(4-hydroxy-3-methylphenyl)(2-methylphenyl)methanone | 147029-76-3
中文名称
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中文别名
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英文名称
(4-hydroxy-3-methylphenyl)(2-methylphenyl)methanone
英文别名
4-Hydroxy-2',3-dimethylbenzophenone;(4-hydroxy-3-methylphenyl)-(2-methylphenyl)methanone
CAS
147029-76-3
化学式
C15H14O2
mdl
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分子量
226.275
InChiKey
KRZZANHKOVCHLF-UHFFFAOYSA-N
BEILSTEIN
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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
物化性质
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熔点:142°C
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沸点:375.7±37.0 °C(Predicted)
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密度:1.139±0.06 g/cm3(Predicted)
计算性质
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辛醇/水分配系数(LogP):3.6
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重原子数:17
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可旋转键数:2
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环数:2.0
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sp3杂化的碳原子比例:0.13
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拓扑面积:37.3
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氢给体数:1
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氢受体数:2
上下游信息
反应信息
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作为反应物:参考文献:名称:Glycosylated derivatives of benzophenone, benzhydrol and benzhydril as potential venous antithrombotic agents摘要:A series of glycosylated derivatives of benzophenone, benzhydrol, and benzhydril has been synthesized and evaluated for potential activity as venous antithrombotic agents. Studies on structure-activity relationships revealed that compounds having an electron-withdrawing group in the benzhydril or benzhydrol moiety, and specifically those having the beta-D-xylopyranosyl structure in the sugar moiety, were good antithrombotic agents in a rat model of venous thrombosis.DOI:10.1021/jm00059a015
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作为产物:描述:2-methyl-benzoic acid o-tolyl ester 在 aluminum (III) chloride 作用下, 以 neat (no solvent) 为溶剂, 以80%的产率得到(4-hydroxy-3-methylphenyl)(2-methylphenyl)methanone参考文献:名称:设计和合成二酰胺偶联的二苯甲酮作为潜在的抗癌药。摘要:一系列二酰胺偶联的二苯甲酮2-(4-苯甲酰基-苯氧基)-N- {2- [2-(2-(4-苯甲酰基-苯氧基)-乙酰氨基]-苯基}-乙酰胺类似物(9a-1)的合成多步反应和所有化合物都得到了很好的表征。在系列(9a-1)中,通过对多种癌细胞类型进行筛选,选择了在环A,B和D的邻位具有三个甲基,在环E的对位具有溴基的化合物9k作为先导化合物。体外细胞毒性和抗增殖测定系统。而且,化合物9k的细胞毒性性质导致体内肿瘤生长的退化,这可能是由于小鼠腹膜衬里血管生成减少导致肿瘤生长退化的缘故。DOI:10.1016/j.ejmech.2016.03.040
文献信息
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Synthesis, molecular docking, and apoptogenic efficacy of novel N-heterocycle analogs to target B-cell lymphoma 2/X-linked inhibitors of apoptosis proteins to regress melanoma作者:Zabiulla Zabiulla、Vikas H. Malojirao、Yasser Hussein Eissa Mohammed、Prabhu Thirusangu、B. T. Prabhakar、Shaukath Ara KhanumDOI:10.1007/s00044-019-02357-x日期:2019.8compounds were confirmed by IR, 1H, 13C, NMR, and mass spectra and also by elemental analyses. The newly synthesized molecules were screened for selectivity against cancers of different origin through cell based assay system using B16F10, A375, A549, HepG2, ACHN, and MCF7 cells. The results postulated that compound 11f with two bromo groups at the para position in rings A and E and two methyl groups at ortho通过多步过程合成了一系列具有酰胺键11a - 1的新型哌啶共轭二苯甲酮类似物。这些化合物的结构通过IR,1 H,13 C,NMR和质谱以及元素分析确认。通过基于细胞的测定系统,使用B16F10,A375,A549,HepG2,ACHN和MCF7细胞筛选新合成的分子对不同来源的癌症的选择性。结果假定化合物11f在环A和E的对位上有两个溴基,在环B和D的邻位上有两个甲基,具有针对黑素瘤的靶向特异性作用,突出了取代基的重要性。线下研究进一步推断化合物11f引发导致细胞死亡的凋亡性细胞事件。最终机制的研究表明,化合物11f成为B细胞淋巴瘤2的双重抑制剂和X连锁的凋亡抑制剂,导致Bax和Bad的上调。此外,在小鼠黑素瘤中具有相似的机制模拟了抗增殖作用。分子对接实验进一步证实了化合物11f通过强大的氢键具有对B细胞淋巴瘤2和X连锁凋亡抑制剂的超强亲和力。该研究暗示通过诱导凋亡作用鉴定具有针对黑素瘤的选
