ''Little organ''</ref> with an inner and an outer membrane. The [[outer membrane]] limits the organelle. The [[inner membrane]] folds in on itself forming the [[cristae mitochondriales]], giving the appearance of partitions and chambers within the organelle in cross section.<ref>[http://cellbio.utmb.edu/cellbio/mitoch1.htm  Mitochondria: Architecture dictates function] Cell Biology Graduate Program, University of Texas Medical Branch</ref>  The cristae number and shape vary according to the type of tissue and organism. Cristae serve to increase the surface area of the inner membrane.<ref name=NCBICell/>.


Mitochondria contain their own [[genome]] which is separate and distinct from the genome of the cell.<ref name=NCBICell/> Theoretically, mitochondria may have been separate [[unicellular organisms]] at one time and were subsumed in a [[symbiotic relationship]] into eukaryotic cells at some point in the evolutionary process.<ref name=AlbertsMBioCellMitoandChloro>[http://www.ncbi.nlm.nih.gov/books/bv.fcgi?highlight=mitochondria&rid=mboc4.chapter.2489 Energy Conversion: Mitochondria and Chloroplasts] Alberts, B., Johnson, A., Lewis, J., Raff, M., Roberts, K., Walter, P. (2002) ''Molecular Biology of the Cell''. NY:Taylor & Francis Group, Garland Science</ref>
Mitochondria contain their own [[genome]] which is separate and distinct from the genome of the cell.<ref name=NCBICell/> Theoretically, mitochondria may have been separate [[unicellular organisms]] at one time and were subsumed in a [[symbiotic relationship]] into eukaryotic cells at some point in the evolutionary process.<ref name=AlbertsMBioCellMitoandChloro>[http://www.ncbi.nlm.nih.gov/books/bv.fcgi?highlight=mitochondria&rid=mboc4.chapter.2489 Energy Conversion: Mitochondria and Chloroplasts] Alberts, B., Johnson, A., Lewis, J., Raff, M., Roberts, K., Walter, P. (2002) ''Molecular Biology of the Cell''. NY:Taylor & Francis Group, Garland Science</ref> The similarity of genes between the mitochondrial genome and the ''[[Rickettsia prowazekii]]'' genome suggests this bacteria is the most closely related to mitochondria to date.<ref name=Andersson>{{citation
 
| journal = Nature
{{editintro}}
| volume = 396
| pages =133-140
| date = 12 November 1998
| doi=10.1038/24094
| title = The genome sequence of ''Rickettsia prowazekii'' and the origin of mitochondria
| author =Andersson SGE ''et al.''
| url =http://www.nature.com/nature/journal/v396/n6707/full/396133a0.html}}</ref>


==General characteristics==
==General characteristics==
Line 15: Line 24:
Mitochondria were first seen in a light microscope in the nineteenth century but were not really understood until procedures for isolating intact samples were developed in 1948. Mitochondria are often retrieved from purified liver cells which contain from 1000 to 2000 mitochondria each, occupying about one-fifth of the cell volume.<ref name=AlbertTheMito/>
Mitochondria were first seen in a light microscope in the nineteenth century but were not really understood until procedures for isolating intact samples were developed in 1948. Mitochondria are often retrieved from purified liver cells which contain from 1000 to 2000 mitochondria each, occupying about one-fifth of the cell volume.<ref name=AlbertTheMito/>
==Function==
==Function==
[[Pyruvate]] formed in glycolysis in the second stage of anaerobic oxidation is transported into mitochondria. Mitochondria oxidize the pyruvate with O<sub>2</sub> to CO<sub>2</sub> generating 34 of 36 ATP  molecules generated when glucose is converted to CO<sub>2</sub><ref name=LodishOxidation>[http://www.ncbi.nlm.nih.gov/books/bv.fcgi?highlight=mitochondria&rid=mcb.section.4337#4345Oxidation of Glucose and Fatty Acids to CO2] Lodish, Harvey; Berk, Arnold; Zipursky, S. Lawrence; Matsudaira, Paul; Baltimore, David; Darnell, James E. (2000) Molecular Cell Biology. 4th ed. New York: W. H. Freeman & Co.</ref>
[[Pyruvate]] formed in glycolysis in the second stage of anaerobic oxidation is transported into mitochondria. Mitochondria oxidize the pyruvate with O<sub>2</sub> to CO<sub>2</sub> generating 34 of 36 ATP  molecules when glucose is converted to CO<sub>2</sub><ref name=LodishOxidation>[http://www.ncbi.nlm.nih.gov/books/bv.fcgi?highlight=mitochondria&rid=mcb.section.4337#4345 Oxidation of Glucose and Fatty Acids to CO2] Lodish, Harvey; Berk, Arnold; Zipursky, S. Lawrence; Matsudaira, Paul; Baltimore, David; Darnell, James E. (2000) Molecular Cell Biology. 4th ed. New York: W. H. Freeman & Co.</ref>


