Double screening of suramin derivatives on human colon cancer cells and on neural cells provides new therapeutic agents with reduced toxicity

S Baghdiguian, P Nickel, J Fantini - Cancer letters, 1991 - Elsevier
S Baghdiguian, P Nickel, J Fantini
Cancer letters, 1991Elsevier
Suramin is a polyanionic compound currently used under evaluation for antineoplastic
activity. One of the main problems encountered during clinical trials was an adverse
neurotoxic effect, probably due to a direct cytotoxic effect on neural cells. Suramin is also
known to trigger differentiation of human colon cancer cells, yet a chronic treatment induces
a lysosomal storage disorder. The aim of this study was to evaluate suramin analogs for their
effect:(i) on the lysosomal system of the human colon cancer cell clone HT29-D4; and (ii) on …
Abstract
Suramin is a polyanionic compound currently used under evaluation for antineoplastic activity. One of the main problems encountered during clinical trials was an adverse neurotoxic effect, probably due to a direct cytotoxic effect on neural cells. Suramin is also known to trigger differentiation of human colon cancer cells, yet a chronic treatment induces a lysosomal storage disorder. The aim of this study was to evaluate suramin analogs for their effect: (i) on the lysosomal system of the human colon cancer cell clone HT29-D4; and (ii) on C6 glioma cell growth and morphology. One of the derivatives tested, NF036, induced terminal differentiation of HT29-D4 cells without any impairment of the lysosomal system. Furthermore, in contrast to suramin, NF036 did not alter C6 cell growth and morphology. We conclude that there is a relationship between the ability of a suramin derivative to induce a lysosomal storage disorder in human colon cancer cells and its neurotoxic effect. A double screening of suramin analogs on HT29-D4 and C6 cells allowed us to identify a new candidate antineoplastic drug: NF036.
Elsevier
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