Novel metal chelating molecules with anticancer activity. Striking effect of the imidazole substitution of the histidine-pyridine-histidine system.

Taha F S Ali Kana Iwamaru Halil Ibrahim Ciftci Ryoko Koga Masahiro Matsumoto Yasunori Oba Hiromasa Kurosaki Mikako Fujita Yoshinari Okamoto Kazuo Umezawa Mitsuyoshi Nakao Takuichiro Hide Keishi Makino Jun-ichi Kuratsu Mohamed Abdel-Aziz Gamal El-Din A A Abuo-Rahma Eman A M Beshr Masami Otsuka

Bioorg Med Chem

Department of Bioorganic Medicinal Chemistry, Faculty of Life Sciences, Kumamoto University, 5-1 Oe-honmachi, Chuo-ku, Kumamoto 862-0973, Japan. Electronic address:

Published: September 2015

Previously we have reported a metal chelating histidine-pyridine-histidine system possessing a trityl group on the histidine imidazole, namely HPH-2Trt, which induces apoptosis in human pancreatic adenocarcinoma AsPC-1 cells. Herein the influence of the imidazole substitution of HPH-2Trt was examined. Five related compounds, HPH-1Trt, HPH-2Bzl, HPH-1Bzl, HPH-2Me, and HPH-1Me were newly synthesized and screened for their activity against AsPC-1 and brain tumor cells U87 and U251. HPH-1Trt and HPH-2Trt were highly active among the tested HPH compounds. In vitro DNA cleavage assay showed both HPH-1Trt and HPH-2Trt completely disintegrate pUC19 DNA. The introduction of trityl group decisively potentiated the activity.

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http://dx.doi.org/10.1016/j.bmc.2015.07.044	DOI Listing

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