4-[5-(氯甲基)-1,2,4-噁二唑-3-基]吡啶 | 50737-35-4
中文名称
4-[5-(氯甲基)-1,2,4-噁二唑-3-基]吡啶
中文别名
——
英文名称
5-(chloromethyl)-3-(pyridin-4-yl)-1,2,4-oxadiazole
英文别名
4-(5-(chloromethyl)-1,2,4-oxadiazol-3-yl)pyridine;4-[5-(Chloromethyl)-1,2,4-oxadiazol-3-yl]pyridine;5-(chloromethyl)-3-pyridin-4-yl-1,2,4-oxadiazole
![4-[5-(氯甲基)-1,2,4-噁二唑-3-基]吡啶化学式](data:image/svg+xml;base64,<?xml version="1.0" encoding="UTF-8"?>
<svg xmlns="http://www.w3.org/2000/svg" xmlns:xlink="http://www.w3.org/1999/xlink" width="300" height="300" viewBox="0 0 300 300">
<defs>
<g>
<g id="glyph-0-0">
<path d="M 0.890625 3.15625 L 0.890625 -12.5625 L 9.796875 -12.5625 L 9.796875 3.15625 Z M 1.890625 2.15625 L 8.796875 2.15625 L 8.796875 -11.5625 L 1.890625 -11.5625 Z M 1.890625 2.15625 "/>
</g>
<g id="glyph-0-1">
<path d="M 1.75 -12.984375 L 4.109375 -12.984375 L 9.875 -2.125 L 9.875 -12.984375 L 11.578125 -12.984375 L 11.578125 0 L 9.203125 0 L 3.453125 -10.859375 L 3.453125 0 L 1.75 0 Z M 1.75 -12.984375 "/>
</g>
<g id="glyph-0-2">
<path d="M 7.015625 -11.796875 C 5.742188 -11.796875 4.734375 -11.316406 3.984375 -10.359375 C 3.234375 -9.410156 2.859375 -8.117188 2.859375 -6.484375 C 2.859375 -4.847656 3.234375 -3.550781 3.984375 -2.59375 C 4.734375 -1.644531 5.742188 -1.171875 7.015625 -1.171875 C 8.296875 -1.171875 9.304688 -1.644531 10.046875 -2.59375 C 10.796875 -3.550781 11.171875 -4.847656 11.171875 -6.484375 C 11.171875 -8.117188 10.796875 -9.410156 10.046875 -10.359375 C 9.304688 -11.316406 8.296875 -11.796875 7.015625 -11.796875 Z M 7.015625 -13.21875 C 8.835938 -13.21875 10.289062 -12.609375 11.375 -11.390625 C 12.46875 -10.171875 13.015625 -8.535156 13.015625 -6.484375 C 13.015625 -4.429688 12.46875 -2.796875 11.375 -1.578125 C 10.289062 -0.359375 8.835938 0.25 7.015625 0.25 C 5.191406 0.25 3.734375 -0.359375 2.640625 -1.578125 C 1.546875 -2.796875 1 -4.429688 1 -6.484375 C 1 -8.535156 1.546875 -10.171875 2.640625 -11.390625 C 3.734375 -12.609375 5.191406 -13.21875 7.015625 -13.21875 Z M 7.015625 -13.21875 "/>
</g>
<g id="glyph-0-3">
