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  • 1
    ISSN: 1432-0827
    Keywords: Radioautography ; Mineralization ; Incisors ; Odontoblasts ; Ameloblasts
    Source: Springer Online Journal Archives 1860-2000
    Topics: Biology , Medicine , Physics
    Notes: Abstract To find out whether the calcium phosphate of dentin and enamel is elaborated in the cells prior to passing into the organic matrix or is initially deposited into the matrix, rats were injected intravenously with45Ca and killed 30 sec or 5 min later by glutaraldehyde perfusion; semithin sections of the undecalcified incisor teeth were then radioautographed for detection of the incorporated45Ca. Rat incisor teeth were selected since there is evidence that the calcium they take up is “stable”; that is, not subject to significant loss by exchange or by other physiocochemical processes. Whendentin is examined after45Ca injection, the maximum radioautographic reaction is observed next to the junction with predentin and a gradual decrease up to the dentin enamel border. No radioactivity is detected in odontoblasts. These observations are interpreted as indicating that the initial site of calcium phosphate deposition is in the matrix of dentin. In theenamel, the radioautographic reaction is spread fairly uniformly throughout the matrix, with a weak reaction over ameloblasts attributed to radiation scatter. The interpretation is again that calcium phosphate is deposited into the matrix; and, furthermore, that this deposition begins as soon as the matrix is laid down and continues at about the same rate up to an advanced stage of mineralization.
    Type of Medium: Electronic Resource
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  • 2
    Electronic Resource
    Electronic Resource
    Springer
    Protoplasma 160 (1991), S. 5-38 
    ISSN: 1615-6102
    Keywords: Radioautography ; Cell classification ; Cell renewal ; Protein turnover ; extracellular matrix stability
    Source: Springer Online Journal Archives 1860-2000
    Topics: Biology
    Notes: Summary Some 50 years ago, Schoenheimer, Hevesy, and their followers discovered that the substances making up the organs of the body were in a dynamic state. When a precise method was devised for radioautography in 1946, it became possible to examine how whole cells, intracellular components, and extracellular matrix participated in this dynamism. Whole cells have been classified according to their ability to proliferate, as measured in3H-thymidine radioautographs. Some cell populations, such as cortical neurons, do not proliferate and are calledstatic. Many others, such as kidney cell populations, proliferate at a slow rate that decreases with age and are calledexpanding. The cells in these two groups appear to live on as long as the individual. In a third group, cell populations such as those of surface epithelia and blood proliferate at a rapid rate and are calledrenewing; new cells continually arise from mitosis, differentiate to a functional stage and, thereafter, die. Renewing cell populations are under the dual control of genetic and environmental factors. Intracellular components turn over at variable but generally rapid rates. Thus, all cells, whether they belong to static, expanding or renewing populations, are labeled in radioautographs prepared after injection of3H-amino acids and, therefore, continually synthesize proteins. The newly-synthesized proteins migrate from ribosomes to nucleus, mitochondria and endoplasmic reticulum. From the latter, they may be traced to the Golgi apparatus, where their glycosylation is completed; they are then delivered to lysosomes, plasma membrane and, outside of some cells, by means of secretory granules. Like proteins, other intracellular components, namely RNAs, carbohydrates and lipids undergo turnover. However, while DNA and associated histones may be duplicated for mitosis, they otherwise remain completely stable. Extracellular matrices are of two main types: stromal matrices and basement membranes. Stromal matrices include a series of compact structures, such as dentin, elastic tissue and bone, whose components are mainly stable, with the exception of bone remodeling areas. As for connective tissue components, the turnover rate seems to decrease with the compactness. In basement membrane, limited evidence indicates that laminin turns over at a slow rate and heparan sulfate proteoglycan at a rapid rate, while type IV collagen might be stable. Thus, with few exceptions, extracellular matrix components turn over slowly or not at all. In conclusion, the dynamic state of body components arises from three different sources: (1) the extracellular matrix provides a rather small contribution; (2) cells in renewing populations provide an important share; (3) the turnover of intracellular components, that is proteins, RNAs, and other substances is the major factor in the dynamism of body components. The renewal of intracellular components occurs from bacteria to man. It is an essential feature of life.
    Type of Medium: Electronic Resource
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