phenanthrene-2-carbonyl chloride | 16331-53-6
中文名称
——
中文别名
——
英文名称
phenanthrene-2-carbonyl chloride
英文别名
Phenanthren-2-carbonylchlorid;2-carboxyphenanthrene chloride;2-Phenanthroyl chloride
CAS
16331-53-6
化学式
C15H9ClO
mdl
——
分子量
240.689
InChiKey
YEKHRSMVHYXZQB-UHFFFAOYSA-N
BEILSTEIN
——
EINECS
——
-
物化性质
-
计算性质
-
ADMET
-
安全信息
-
SDS
-
制备方法与用途
-
上下游信息
-
文献信息
-
表征谱图
-
同类化合物
-
相关功能分类
-
相关结构分类
计算性质
-
辛醇/水分配系数(LogP):5.5
-
重原子数:17
-
可旋转键数:1
-
环数:3.0
-
sp3杂化的碳原子比例:0.0
-
拓扑面积:17.1
-
氢给体数:0
-
氢受体数:1
上下游信息
反应信息
-
作为反应物:描述:phenanthrene-2-carbonyl chloride 在 RhCl(PPh3)3 作用下, 生成 2-氯菲参考文献:名称:Decarbonylation of aromatic carbonyl compounds catalyzed by rhodium complexes摘要:DOI:10.1021/ja00986a017
-
作为产物:描述:参考文献:名称:N1-取代的哌嗪-2,3-二羧酸衍生物作为NMDA受体拮抗剂的合成与药理作用。摘要:竞争性NMDA受体拮抗剂的结合位点位于NR2亚基上,其中有四种类型(NR2A-D)。典型的拮抗剂,例如(R)-AP5,具有亚单位选择性为NR2A> NR2B> NR2C> NR2D。竞争性NMDA受体拮抗剂(2R,3S)-(1-联苯基-4-羰基)哌嗪-2,3-二羧酸(PBPD,16b)与NR2A和NR2B相比,对NR2C和NR2D的相对亲和力增强,显示出非同寻常的选择性。合成了16b的带有芳基或芳基取代基的哌啶-2,3-二羧酸的N(1)连接基团的类似物,以探讨NR2C / NR2D选择性的结构要求。菲-2-羰基类似物16e对NR2C和NR2D的亲和力高> 60倍,对NR2C / NR2D的选择性是NR2A / NR2B的3-5倍。菲-3-羰基类似物(16f)的效力较低,但选择性更高,分别对NR2D的选择性是NR2A和NR2B的5倍和7倍。因此,带有大量疏水残基的拮抗剂具有与典型拮抗剂不同的NR2亚基选择性。DOI:10.1021/jm0492498
文献信息
-
Linear Conjugated Systems Bearing Aromatic Terminal Groups. IV. The Syntheses of Some Diarylacetylenes作者:Shuzo Akiyama、Kazuhiro Nakasuji、Masazumi NakagawaDOI:10.1246/bcsj.44.2231日期:1971.8The syntheses of 1,1′-, 9,9′-, and 1,9′-dianthryl-, 2,2′-, 3,3′-, and 9,9′-diphenanthryl-, 1,1′-and 2,2′-dipyrenyl-, and 6,6′-dichrysenylacetylenes according to the pyrolytic reactions of the corresponding β-ketoalkylidenetriphenylphosphorane derivatives (intramolecular Wittig reaction) were described.1,1'-、9,9'-和1,9'-二蒽基-、2,2'-、3,3'-和9,9'-二菲基-、1,1'-的合成根据相应的 β-酮亚烷基三苯基正膦衍生物(分子内 Wittig 反应)的热解反应,描述了 2,2'-二芘基-和 6,6'-二炔基乙炔。
-
2-[(Arylmethyl)amino]-2-methyl-1,3-propanediol DNA intercalators. An examination of the effects of aromatic ring variation on antitumor activity and DNA binding作者:Kenneth W. Bair、C. Webster Andrews、Richard L. Tuttle、Vincent C. Knick、Michael Cory、David D. McKeeDOI:10.1021/jm00111a010日期:1991.7The effects of variation of aromatic ring size, shape, and side-chain position on antitumor activity and DNA binding in a series of carbocyclic 2-[(arylmethyl)amino]-2-methyl-1,3-propanediols (AMAPs) were examined. In general, the interaction of AMAPs with DNA increases as the intercalating ring system grows in area, with three distinct binding levels evident. Isomers from a specific ring system appear to bind DNA similarly. DNA binding is not the sole criterion for antitumor activity for the AMAPs studied; the magnitude of the DELTA-T(m) does not correlate with the antitumor activity observed. Significant in vivo P388 activity was seen for AMAP congeners from several tetracyclic ring systems. However, isomers from each of the specific ring systems produced a wide range of in vivo P388 activity. Thus, AMAP antitumor activity is not a function of the ring system per se, but rather appears to be related to the shape of the specific molecule. Three AMAP congeners (crisnatol (770U82, 773U82, and 502U83) are currently in clinical trials.
