N-(4-methoxyphenyl)imidodicarbonimidic diamide hydrochloride | 4838-56-6
中文名称
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中文别名
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英文名称
N-(4-methoxyphenyl)imidodicarbonimidic diamide hydrochloride
英文别名
1-(4-methoxy-phenyl)-biguanide; hydrochloride;1-(4-Methoxy-phenyl)-biguanid; Hydrochlorid;1-(p-Methoxyphenyl)biguanide hydrochloride;diaminomethylidene-[N'-(4-methoxyphenyl)carbamimidoyl]azanium;chloride
CAS
4838-56-6
化学式
C9H13N5O*ClH
mdl
MFCD01740304
分子量
243.696
InChiKey
GSHFIBZGCAWOEW-UHFFFAOYSA-N
BEILSTEIN
——
EINECS
——
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物化性质
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计算性质
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ADMET
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安全信息
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SDS
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制备方法与用途
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上下游信息
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文献信息
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表征谱图
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同类化合物
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相关功能分类
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相关结构分类
计算性质
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辛醇/水分配系数(LogP):0.57
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重原子数:16
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可旋转键数:3
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环数:1.0
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sp3杂化的碳原子比例:0.111
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拓扑面积:112
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氢给体数:4
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氢受体数:2
SDS
反应信息
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作为反应物:参考文献:名称:Synthesis and antiviral activity of benzimidazolyl- and triazolyl-1,3,5-triazines摘要:A novel series of 1,3,5-triazine analogs was successfully synthesized through conjugation with benzimidazole or 1,2,4-triazole derivatives via a methylenethio linker. The new analogs were in vitro evaluated against HSV-1 in Vero cells; among these analogs, two compounds exhibited good effect in inhibiting HSV-1 replication (for compound 5p: EC50 = 3.5 mu g/ml, SI = 358; for compound 5r: EC50 = 5.0 mu g/ml, SI = 300) in comparison to acyclovir.DOI:10.1007/s00044-011-9574-8
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作为产物:参考文献:名称:使用多药理学浏览器PPB2从表型筛选中鉴定溶血磷脂酸酰基转移酶β(LPAAT-β)为纳摩尔血管生成抑制剂的靶标。摘要:通过在表型共培养测定中筛选激酶抑制剂类似物的聚焦库以抑制血管生成,我们确定了一种氨基三嗪,它可作为一种抑制细胞生长的纳摩尔抑制剂。但是,发现该氨基三嗪在全基因组谱分析中完全没有活性。为了解释其作用机理,我们使用了在线靶标预测工具PPB2(http://ppb2.gdb.tools),该工具建议溶血磷脂酸酰基转移酶β(LPAAT-β)作为该氨基三嗪和其他类似物的可能靶标。通过结构-活动关系分析来识别。与已知的LPAAT-β抑制剂相比,在生化分析中证实了LPAAT-β抑制(IC50≈15 nm),并且抑制了它对细胞增殖的作用。DOI:10.1002/cmdc.201800554
文献信息
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Synthesis and in vitro anticancer evaluation of some 4,6-diamino-1,3,5-triazine-2-carbohydrazides as Rad6 ubiquitin conjugating enzyme inhibitors作者:Hend Kothayer、Sebastian M. Spencer、Kaushlendra Tripathi、Andrew D. Westwell、Komaraiah PalleDOI:10.1016/j.bmcl.2016.02.085日期:2016.4abbreviate our compound names as 'new triazines', have been synthesized, based on the previously reported Rad6B-inhibitory diamino-triazinylmethyl benzoate anticancer agents TZ9 and 4-amino-N'-phenyl-6-(arylamino)-1,3,5-triazine-2-carbohydrazides. Synthesis of the target compounds was readily accomplished in two steps from either bis-aryl/aryl biguanides via reaction of phenylhydrazine or hydrazinehydrate4-氨基-6-(芳基氨基)-1,3,5-三嗪-2-碳酰肼(3a-e)和N'-苯基-4,6-双(芳基氨基)-1,3,5-三嗪系列为方便读者阅读,我们合成了-2-碳酰肼(6a-e),根据先前报道的Rad6B抑制性二氨基三嗪基甲基苯甲酸酯苯甲酸酯类抗癌剂TZ9和4-氨基合成了我们的化合物名称“新三嗪”。 -N′-苯基-6-(芳基氨基)-1,3,5-三嗪-2-碳酰肼。通过苯肼或肼与关键的4-氨基-6-双(芳基氨基)/(芳基氨基)-1,3,5-三嗪- 2-羧酸盐中间体。评估了这些新的三嗪衍生物抑制Rad6B泛素结合的能力以及针对几种人类癌细胞系的体外抗癌活性:卵巢癌(OV90和A2780),肺部(H1299和A549),乳腺(MCF-7和MDA-MB231) MTS分析检测结肠癌和结肠癌(HT29)细胞。与先前报道的选择性Rad6抑制剂TZ9相比,所有10种新的三嗪均表现出优异的Rad6B抑制活性。
