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Titlebook: Assessment of Cell Proliferation in Clinical Practice; Peter A. Hall (Professor of Histopathology),David Book 1992 Springer-Verlag London

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The Treatment of Electronic Organizers, preserving the spatial orientation of cells. Antibodies may recognise endogenous cell cycle related molecules occurring naturally within the tissue to be studied, or exogenous substances, such as bromodeoxyuridine (BUdR), a thymidine analogue incorporated during the S (DNA synthetic) phase of the c
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PC Hardware and Inside the Box,n patient management. This chapter will outline the techniques currently clinically available and discuss their practical advantages and disadvantages. In addition, the clinical situations in which assessment of cell proliferation may prove to be of use will be reviewed.
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https://doi.org/10.1007/978-1-84628-732-91960s (Skipper et al. 1964, 1967). As a result of his investigations of experimental tumour systems, Skipper concluded that a given dose or course of (chemo)therapy will kill a constant . of the cell population, rather than a constant number of cells. He went on to consider the consequences of tumou
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https://doi.org/10.1007/978-3-540-78716-7 and indirect mechanisms mediated through factors carried by organ vasculature. Disruption of the functional integrity of growth regulatory systems may lead to uncontrolled proliferation and abnormal cellular behaviour manifest in a most extreme form in the development of malignant tumours.
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PC Hardware and Inside the Box,n patient management. This chapter will outline the techniques currently clinically available and discuss their practical advantages and disadvantages. In addition, the clinical situations in which assessment of cell proliferation may prove to be of use will be reviewed.
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Clinical Aspects of Assessing Cell Proliferation,n patient management. This chapter will outline the techniques currently clinically available and discuss their practical advantages and disadvantages. In addition, the clinical situations in which assessment of cell proliferation may prove to be of use will be reviewed.
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Regulation of the Eukaryotic Cell Cycle,rs primarily in G. (Smith 1982). Thus, though not invariant, the duration of S + G. + M generally changes far less than does the duration of G. with changes in proliferation rate. Furthermore, cells which cease proliferation, either reversibly (e.g. hepatocytes, lymphocytes) or permanently (e.g. neu
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