-
[EN] KETONES AND REDUCED KETONES AS THERAPEUTIC AGENTS FOR THE TREATMENT OF BONE CONDITIONS<br/>[FR] CETONES ET CETONES REDUITES EN TANT QU'AGENTS THERAPEUTIQUES DESTINES AU TRAITEMENT D'AFFECTIONS OSSEUSES申请人:UNIV ABERDEEN公开号:WO2004098582A3公开(公告)日:2005-04-21
-
Studies in the Phenanthrene Series. IV. Phenanthrene-2-, 3- and 9-Aldehydes<sup>1</sup>作者:Erich Mosettig、Jacob van de KampDOI:10.1021/ja01334a065日期:1933.7
-
Synthesis and Pharmacology of <i>N</i>-Substituted Piperazine-2,3-dicarboxylic Acid Derivatives Acting as NMDA Receptor Antagonists作者:Richard M. Morley、Heong-Wai Tse、Bihua Feng、Jacqueline C. Miller、Daniel T. Monaghan、David E. JaneDOI:10.1021/jm0492498日期:2005.4.1The binding site for competitive NMDA receptor antagonists is on the NR2 subunit, of which there are four types (NR2A-D). Typical antagonists such as (R)-AP5 have a subunit selectivity of NR2A > NR2B > NR2C > NR2D. The competitive NMDA receptor antagonist (2R,3S)-(1-biphenylyl-4-carbonyl)piperazine-2,3-dicarboxylic acid (PBPD, 16b) displays an unusual selectivity with improved relative affinity for竞争性NMDA受体拮抗剂的结合位点位于NR2亚基上,其中有四种类型(NR2A-D)。典型的拮抗剂,例如(R)-AP5,具有亚单位选择性为NR2A> NR2B> NR2C> NR2D。竞争性NMDA受体拮抗剂(2R,3S)-(1-联苯基-4-羰基)哌嗪-2,3-二羧酸(PBPD,16b)与NR2A和NR2B相比,对NR2C和NR2D的相对亲和力增强,显示出非同寻常的选择性。合成了16b的带有芳基或芳基取代基的哌啶-2,3-二羧酸的N(1)连接基团的类似物,以探讨NR2C / NR2D选择性的结构要求。菲-2-羰基类似物16e对NR2C和NR2D的亲和力高> 60倍,对NR2C / NR2D的选择性是NR2A / NR2B的3-5倍。菲-3-羰基类似物(16f)的效力较低,但选择性更高,分别对NR2D的选择性是NR2A和NR2B的5倍和7倍。因此,带有大量疏水残基的拮抗剂具有与典型拮抗剂不同的NR2亚基选择性。
同类化合物
2,9-二(2-苯乙基)蒽并[2,1,9-DEF:6,5,10-D’E’F’]二异喹啉-1,3,8,10(2H,9H)-四酮
高雌二醇
马兜铃酸盐
马兜铃酸C
马兜铃酸B
马兜铃酸(1:1MIXTUREOFARISTOLOCHICACIDIANDARISTOLOCHICACIDII)
马兜铃酸 Ia
马兜铃酸 IVa
马兜铃酸
颜料黑32
颜料红179
颜料红178
颜料红149
颜料红123
顺式-菲-1,2-二醇-3,4-环氧化物
顺式-苯并(a)屈-11,12-二醇-13,14-环氧化物
雷公藤酚A
镁二(1,4,5,6,7,16,17,18,19,19,20,20-十二氯六环[14.2.1.14,7.02,15.03,8.09,14]二十-5,9,11,13,17-五烯-11-磺酸酯)
钩大青酮
钩大青酮
钙(2+)12-羟基十八烷酸酯
那布扶林
还原红32
足球烯
贝那他汀B
贝母兰素
萘并[2,3-b]荧蒽
萘并[2,1-e][1]苯并二硫杂环戊烷
萘并[2,1-C:7,8-C']二菲
萘并[1,2-e][2]苯并呋喃-1,3-二酮
萘并[1,2-b]屈
萘并[1,2-a]蒽
萘并[1,2-B]菲-6-醇
萘二(六氯环戊二烯)加合物
菲醌单缩氨基硫脲
菲醌
菲并[9,10]呋喃
菲并[9,10-e]醋菲烯
菲并[4,5-bcd]噻吩
菲并[4,5-bcd]呋喃-3-醇
菲并[4,3-d]-1,3-二噁唑-5-羧酸,10-羟基-9-甲氧基-6-硝基-
菲并[3,2-b]噻吩
菲并[2,1-d]噻唑
菲并[2'',1'',10'':4,5,6;7'',8'',9'':4',5',6']二异喹啉并[2,1-a:2',1'-a']二萘嵌间二氮杂苯-8,13-二酮
菲并(3,4-b)噻吩
菲并(1,2-b)噻吩
菲<2,3-H>异喹啉
菲<2,3-B>噻吩
菲9,10-亚胺
菲3,4-氧化物
联系我们
关注我们
公众号