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Design, Synthesis, and Anticancer Properties of Novel Benzophenone-Conjugated Coumarin Analogs作者:V. Lakshmi Ranganatha、Farhan Zameer、S. Meghashri、N. D. Rekha、V. Girish、H. D. Gurupadaswamy、Shaukath Ara KhanumDOI:10.1002/ardp.201300298日期:2013.12of anticancer drugs with specific targets is of prime importance in modern chemical biology. Observing the importance of benzophenone and coumarin nucleus, it would be worthwhile to design and synthesize novel benzophenone derivatives (8a–o) bearing the coumarin nucleus. Further, they were screened for prospective anticancer activities in vitro against the Michigan Cancer Foundation‐7 (MCF‐7) and Ehrlich's在当前情况下,开发具有特定靶点的抗癌药物在现代化学生物学中至关重要。观察到二苯甲酮和香豆素核的重要性,设计和合成带有香豆素核的新型二苯甲酮衍生物 (8a-o) 是值得的。此外,还筛选了它们在体外针对密歇根癌症基金会-7 (MCF-7) 和埃利希腹水瘤 (EAT) 细胞系及其生物标志物的前瞻性抗癌活性,然后进行了有关磷酸肌醇 3-激酶 (PI3K) 和caspase 通过分子对接。据报道,二苯甲酮是靶向肿瘤血管生成的潜在药物。因此,在存在化合物 8a-o 的情况下,观察到血管生成依赖的 CAM 等体内模型系统中新血管的形成。
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Synthesis of some newer analogues of substituted dibenzoyl phenol as potent anti-inflammatory agents作者:Shaukath Ara. Khanum、Venu T. D、Sheena Shashikanth、Aiysha FirdouseDOI:10.1016/j.bmcl.2004.08.014日期:2004.113a-f, which on Fries rearrangement using microwave irradiation led to a facile synthesis of solely dibenzoyl phenols 4a-f in excellent yield. The newly synthesized compounds were screened for their anti-inflammatory activity and were compared with standard drugs. Out of the compounds studied, the compound 4e showed more potent activity than the standard drugs at all doses tested.羟基二苯甲酮1a-f的苯甲酰化作用提供了取代的苯甲酰基苯基苯甲酸酯3a-f,使用微波辐射进行弗里斯重排后,可以轻松地以优异的产率轻松合成仅二苯甲酰基苯酚4a-f。筛选新合成的化合物的抗炎活性,并与标准药物进行比较。在所研究的化合物中,化合物4e在所有测试剂量下均显示出比标准药物更强的活性。
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Synthesis, analgesic, anti-inflammatory, ulcerogenic evaluation, and docking study of (benzoylphenoxy)-N-{5-[2-methylphenyl-6-chlorobenzoxazole]} acetamides as COX/5-LOX inhibitor作者:M.J. Nagesh Khadri、Hussien Ahmed Khamees、Salma Kouser、Zabiulla、Shaukath Ara KhanumDOI:10.1016/j.molstruc.2022.134240日期:2023.15-LOX inhibitors with analgesic and anti-inflammatory effectiveness and very less gastrointestinal toxicity have been recognized as constructive and sustainable agents for inflammatory treatment. In this approach, a series of titled compounds (10a-j) were developed, synthesized, and evaluated in terms of in-vitro COX and LOX enzyme inhibition followed by analgesic, anti-inflammatory, and the ulcerogenicCOX 和 5-LOX 抑制剂具有镇痛和抗炎效果以及极低的胃肠道毒性,已被公认为炎症治疗的建设性和可持续药物。在这种方法中,开发、合成了一系列标题化合物 ( 10a-j ),并在体外COX 和 LOX 酶抑制以及镇痛、抗炎和致溃疡活性方面进行了评估。对表现出潜在镇痛活性的化合物10a-c、10e和10g-10i进行了抗炎评估,随后验证了强效抗炎化合物的致溃疡作用。化合物10b苯环上的甲基邻位取代和氯基对位取代,苯并恶唑上的二苯甲酮苯甲酰基环上氯基的间位取代,观察到具有良好的抑制效力。此外,使用 Autodock 工具对接软件进行计算机研究。
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Synthesis and evaluation of novel benzophenone-thiazole derivatives as potent VEGF-A inhibitors作者:T. Prashanth、Prabhu Thirusangu、B.R. Vijay Avin、V. Lakshmi Ranganatha、B.T. Prabhakar、Shaukath Ara KhanumDOI:10.1016/j.ejmech.2014.09.069日期:2014.11A series of 2-(4-benzoyl-phenoxy)-N-(4-phenyl-thiazol-2-yl)-acetamides (10a-n) were synthesized by multistep reaction sequence and all the compounds were well characterized for structural elucidation. The in vitro cytotoxicity of compounds 10a-n was evaluated against EAC and DLA cell lines using trypan blue dye exclusion method. Further MTT assay and LDH release assay, followed by in vivo studies on murine model were also evaluated. The compound 10h with a methyl and fluor groups at benzophenone moiety and methoxy group at phenyl ring was in a leading position to exhibit the promising antiproliferative effect through translational VEGF-A inhibition. (C) 2014 Elsevier Masson SAS. All rights reserved.
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