4-(4-phenylbutanamido)benzoic acid | 83700-60-1

• 分子结构分类: 有机化合物 - 苯类化合物 - 苯和取代衍生物
• 英文名称: 4-(4-phenylbutanamido)benzoic acid
• 英文别名: 4-[(4-Phenylbutanoyl)amino]benzoic acid；4-(4-phenylbutanoylamino)benzoic acid
• CAS: 83700-60-1
• 化学式: C₁₇H₁₇NO₃
• 分子量: 283.327
• InChiKey: GUKZHIRIDPOHFA-UHFFFAOYSA-N

物化性质

• 沸点：
  541.2±43.0 °C(Predicted)
• 密度：
  1.238±0.06 g/cm3(Predicted)

计算性质

• 辛醇/水分配系数(LogP)：
  2.9
• 重原子数：
  21
• 可旋转键数：
  6
• 环数：
  2.0
• sp3杂化的碳原子比例：
  0.18
• 拓扑面积：
  66.4
• 氢给体数：
  2
• 氢受体数：
  3

反应信息

• 作为反应物：
  描述：

  4-(4-phenylbutanamido)benzoic acid 在 palladium on activated charcoal TEA 、 氢气 、 双(2-氧代-3-恶唑烷基)次磷酰氯 作用下， 以 四氢呋喃 、 甲醇 为溶剂， 反应 2.0h， 生成 HTPB
  参考文献：
  名称：

  Zn²⁺-Chelating Motif-Tethered Short-Chain Fatty Acids as a Novel Class of Histone Deacetylase Inhibitors

  摘要：

  Among various classes of histone deacetylase (HDAC) inhibitors, short-chain fatty acids exhibit the least potency, with IC50 in the millimolar range. We rationalized that this weak potency was, in part, attributable to their inability to access the zinc cation in the HDAC active-site pocket, which is pivotal to the deacetylation catalysis. We thus explored the structural optimization of valproate, butyrate, phenylacetate, and phenylbutyrate by coupling them with Zn2+-chelating motifs (hydroxamic acid and o-phenylenediamine) through aromatic W-amino acid linkers. This strategy has led to a novel class of Zn2+ -chelating, motif-tethered, short-chain fatty acids that exhibited varying degrees of HDAC inhibitory potency. One hydroxamate-tethered phenylbutyrate compound, N-hydroxy-4-(4-phenylbutyrylamino)benzamide (HTPB), displayed nanomolar potency in inhibiting HDAC activity. Exposure of several cancer cell lines to HTPB at the submicromolar level showed reduced cell proliferation accompanied by histone hyperacetylation and elevated p21(WAF/CIPI) expression, which are hallmark features associated with intracellular HDAC inhibition.

  DOI：

  10.1021/jm0303655
• 作为产物：
  描述：

  Methyl 4-(4-phenylbutanoylamino)benzoate 在 氢氧化钾 作用下， 以 甲醇 为溶剂， 反应 1.0h， 生成 4-(4-phenylbutanamido)benzoic acid
  参考文献：
  名称：

  Zn²⁺-Chelating Motif-Tethered Short-Chain Fatty Acids as a Novel Class of Histone Deacetylase Inhibitors

  摘要：

  Among various classes of histone deacetylase (HDAC) inhibitors, short-chain fatty acids exhibit the least potency, with IC50 in the millimolar range. We rationalized that this weak potency was, in part, attributable to their inability to access the zinc cation in the HDAC active-site pocket, which is pivotal to the deacetylation catalysis. We thus explored the structural optimization of valproate, butyrate, phenylacetate, and phenylbutyrate by coupling them with Zn2+-chelating motifs (hydroxamic acid and o-phenylenediamine) through aromatic W-amino acid linkers. This strategy has led to a novel class of Zn2+ -chelating, motif-tethered, short-chain fatty acids that exhibited varying degrees of HDAC inhibitory potency. One hydroxamate-tethered phenylbutyrate compound, N-hydroxy-4-(4-phenylbutyrylamino)benzamide (HTPB), displayed nanomolar potency in inhibiting HDAC activity. Exposure of several cancer cell lines to HTPB at the submicromolar level showed reduced cell proliferation accompanied by histone hyperacetylation and elevated p21(WAF/CIPI) expression, which are hallmark features associated with intracellular HDAC inhibition.