<path d="M 11.46875 -11.984375 L 11.46875 -10.125 C 10.875 -10.675781 10.242188 -11.085938 9.578125 -11.359375 C 8.910156 -11.640625 8.195312 -11.78125 7.4375 -11.78125 C 5.957031 -11.78125 4.820312 -11.320312 4.03125 -10.40625 C 3.25 -9.5 2.859375 -8.191406 2.859375 -6.484375 C 2.859375 -4.765625 3.25 -3.453125 4.03125 -2.546875 C 4.820312 -1.640625 5.957031 -1.1875 7.4375 -1.1875 C 8.195312 -1.1875 8.910156 -1.320312 9.578125 -1.59375 C 10.242188 -1.875 10.875 -2.285156 11.46875 -2.828125 L 11.46875 -1 C 10.851562 -0.582031 10.203125 -0.269531 9.515625 -0.0625 C 8.828125 0.144531 8.101562 0.25 7.34375 0.25 C 5.375 0.25 3.820312 -0.347656 2.6875 -1.546875 C 1.5625 -2.753906 1 -4.398438 1 -6.484375 C 1 -8.566406 1.5625 -10.207031 2.6875 -11.40625 C 3.820312 -12.613281 5.375 -13.21875 7.34375 -13.21875 C 8.113281 -13.21875 8.84375 -13.113281 9.53125 -12.90625 C 10.21875 -12.707031 10.863281 -12.398438 11.46875 -11.984375 Z M 11.46875 -11.984375 "/>
</g>
<g id="glyph-0-4">
<path d="M 1.671875 -13.53125 L 3.28125 -13.53125 L 3.28125 0 L 1.671875 0 Z M 1.671875 -13.53125 "/>
</g>
</g>
</defs>
<path fill="none" stroke-width="0.0333333" stroke-linecap="butt" stroke-linejoin="miter" stroke="rgb(0%, 0%, 0%)" stroke-opacity="1" stroke-miterlimit="10" d="M 1.094217 3.009751 L 1.097199 1.992612 " transform="matrix(44.525921, 0, 0, 44.525921, 104.653997, 10.42166)"/>
<path fill="none" stroke-width="0.0333333" stroke-linecap="butt" stroke-linejoin="miter" stroke="rgb(0%, 0%, 0%)" stroke-opacity="1" stroke-miterlimit="10" d="M 1.10106 2.996241 L 0.528798 3.41015 " transform="matrix(44.525921, 0, 0, 44.525921, 104.653997, 10.42166)"/>
<path fill="none" stroke-width="0.0333333" stroke-linecap="butt" stroke-linejoin="miter" stroke="rgb(0%, 0%, 0%)" stroke-opacity="1" stroke-miterlimit="10" d="M 1.094217 3.001241 L 1.658232 3.413747 " transform="matrix(44.525921, 0, 0, 44.525921, 104.653997, 10.42166)"/>
<path fill="none" stroke-width="0.0333333" stroke-linecap="butt" stroke-linejoin="miter" stroke="rgb(0%, 0%, 0%)" stroke-opacity="1" stroke-miterlimit="10" d="M 1.09369 3.207318 L 1.559799 3.548236 " transform="matrix(44.525921, 0, 0, 44.525921, 104.653997, 10.42166)"/>
<path fill="none" stroke-width="0.0333333" stroke-linecap="butt" stroke-linejoin="miter" stroke="rgb(0%, 0%, 0%)" stroke-opacity="1" stroke-miterlimit="10" d="M 1.097112 2.002262 L 1.972567 1.502202 " transform="matrix(44.525921, 0, 0, 44.525921, 104.653997, 10.42166)"/>
<path fill="none" stroke-width="0.0333333" stroke-linecap="butt" stroke-linejoin="miter" stroke="rgb(0%, 0%, 0%)" stroke-opacity="1" stroke-miterlimit="10" d="M 1.097726 1.809958 L 1.805881 1.405524 " transform="matrix(44.525921, 0, 0, 44.525921, 104.653997, 10.42166)"/>
