Literature DB >> 6159093

Synchronization of 9L rat brain tumor cells by centrifugal elutriation.

P C Keng, C K Li, K T Wheeler.   

Abstract

Asynchronous 9L cells were separated into relatively homogeneously-sized populations using centrifugal elutriation with both a conventional collection method and a long collection method. A substantial increase in the homogeneity of the volume distributions and in the degree of synchrony of the separated fractions was obtained using the long collection method. Autoradiographic data indicated that fractions containing greater than or equal to 97% G1 cells, greater than or equal to 80% S cells, and 70-75% G2 cells could be routinely recovered with this procedure. Recovery in these fractions varied from 5 to 8% of the total number of cells elutriated. The colony forming efficiency (CFE) of cells from fractions representing each phase of the cell cycle was a constant 60-70%, which was comparable to the 60-80% usually found for asynchronous 9L cells. The percentage of cells in the G1, S, and G2 phases in the elutriated fractions was more accurately determined from the volume distribution than from computer fits of the DNA histogram obtained from flow cytometry. In genereal, the degree of synchrony was related to the coefficient of variation (CV) of the volume distributions of the elutriated fractions. The CV was about 14% for all elutriated fractions. When the greater than or equal to 97% G1 population was allowed to progress to S and G2, the CVs were about 17 and 20.2%, respectively. Thus, the best nonperturbing method for obtaining synchronous 9L cells in the S or G2 phases was direct elutriation with the long collection method.

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Year:  1980        PMID: 6159093     DOI: 10.1007/BF02790449

Source DB:  PubMed          Journal:  Cell Biophys        ISSN: 0163-4992


  27 in total

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2.  Factors influencing the survival of rat brain tumor cells after in vitro treatment with 1,3-bis(2-chloroethyl)-1-nitrosourea.

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5.  Cell-cycle phase-dependence of drug-induced cycle progression delay.

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6.  Selection of optimal model for the DNA histogram by analysis of error of estimated parameters.

Authors:  T Lindmo; E Aarnaes
Journal:  J Histochem Cytochem       Date:  1979-01       Impact factor: 2.479

7.  Use of zonal centrifugation for preparing synchronous cultures from Ehrlich ascites cells grown in vivo.

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8.  Density invariance of cultured Chinese hamster cells with stage of the mitotic cycle.

Authors:  E C Anderson; D F Petersen; R A Tobey
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Authors:  H R Macdonald; R G Miller
Journal:  Biophys J       Date:  1970-09       Impact factor: 4.033

10.  Morphological studies of rat brain tumors induced by N-nitrosomethylurea.

Authors:  H H Schmidek; S L Nielsen; A L Schiller; J Messer
Journal:  J Neurosurg       Date:  1971-03       Impact factor: 5.115

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  11 in total

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Authors:  P C Keng; C K Li; K T Wheeler
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Authors:  M A Tsai; R E Waugh; P C Keng
Journal:  Biophys J       Date:  1996-04       Impact factor: 4.033

3.  Treatment of artificially-induced pulmonary metastases with fractionated doses of vincristine and/or radiation therapy.

Authors:  D J Grdina; R A White
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Authors:  F M Domurat; P Keng; D J Mock; N J Roberts
Journal:  Cell Biophys       Date:  1989-12

5.  Changes in growth characteristics and macromolecular synthesis on recovery from severe hypoxia.

Authors:  R E Wilson; P C Keng; R M Sutherland
Journal:  Br J Cancer       Date:  1990-01       Impact factor: 7.640

6.  Radiation response of proliferating and quiescent subpopulations isolated from multicellular spheroids.

Authors:  C K Luk; P C Keng; R M Sutherland
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7.  Cell subpopulations dispersed from solid tumours and separated by centrifugal elutriation.

Authors:  D W Siemann; E M Lord; P C Keng; K T Wheeler
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8.  Characterization of radiation sensitivity of human squamous carcinoma A431 cells.

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9.  Lymphoma models for B cell activation and tolerance. III. Cell cycle dependence for negative signalling of WEHI-231 B lymphoma cells by anti-mu.

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10.  Comparison of tumour age response to radiation for cells derived from tissue culture or solid tumours.

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