Beryl Hartley-Asp

TL;DR: The clastogenic effect of mitomycin C (MC) was determined in two normal fibroblast cell lines and two xeroderma pigmentosum (XP) cell lines, a variant and a group A excision-deficient line, with a distinctly higher sensitivity to caffeine than the classical XP or the normal human cell line.

TL;DR: Karyotype analysis using G‐banding revealed that DU 145 had retained several of its original markers, and demonstrated multiple marker chromosomes in 1013L.

TL;DR: The results extend the knowledge concerning EM and demonstrate that the cell line 1013L is a relevant model system for studying drugs active against human prostatic tumours.

TL;DR: In vivo studies with specific alkylating agent-sensitive, or antimetabolite-sensitive tumours showed no antitumour activity although significant inhibition of Ehrlich ascites tumour cell growth was observed at high doses, suggesting a possible antimetabolic mode of action.

TL;DR: The influence on macromolecular synthesis in the human prostatic tumour cell line 1013L was investigated and an inhibition of overall RNA synthesis was predominant, indicating disturbances in either RNA processing or RNA transport.