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Mitochondria are thought to have originated from an ancient symbiosis that resulted when a nucleated cell engulfed an aerobic prokaryote. The engulfed cell came to rely on the protective environment of the host cell, and, conversely, the host cell came to rely on the engulfed prokaryote for energy production. Over time, the descendants of the engulfed prokaryote developed into mitochondria, and the work of these organelles — using oxygen to create energy — became critical to eukaryotic evolution (Figure 1).
Modern mitochondria have striking similarities to some modern prokaryotes, even though they have diverged significantly since the ancient symbiotic event. For example, the inner mitochondrial membrane contains electron transport proteins like the plasma membrane of prokaryotes, and mitochondria also have their own prokaryote-like circular genome. One difference is that these organelles are thought to have lost most of the genes once carried by their prokaryotic ancestor. Although present-day mitochondria do synthesize a few of their own proteins, the vast majority of the proteins they require are now encoded in the nuclear genome.
As previously mentioned, mitochondria contain two major membranes. The outer mitochondrial membrane fully surrounds the inner membrane, with a small intermembrane space in between. The outer membrane has many protein-based pores that are big enough to allow the passage of ions and molecules as large as a small protein. In contrast, the inner membrane has much more restricted permeability, much like the plasma membrane of a cell. The inner membrane is also loaded with proteins involved in electron transport and ATP synthesis. This membrane surrounds the mitochondrial matrix, where the citric acid cycle produces the electrons that travel from one protein complex to the next in the inner membrane. At the end of this electron transport chain, the final electron acceptor is oxygen, and this ultimately forms water (H20). At the same time, the electron transport chain produces ATP. (This is why the the process is called oxidative phosphorylation.)
During electron transport, the participating protein complexes push protons from the matrix out to the intermembrane space. This creates a concentration gradient of protons that another protein complex, called ATP synthase, uses to power synthesis of the energy carrier molecule ATP (Figure 2).
Mitochondrial genomes are very small and show a great deal of variation as a result of divergent evolution. Mitochondrial genes that have been conserved across evolution include rRNA genes, tRNA genes, and a small number of genes that encode proteins involved in electron transport and ATP synthesis. The mitochondrial genome retains similarity to its prokaryotic ancestor, as does some of the machinery mitochondria use to synthesize proteins. In fact, mitochondrial rRNAs more closely resemble bacterial rRNAs than the eukaryotic rRNAs found in cell cytoplasm. In addition, some of the codons that mitochondria use to specify amino acids differ from the standard eukaryotic codons.
Still, the vast majority of mitochondrial proteins are synthesized from nuclear genes and transported into the mitochondria. These include the enzymes required for the citric acid cycle, the proteins involved in DNA replication and transcription, and ribosomal proteins. The protein complexes of the respiratory chain are a mixture of proteins encoded by mitochondrial genes and proteins encoded by nuclear genes. Proteins in both the outer and inner mitochondrial membranes help transport newly synthesized, unfolded proteins from the cytoplasm into the matrix, where folding ensues (Figure 3).
Mitochondria cannot be made "from scratch" because they need both
mitochondrial and nuclear gene products. These organelles replicate by
dividing in two, using a process similar to the simple, asexual form of
cell division employed by bacteria. Video microscopy shows that
mitochondria are incredibly dynamic. They are constantly dividing,
fusing, and changing shape. Indeed, a single mitochondrion may contain
multiple copies of its genome at any given time.
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