(3-(2-(cyclopropanecarboxamido)-N-hydroxyacetamido)propyl)phosphonic acid | 853078-13-4
中文名称
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中文别名
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英文名称
(3-(2-(cyclopropanecarboxamido)-N-hydroxyacetamido)propyl)phosphonic acid
英文别名
3-[[2-(Cyclopropanecarbonylamino)acetyl]-hydroxy-amino]propylphosphonic acid;3-[[2-(cyclopropanecarbonylamino)acetyl]-hydroxyamino]propylphosphonic acid
CAS
853078-13-4
化学式
C9H17N2O6P
mdl
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分子量
280.218
InChiKey
UHCOSYOZVSEXPK-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
计算性质
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辛醇/水分配系数(LogP):-2.4
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重原子数:18
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可旋转键数:7
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环数:1.0
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sp3杂化的碳原子比例:0.78
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拓扑面积:127
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氢给体数:4
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氢受体数:6
反应信息
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作为产物:描述:2-[(环丙基羰基)氨基]乙酸 在 三甲基溴硅烷 、 palladium 10% on activated carbon 、 氢气 、 N,N-二异丙基乙胺 、 N-[(dimethylamino)-3-oxo-1H-1,2,3-triazolo[4,5-b]pyridin-1-yl-methylene]-N-methylmethanaminium hexafluorophosphate 作用下, 以 甲醇 、 二氯甲烷 、 N,N-二甲基甲酰胺 为溶剂, 20.0 ℃ 、101.33 kPa 条件下, 反应 32.17h, 生成 (3-(2-(cyclopropanecarboxamido)-N-hydroxyacetamido)propyl)phosphonic acid参考文献:名称:强大的单取代和双取代的磷霉素类似物对DXR的抑制作用摘要:抗疟药磷酰胺霉素靶向DXR,该酶催化MEP途径中第一个关键步骤,产生必需的类异戊二烯前体,异戊烯基二磷酸酯和二甲基烯丙基二磷酸酯。MEP途径被多种病原体所利用,包括结核分枝杆菌和apicomplexan寄生虫,并且不同于人类必需的经典甲羟戊酸途径。使用基于结构的方法,我们设计了许多磷酰胺霉素类似物,包括在Cα和异羟肟酸酯位置上均被取代的一系列类似物。事实证明,后者是设计抑制剂的稳定框架,该抑制剂从极性和局促的(因此不易药物化)底物结合位点延伸,并且可以首次桥接底物和辅因子结合位点。就在体外试验中杀死恶性疟原虫而言,许多这类化合物比磷霉素更有效。最好的IC 50为40 nM。DOI:10.1021/jm4006498
文献信息
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INHIBITION OF ISOPRENOID BIOSYNTHETIC PATHWAYS TO TREAT NEUROINFLAMMATORY DISORDERS申请人:TABACZYNSKI David A.公开号:US20160303146A1公开(公告)日:2016-10-20This invention provides methods and pharmaceutical compositions that can treat neuroinflammatory disease by reducing the production of pyrophosphate intermediates produced during the biosynthesis of isoprenoids. The pyrophosphate compounds being inhibited are normally produced through the mevalonate and non-mevalonate pathways of the host vertebrate organisms and their symbiotic and pathogenic microorganisms. The methods involve administering to a patient an inhibitor of the mevalonate-dependent pathway, an inhibitor of the non-mevalonate pathway, or combination of such inhibitors.
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INHIBITION OF ISOPRENOID BIOSYNTHETIC PATHWAYS TO TREAT AUTOIMMUNE DISORDERS申请人:TABACZYNSKI David A.公开号:US20160375041A1公开(公告)日:2016-12-29The invention provides methods and pharmaceutical compositions that can treat autoimmune disease by reducing the production of pyrophosphate intermediates produced during the biosynthesis of isoprenoids. The pyrophosphate compounds being inhibited are normally produced through the mevalonate and non-mevalonate pathways of the host vertebrate organisms and their symbiotic and pathogenic microorganisms. The methods involve administering to a patient an inhibitor of the mevalonate-dependent pathway, an inhibitor of the non-mevalonate pathway, or combination of such inhibitors.
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[EN] INHIBITION OF ISOPRENOID BIOSYNTHETIC PATHWAYS TO TREAT AUTOIMMUNE DISORDERS<br/>[FR] INHIBITION DE VOIES DE BIOSYNTHÈSE D'ISOPRÉNOÏDES POUR TRAITER DES TROUBLES AUTO-IMMUNS申请人:TABACZYNSKI DAVID A公开号:WO2015084721A1公开(公告)日:2015-06-11The invention provides methods and pharmaceutical compositions that can treat autoimmune disease by reducing the production of pyrophosphate intermediates produced during the biosynthesis of isoprenoids. The pyrophosphate compounds being inhibited are normally produced through the mevalonate and non-mevalonate pathways of the host vertebrate organisms and their symbiotic and pathogenic microorganisms. The methods involve administering to a patient an inhibitor of the mevalonate-dependent pathway, an inhibitor of the non-mevalonate pathway, or combination of such inhibitors.
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DXR Inhibition by Potent Mono- and Disubstituted Fosmidomycin Analogues作者:Anna M. Jansson、Anna Więckowska、Christofer Björkelid、Samir Yahiaoui、Sanjeewani Sooriyaarachchi、Martin Lindh、Terese Bergfors、Shyamraj Dharavath、Matthieu Desroses、Surisetti Suresh、Mounir Andaloussi、Rautela Nikhil、Sharma Sreevalli、Bachally R. Srinivasa、Mats Larhed、T. Alwyn Jones、Anders Karlén、Sherry L. MowbrayDOI:10.1021/jm4006498日期:2013.8.8including Mycobacterium tuberculosis and apicomplexan parasites, and differs from the classical mevalonate pathway that is essential in humans. Using a structure-based approach, we designed a number of analogues of fosmidomycin, including a series that are substituted in both the Cα and the hydroxamate positions. The latter proved to be a stable framework for the design of inhibitors that extend from the抗疟药磷酰胺霉素靶向DXR,该酶催化MEP途径中第一个关键步骤,产生必需的类异戊二烯前体,异戊烯基二磷酸酯和二甲基烯丙基二磷酸酯。MEP途径被多种病原体所利用,包括结核分枝杆菌和apicomplexan寄生虫,并且不同于人类必需的经典甲羟戊酸途径。使用基于结构的方法,我们设计了许多磷酰胺霉素类似物,包括在Cα和异羟肟酸酯位置上均被取代的一系列类似物。事实证明,后者是设计抑制剂的稳定框架,该抑制剂从极性和局促的(因此不易药物化)底物结合位点延伸,并且可以首次桥接底物和辅因子结合位点。就在体外试验中杀死恶性疟原虫而言,许多这类化合物比磷霉素更有效。最好的IC 50为40 nM。
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