'Cellular respiration' describes the metabolism reactions and processes that take place in a
cell to obtain
biochemical energy from fuel molecules and the release of the cells' waste products. Energy is released by the
oxidation of fuel molecules and is stored as "high-energy" carriers. The reactions involved in respiration are
catabolic reactions in metabolism.
Fuel molecules commonly used by cells in respiration include
glucose,
amino acids and
fatty acids, and a common
oxidizing agent (
electron acceptor) is molecular
oxygen (O
2). There are organisms, however, that can respire using other
organic molecules as electron acceptors instead of oxygen. Organisms that use oxygen as a final electron acceptor in respiration are described as
aerobic, while those that do not are referred to as
anaerobic.
The energy released in respiration is used to synthesize molecules that act as a chemical storage of this energy. One of the most widely used compounds in a cell is
adenosine triphosphate (ATP) and its stored chemical energy can be used for many processes requiring energy, including
biosynthesis,
locomotion or transportation of molecules across
cell membranes. Because of its ubiquitous nature, ATP is also known as the "universal energy currency", since the amount of it in a cell indicates how much energy is available for energy-consuming processes.
Aerobic respiration
''Aerobic respiration'' requires
oxygen in order to generate energy (
ATP). It is the preferred method of
pyruvate breakdown from
glycolysis and requires that pyruvate enter the
mitochondrion to be fully oxidized by the
Krebs cycle. The product of this process is energy in the form of ATP (Adenosine Triphosphate), by
substrate-level phosphorylation,
NADH and
FADH2.
'Simplified Reaction:' C
6H
12O
6 (aq) + 6O
2 (g) → 6CO
2 (g) + 6H
2O
(l) ΔH
c -2880KJ
The reducing potential of NADH and FADH
2 is converted to more ATP through an
electron transport chain with oxygen as the "terminal electron acceptor". Most of the ATP produced by cellular respiration is by
oxidative phosphorylation, ATP molecules are made to the
chemiosmotic potential driving ATP synthase. Respiration is the process by which cells obtain energy when oxygen is present in the cell. Biology text books often quote that between 36-38 ATP molecules can be made per oxidised glucose molecule during cellular respiration (2 from glycolysis 2 from the Krebs cycle, and about 32-34 from the electron transport system). Such conditions are never realized due to losses (leaky membranes) as well as the cost of moving pyruvate and ADP into the mitochondrial matrix.
Aerobic metabolism is more efficient than anaerobic metabolism (which yields 2 mol ATP per 1 mol glucose). They share the initial pathway of
glycolysis but aerobic metabolism continues with the Krebs cycle and oxidative phosphorylation. The post glycolytic reactions take place in the mitochondria in
eukaryotic cells, and in the
cytoplasm in
prokaryotic cells.
Glycolysis
Main articles: Glycolysis
Glycolysis is a
metabolic pathway that is found in the cytoplasm of cells in all living organisms and does not require
oxygen. The process converts one molecule of
glucose into two molecules of
pyruvate, and makes energy in the form of two net molecules of
ATP. Four molecules of ATP per glucose are actually produced; however, two are consumed for the
preparatory phase. The initial
phosphorylation of glucose is required to destabilize the molecule for cleavage into two
triose sugars. During the
pay-off phase of glycolysis four
phosphate groups are transferred to ADP by
substrate-level phosphorylation to make four ATP and two NADH are produced when the triose sugars are oxidized. Glycolysis takes place in the
cytoplasm of the
cell. The overall reaction can be expressed this way:
:Glucose + 2 ATP + 2 NAD
+ + 2 P
i + 4 ADP → 2 pyruvate + 2 ADP + 2 NADH + 4 ATP + 2 H
2O
Oxidative decarboxylation of pyruvate
Main articles: Pyruvate decarboxylation
Produces
acetyl-CoA from pyruvate inside the
mitochondrial matrix. This oxidation reaction also releases carbon dioxide as a product. In the process one molecule of NADH is formed per pyruvate oxidized.
Citric Acid cycle/Krebs cycle
Main articles: Citric acid cycle
When oxygen is present,
acetyl-CoA is produced from pyruvate. If oxygen is not present the cell undergoes fermentation of the pyruvate molecule. If
acetyl-CoA is produced the molecule then enters the
citric acid cycle (Krebs cycle) inside the mitochondrial matrix, and gets oxidized to
CO2 while at the same time reducing
NAD to
NADH.
NADH can be used by the
electron transport chain to create further
ATP as part of oxidative phosphorylation. To fully oxidize the equivalent of one glucose molecule two acetyl-CoA must be metabolized by the Krebs cycle. Two
waste products, H
2O and CO
2 are created during this cycle.
Oxidative phosphorylation
Main articles: Oxidative phosphorylation,
Electron transport chain,
Electrochemical gradient,
ATP synthase
In eukaryotes, oxidative phosphorylation occurs in the mitochondrial
cristae. It comprises the electron transport chain that establishes a
proton gradient (chemiosmotic potential) across the inner membrane by oxidizing the NADH produced from the Krebs cycle. ATP is synthesised by the ATP synthase enzyme when the chemiosmotic gradient is used to drive the phosphorylation of ADP.