<path fill="none" stroke-width="0.0333333" stroke-linecap="butt" stroke-linejoin="miter" stroke="rgb(0%, 0%, 0%)" stroke-opacity="1" stroke-miterlimit="10" d="M 1.105446 2.007087 L 0.225955 1.497289 " transform="matrix(44.525921, 0, 0, 44.525921, 104.653997, 10.42166)"/>
<path fill="none" stroke-width="0.0333333" stroke-linecap="butt" stroke-linejoin="miter" stroke="rgb(0%, 0%, 0%)" stroke-opacity="1" stroke-miterlimit="10" d="M 0.373955 3.866871 L 0.590121 4.539408 " transform="matrix(44.525921, 0, 0, 44.525921, 104.653997, 10.42166)"/>
<path fill="none" stroke-width="0.0333333" stroke-linecap="butt" stroke-linejoin="miter" stroke="rgb(0%, 0%, 0%)" stroke-opacity="1" stroke-miterlimit="10" d="M 0.532658 3.8159 L 0.711715 4.373072 " transform="matrix(44.525921, 0, 0, 44.525921, 104.653997, 10.42166)"/>
<path fill="none" stroke-width="0.0333333" stroke-linecap="butt" stroke-linejoin="miter" stroke="rgb(0%, 0%, 0%)" stroke-opacity="1" stroke-miterlimit="10" d="M 1.810443 3.871872 L 1.685165 4.253145 " transform="matrix(44.525921, 0, 0, 44.525921, 104.653997, 10.42166)"/>
<path fill="none" stroke-width="0.0333333" stroke-linecap="butt" stroke-linejoin="miter" stroke="rgb(0%, 0%, 0%)" stroke-opacity="1" stroke-miterlimit="10" d="M 1.964145 1.516678 L 1.964145 0.495503 " transform="matrix(44.525921, 0, 0, 44.525921, 104.653997, 10.42166)"/>
<path fill="none" stroke-width="0.0333333" stroke-linecap="butt" stroke-linejoin="miter" stroke="rgb(0%, 0%, 0%)" stroke-opacity="1" stroke-miterlimit="10" d="M 0.234201 1.511677 L 0.234201 0.490414 " transform="matrix(44.525921, 0, 0, 44.525921, 104.653997, 10.42166)"/>
<path fill="none" stroke-width="0.0333333" stroke-linecap="butt" stroke-linejoin="miter" stroke="rgb(0%, 0%, 0%)" stroke-opacity="1" stroke-miterlimit="10" d="M 0.400888 1.415701 L 0.400888 0.586566 " transform="matrix(44.525921, 0, 0, 44.525921, 104.653997, 10.42166)"/>
<path fill="none" stroke-width="0.0333333" stroke-linecap="butt" stroke-linejoin="miter" stroke="rgb(0%, 0%, 0%)" stroke-opacity="1" stroke-miterlimit="10" d="M 0.581611 4.53932 L 1.344948 4.541601 " transform="matrix(44.525921, 0, 0, 44.525921, 104.653997, 10.42166)"/>
