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Efficient Utilization of 6-Aminouracil to Synthesize Fused and Related Heterocyclic Compounds and Their Evaluation as Prostate Cytotoxic Agents with Cathepsin B Inhibition
Efficient Utilization of 6-Aminouracil to Synthesize Fused and Related Heterocyclic Compounds and Their Evaluation as Prostate Cytotoxic Agents with Cathepsin B Inhibition
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摘要:
6-aminouracil 1 was utilized to introduce different heterocyclic rings at C-6 position through various synthetic strategies. The synthesized compounds bear rings that are either directly attached to the uracil back bone as in compounds 6, 12a-c and 15, or attached through an amino bridge as compounds 3a-c, 5a, b, 7a, b, 9 and 10, or through an imino bridge as compound 18. Also, compounds 4, 8, 11a-c, 14, 16 and 17 bearing biologically active side chains were synthesized. In addition to, compounds 13, 19, 20, 21 and 22 bear fused rings to the uracil backbone. All synthesized compounds were evaluated for their anticancer activity against prostate PC3 cell line using in-vitro sulforhodamine-B (SRB) method, from which compounds 3a, c, 4, 5a, b, 6, 7a, b, 11a-c, 12a, b, 17 and 20 were the most active. These active compounds were further evaluated for their ability to inhibit cathepsin B enzyme by using enzyme-linked immunosorbent assay, which revealed that compounds 5a, b, 7a, 11a, 12a and 17 exhibited more than 50% inhibition of cathepsin B. Among which the phenyl thiourea derivative 17 was the most active exhibiting 82.3% inhibition, while the reference doxorubicin exerted 18.7% inhibition.
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| 篇名 | Efficient Utilization of 6-Aminouracil to Synthesize Fused and Related Heterocyclic Compounds and Their Evaluation as Prostate Cytotoxic Agents with Cathepsin B Inhibition | ||
| 来源期刊 | 药物化学期刊(英文) | 学科 | 医学 |
| 关键词 | URACIL Cytotoxicity PC3 Cell Line CATHEPSIN B | ||
| 年,卷(期) | ywhxqkyw,(2) | 所属期刊栏目 | |
| 研究方向 | 页码范围 | 39-60 | |
| 页数 | 22页 | 分类号 | R73 |
| 字数 | 语种 | ||
| DOI | |||
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URACIL
Cytotoxicity
PC3
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CATHEPSIN
B
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药物化学期刊(英文)
主办单位:
美国科研出版社
出版周期:
季刊
ISSN:
2164-3121
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出版地:
武汉市江夏区汤逊湖北路38号光谷总部空间
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