Actin Organization as an in Vitro Assay for Tumorigenicity
Robert Pollack,
Nancy Nicholson,
David Alcorta,
Michael Verderame,
Katy Smith and
Bettie Steinberg
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Robert Pollack: Columbia University, Department of Biological Sciences
Nancy Nicholson: Columbia University, Department of Biological Sciences
David Alcorta: Columbia University, Department of Biological Sciences
Michael Verderame: Columbia University, Department of Biological Sciences
Katy Smith: Columbia University, Department of Biological Sciences
Bettie Steinberg: Columbia University, Department of Biological Sciences
Chapter 1 in Cell and Muscle Motility, 1982, pp 1-13 from Springer
Abstract:
Abstract The endpoints of in vivo and in vitro assays applied to cells after exposure to a potential oncogenic transforming agent are cellular tumorigenicity and transformation. Tumors are failures of in vivo growth control; transformations are failures of in vitro growth control. Many agents cause tumors in vivo, many agents transform normal cultured cells, and some agents do both. However, even when caused by a single agent, the in vivo and in vitro endpoint assays show only a partial overlap. That is, some but not all tumors will grow as transformed cells in culture, and some but not all in vitro transformants will be tumorigenic on injection into susceptible animals (Shin et al., 1975). Recently, we have described a subset of in vitro phenotypic changes that correlate with in vivo tumorigenicity (Steinberg et al., 1979; Barrett et al., 1979; Pollack, 1981). In this chapter, we will describe recent studies on one of the in vitro changes linked to tumorigenicity, the disruption in organization of cyto-skeletal actin.
Keywords: Skin Fibroblast; Human Skin Fibroblast; Asymptomatic Child; Actin Organization; Actin Cable (search for similar items in EconPapers)
Date: 1982
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Persistent link: https://EconPapers.repec.org/RePEc:spr:sprchp:978-1-4684-4037-9_1
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DOI: 10.1007/978-1-4684-4037-9_1
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