<path fill="none" stroke-width="0.0333333" stroke-linecap="butt" stroke-linejoin="miter" stroke="rgb(0%, 0%, 0%)" stroke-opacity="1" stroke-miterlimit="10" d="M 0.595122 4.532477 L -0.00565183 5.354242 " transform="matrix(44.525921, 0, 0, 44.525921, 104.653997, 10.42166)"/>
<path fill="none" stroke-width="0.0333333" stroke-linecap="butt" stroke-linejoin="miter" stroke="rgb(0%, 0%, 0%)" stroke-opacity="1" stroke-miterlimit="10" d="M 1.972392 0.50989 L 1.353721 0.148619 " transform="matrix(44.525921, 0, 0, 44.525921, 104.653997, 10.42166)"/>
<path fill="none" stroke-width="0.0333333" stroke-linecap="butt" stroke-linejoin="miter" stroke="rgb(0%, 0%, 0%)" stroke-opacity="1" stroke-miterlimit="10" d="M 1.805705 0.605604 L 1.269676 0.292584 " transform="matrix(44.525921, 0, 0, 44.525921, 104.653997, 10.42166)"/>
<path fill="none" stroke-width="0.0333333" stroke-linecap="butt" stroke-linejoin="miter" stroke="rgb(0%, 0%, 0%)" stroke-opacity="1" stroke-miterlimit="10" d="M 0.225867 0.504802 L 0.844362 0.147303 " transform="matrix(44.525921, 0, 0, 44.525921, 104.653997, 10.42166)"/>
<path fill="none" stroke-width="0.0333333" stroke-linecap="butt" stroke-linejoin="miter" stroke="rgb(0%, 0%, 0%)" stroke-opacity="1" stroke-miterlimit="10" d="M -0.00389723 5.337661 L 0.271662 5.960981 " transform="matrix(44.525921, 0, 0, 44.525921, 104.653997, 10.42166)"/>
<g fill="rgb(19%, 31%, 97.000003%)" fill-opacity="1">
<use xlink:href="#glyph-0-1" x="110.640625" y="176.636719"/>
</g>
<g fill="rgb(19%, 31%, 97.000003%)" fill-opacity="1">
<use xlink:href="#glyph-0-1" x="182.691406" y="176.863281"/>
</g>
<g fill="rgb(100%, 5.1%, 5.1%)" fill-opacity="1">
<use xlink:href="#glyph-0-2" x="168.449219" y="219.15625"/>
</g>
<g fill="rgb(19%, 31%, 97.000003%)" fill-opacity="1">
<use xlink:href="#glyph-0-1" x="146.933594" y="16.914062"/>
</g>
<g fill="rgb(9.977717%, 78.158784%, 9.977717%)" fill-opacity="1">
<use xlink:href="#glyph-0-3" x="114.292969" y="295.816406"/>
<use xlink:href="#glyph-0-4" x="126.72892" y="295.816406"/>
</g>
</svg>
)
CAS
50737-35-4
化学式
C8H6ClN3O
mdl
MFCD09034189
分子量
195.608
InChiKey
TTYRVRZPJAJSGJ-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):1.2
-
重原子数:13
-
可旋转键数:2
-
环数:2.0
-
sp3杂化的碳原子比例:0.12
-
拓扑面积:51.8
-
氢给体数:0
-
氢受体数:4
安全信息
-
危险等级:IRRITANT
-
海关编码:2934999090
SDS
上下游信息
-
下游产品
