Genetic content
The genetic information of all cells resides in the sequence of nitrogenous bases in the extremely long molecules of DNA. Unlike the DNA in eukaryotic cells, which resides in the nucleus, DNA in bacterial cells is not sequestered in a membrane-bound organelle but appears as a long coil distributed through the cytoplasm. In many bacteria the DNA is present as a single circular chromosome, although some bacteria may contain two chromosomes, and in some cases the DNA is linear rather than circular. A variable number of smaller, usually circular (though sometimes linear) DNA molecules, called plasmids, can carry auxiliary information.
The sequence of bases in the DNA has been determined for hundreds of bacteria. The amount of DNA in bacterial chromosomes ranges from 580,000 base pairs in Mycoplasma genitalium to 4,700,000 base pairs in E. coli to roughly 9,450,000 base pairs in Myxococcus xanthus. Sorangium cellulosum, a myxobacterium, has one of the largest bacterial genomes, containing in excess of 13 million base pairs. The length of the E. coli chromosome, if removed from the cell and stretched to its fullest extent, is about 1.2 mm, which is striking in view of the fact that the length of the cell is about 0.001 mm.
As in all organisms, bacterial DNA contains the four nitrogenous bases adenine (A), cytosine (C), guanine (G), and thymine (T). The rules of base pairing for double-stranded DNA molecules require that the number of adenine and thymine bases be equal and that the number of cytosine and guanine bases also be equal. The relationship between the number of pairs of G and C bases and the number of pairs of A and T bases is an important indicator of evolutionary and adaptive genetic changes within an organism. The proportion, or molar ratio, of G + C can be measured as G + C divided by the sum of all the bases (A + T + G + C) multiplied by 100 percent. The extent to which G + C ratios vary between organisms may be considerable. In plants and animals, the proportion of G + C is about 50 percent. A far wider range in the proportion of G + C is seen in prokaryotes, extending from about 25 percent in most Mycoplasma to about 50 percent in E. coli to nearly 75 percent in Micrococcus, actinomycetes, and fruiting myxobacteria. The G + C content within a species in a single genus, however, is very similar.
Cytoplasmic structures
The cytoplasm of bacteria contains high concentrations of enzymes, metabolites, and salts. In addition, the proteins of the cell are made on ribosomes that are scattered throughout the cytoplasm. Bacterial ribosomes are different from ribosomes in eukaryotic cells in that they are smaller, have fewer constituents (consist of three types of ribosomal RNA [rRNA] and 55 proteins, as opposed to four types of rRNA and 78 proteins in eukaryotes), and are inhibited by different antibiotics than those that act on eukaryotic ribosomes.
There are numerous inclusion bodies, or granules, in the bacterial cytoplasm. These bodies are never enclosed by a membrane and serve as storage vessels. Glycogen, which is a polymer of glucose, is stored as a reserve of carbohydrate and energy. Volutin, or metachromatic granules, contains polymerized phosphate and represents a storage form for inorganic phosphate and energy. Many bacteria possess lipid droplets that contain polymeric esters of poly-β-hydroxybutyric acid or related compounds. This is in contrast to eukaryotes, which use lipid droplets to store triglycerides. In bacteria, storage granules are produced under favourable growth conditions and are consumed after the nutrients have been depleted from the medium. Many aquatic bacteria produce gas vacuoles, which are protein-bound structures that contain air and allow the bacteria to adjust their buoyancy. Bacteria can also have internal membranous structures that form as outgrowths of the cytoplasmic membrane.
Biotypes of bacteria
The fact that pathogenic bacteria are constantly battling their host’s immune system might account for the bewildering number of different strains, or types, of bacteria that belong to the same species but are distinguishable by serological tests. Microbiologists often identify bacteria by the presence of specific molecules on their cell surfaces, which are detected with specific antibodies. Antibodies are serum proteins that bind very tightly to foreign molecules (antigens) in an immune reaction aimed at removing or destroying the antigens. Antibodies have remarkable specificity, and the substitution of even one amino acid in a protein might prevent that protein from being recognized by an antibody.
For many bacterial species there are thousands of different strains (called serovars, for serological variants), which differ from one another mainly or solely in the antigenic identity of their lipopolysaccharide, flagella, or capsule. Different serovars of enteric bacteria—such as E. coli and Salmonella enterica, for example—are often found to be associated with the ability to inhabit different host animals or to cause different diseases. Formation of these numerous serovars reflects the ability of bacteria to respond effectively to the intense defensive actions of the immune system.
Bacterial reproduction
Reproductive processes
Binary fission
Most prokaryotes reproduce by a process of binary fission, in which the cell grows in volume until it divides in half to yield two identical daughter cells. Each daughter cell can continue to grow at the same rate as its parent. For this process to occur, the cell must grow over its entire surface until the time of cell division, when a new hemispherical pole forms at the division septum in the middle of the cell. In gram-positive bacteria the septum grows inward from the plasma membrane along the midpoint of the cell; in gram-negative bacteria the walls are more flexible, and the division septum forms as the side walls pinch inward, dividing the cell in two. In order for the cell to divide in half, the peptidoglycan structure must be different in the hemispherical cap than in the straight portion of the cell wall, and different wall-cross-linking enzymes must be active at the septum than elsewhere.