==Substructure==
==Substructure==
There are two structurally and distinct membranes and two internal compartments or spaces. The two membranes are separated by the inter-membrane space. The space enclosed within the inner memberane is the [[matrix]], a moderately dense region with strands of [[DNA]], [[ribosome]]s, or small [[granule]]s with which the mitochondria code for a portion of their own proteins.<ref name=UTMedMitoStrx/><ref name=LodishOxidation/>
There are two structurally and distinct membranes and two internal compartments or spaces. The two membranes are separated by the inter-membrane space. The space enclosed within the inner membrane is the [[matrix]], a moderately dense region with strands of [[DNA]], [[ribosome]]s, or small [[granule]]s with which the mitochondria code for a portion of their own proteins.<ref name=UTMedMitoStrx/><ref name=LodishOxidation/>


===Outer membrane===
===Outer membrane===
Line 30: Line 39:
Extremely convoluted, its infolding form the cristae that project into the matrix of the inner compartment of the mitochondrion and significantly increase the area of the inner membrane. Cristae vary in volume for different types of cells. The number of cristae in a mitochondria in a myocardial cell, for example, is three times that of mitochondria in a liver cell. There is also a greater demand for ATP in myocardial cells than in liver cells.<ref name=AlbertTheMito/>
Extremely convoluted, its infolding form the cristae that project into the matrix of the inner compartment of the mitochondrion and significantly increase the area of the inner membrane. Cristae vary in volume for different types of cells. The number of cristae in a mitochondria in a myocardial cell, for example, is three times that of mitochondria in a liver cell. There is also a greater demand for ATP in myocardial cells than in liver cells.<ref name=AlbertTheMito/>


In [[Prokaryote|prokaryotes]], the plasma membrane is used to produce ATP. However, eukaryotic cells reserve this function for membranes in energy converting organells, mitochondria and [[plastids]]<ref>notably chloroplasts—occuring only in plants</ref> and the plasma membrane is reserved for other transport processes. Mitochondria and plastids are morphologically notable for their extensive inner membranes.<ref name=AlbertsMBioCellMitoandChloro/>
In [[Prokaryote|prokaryotes]], the plasma membrane is used to produce ATP. However, eukaryotic cells reserve this function for membranes in energy converting organelles, mitochondria and [[plastids]]<ref>notably chloroplasts—occurring only in plants</ref> and the plasma membrane is reserved for other transport processes. Mitochondria and plastids are morphologically notable for their extensive inner membranes.<ref name=AlbertsMBioCellMitoandChloro/>


The inner membrane is a lipid bilayer containing a high proportion of [[cardiolipin]] (diphosphatidylglycerol).<ref>A double [[phospholipid]], cardiolipin contains four rather then two [[fatty acid]]s</ref> It sufficiently reduces the membrane’s permeability to protons making the membrane especially impermeable to ions and establishing the conditions that allow a proton-motive force to be established across it. The inner membrane also holds a number of different transport proteins which make it selectively permeable to smaller molecules that are metabolised or utilised in mitochondrial enzymes in the matrix.<ref name=AlbertTheMito/><ref name=LodishOxidation/>
The inner membrane is a lipid bilayer containing a high proportion of [[cardiolipin]] (diphosphatidylglycerol).<ref>A double [[phospholipid]], cardiolipin contains four rather then two [[fatty acid]]s</ref> It sufficiently reduces the membrane’s permeability to protons making the membrane especially impermeable to ions and establishing the conditions that allow a proton-motive force to be established across it. The inner membrane also holds a number of different transport proteins which make it selectively permeable to smaller molecules that are metabolised or utilised in mitochondrial enzymes in the matrix.<ref name=AlbertTheMito/><ref name=LodishOxidation/>