中文名称 英文名称 CAS号 化学式 分子量 —— N-((3-(pyridin-4-yl)-1,2,4-oxadiazol-5-yl)methyl)propan-2-amine 1179621-88-5 C11H14N4O 218.258
反应信息
-
作为反应物:描述:4-[5-(氯甲基)-1,2,4-噁二唑-3-基]吡啶 在 potassium carbonate 、 三乙胺 作用下, 以 四氢呋喃 、 乙腈 为溶剂, 反应 0.75h, 生成 N-isopropyl-N-((3-(pyridin-4-yl)-1,2,4-oxadiazol-5-yl)methyl)-2-(p-tolyloxy)acetamide参考文献:名称:恶二唑-异丙基酰胺作为有效的非共价蛋白酶体抑制剂摘要:对 50 000 ChemBridge 化合物库的筛选导致鉴定出恶二唑-异丙基酰胺1 (PI-1833),其抑制胰凝乳蛋白酶样 (CT-L) 活性(IC 50 = 0.60 μM),对其他两种主要蛋白酶体几乎没有影响蛋白水解活性,胰蛋白酶样 (TL) 和谷氨酰肽水解样 (PGPH-L)。LC-MS/MS 和透析表明1是一种非共价且快速可逆的 CT-L 抑制剂。集中文库合成为11ad (PI-1840) 提供了 CT-L 活性 (IC 50= 27 纳米)。详细的 SAR 研究表明酰胺部分和两个苯环对修饰敏感。疏水性残基,如在对位丙基或丁基(未邻位或间位)的A环和一个的米-吡啶基团作为B环,显著提高活性。化合物11ad (IC 50 = 0.37 μM)在抑制完整 MDA-MB-468 人乳腺癌细胞中的 CT-L 活性和抑制其存活方面比1 (IC 50 = 3.5 μM)更有效。11ad的活DOI:10.1021/jm400221d
-
作为产物:描述:(Z)-N'-(2-chloroacetoxy)isonicotinimidamide 以 甲苯 为溶剂, 反应 2.0h, 以84%的产率得到4-[5-(氯甲基)-1,2,4-噁二唑-3-基]吡啶参考文献:名称:恶二唑-异丙基酰胺作为有效的非共价蛋白酶体抑制剂摘要:对 50 000 ChemBridge 化合物库的筛选导致鉴定出恶二唑-异丙基酰胺1 (PI-1833),其抑制胰凝乳蛋白酶样 (CT-L) 活性(IC 50 = 0.60 μM),对其他两种主要蛋白酶体几乎没有影响蛋白水解活性,胰蛋白酶样 (TL) 和谷氨酰肽水解样 (PGPH-L)。LC-MS/MS 和透析表明1是一种非共价且快速可逆的 CT-L 抑制剂。集中文库合成为11ad (PI-1840) 提供了 CT-L 活性 (IC 50= 27 纳米)。详细的 SAR 研究表明酰胺部分和两个苯环对修饰敏感。疏水性残基,如在对位丙基或丁基(未邻位或间位)的A环和一个的米-吡啶基团作为B环,显著提高活性。化合物11ad (IC 50 = 0.37 μM)在抑制完整 MDA-MB-468 人乳腺癌细胞中的 CT-L 活性和抑制其存活方面比1 (IC 50 = 3.5 μM)更有效。11ad的活DOI:10.1021/jm400221d
文献信息
-
[EN] 1-AZA-BICYCLO [2.2.2] OCTANE DERIVATIVES USEFUL AS MUSCARINIC RECEPTOR ANTAGONISTS<br/>[FR] DÉRIVÉS DE 1-AZA-BICYCLO [2.2.2] OCTANE UTILES EN TANT QU'ANTAGONISTES DES RÉCEPTEURS MUSCARINIQUES申请人:ARGENTA DISCOVERY LTD公开号:WO2009153536A1公开(公告)日:2009-12-23The invention provides named compounds of formula (I), pharmaceutical compositions containing them, a process for preparing the pharmaceutical compositions and their use in therapy.本发明提供了公式(I)的命名化合物、含有它们的药物组合物、制备所述药物组合物的方法以及它们在治疗中的用途。
-
Design, Synthesis, and Evaluation of the Highly Selective and Potent G-Protein-Coupled Receptor Kinase 2 (GRK2) Inhibitor for the Potential Treatment of Heart Failure作者:Tomohiro Okawa、Yoshio Aramaki、Mitsuo Yamamoto、Toshitake Kobayashi、Shoji Fukumoto、Yukio Toyoda、Tsutomu Henta、Akito Hata、Shota Ikeda、Manami Kaneko、Isaac D. Hoffman、Bi-Ching Sang、Hua Zou、Tetsuji KawamotoDOI:10.1021/acs.jmedchem.7b00443日期:2017.8.24for heart failure, highly potent and selective GRK2 inhibitors, exhibit potentiation of β-adrenergic signaling in vitro studies. Hydrazone derivative 5 and 1,2,4-triazole derivative 24a were identified as hit compounds by HTS. New scaffold generation and SAR studies of all parts resulted in a 4-methyl-1,2,4-triazole derivative with an N-benzylcarboxamide moiety with highly potent activity toward GRK2用于心力衰竭的一类新型治疗药物,高效和选择性的GRK2抑制剂,在体外研究中表现出增强的β-肾上腺素信号传导能力。