@article{oai:repo.qst.go.jp:00046642,
 author = {Ishikawa, J and Takahashi, Y and Hazawa, Masaharu and Fukushi, Y and Yoshozawa, A and Kashiwakura, Ikuo and 羽澤 勝治},
 issue = {3},
 journal = {Cancer Cell International (Online Only URL:Thhp://www.pubmedcentral.nih.gov/tocrender.fcgi?journal=96&action=archive)},
 month = {Jan},
 note = {BACKGROUND: 
\nThe aim of this study was to evaluate the biological and pharmaceutical activities of 14 amphiphilic liquid-crystalline compounds (LCs), i.e, phenylpyrimidine derivatives possessing D-glucamine and cyanobiphenyl derivatives with a terminal hydroxyl unit.
\nRESULTS: 
\nThe cytotoxic properties of the LCs on the cell growth, cell cycle distribution, and cell signaling pathway of U937 human leukemic monocyte lymphoma cells were assessed by flow cytometry and western blot analysis. Some LCs showed cytostatic effects, suppressing cell growth via S-phase arrest and without apoptosis in U937 cells. To investigate the mechanisms of the LC-induced S-phase arrest, proteins relevant to cell cycle regulation were investigated by western blot analysis. The rate of LC-induced S-phase arrest was congruent with the decreased expression of MCM2, cyclin A, cyclin B, CDK2, phospho-CDK1 and Cdc25C. Observed changes in cell cycle distribution by LC treated might be caused by insufficient preparation for G2/M transition. Considering the structure of the LCs, the rod-like molecules displaying cytotoxicity against U937 cells possessed flexible spacers with no bulky polar group attached via the flexible spacer.
\nCONCLUSIONS: 
\nOur results revealed that some LCs showed cytotoxic properties against non-solid type tumor human leukemic cells via LC-induced S-phase arrest and decreasing expression of several cell cycle related proteins.},
 pages = {12--13},
 title = {Suppressive effects of liquid crystal compounds on the growth of U937 human leukemic monocyte lymphoma cells.},
 volume = {12},
 year = {2012}
}