Protein constitutes a higher percentage of the inner membrane than in any other membrane of the cell, 76 percent. The inner membrane contains many protein-rich intramembrane particles including the F<sub>0</sub>F<sub>1</sub> complexes that synthesize ATP and those that transport electrons to O<sub>2</sub> from NADH or reduced flavin adenine dinucleotide (FADH<sub>2</sub>.  
Protein constitutes a higher percentage of the inner membrane than in any other membrane of the cell, 76 percent. The inner membrane contains many protein-rich intramembrane particles including the F<sub>0</sub>F<sub>1</sub> complexes that synthesize ATP and those that transport electrons to O<sub>2</sub> from NADH or reduced flavin adenine dinucleotide (FADH<sub>2</sub>).  


The inner membrane also hold transport proteins which pass impermeable molecules, such as ADP and P<sub>i</sub>, to pass from the cytosol of the inter-membrane space through the inner membrane to the internal matrix. The proteins also transport other molecules in reverse, such as ATP, from the matrix into the cytosol.<ref name=LodishOxidation/>
The inner membrane also hold transport proteins which pass impermeable molecules, such as ADP and P<sub>i</sub>, to pass from the cytosol of the inter-membrane space through the inner membrane to the internal matrix. The proteins also transport other molecules in reverse, such as ATP, from the matrix into the cytosol.<ref name=LodishOxidation/>
Line 44: Line 53:
===Replication===
===Replication===
In a process similar to replication in bacterial cells, when a mitochondrion reaches a certain size, they undergo fission, the furrowing of the inner and outermembrane which pinches them into two daughter mitochondria. Prior to fission they replicate their DNA.<ref name=UTexasMitoLifeCycle>[http://cellbio.utmb.edu/cellbio/mitoch2.htm The mitochondrial life cycle] Cell Biology Graduate Program, University of Texas Medical Branch</ref>
In a process similar to replication in bacterial cells, when a mitochondrion reaches a certain size, they undergo fission, the furrowing of the inner and outermembrane which pinches them into two daughter mitochondria. Prior to fission they replicate their DNA.<ref name=UTexasMitoLifeCycle>[http://cellbio.utmb.edu/cellbio/mitoch2.htm The mitochondrial life cycle] Cell Biology Graduate Program, University of Texas Medical Branch</ref>
===Death===
===Death===
Mitochondrion at the end of their life are disposed of through [[autophagy]].  Cellular [[endoplasmic reticulum]] are wrapped around the mitochondrion forming a vacuole. [[Golgi complex]] vesicles containing hydrolases then join with the autophagic vacuole which then degrades the contents of the vacuole, the mitochondrion.<ref name=UTexasMitoLifeCycle/>
Mitochondrion at the end of their life are disposed of through [[autophagy]].  Cellular [[endoplasmic reticulum]] are wrapped around the mitochondrion forming a vacuole. [[Golgi complex]] vesicles containing hydrolases then join with the autophagic vacuole which then degrades the contents of the vacuole, the mitochondrion.<ref name=UTexasMitoLifeCycle/>


==Ca<sup>2+</sup> homeostasis==
==Ca<sup>2+</sup> homeostasis==
Mitochondrial uniporter<ref> cell membrane transport proteins whose function involves the passage of small hydrophilic ions and molecules through a cell membrane down a concentration gradient. [http://www.mercksource.com/pp/us/cns/cns_hl_dorlands.jspzQzpgzEzzSzppdocszSzuszSzcommonzSzdorlandszSzdorlandzSzdmd_u_02zPzhtm] Dorlands Medical Dictionary</ref> in the inner membrane move Ca<sup>2+</sup> into the matrix which in turn initiates activation of dehydrogenases in the citric acid cycle, the cellular concentrations of Ca<sup>2+</sup> essentially triggering variations in mitochondrion activity. This establishes a clear link between energy metabolism and cellular activity involving a functional relationship with endoplasmic reticulum.


