Characterization of a novel barbituric acid and two thiobarbituric acid compounds for lung cancer treatment

Sang Y. Lee; Becky Slagle-Webb; Arun K. Sharma; James R. Connor

doi:10.21873/anticanres.14625

Characterization of a novel barbituric acid and two thiobarbituric acid compounds for lung cancer treatment

Sang Y. Lee, Becky Slagle-Webb, Arun K. Sharma, James R. Connor

Research output: Contribution to journal › Article › peer-review

Abstract

Background/Aim: Previously, we reported the identification of a cytotoxic chemotype compound CC-I (1a), a derivative of thiobarbituric acid. We also reported the anticancer activity of a series of novel thio- and seleno-barbituric acid analogs. Materials and Methods: We herein evaluated the effect of 1a and its modified compounds on in vitro and in vivo lung cancer models. Results: The compounds 1b and 2a showed more potent cytotoxicity than 1a to lung cancer cells. Moreover, 1b did not have any cytotoxicity on normal cells, such as fibroblasts. In the human lung cancer A549 mouse tumor xenograft model, 1b and 2a showed more pronounced antitumor effects than 1a. In the A549 lung cancer cells, 1a induced cell death mainly via JNK and p38 MAPK activation. However, compound 1b and 2a induced lung cancer cell death mostly through JNK activation. Conclusion: The results suggest that 1b and 2a can be useful therapeutic agents for lung cancer.

Original language	English (US)
Pages (from-to)	6039-6049
Number of pages	11
Journal	Anticancer research
Volume	40
Issue number	11
DOIs	https://doi.org/10.21873/anticanres.14625
State	Published - Nov 2020
Externally published	Yes

Keywords

Barbituric acid
Cytotoxicity
In vivo tumor model
Lung cancer
Thiobarbituric acid

ASJC Scopus subject areas

Oncology
Cancer Research

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10.21873/anticanres.14625

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title = "Characterization of a novel barbituric acid and two thiobarbituric acid compounds for lung cancer treatment",

abstract = "Background/Aim: Previously, we reported the identification of a cytotoxic chemotype compound CC-I (1a), a derivative of thiobarbituric acid. We also reported the anticancer activity of a series of novel thio- and seleno-barbituric acid analogs. Materials and Methods: We herein evaluated the effect of 1a and its modified compounds on in vitro and in vivo lung cancer models. Results: The compounds 1b and 2a showed more potent cytotoxicity than 1a to lung cancer cells. Moreover, 1b did not have any cytotoxicity on normal cells, such as fibroblasts. In the human lung cancer A549 mouse tumor xenograft model, 1b and 2a showed more pronounced antitumor effects than 1a. In the A549 lung cancer cells, 1a induced cell death mainly via JNK and p38 MAPK activation. However, compound 1b and 2a induced lung cancer cell death mostly through JNK activation. Conclusion: The results suggest that 1b and 2a can be useful therapeutic agents for lung cancer.",

keywords = "Barbituric acid, Cytotoxicity, In vivo tumor model, Lung cancer, Thiobarbituric acid",

author = "Lee, {Sang Y.} and Becky Slagle-Webb and Sharma, {Arun K.} and Connor, {James R.}",

note = "Funding Information: This study was supported by the National Cancer Institute [grant number R21CA167406] and the Elsa U. Pardee Foundation [grant number 125000]. The content is solely the responsibility of the authors and does not necessarily represent the official views of the funders. Publisher Copyright: {\textcopyright} 2020 International Institute of Anticancer Research. All rights reserved.",

year = "2020",

month = nov,

doi = "10.21873/anticanres.14625",

language = "English (US)",

volume = "40",

pages = "6039--6049",

journal = "Anticancer research",

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publisher = "International Institute of Anticancer Research",

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T1 - Characterization of a novel barbituric acid and two thiobarbituric acid compounds for lung cancer treatment

AU - Lee, Sang Y.

AU - Slagle-Webb, Becky

AU - Sharma, Arun K.

AU - Connor, James R.

N1 - Funding Information: This study was supported by the National Cancer Institute [grant number R21CA167406] and the Elsa U. Pardee Foundation [grant number 125000]. The content is solely the responsibility of the authors and does not necessarily represent the official views of the funders. Publisher Copyright: © 2020 International Institute of Anticancer Research. All rights reserved.

PY - 2020/11

Y1 - 2020/11

N2 - Background/Aim: Previously, we reported the identification of a cytotoxic chemotype compound CC-I (1a), a derivative of thiobarbituric acid. We also reported the anticancer activity of a series of novel thio- and seleno-barbituric acid analogs. Materials and Methods: We herein evaluated the effect of 1a and its modified compounds on in vitro and in vivo lung cancer models. Results: The compounds 1b and 2a showed more potent cytotoxicity than 1a to lung cancer cells. Moreover, 1b did not have any cytotoxicity on normal cells, such as fibroblasts. In the human lung cancer A549 mouse tumor xenograft model, 1b and 2a showed more pronounced antitumor effects than 1a. In the A549 lung cancer cells, 1a induced cell death mainly via JNK and p38 MAPK activation. However, compound 1b and 2a induced lung cancer cell death mostly through JNK activation. Conclusion: The results suggest that 1b and 2a can be useful therapeutic agents for lung cancer.

AB - Background/Aim: Previously, we reported the identification of a cytotoxic chemotype compound CC-I (1a), a derivative of thiobarbituric acid. We also reported the anticancer activity of a series of novel thio- and seleno-barbituric acid analogs. Materials and Methods: We herein evaluated the effect of 1a and its modified compounds on in vitro and in vivo lung cancer models. Results: The compounds 1b and 2a showed more potent cytotoxicity than 1a to lung cancer cells. Moreover, 1b did not have any cytotoxicity on normal cells, such as fibroblasts. In the human lung cancer A549 mouse tumor xenograft model, 1b and 2a showed more pronounced antitumor effects than 1a. In the A549 lung cancer cells, 1a induced cell death mainly via JNK and p38 MAPK activation. However, compound 1b and 2a induced lung cancer cell death mostly through JNK activation. Conclusion: The results suggest that 1b and 2a can be useful therapeutic agents for lung cancer.

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KW - Cytotoxicity

KW - In vivo tumor model

KW - Lung cancer

KW - Thiobarbituric acid

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Characterization of a novel barbituric acid and two thiobarbituric acid compounds for lung cancer treatment

Abstract

Keywords

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