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Estimation of kinetic cell-cycle-related gene expression in G1 and G2 phases from immunofluorescence flow cytometry data.

Authors :
Jacobberger JW
Sramkoski RM
Wormsley SB
Bolton WE
Source :
Cytometry [Cytometry] 1999 Mar 01; Vol. 35 (3), pp. 284-9.
Publication Year :
1999

Abstract

Background: Flow cytometry of immunofluorescence and DNA content provides measures of cell-cycle-related gene expression (protein and/or epitope levels) for asynchronously growing cells. From these data, time-related expression through S phase can be directly measured. However, for G1, G2, and M phases, this information is unavailable. We present an objective method to model G1 and G2 kinetic expression from an estimate of a minimum biological unit of positive immunofluorescence derived from the distribution of specific immunofluorescence of mitotic cells.<br />Methods: DU 145 cells were stained for DNA, cyclin B1, and a mitotic marker (p105) and analyzed by flow cytometry. The cyclin B1 immunofluorescence (B1) distribution of p105-positive cells was used to model the B1 distribution of G2 and G1 cells. The G1/S and S/G2 interface measurements were used to calculate expression in S phase and test the validity of the approach.<br />Results: B1 at S/G2 closely matched the earliest modeled estimate of B1 in G2. B1 increased linearly through G1 and S but exponentially through G2; mitotic levels were equivalent to the highest G2 levels. G1 modeling of B1 was less certain than that of G2 due to low levels of expression but demonstrated general feasibility.<br />Conclusions: By this method, the upper and lower bounds of cyclin B1 expression could be estimated and kinetic expression through G1, G2, and M modeled. Together with direct measurements in S phase, expression of B1 throughout the entire cell cycle of DU 145 cells could be modeled. The method should be generally applicable given model-specific assumptions.

Details

Language :
English
ISSN :
0196-4763
Volume :
35
Issue :
3
Database :
MEDLINE
Journal :
Cytometry
Publication Type :
Academic Journal
Accession number :
10082310
Full Text :
https://doi.org/10.1002/(sici)1097-0320(19990301)35:3<284::aid-cyto12>3.0.co;2-k