Mitochondrial uniporter<ref> cell membrane transport proteins whose function involves the passage of small hydrophilic ions and molecules through a through a cell membrane down a concentration gradient. [http://www.mercksource.com/pp/us/cns/cns_hl_dorlands.jspzQzpgzEzzSzppdocszSzuszSzcommonzSzdorlandszSzdorlandzSzdmd_u_02zPzhtm] Dorlands Medical Dictionary</ref> in the inner membrane move Ca<sup>2+</sup> into the matrix which in turn initiates activation of dehydrogenases in the citric acid cycle, the cellular concentrations of Ca<sup>2+</sup> essentially triggering variations in mitochondrion activity. This establishes a clear link between energy metabolism and cellular activity involving a functional relationship with endoplasmic reticulum.
Ca<sup>2+</sup> uptake is apparently rapid while the Ca<sup>2+</sup>is then released  back into the cell over a longer period, indicating that the mitochondria act as a buffer. This buffering function has an impact on presynaptic terminal potentials and may be involved in the propagation of cytosolic Ca<sup>2+</sup> waves.<ref>[http://www.ncbi.nlm.nih.gov/books/bv.fcgi?highlight=mitochondria&rid=eurekah.section.2009 Mitochondria and Ca2+ homeostasis] Eurekah Bioscience Collection (2003) Landes Bioscience; [http://www.ncbi.nlm.nih.gov/books/bv.fcgi?rid=eurekah.section.2007 The endoplasmic reticulum Ca<sup>2+</sup> store]Eurekah Bioscience Collection (2003) Landes Bioscience; [http://www.ncbi.nlm.nih.gov/books/bv.fcgi?rid=eurekah.section.2005  Cytosolic Ca<sup>2+</sup> buffering] Eurekah Bioscience Collection (2003) Landes Bioscience</ref>


Ca<sup>2+</sup> uptake is apparently rapid while the Ca<sup>2+</sup>is then released  back into the cell over a longer period, indicating that the mitochondria act as a buffer. This buffering function has an impact on presynaptic terminal potentials and and may be involved in the propagation of cytosolic Ca<sup>2+</sup> waves.<ref>[http://www.ncbi.nlm.nih.gov/books/bv.fcgi?highlight=mitochondria&rid=eurekah.section.2009 Mitochondria and Ca2+ homeostasis] Eurekah Bioscience Collection (2003) Landes Bioscience</ref><ref>[http://www.ncbi.nlm.nih.gov/books/bv.fcgi?rid=eurekah.section.2007 The endoplasmic reticulum Ca<sup>2+</sup> store]Eurekah Bioscience Collection (2003) Landes Bioscience</ref><ref>[http://www.ncbi.nlm.nih.gov/books/bv.fcgi?rid=eurekah.section.2005  Cytosolic Ca<sup>2+</sup> buffering] Eurekah Bioscience Collection (2003) Landes Bioscience</ref>
===Neurotoxicity and neuroprotection===
Overloading mitochondria with Ca<sup>2+</sup> may be linked to neuron apoptosis (cell death) through two possible results: (a) decrease or loss of inner mitochondrial membrane proton gradient leading to termination of the production of ATP; (b) proactive substances such as cytochrome ''c'' may be released into the protoplasm of the cell. These proactive substances will in turn activate caspases<ref>Enzymes of the cysteine endopeptidases family that function in apoptosis [http://www.mercksource.com/pp/us/cns/cns_hl_dorlands.jspzQzpgzEzzSzppdocszSzuszSzcommonzSzdorlandszSzdorlandzSzdmd-a-b-000zPzhtm] Dorland's Illustrated Medical Dictionary </ref> which will result in necrosis<ref>Necrosis is irreversible tissue death resulting from various causes such as insufficient blood supply, injury, radiation toxins.[ [http://www.mercksource.com/pp/us/cns/cns_hl_dorlands.jspzQzpgzEzzSzppdocszSzuszSzcommonzSzdorlandszSzdorlandzSzdmd-a-b-000zPzhtm] Dorland's Illustrated Medical Dictionary </ref>
or apoptosis<ref> from the Greek meaning“a falling off,” from apo off + ptosis fall.  Apoptosis is a morphologic pattern of cell death which effects single cells. Changes in apoptosis are cell shrinkage, chromatin condensation, cytoplasmic bleb formation, and the cell is fragmented into apoptotic bodies disposed of through the process of phagocytosis. It is a normal mechanism for the regulation of cell populations which deletes cells. It is synonymous with programmed cell death. [http://www.mercksource.com/pp/us/cns/cns_hl_dorlands.jspzQzpgzEzzSzppdocszSzuszSzcommonzSzdorlandszSzdorlandzSzdmd-a-b-000zPzhtm] Dorland's Illustrated Medical Dictionary </ref> according the extent of the loss ATP production and survival of sufficient numbers of mitochondria.<ref>[http://www.ncbi.nlm.nih.gov/books/bv.fcgi?highlight=mitochondria&rid=eurekah.section.2010 Mitochondria, neurotoxicity and neuroprotection]Eurekah Bioscience Collection (2003) Landes Bioscience</ref>


