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Autor(en): 
  • Zbigniew Darzynkiewicz
  • Joe W. Gray
  • Techniques in Cell Cycle Analysis 
     

    (Buch)
    Dieser Artikel gilt, aufgrund seiner Grösse, beim Versand als 3 Artikel!


    Übersicht

    Auf mobile öffnen
     
    Lieferstatus:   i.d.R. innert 5-10 Tagen versandfertig
    Veröffentlichung:  November 2013  
    Genre:  Naturwissensch., Medizin, Technik 
     
    Biologie / Mikrobiologie / Biologie / Molekularbiologie / Biologie / Zellbiologie / Biowissenschaften, allgemein / C; SCL16008 - Cell Biology; SUCO11642 - Biomedical and Life Sciences / Cytologie / Mikrobiologie (nicht-medizinisch) / Mikrobiologie - Mikroorganismus / Molekularbiologie / SCIENCE / Life Sciences / Molecular Biology / ZELLBIOLOGIE / Zelle (biologisch) / Zellbiologie / Zelle (biologisch) / Zytologie / Zytologie
    ISBN:  9781489941015 
    EAN-Code: 
    9781489941015 
    Verlag:  Humana Press 
    Einband:  Kartoniert  
    Sprache:  English  
    Dimensionen:  H 235 mm / B 155 mm / D 24 mm 
    Gewicht:  645 gr 
    Seiten:  428 
    Zus. Info:  Paperback 
    Bewertung: Titel bewerten / Meinung schreiben
    Inhalt:
    Quantification of the proliferative characteristics of normal and malignant cells has been of interest to oncolo­ gists and cancer biologists for almost three decades. This interest stems from (a) the fact that cancer is a disease of uncontrolled proliferation, (b) the finding that many of the commonly used anticancer agents are preferentially toxic to cells that are actively proliferating, and (c) the observa­ tion that significant differences in proliferation characteristics exist between normal and malignant cells. Initially, cell cycle analysis was pursued enthusiastically in the hope of gener­ ating information useful for the development of rational cancer therapy strategies; for example, by allowing identi­ fication of rapidly proliferating tumors against which cell cycle-specific agents could be used with maximum effec­ tiveness and by allowing rational scheduling of cell cyc- specific therapeutic agents to maximize the therapeutic ratio. Unfortunately, several difficulties haveprevented realiza­ tion of the early promise of cell cycle analysis: Proliferative patterns of the normal and malignant tissues have been found to be substantially more complex than originally an­ ticipated, and synchronization of human tumors has proved remarkably difficult. Human tumors of the same type have proved highly variable, and the cytokinetic tools available for cell cycle analysis have been labor intensive, as well as somewhat subjective and in many cases inapplicable to humans. However, the potential for substantially improved cancer therapy remains if more accurate cytokinetic infor­ mation about human malignancies and normal tissues can be obtained in a timely fashion.

      



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