  DOI：

  10.1021/jm0303655

文献信息

• Tungsten-Catalyzed Transamidation of Tertiary Alkyl Amides
  作者：Fang-Fang Feng、Xuan-Yu Liu、Chi Wai Cheung、Jun-An Ma

  DOI：10.1021/acscatal.1c01840

  日期：2021.6.18

  chloride as a catalyst and chlorotrimethylsilane as an additive. The highly electrophilic and oxophilic tungsten catalyst enables the selective scission of a C–N bond of tertiary alkyl amides to effect transamidation of a myriad of structurally and electronically diverse tertiary alkyl amides and amines. Mechanistic study implies that the synergistic effect of the catalyst and the additive could pronouncedly

  转酰胺最近已成为使酰胺多样化的一种简单方便的方法。然而，臭名昭著的、完全烷基取代的叔酰胺的动力学和热力学要求的转酰胺化仍然是一个长期的挑战。在这里，我们描述了一种使用简单的氯化钨 (VI) 作为催化剂和三甲基氯硅烷作为添加剂来活化叔烷基酰胺以简化转酰胺化的方法。高度亲电和亲氧的钨催化剂能够选择性地切断叔烷基酰胺的 C-N 键，从而实现无数结构和电子不同的叔烷基酰胺和胺的转酰胺化。
• Small molecule inhibitors of STAT3 with anti-tumor activity
  申请人：Turkson James

  公开号：US20090069420A1

  公开（公告）日：2009-03-12

  The present invention concerns compounds, compositions containing these compounds, and methods of using these compounds and compositions as inhibitors of Stat3 signaling, Stat3 dimerization, Stat3-DNA binding, Stat5-DNA binding, and/or aberrant cell growth in vitro or in vivo, e.g., as anti-cancer agents for treatment of cancer, such as breast cancer. The compounds of the invention include, but are not limited to, NSC 74859 (S3I-201), NSC 42067, NSC 59263, NSC 75912, NSC 11421, NSC 91529, NSC 263435, and pharmaceutically acceptable salts and analogs of the foregoing. Other non-malignant diseases characterized by proliferation of cells that may be treated using the compounds of the invention, but are not limited to, cirrhosis of the liver; graft rejection; restenosis; and disorders characterized by a proliferation of T cells such as autoimmune diseases, e.g., type 1 diabetes, lupus and multiple sclerosis. The invention further includes an in-vitro screening test for the presence of malignant cells in a mammalian tissue; a method of identifying inhibitors of constitutive Stat3 activation, Stat3-DNA binding, Stat5-DNA binding, and/or Stat3 dimerization; and a method of identifying anti-cancer agents.

  本发明涉及化合物、含有这些化合物的组合物以及使用这些化合物和组合物作为Stat3信号传导、Stat3二聚化、Stat3-DNA结合、Stat5-DNA结合和/或体内或体外异常细胞生长的抑制剂的方法，例如用作治疗癌症（如乳腺癌）的抗癌剂。本发明的化合物包括但不限于NSC 74859（S3I-201）、NSC 42067、NSC 59263、NSC 75912、NSC 11421、NSC 91529、NSC 263435以及上述的药物可接受的盐和类似物。其他非恶性疾病，其特征为细胞增殖，可以使用本发明的化合物进行治疗，但不限于肝硬化、移植排斥、再狭窄以及以T细胞增殖为特征的疾病，例如自身免疫疾病，如1型糖尿病、狼疮和多发性硬化症。本发明还包括一种用于检测哺乳动物组织中恶性细胞存在的体外筛选测试；一种识别组成Stat3激活、Stat3-DNA结合、Stat5-DNA结合和/或Stat3二聚化抑制剂的方法；以及一种识别抗癌剂的方法。
• Small molecule inhibitors of stat3 with anti-tumor activity
  申请人：Turkson James

  公开号：US20110201576A1

  公开（公告）日：2011-08-18

  The present invention concerns compounds, compositions containing these compounds, and methods of using these compounds and compositions as inhibitors of Stat3 signaling, Stat3 dimerization, Stat3-DNA binding, Stat5-DNA binding, and/or aberrant cell growth in vitro or in vivo, e.g., as anti-cancer agents for treatment of cancer, such as breast cancer. The compounds of the invention include, but are not limited to, NSC 74859 (S3I-201), NSC 42067, NSC 59263, NSC 75912, NSC 11421, NSC 91529, NSC 263435, and pharmaceutically acceptable salts and analogs of the foregoing. Other non-malignant diseases characterized by proliferation of cells that may be treated using the compounds of the invention, but are not limited to, cirrhosis of the liver; graft rejection; restenosis; and disorders characterized by a proliferation of T cells such as autoimmune diseases, e.g., type 1 diabetes, lupus and multiple sclerosis. The invention further includes an in-vitro screening test for the presence of malignant cells in a mammalian tissue; a method of identifying inhibitors of constitutive Stat3 activation, Stat3-DNA binding, Stat5-DNA binding, and/or Stat3 dimerization; and a method of identifying anti-cancer agents.