==Notes==
==Notes==
<div class="references-small" style="-moz-column-count:3; column-count:3;">
{{reflist|2}}[[Category:Suggestion Bot Tag]]
<references/>
</div>

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Mitochondria (singular mitochondrion) are the source of energy production within eukaryotic cells. They are semiautonomous and self reproducing organelles, residing in the cytoplasm. Converting cellular energy metabolites in the Krebs Cycle, through the process of oxidative phosphorylation they produce adenosine triphosphate (ATP), which is used to power other processes in the cell.[1][2][3][4]

Mitochondria are the 'power plants' of cells that convert organic materials into energy. Mitochondria have their own DNA

Their function is essential to efficient energy production. Without them eukaryotic cells would be dependent on anaerobic glycolysis for their ATP. Glycolysis releases very little free energy but in the mitochondria the metabolism of sugars is much more efficient and provides 15 times more ATP than is produced through glycolysis.[5]

Mitochondria take up a large portion of the cytoplasmic volume of eukaryotic cells. They are rod shaped[6]organelles[7] with an inner and an outer membrane. The outer membrane limits the organelle. The inner membrane folds in on itself forming the cristae mitochondriales, giving the appearance of partitions and chambers within the organelle in cross section.[8] The cristae number and shape vary according to the type of tissue and organism. Cristae serve to increase the surface area of the inner membrane.[2].

Mitochondria contain their own genome which is separate and distinct from the genome of the cell.[2] Theoretically, mitochondria may have been separate unicellular organisms at one time and were subsumed in a symbiotic relationship into eukaryotic cells at some point in the evolutionary process.[9] The similarity of genes between the mitochondrial genome and the Rickettsia prowazekii genome suggests this bacteria is the most closely related to mitochondria to date.[10]

General characteristics

Usually seen as inflexible cylinders of roughly 0.5–1 μm, mitochondria resemble bacteria. Mitochondria are actual very mobile and frequently change shape. They may even fuse with other mitochondria and then separate. They are often associated with microtubules in the cytoplasm which determine mitochondrial orientation and distribution. In some cells they form long moving chains and in other types of cells they remain fixed in a position providing ATP directly to a site of high ATP consumption such as the adjacent myofibrils of cardiac muscle or the flagellum of sperm.[5]

Mitochondria were first seen in a light microscope in the nineteenth century but were not really understood until procedures for isolating intact samples were developed in 1948. Mitochondria are often retrieved from purified liver cells which contain from 1000 to 2000 mitochondria each, occupying about one-fifth of the cell volume.[5]

Function

Pyruvate formed in glycolysis in the second stage of anaerobic oxidation is transported into mitochondria. Mitochondria oxidize the pyruvate with O2 to CO2 generating 34 of 36 ATP molecules when glucose is converted to CO2[11]

Substructure

There are two structurally and distinct membranes and two internal compartments or spaces. The two membranes are separated by the inter-membrane space. The space enclosed within the inner membrane is the matrix, a moderately dense region with strands of DNA, ribosomes, or small granules with which the mitochondria code for a portion of their own proteins.[3][11]

Outer membrane

The external membrane of the mitochondria contain the transport protein porin. Porin forms aqueous channels through the lipid bilayer of the mitochondria, resembling a permeable sieve through which molecules, including small proteins, of 5 kiloDaltons or less may pass into the inter-membrane space.