HTS将衍生物5和1,2,4-三唑衍生物24a鉴定为命中化合物。新一代的脚手架和所有部分的SAR研究都产生了带有N-苄基羧酰胺部分的4-甲基-1,2,4-三唑衍生物,对GRK2的活性很高,对其他激酶的选择性更高。在亚型选择性方面,这些化合物对GRK1、5、6和7表现出足够的选择性,并且对GRK3具有几乎相同的抑制作用。我们的药物化学努力导致发现了115h(GRK2 IC 50= 18 nM),获得了与人GRK2和GRK2抑制剂的共晶体结构,该抑制剂增强了β-肾上腺素能受体(βAR)介导的cAMP积累,并防止了用异丙肾上腺素处理过的表达β2AR的HEK293细胞中βAR的内在化。因此,115h似乎是心力衰竭治疗的一种新型疗法。
-
PROTEASOME CHYMOTRYPSIN-LIKE INHIBITION USING PI-1833 ANALOGS申请人:H. Lee Moffitt Cancer Center and Research Institute, Inc公开号:US20140073650A1公开(公告)日:2014-03-13Focused library synthesis and medicinal chemistry on an oxadiazole-isopropylamide core proteasome inhibitor provided the lead compound that strongly inhibits CT-L activity. Structure activity relationship studies indicate the amide moiety and two phenyl rings are sensitive toward synthetic modifications. Only para-substitution in the A-ring was important to maintain potent CT-L inhibitory activity. Hydrophobic residues in the A-ring's para-position and meta-pyridyl group at the B-ring significantly improved inhibition. The meta-pyridyl moiety improved cell permeability. The length of the aliphatic chain at the para position of the A-ring is critical with propyl yielding the most potent inhibitor, whereas shorter (i.e. ethyl, methyl or hydrogen) or longer (i.e. butyl, propyl and hexyl) chains demonstrating progressively less potency. Introduction of a stereogenic center next to the ether moiety (i.e. substitution of one of the hydrogens by methyl) demonstrated chiral discrimination in proteasome CT-L activity inhibition (the S-enantiomer was 35-40 fold more potent than the R-enantiomer).聚焦于氧代二唑-异丙酰胺核心蛋白酶体抑制剂的合成和药物化学,提供了一种强烈抑制CT-L活性的先导化合物。结构活性关系研究表明,酰胺基团和两个苯环对合成修饰非常敏感。只有在A环上的对位取代对维持强效的CT-L抑制活性至关重要。A环对位的疏水基团和B环的间吡啶基团显著提高了抑制作用。间吡啶基团提高了细胞渗透性。A环对位的脂肪链长度是关键,丙基产生了最有效的抑制剂,而较短(即乙基,甲基或氢)或较长(即丁基,异丙基和己基)的链逐渐表现出较少的效力。在醚基团旁引入一个立体异构中心(即将一个氢原子取代为甲基)表明在蛋白酶体CT-L活性抑制中具有手性歧视(S-对映体比R-对映体更有效,效力提高了35-40倍)。
-