  本发明涉及化合物、含有这些化合物的组合物以及使用这些化合物和组合物作为Stat3信号、Stat3二聚化、Stat3-DNA结合、Stat5-DNA结合和/或体内或体外异常细胞增长的抑制剂的方法，例如作为治疗癌症（如乳腺癌）的抗癌剂。本发明的化合物包括但不限于NSC 74859（S3I-201）、NSC 42067、NSC 59263、NSC 75912、NSC 11421、NSC 91529、NSC 263435及其药学上可接受的盐和类似物。本发明还包括使用该化合物治疗其他非恶性疾病，这些疾病以细胞增生为特征，但不限于肝硬化、移植排斥、再狭窄和以T细胞增殖为特征的疾病，例如自身免疫性疾病，如1型糖尿病、红斑狼疮和多发性硬化症。本发明还包括一种体外筛选恶性细胞的方法；一种识别组成性Stat3激活、Stat3-DNA结合、Stat5-DNA结合和/或Stat3二聚化抑制剂的方法；以及一种识别抗癌剂的方法。
• SMALL MOLECULE INHIBITORS OF STAT3 WITH ANTI-TUMOR ACTIVITY
  申请人：H. Lee Moffitt Cancer Center And Research Institute, Inc.

  公开号：US20140329900A1

  公开（公告）日：2014-11-06

  The present invention concerns compounds, compositions containing these compounds, and methods of using these compounds and compositions as inhibitors of Stat3 signaling, Stat3 dimerization, Stat3-DNA binding, Stat5-DNA binding, and/or aberrant cell growth in vitro or in vivo, e.g., as anti-cancer agents for treatment of cancer, such as breast cancer. The compounds of the invention include, but are not limited to, NSC 74859 (S31-201), NSC 42067, NSC 59263, NSC 75912, NSC 11421, NSC 91529, NSC 263435, and pharmaceutically acceptable salts and analogs of the foregoing. Other non-malignant diseases characterized by proliferation of cells that may be treated using the compounds of the invention, but are not limited to, cirrhosis of the liver; graft rejection; restenosis; and disorders characterized by a proliferation of T cells such as autoimmune diseases, e.g., type 1 diabetes, lupus and multiple sclerosis. The invention further includes an in-vitro screening test for the presence of malignant cells in a mammalian tissue; a method of identifying inhibitors of constitutive Stat3 activation, Stat3-DNA binding, Stat5-DNA binding, and/or Stat3 dimerization; and a method of identifying anti-cancer agents.

  本发明涉及化合物、含有这些化合物的组合物以及使用这些化合物和组合物作为Stat3信号通路、Stat3二聚化、Stat3-DNA结合、Stat5-DNA结合和/或体外或体内异常细胞生长的抑制剂的方法，例如作为治疗癌症，如乳腺癌的抗癌剂。本发明的化合物包括但不限于NSC 74859（S31-201）、NSC 42067、NSC 59263、NSC 75912、NSC 11421、NSC 91529、NSC 263435以及其药学上可接受的盐和类似物。其他非恶性疾病，其特征为细胞增殖，可以使用本发明的化合物进行治疗，但不限于肝硬化、移植排斥反应、再狭窄以及T细胞增殖的疾病，例如自身免疫性疾病，如1型糖尿病、狼疮和多发性硬化等。本发明还包括一种用于检测哺乳动物组织中恶性细胞存在的体外筛选测试；一种识别组成性Stat3激活、Stat3-DNA结合、Stat5-DNA结合和/或Stat3二聚化抑制剂的方法；以及一种识别抗癌剂的方法。
• 4-[4-[(2-Hydroxybenzoyl)amino]phenyl]butyric Acid as a Novel Oral Delivery Agent for Recombinant Human Growth Hormone
  作者：Andrea Leone-Bay、Koc-Kan Ho、Rajesh Agarwal、Robert A. Baughman、Kiran Chaudhary、Frenel DeMorin、Lise Genoble、Campbell McInnes、Christine Lercara、Sam Milstein、Doris O'Toole、Donald Sarubbi、Bruce Variano、Duncan R. Paton

  DOI：10.1021/jm960038f

  日期：1996.1.1

  A series of N-acetylated, non-alpha, aromatic amino acids was prepared and shown to promote the absorption of recombinant human growth hormone (rhGH) from the gastrointestinal tract. Seventy compounds in this family were tested in vivo in rats. Of the compounds tested, 4-[4-[(2-hydroxybenzoyl)amino]phenyl]butyric acid was identified as a preclinical candidate and was used to demonstrate the oral delivery of rhGH in primates. A significant positive correlation was found between the relative log k' of the delivery agents, as determined by HPLC on an immobilized artificial membrane (IAM) column, and serum rhGH concentrations following oral or colonic dosing in rats. Structure-activity relationships have also been developed on the basis of electronic effects and hydrogen-bonding characteristics of the aromatic amide substituents.