The inner membrane, by comparison, is impermeable to most molecules. In other words, the inter-membrane space is chemically like the cytosol while the internal matrix of the mitochondria contains a select set of molecules.[5][11]

Inner membrane

The inner membrane constitutes the framework for electron-transport processes that produce most of the cell's ATP. Enzymes embedded in the inner mitochondrial membrane are essential to the process of oxidative phosphorylation generating most of the animal cell ATP.[9]

Extremely convoluted, its infolding form the cristae that project into the matrix of the inner compartment of the mitochondrion and significantly increase the area of the inner membrane. Cristae vary in volume for different types of cells. The number of cristae in a mitochondria in a myocardial cell, for example, is three times that of mitochondria in a liver cell. There is also a greater demand for ATP in myocardial cells than in liver cells.[5]

In prokaryotes, the plasma membrane is used to produce ATP. However, eukaryotic cells reserve this function for membranes in energy converting organelles, mitochondria and plastids[12] and the plasma membrane is reserved for other transport processes. Mitochondria and plastids are morphologically notable for their extensive inner membranes.[9]

The inner membrane is a lipid bilayer containing a high proportion of cardiolipin (diphosphatidylglycerol).[13] It sufficiently reduces the membrane’s permeability to protons making the membrane especially impermeable to ions and establishing the conditions that allow a proton-motive force to be established across it. The inner membrane also holds a number of different transport proteins which make it selectively permeable to smaller molecules that are metabolised or utilised in mitochondrial enzymes in the matrix.[5][11]

Protein constitutes a higher percentage of the inner membrane than in any other membrane of the cell, 76 percent. The inner membrane contains many protein-rich intramembrane particles including the F0F1 complexes that synthesize ATP and those that transport electrons to O2 from NADH or reduced flavin adenine dinucleotide (FADH2).

The inner membrane also hold transport proteins which pass impermeable molecules, such as ADP and Pi, to pass from the cytosol of the inter-membrane space through the inner membrane to the internal matrix. The proteins also transport other molecules in reverse, such as ATP, from the matrix into the cytosol.[11]

Matrix

Along with the inner membrane, the matrix contained in the internal compartment of the mitochondria is the primary functional area of the mitochondria. The matrix includes enzymes that metabolise pyruvate and fatty acids to produce acetyl CoA[14] along with enzymes that oxidise acetyl CoA in the Kreb's cycle.[15] The Kreb's cycle produces, amongst other things, NDAH which is the primary source of electrons transported through the respiratory chain.[16] The respiratory chain enzymes are embedded in the inner mitochondrial membrane, essential there to the process of oxidative phosphorylation.[5]

Life cycle

Replication

In a process similar to replication in bacterial cells, when a mitochondrion reaches a certain size, they undergo fission, the furrowing of the inner and outermembrane which pinches them into two daughter mitochondria. Prior to fission they replicate their DNA.[17]

Death

Mitochondrion at the end of their life are disposed of through autophagy. Cellular endoplasmic reticulum are wrapped around the mitochondrion forming a vacuole. Golgi complex vesicles containing hydrolases then join with the autophagic vacuole which then degrades the contents of the vacuole, the mitochondrion.[17]

Ca2+ homeostasis

Mitochondrial uniporter[18] in the inner membrane move Ca2+ into the matrix which in turn initiates activation of dehydrogenases in the citric acid cycle, the cellular concentrations of Ca2+ essentially triggering variations in mitochondrion activity. This establishes a clear link between energy metabolism and cellular activity involving a functional relationship with endoplasmic reticulum.

