Structural properties of dibenzosuberanylpiperazine derivatives for efficient reversal of chloroquine resistance in Plasmodium chabaudi

Yumiko Osa; Seiki Kobayashi; Yoko Sato; Yumiko Suzuki; Kouichi Takino; Tsutomu Takeuchi; Yoshiyuki Miyata; Masakazu Sakaguchi; Hiroaki Takayanagi

doi:10.1021/jm020379v

Structural properties of dibenzosuberanylpiperazine derivatives for efficient reversal of chloroquine resistance in Plasmodium chabaudi

J Med Chem. 2003 May 8;46(10):1948-56. doi: 10.1021/jm020379v.

Authors

Yumiko Osa¹, Seiki Kobayashi, Yoko Sato, Yumiko Suzuki, Kouichi Takino, Tsutomu Takeuchi, Yoshiyuki Miyata, Masakazu Sakaguchi, Hiroaki Takayanagi

Affiliation

¹ School of Pharmaceutical Sciences, Kitasato University, 5-9-1, Shirokane, Minato-ku, Tokyo 108-8641, Japan. osay@pharm.kitasato-u.ac.jp

PMID: 12723957
DOI: 10.1021/jm020379v

Abstract

For the purpose of developing chemosensitizers to reverse chloroquine (CQ) resistance in Plasmodium chabaudi in vivo, dibenzosuberanylpiperazine (1-(10,11-dihydro-5H-dibenzo[a,d]cyclohepten-5-yl)piperazine) (DSP) and its piperazin-1-yl derivatives were synthesized systematically. DSP hydrochloride (3) was obtained from the reaction of dibenzosuberanyl chloride with piperazine in the presence of 1,8-diazabicyclo[5,4,0]-7-undecene (DBU). To understand the relationship between the substituent patterns of DSP derivatives and their biological activities, 13 hydroxyalkyl or hydroxyalkenyl derivatives were synthesized by an attack of the piperazine secondary amine of 3 on commercially available epoxides in the presence of triethylamine or DBU, and three alkyl or alkynyl derivatives were synthesized by the reactions of 3 with the corresponding organic chlorides in the presence of DBU. In both reactions, the yield was a maximum of 90%. The biological activities of the synthesized compounds were evaluated on the basis of two values: antimalarial activity and reversal activity. The values of antimalarial activities by single administration of 17 test compounds were not effective, being in the range 67-152% on day 4 after infection of Plasmodium chabaudi to mice except for the administration of 3-(dibenzosuberanylpiperazin-1-yl)-1-butene (29, 22%). On the other hand, administration of the seven test compounds (50 mg/kg dose) combined with CQ (3-4 mg/kg) gave high reversal activities, namely, low values (0% on day 4). The effective test compounds were those obtained by introducing the following substituents: 2-hydroxybutyl (24), 2-hydroxyhexen-5-yl (27), 2-hydroxybuten-3-yl (28a), 2-substituted 1-hydroxybuten-3-yl (28b), 4-acetoxybutyn-2-yl (30), 4-hydroxybutyn-2-yl (31), and 3-substituted buten-1-yl (29), which correspond to the nonbulky groups of hydroxyalkyl (C4), hydroxyalkenyl (C4-C6), hydroxyalkynyl (C4), or alkenyl (C4). These results may lead to the development of an approach to developing clinically applicable chemosensitizers for drug-resistant malaria.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Antimalarials / chemical synthesis*
Antimalarials / chemistry
Antimalarials / pharmacology
Chloroquine / pharmacology*
Crystallography, X-Ray
Dibenzocycloheptenes / chemical synthesis*
Dibenzocycloheptenes / chemistry
Dibenzocycloheptenes / pharmacology
Drug Resistance, Multiple
Female
Malaria / drug therapy
Mice
Piperazines / chemical synthesis*
Piperazines / chemistry
Piperazines / pharmacology
Plasmodium chabaudi / drug effects*
Structure-Activity Relationship

Substances

Antimalarials
Dibenzocycloheptenes
Piperazines
dibenzosuberanylpiperazine
Chloroquine