Parallel synthesis and biological evolution of quinic acid derivatives as immuno-suppressing agents against T-cell receptors

Chih Yu Huang; Li Hsun Chen; Hsuan Yu Huang; Feng Sheng Kao; Yun Ta Lee; Manikandan Selvaraju; Chung-Ming Sun; Hueih Min Chen

doi:10.1039/c5ra06095h

Parallel synthesis and biological evolution of quinic acid derivatives as immuno-suppressing agents against T-cell receptors

Chih Yu Huang, Li Hsun Chen, Hsuan Yu Huang, Feng Sheng Kao, Yun Ta Lee, Manikandan Selvaraju, Chung-Ming Sun^*, Hueih Min Chen

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摘要

A simple protocol for the synthesis of quinic acid derivatives was established and their biological evolution against T-cells is studied. Results showed that one of the derivatives, Cyn-1324, has low toxicity on T-cells and a high effect on reducing Signal 2 of T-cell immune responses. In vitro binding measurements of atomic force spectroscopy further indicated that the blocking effect of Cyn-1324 between CD28 and CD80 was about 31 ± 4%. In vivo animal tests also confirmed that Cyn-1324 can reduce the allergic responses from ovalbumin-induced mice with little toxicity. Based on these observations, Cyn-1324 can be a mild immuno-suppressive candidate for future drug development.

原文	English
頁（從 - 到）	50801-50806
頁數	6
期刊	RSC Advances
卷	5
發行號	63
DOIs	https://doi.org/10.1039/c5ra06095h
出版狀態	Published - 2015

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title = "Parallel synthesis and biological evolution of quinic acid derivatives as immuno-suppressing agents against T-cell receptors",

abstract = "A simple protocol for the synthesis of quinic acid derivatives was established and their biological evolution against T-cells is studied. Results showed that one of the derivatives, Cyn-1324, has low toxicity on T-cells and a high effect on reducing Signal 2 of T-cell immune responses. In vitro binding measurements of atomic force spectroscopy further indicated that the blocking effect of Cyn-1324 between CD28 and CD80 was about 31 ± 4%. In vivo animal tests also confirmed that Cyn-1324 can reduce the allergic responses from ovalbumin-induced mice with little toxicity. Based on these observations, Cyn-1324 can be a mild immuno-suppressive candidate for future drug development.",

author = "Huang, {Chih Yu} and Chen, {Li Hsun} and Huang, {Hsuan Yu} and Kao, {Feng Sheng} and Lee, {Yun Ta} and Manikandan Selvaraju and Chung-Ming Sun and Chen, {Hueih Min}",

note = "Publisher Copyright: {\textcopyright} The Royal Society of Chemistry 2015.",

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doi = "10.1039/c5ra06095h",

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T1 - Parallel synthesis and biological evolution of quinic acid derivatives as immuno-suppressing agents against T-cell receptors

AU - Huang, Chih Yu

AU - Chen, Li Hsun

AU - Huang, Hsuan Yu

AU - Kao, Feng Sheng

AU - Lee, Yun Ta

AU - Selvaraju, Manikandan

AU - Sun, Chung-Ming

AU - Chen, Hueih Min

PY - 2015

Y1 - 2015

N2 - A simple protocol for the synthesis of quinic acid derivatives was established and their biological evolution against T-cells is studied. Results showed that one of the derivatives, Cyn-1324, has low toxicity on T-cells and a high effect on reducing Signal 2 of T-cell immune responses. In vitro binding measurements of atomic force spectroscopy further indicated that the blocking effect of Cyn-1324 between CD28 and CD80 was about 31 ± 4%. In vivo animal tests also confirmed that Cyn-1324 can reduce the allergic responses from ovalbumin-induced mice with little toxicity. Based on these observations, Cyn-1324 can be a mild immuno-suppressive candidate for future drug development.

AB - A simple protocol for the synthesis of quinic acid derivatives was established and their biological evolution against T-cells is studied. Results showed that one of the derivatives, Cyn-1324, has low toxicity on T-cells and a high effect on reducing Signal 2 of T-cell immune responses. In vitro binding measurements of atomic force spectroscopy further indicated that the blocking effect of Cyn-1324 between CD28 and CD80 was about 31 ± 4%. In vivo animal tests also confirmed that Cyn-1324 can reduce the allergic responses from ovalbumin-induced mice with little toxicity. Based on these observations, Cyn-1324 can be a mild immuno-suppressive candidate for future drug development.

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U2 - 10.1039/c5ra06095h

DO - 10.1039/c5ra06095h

M3 - Article

AN - SCOPUS:84935889876

SN - 2046-2069

VL - 5

SP - 50801

EP - 50806

JO - RSC Advances

JF - RSC Advances

IS - 63

ER -

Parallel synthesis and biological evolution of quinic acid derivatives as immuno-suppressing agents against T-cell receptors

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