Design and synthesis of aralkyl-ketone piperazine derivatives and their antalgic activities

Jian-qi LI; Li-ying HUANG; Jian-xin CHEN; Zhi-jie WENG; Chun-nian ZHANG; Jian-qi LI; Li-ying HUANG; Jian-xin CHEN; Zhi-jie WENG; Chun-nian ZHANG

Design and synthesis of aralkyl-ketone piperazine derivatives and their antalgic activities / 药学学报

Jian-qi LI; Li-ying HUANG; Jian-xin CHEN; Zhi-jie WENG; Chun-nian ZHANG; Jian-qi LI; Li-ying HUANG; Jian-xin CHEN; Zhi-jie WENG; Chun-nian ZHANG.

Yao Xue Xue Bao ; (12): 1166-1175, 2007.

Article in Zh | WPRIM | ID: wpr-268210

Responsible library: WPRO

ABSTRACT

ABSTRACT

To synthesize aralkyl-ketone piperazine derivatives as analgesic agents, the N atom of the one side of piperazine ring is protected by formyl group firstly, then the unprotected N atom is alkylated to prepare aralkyl-ketone piperazine derivatives. Their analgesic biological activities were well studied by mice writhing model, rat hot plate model and rat tail flick model. Sixty four compounds were synthesized and pharmacological tests in vivo revealed these compounds have potent analgesic activities, especially compound I12, I14, I14 I21 and I37. These four compounds are more worthy for further research.

Subject(s)

Animals; Female; Male; Mice; Rats; Analgesics; Pharmacology; Molecular Structure; Pain Measurement; Piperazines; Pharmacology; Random Allocation; Rats, Sprague-Dawley

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Full text: 1 Index: WPRIM Main subject: Pharmacology / Piperazines / Pain Measurement / Molecular Structure / Random Allocation / Rats, Sprague-Dawley / Analgesics Limits: Animals Language: Zh Journal: Yao Xue Xue Bao Year: 2007 Type: Article

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