Biologically active sulfur-containing polyamides as promising anticancer materials.

IF 1.8 4区 化学 Q3 POLYMER SCIENCE Designed Monomers and Polymers Pub Date : 2023-01-01 DOI:10.1080/15685551.2023.2205734
Gadeer R Ashour, Sara A Alqarni, Youssef O Al-Ghamdi, W Abd El-Fattah, Abeer M Alosaimi, Mahmoud A Hussein
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Abstract

Thiazol-based molecules have practically infinite biological implementation. Today, there are many medical applications for compounds containing the thiazole moiety owing to their presence in most clinically applied anticancer drugs, such as dasatinib, dabrafenib, ixabepilone, patellamide A and epothilone. In this study, the polycondensation, of a new group of thiazole-containing polyamides with the formulas PA1-4 was carried out by the interaction of 2-aminothiazole diphenyl sulfide and variable diacid chlorides in dimethyl formamide in the presence of potassium carbonate anhydrous as a catalyst. Fourier transform-infrared spectroscopy (FTIR) was initially used to figure out the PA1-4 structures, which were further characterized using solubility, gel permeation chromatography (GPC), X-ray diffraction analyses (XRD) and scanning electron microscopy (SEM). The solubility results revealed that the presence of heteroaromatic thiazole ring units and sulfur content in the polyamides main chain, made the solubility easier as it increases the chain packing distance. From the values of average molecular weight, it was clear that all synthesized polyamides have almost the same chain length which ranged from 37,561.80 to 39,827.66. Moreover, the thermogravimetric analysis (TGA) confirm that PA1-4 were thermally stable even at high temperatures especially the polyamides which were synthesized from aromatic diacid chlorides. Furthermore, the newly synthesized polyamides were investigated for their antimicrobial properties against different species of Gram-positive and Gram-negative bacteria and also against different fungi. The results revealed that compound PA2 showed the highest antibacterial activity. Also, their inhibitory activity against breast carcinoma cells (MCF-7 cell line) and colon carcinoma cells (HCT cell line) was evaluated. It was clear that there was an enhancement in the anticancer activity for the synthesized polyamides owing to the presence of the thiazole moiety as well as sulfur linkage. According to the results of the 50% inhibitory concentration (IC50), the synthesized polymers were found to be more active against the MCF-7 cell line than the HCT cell line.

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具有生物活性的含硫聚酰胺是很有前景的抗癌材料。
以噻唑为基础的分子实际上具有无限的生物用途。今天,含有噻唑部分的化合物有许多医疗应用,因为它们存在于大多数临床应用的抗癌药物中,如达沙替尼、达非尼、伊沙匹龙、帕特拉胺A和埃泊替龙。在无水碳酸钾的催化下,2-氨基噻唑二苯硫醚与可变二酸氯化物在二甲基甲酰胺中相互作用,缩聚得到了一组新的含噻唑聚酰胺,分子式为PA1-4。采用傅里叶变换红外光谱(FTIR)初步确定了PA1-4的结构,并利用溶解度、凝胶渗透色谱(GPC)、x射线衍射分析(XRD)和扫描电镜(SEM)对PA1-4进行了进一步的表征。溶解度结果表明,杂芳噻唑环单元的存在和聚酰胺主链中硫含量的增加,使得聚酰胺的溶解度随着链填充距离的增加而增加。从平均分子量的值可以看出,所有合成的聚酰胺具有几乎相同的链长,在37,561.80 ~ 39,827.66之间。此外,热重分析(TGA)证实了PA1-4在高温下的热稳定性,特别是芳香族二酸氯化物合成的聚酰胺。此外,还研究了新合成的聚酰胺对不同种类的革兰氏阳性菌和革兰氏阴性菌以及不同真菌的抗菌性能。结果表明,化合物PA2抗菌活性最高。并对其对乳腺癌细胞(MCF-7细胞系)和结肠癌细胞(HCT细胞系)的抑制活性进行了评价。显然,由于噻唑基团和硫键的存在,合成的聚酰胺的抗癌活性有所增强。根据50%抑制浓度(IC50)的结果,发现合成的聚合物对MCF-7细胞株的活性比HCT细胞株更强。
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来源期刊
Designed Monomers and Polymers
Designed Monomers and Polymers 化学-高分子科学
CiteScore
3.30
自引率
0.00%
发文量
28
审稿时长
2.1 months
期刊介绍: Designed Monomers and Polymers ( DMP) publishes prompt peer-reviewed papers and short topical reviews on all areas of macromolecular design and applications. Emphasis is placed on the preparations of new monomers, including characterization and applications. Experiments should be presented in sufficient detail (including specific observations, precautionary notes, use of new materials, techniques, and their possible problems) that they could be reproduced by any researcher wishing to repeat the work. The journal also includes macromolecular design of polymeric materials (such as polymeric biomaterials, biomedical polymers, etc.) with medical applications. DMP provides an interface between organic and polymer chemistries and aims to bridge the gap between monomer synthesis and the design of new polymers. Submssions are invited in the areas including, but not limited to: -macromolecular science, initiators, macroinitiators for macromolecular design -kinetics, mechanism and modelling aspects of polymerization -new methods of synthesis of known monomers -new monomers (must show evidence for polymerization, e.g. polycondensation, sequential combination, oxidative coupling, radiation, plasma polymerization) -functional prepolymers of various architectures such as hyperbranched polymers, telechelic polymers, macromonomers, or dendrimers -new polymeric materials with biomedical applications
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