Theoretical yields
The yields in the table below are for one glucose molecule being fully oxidized into carbon dioxide. It is assumed that all the
reduced coenzymes are oxidized by the electron transport chain and used for oxidative phosphorylation.
| Step | coenzyme yield | ATP yield | Source of ATP |
|---|
| Glycolysis preparatory phase | | -2 | Phosphorylation of glucose and fructose 6-phosphate uses two ATP from the cytoplasm. |
| Glycolysis pay-off phase | | 4 | Substrate-level phosphorylation |
| 2 NADH | 4 (6) | Oxidative phosphorylation. Only 2 ATP per NADH since the coenzyme must feed into the electron transport chain from the cytoplasm rather than the mitochondrial matrix. If the malate shuttle is used to move NADH into the mitochondria this might count as 3 ATP per NADH. |
| Oxidative decarboxylation | 2 NADH | 6 | Oxidative phosphorylation |
| Krebs cycle | | 2 | Substrate-level phosphorylation |
| 6 NADH | 18 | Oxidative phosphorylation |
| 2 FADH2 | 4 | Oxidative phosphorylation |
| 'Total yield' | '36 (38) ATP' | From the complete oxidation of one glucose molecule to carbon dioxide and oxidation of all the reduced coenzymes. |
Although there is a theoretical yield of 36-38 ATP molecules per glucose during cellular respiration, such conditions are generally not realized due to losses such as the cost of moving pyruvate (from glycolysis), phosphate and ADP (substrates for ATP syhthesis) into the mitochondria. All are actively transported using carriers that utilise the stored energy in the proton
electrochemical gradient.
★ The '
pyruvate carrier' is a
symporter and the driving force for moving pyruvate into the mitochondria is the movement of protons from the
intermembrane space to the matrix.
★ The '
phosphate carrier' is an
antiporter and the driving force for moving phosphate ions into the mitochondria is the movement of hydroxyls ions from the matrix to the intermembrane space.
★ The '
adenine nucleotide carrier' is an antiporter and exchanges ADP and ATP across the
inner membrane. The driving force is due to the ATP (-4) having a more negative charge than the ADP (-3) and thus it dissipates some of the electrical component of the proton electrochemical gradient.
The outcome of these transport processes using the proton electrochemical gradient is that more than 3 H
+ are needed to make 1 ATP. Obviously this reduces the theoretical efficiency of the whole process and the likely maximum is closer to 28-30 ATP molecules.
[1] In practice the efficiency may be even lower due to the inner membrane of the mitochondira being slightly leaky to protons.
[2] Other factors may also dissipate the proton gradient creating an apparently leaky mitochondria. An uncoupling protein known as
thermogenin is expressed in some cell types and is a channel that can transport protons. When this protein is active in the inner membrane it short circuits the coupling between the
electron transport chain and
ATP synthesis. The potential energy from the proton gradient is not used to make ATP but generates heat. This is particularly important in a baby's brown fat, for thermogenesis, and hibernating animals.
Anaerobic respiration
:''Main article:
Anaerobic respiration''
Without oxygen, pyruvate is not metabolized by cellular respiration but undergoes a process of
fermentation. The pyruvate is not transported into the mitochondrion, but remains in the cytoplasm, where it is converted to
waste products that may be removed from the cell. This serves the purpose of oxidizing the hydrogen carriers so that they can perform glycolysis again and removing the excess pyruvate. This waste product varies depending on the organism. In skeletal muscles, the waste product is
lactic acid. This type of fermentation is called
lactic acid fermentation. In yeast, the waste products are
ethanol and
carbon dioxide. This type of fermentation is known as alcoholic or
ethanol fermentation.
Anaerobic respiration is less efficient at using the energy from glucose since 2 ATP are produced during anaerobic respiration per glucose, compared to the 30 ATP per glucose produced by aerobic respiration. This is because the
waste products of anaerobic respiration still contain plenty of energy.
Ethanol, for example, can be used in gasoline (petrol) solutions. Glycolytic ATP, however, is created more quickly. For prokaryotes to continue a rapid growth rate when they are shifted from an aerobic environment to an anaerobic environment, they must increase the rate of the glycolytic reactions. Thus, during short bursts of strenuous activity, muscle cells use anaerobic respiration to supplement the ATP production from the slower aerobic respiration, so anaerobic respiration may be used by a cell even before the oxygen levels are depleted, as is the case in sports that do not require athletes to pace themselves, such as
sprinting.
See also
★
Tetrazolium chloride: cellular respiration indicator
References
1. The molecular machinery of Keilin's respiratory chain, Rich PR, , , Biochem. Soc. Trans., 2003
2. Mitochondrial proton conductance and H+/O ratio are independent of electron transport rate in isolated hepatocytes, Porter RK, Brand MD, , , Biochem. J., 1995
External links
★
Chart of Important Metabolic Products
★
A detailed description of respiration vs. fermentation
★
Kimball's online resource to cellular respiration
★
Cellular Respiration and Fermentation at Clermont College
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