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Discovery of Small-Molecule Cyclic GMP-AMP Synthase Inhibitors作者:Rosaura Padilla-Salinas、Lijun Sun、Rachel Anderson、Xikang Yang、Shuting Zhang、Zhijian J. Chen、Hang YinDOI:10.1021/acs.joc.9b02666日期:2020.2.7exists for inhibiting cGAS in cells, while others are limited by their poor cellular activity or specificity, which underscores the urgency for discovering new cGAS inhibitors. Here, we describe the development of new small-molecule human cGAS (hcGAS) inhibitors (80 compounds synthesized) with high binding affinity in vitro and cellular activity. Our studies show CU-32 and CU-76 selectively inhibit the DNA
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[EN] HETEROARYL COMPOUNDS AND THEIR USE<br/>[FR] COMPOSÉS HÉTÉROARYLE ET LEUR UTILISATION申请人:MINORYX THERAPEUTICS S L公开号:WO2018122775A1公开(公告)日:2018-07-05The application is directed to compounds of formula (I): and their salts and solvates, wherein R1, R2, R3, A1, A2, A3, and n are as set forth in the specification, as well as to a method for their preparation, pharmaceutical compositions comprising the same, and use thereof for the treatment and/or prevention of a lysosomal storage disease, such as Gaucher's, and other diseases or disorders that are synucleinopathies.该申请涉及式(I)的化合物及其盐和溶剂合物,其中R1、R2、R3、A1、A2、A3和n如规范中所述,以及它们的制备方法,包含它们的药物组合物,以及用于治疗和/或预防溶酶体贮积病(如高雪氏病)和其他α-突触核蛋白病的用途。
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New 2-[(4-Amino-6-N-substituted-1,3,5-triazin-2-yl)methylthio]-N-(imidazolidin-2-ylidene)-4-chloro-5-methylbenzenesulfonamide Derivatives, Design, Synthesis and Anticancer Evaluation作者:Łukasz Tomorowicz、Beata Żołnowska、Krzysztof Szafrański、Jarosław Chojnacki、Ryszard Konopiński、Ewa A. Grzybowska、Jarosław Sławiński、Anna KawiakDOI:10.3390/ijms23137178日期:——In the search for new compounds with antitumor activity, new potential anticancer agents were designed as molecular hybrids containing the structures of a triazine ring and a sulfonamide fragment. Applying the synthesis in solution, a base of new sulfonamide derivatives 20–162 was obtained by the reaction of the corresponding esters 11–19 with appropriate biguanide hydrochlorides. The structures of在寻找具有抗肿瘤活性的新化合物时,设计了新的潜在抗癌剂,它们是包含三嗪环和磺酰胺片段结构的分子杂化物。通过在溶液中进行合成,通过将相应的酯11-19与适当的双胍盐酸盐反应,得到了一系列新的磺酰胺衍生物20-162。这些化合物的结构通过光谱学(红外线,核磁共振),质谱(高分辨质谱或MALDI-TOF / TOF),元素分析(C,H,N)和X射线晶体学得到了证实。检查了所得化合物对三种肿瘤细胞系HCT-116,MCF-7和HeLa的细胞毒性活性。结果表明,一些最活跃的化合物属于R1 = 4-三氟甲基苄基和R1 = 3,5-双(三氟甲基)苄基系列,并且展示了IC50值在3.6 µM到11.0 µM之间。描述了SAR关系,表明R2 = 4-苯基哌嗪-1-基取代基对于针对HCT-116和MCF-7细胞系的细胞毒性活性起关键作用。关于活性化合物作用机理的研究包括评估MDM2-p53相互作用的抑制,细胞周期分析和细胞凋亡诱导检查。结果表明,所研究的化合物不会抑制MDM2-p53相互作用,但以p53独立的方式诱导G0 / G1和G2 / M细胞周期阻滞。此外,活性化合物在携带野生型和突变型p53的细胞中诱导凋亡。化合物设计是逐步进行的,并通过QSAR模型辅助,将化合物对HCT-116细胞系的活性与分子描述符相关联。
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A Series of Biguanide Ligands and Their Cu(II) Complexes: Cholinesterase Inhibitory and Antimicrobial Properties作者:Julide Nacaroglu Ballı、Ozge Gungor、Muhammet KoseDOI:10.1002/cbdv.202301434日期:2024.2donepezil and galantamine. On the other hand, complexation of the biguanide compounds with Cu(II) resulted in dramatic increase in the inhibitory activity. The Cu(II) complexes showed AChE inhibitory activity with the IC50 values of 21.29±0.95–82.53±0.20 μM and those values are comparable to that of donepezil (IC50: 18.54±1.03 μM). The synthesised compounds were also screened for their antimicrobial activity在这项工作中,合成了一系列双胍盐酸盐及其 Cu(II) 配合物,并筛选了它们的乙酰/丁酰胆碱酯酶抑制和抗菌特性。通过常见的光谱和分析方法对合成的化合物的结构进行了表征。与参考药物多奈哌齐和加兰他敏相比,双胍化合物显示出明显较低的抑制活性。另一方面,双胍化合物与 Cu(II) 的络合导致抑制活性显着增加。 Cu(II) 配合物显示出 AChE 抑制活性,IC 50值为 21.29±0.95–82.53±0.20 μM,这些值与多奈哌齐相当(IC 50 :18.54±1.03 μM)。还筛选了合成化合物对革兰氏阳性(+)和革兰氏阴性(-)细菌的抗菌活性。化合物 (12.50 mg/mL) 显示出重要的抗菌特性,对革兰氏阳性和革兰氏阴性微生物的抑制区直径为 8-28 毫米。化合物 A03 和 A08 对大肠杆菌表现出比标准抗生素阿米卡星和庆大霉素更强的抗菌特性。
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