Proteasome chymotrypsin-like inhibition using PI-1833 analogs申请人:H. Lee Moffitt Cancer Center and Research Institute, Inc.公开号:US10662180B2公开(公告)日:2020-05-26Focused library synthesis and medicinal chemistry on an oxadiazole-isopropylamide core proteasome inhibitor provided the lead compound that strongly inhibits CT-L activity. Structure activity relationship studies indicate the amide moiety and two phenyl rings are sensitive toward synthetic modifications. Only para-substitution in the A-ring was important to maintain potent CT-L inhibitory activity. Hydrophobic residues in the A-ring's para-position and meta-pyridyl group at the B-ring significantly improved inhibition. The meta-pyridyl moiety improved cell permeability. The length of the aliphatic chain at the para position of the A-ring is critical with propyl yielding the most potent inhibitor, whereas shorter (i.e. ethyl, methyl or hydrogen) or longer (i.e. butyl, propyl and hexyl) chains demonstrating progressively less potency. Introduction of a stereogenic center next to the ether moiety (i.e. substitution of one of the hydrogens by methyl) demonstrated chiral discrimination in proteasome CT-L activity inhibition (the S-enantiomer was 35-40 fold more potent than the R-enantiomer).通过对一种噁二唑-异丙基酰胺核心蛋白酶体抑制剂进行重点文库合成和药物化学研究,获得了能强烈抑制 CT-L 活性的先导化合物。结构活性关系研究表明,酰胺分子和两个苯基环对合成修饰很敏感。只有 A 环中的对位取代对保持 CT-L 的强效抑制活性非常重要。A 环的对位疏水残基和 B 环的元吡啶基能显著改善抑制作用。偏吡啶基提高了细胞渗透性。A 环对位脂肪族链的长度至关重要,丙基产生的抑制作用最强,而较短的链(即乙基、甲基或氢基)或较长的链(即丁基、丙基和己基)的抑制作用则逐渐减弱。在醚分子旁边引入一个立体中心(即用甲基取代其中一个氢)可在蛋白酶体 CT-L 活性抑制方面显示出手性差异(S-对映体的效力比 R-对映体高 35-40 倍)。
-
US9878999B2申请人:——公开号:US9878999B2公开(公告)日:2018-01-30
同类化合物
(S)-氨氯地平-d4
(R,S)-可替宁N-氧化物-甲基-d3
(R)-N'-亚硝基尼古丁
(5E)-5-[(2,5-二甲基-1-吡啶-3-基-吡咯-3-基)亚甲基]-2-亚磺酰基-1,3-噻唑烷-4-酮
(5-溴-3-吡啶基)[4-(1-吡咯烷基)-1-哌啶基]甲酮
(5-氨基-6-氰基-7-甲基[1,2]噻唑并[4,5-b]吡啶-3-甲酰胺)
(2S)-2-[[[9-丙-2-基-6-[(4-吡啶-2-基苯基)甲基氨基]嘌呤-2-基]氨基]丁-1-醇
(2R,2''R)-(+)-[N,N''-双(2-吡啶基甲基)]-2,2''-联吡咯烷四盐酸盐
黄色素-37
麦斯明-D4
麦司明
麝香吡啶
鲁非罗尼
鲁卡他胺
高氯酸N-甲基甲基吡啶正离子
高氯酸,吡啶
高奎宁酸
马来酸溴苯那敏
马来酸左氨氯地平
顺式-双(异硫氰基)(2,2'-联吡啶基-4,4'-二羧基)(4,4'-二-壬基-2'-联吡啶基)钌(II)
顺式-二氯二(4-氯吡啶)铂
顺式-二(2,2'-联吡啶)二氯铬氯化物
顺式-1-(4-甲氧基苄基)-3-羟基-5-(3-吡啶)-2-吡咯烷酮
顺-双(2,2-二吡啶)二氯化钌(II) 水合物
顺-双(2,2'-二吡啶基)二氯化钌(II)二水合物
顺-二氯二(吡啶)铂(II)
顺-二(2,2'-联吡啶)二氯化钌(II)二水合物
非那吡啶
非洛地平杂质C
非洛地平
非戈替尼
非尼拉朵
非尼拉敏
阿雷地平
阿瑞洛莫
阿培利司N-6
阿伐曲波帕杂质40
间硝苯地平
间-硝苯地平
锇二(2,2'-联吡啶)氯化物
链黑霉素
链黑菌素
银杏酮盐酸盐
铬二烟酸盐
铝三烟酸盐
铜-缩氨基硫脲络合物
铜(2+)乙酸酯吡啶(1:2:1)
铁5-甲氧基-6-甲基-1-氧代-2-吡啶酮
钾4-氨基-3,6-二氯-2-吡啶羧酸酯
钯,二氯双(3-氯吡啶-κN)-,(SP-4-1)-
联系我们
关注我们
公众号