Ca2+ uptake is apparently rapid while the Ca2+is then released back into the cell over a longer period, indicating that the mitochondria act as a buffer. This buffering function has an impact on presynaptic terminal potentials and may be involved in the propagation of cytosolic Ca2+ waves.[19]

Neurotoxicity and neuroprotection

Overloading mitochondria with Ca2+ may be linked to neuron apoptosis (cell death) through two possible results: (a) decrease or loss of inner mitochondrial membrane proton gradient leading to termination of the production of ATP; (b) proactive substances such as cytochrome c may be released into the protoplasm of the cell. These proactive substances will in turn activate caspases[20] which will result in necrosis[21] or apoptosis[22] according the extent of the loss ATP production and survival of sufficient numbers of mitochondria.[23]

Notes

  1. [1] Munich Information Center for Protein Synthesis
  2. 2.0 2.1 2.2 What is a cell? National Center for Biotechnology Information, National Library of Medicine, National Institutes of Health
  3. 3.0 3.1 Mitochondrial substructure Cell Biology Graduate Program, University of Texas Medical Branch
  4. ATP and oxidative phosphorylation reactions Jakubowski, Henry (2006) College of Saint Benedict, Saint John’s University
  5. 5.0 5.1 5.2 5.3 5.4 5.5 5.6 The mitochondrion Alberts, B., Johnson, A., Lewis, J., Raff, M., Roberts, K., Walter, P. (2002) Molecular Biology of the Cell. NY:Taylor & Francis Group, Garland Science
  6. Usually rod shaped. they may also be round.
  7. a word derived from Greek meaning Little organ
  8. Mitochondria: Architecture dictates function Cell Biology Graduate Program, University of Texas Medical Branch
  9. 9.0 9.1 9.2 Energy Conversion: Mitochondria and Chloroplasts Alberts, B., Johnson, A., Lewis, J., Raff, M., Roberts, K., Walter, P. (2002) Molecular Biology of the Cell. NY:Taylor & Francis Group, Garland Science
  10. Andersson SGE et al. (12 November 1998), "The genome sequence of Rickettsia prowazekii and the origin of mitochondria", Nature 396: 133-140, DOI:10.1038/24094
  11. 11.0 11.1 11.2 11.3 11.4 Oxidation of Glucose and Fatty Acids to CO2 Lodish, Harvey; Berk, Arnold; Zipursky, S. Lawrence; Matsudaira, Paul; Baltimore, David; Darnell, James E. (2000) Molecular Cell Biology. 4th ed. New York: W. H. Freeman & Co.
  12. notably chloroplasts—occurring only in plants
  13. A double phospholipid, cardiolipin contains four rather then two fatty acids
  14. acetyl coenzyme A
  15. also referred to as the citric acid cycle
  16. i.e. the electron-transport chain in mitochondria
  17. 17.0 17.1 The mitochondrial life cycle Cell Biology Graduate Program, University of Texas Medical Branch
  18. cell membrane transport proteins whose function involves the passage of small hydrophilic ions and molecules through a cell membrane down a concentration gradient. [2] Dorlands Medical Dictionary
  19. Mitochondria and Ca2+ homeostasis Eurekah Bioscience Collection (2003) Landes Bioscience; The endoplasmic reticulum Ca2+ storeEurekah Bioscience Collection (2003) Landes Bioscience; Cytosolic Ca2+ buffering Eurekah Bioscience Collection (2003) Landes Bioscience
  20. Enzymes of the cysteine endopeptidases family that function in apoptosis [3] Dorland's Illustrated Medical Dictionary
  21. Necrosis is irreversible tissue death resulting from various causes such as insufficient blood supply, injury, radiation toxins.[ [4] Dorland's Illustrated Medical Dictionary
  22. from the Greek meaning“a falling off,” from apo off + ptosis fall. Apoptosis is a morphologic pattern of cell death which effects single cells. Changes in apoptosis are cell shrinkage, chromatin condensation, cytoplasmic bleb formation, and the cell is fragmented into apoptotic bodies disposed of through the process of phagocytosis. It is a normal mechanism for the regulation of cell populations which deletes cells. It is synonymous with programmed cell death. [5] Dorland's Illustrated Medical Dictionary
  23. Mitochondria, neurotoxicity and neuroprotectionEurekah Bioscience Collection (2003) Landes Bioscience