tert-butyl (2S,3S,αS)-3-(N-benzyl-N-α-methylbenzylamino)-2-hydroxybutanoate | 181137-51-9
中文名称
——
中文别名
——
英文名称
tert-butyl (2S,3S,αS)-3-(N-benzyl-N-α-methylbenzylamino)-2-hydroxybutanoate
英文别名
tert-butyl (S,S,S)-2-hydroxy-3-[N-benzyl-N-(α-methylbenzyl)amino]butanoate;tert-butyl (2S,3S,αS)-2-hydroxy-3-[N-benzyl-N-(α-methylbenzyl)amino]butanoate;tert-butyl (2S,3S)-3-[benzyl-[(1S)-1-phenylethyl]amino]-2-hydroxybutanoate
CAS
181137-51-9
化学式
C23H31NO3
mdl
——
分子量
369.504
InChiKey
JRBPZDZFCLSTDV-WFXMLNOXSA-N
BEILSTEIN
——
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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沸点:474.0±40.0 °C(Predicted)
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密度:1.082±0.06 g/cm3(Predicted)
计算性质
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辛醇/水分配系数(LogP):4.3
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重原子数:27
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可旋转键数:9
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环数:2.0
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sp3杂化的碳原子比例:0.43
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拓扑面积:49.8
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氢给体数:1
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氢受体数:4
上下游信息
反应信息
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作为反应物:描述:tert-butyl (2S,3S,αS)-3-(N-benzyl-N-α-methylbenzylamino)-2-hydroxybutanoate 在 palladium dihydroxide 氢气 、 甲烷 作用下, 以 甲醇 、 甲苯 为溶剂, 20.0 ℃ 、506.66 kPa 条件下, 反应 4.0h, 生成 tert-butyl (4S,5S)-4-methyloxazolidin-2-one-5-carboxylate参考文献:名称:抗-(2S,3S)-和顺-(2R,3S)-二氨基丁酸的不对称合成。摘要:将同手性N-苄基-N-α-甲基苄基氨基锂加到(E)-肉桂酸叔丁酯或(E)-巴豆酸叔丁酯中,并用叠氮化三苯胺原位胺化,仅形成相应的2-重氮大于95%de的-3-氨基酯 叔丁基(3S,alphaR)-3-N-苄基-N-α-甲基苄基氨基-3-苯基丙酸酯或叔丁基(3S,alphaS)-3-N-苄基-的(E)-烯醇锂的胺化N-α-甲基苄氨基氨基丁酸酯与三叠氮化物以良好的收率和85%的de和> 95%的de生成(2R,3R,alphaR)-和(2S,3S,alphaS)-抗-2-叠氮基-3-氨基酯分别。或者,可以将叔丁基抗-(2S,3S,αS)-2-羟基-3-N-苄基-N-α-甲基苄基氨基丁酸酯选择性地转化为叔丁基抗-(2S,3S,αS)-2-叠氮基-3-N-苄基-N-α-甲基苄基氨基丁酸通过叠氮鎓离子的形成和与叠氮化物的区域选择性打开。(2S,3S,alphaS)-2-叠氮基-3-氨基丁酸叔丁酯通过DOI:10.1039/b306936m
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作为产物:参考文献:名称:Nine Enzymes Are Required for Assembly of the Pacidamycin Group of Peptidyl Nucleoside Antibiotics摘要:Pacidamycins are a family of uridyl peptide antibiotics that inhibit the translocase MraY, an essential enzyme in bacterial cell wall biosynthesis that to date has not been clinically targeted. The pacidamycin structural skeleton contains a doubly inverted peptidyl chain with a beta-peptide and a ureido linkage as well as a 3'-deoxyuridine nucleoside attached to DABA(3) of the peptidyl chain via an enamide linkage. Although the biosynthetic gene cluster for pacidamycins was identified recently, the assembly line of this group of peptidyl nucleoside antibiotics remained poorly understood because of the highly dissociated nature of the encoded nonribosomal peptide synthetase (NRPS) domains and modules. This work has identified a minimum set of enzymes needed for generation of the pacidamycin scaffold from amino acid and nucleoside monomers, highlighting a freestanding thiolation (T) domain (PacH) as a key carrier component in the peptidyl chain assembly as well as a freestanding condensation (C) domain (PacI) catalyzing the release of the assembled peptide by a nucleoside moiety. On the basis of the substrate promiscuity of this enzymatic assembly line, several pacidamycin analogues were produced using in vitro total biosynthesis.DOI:10.1021/ja2011109
文献信息
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Asymmetric synthesis of vicinal amino alcohols: xestoaminol C, sphinganine and sphingosine作者:Elin Abraham、Stephen G. Davies、Nicholas L. Millican、Rebecca L. Nicholson、Paul M. Roberts、Andrew D. SmithDOI:10.1039/b801357h日期:——beta-unsaturated esters, via conjugate addition of lithium (S)-N-benzyl-N-(alpha-methylbenzyl)amide and subsequent in situ enolate oxidation with (+)-(camphorsulfonyl)oxaziridine, has been used as the key step in the asymmetric synthesis of N,O-diacetyl xestoaminol C (41% yield over 8 steps), N,O,O-triacetyl sphinganine (30% yield over 8 steps) and N,O,O-triacetyl sphingosine (30% yield over 7 steps)
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Microconine [N-methyl-2-methyl-3-methoxy-6-(deca-l’,3′,5′-trienyl)piperidine, an alkaloid from Microcos paniculata]: Synthesis, stereochemistry and spectroscopic data作者:Stephen G. Davies、Ai M. Fletcher、Paul M. Roberts、Cameron E. Taylor、James E. ThomsonDOI:10.1016/j.tet.2020.131860日期:2021.15′-trienyl)piperidine], an alkaloid found in Microcos paniculata, are reported. The asymmetric synthesis of the (2S,3R,6S)- and (2S,3S,6S)-stereoisomeric forms [epimeric at C(3)] of this compound allows the unambiguous assignment of the relative 2,3-cis-3,6-cis-configuration of the natural product. The synthesis uses the conjugate addition of enantiopure lithium (S)-N-benzyl-N-(α-methylbenzyl)amide to明确分离的Microconine原始样品[ N-甲基-2-甲基-3-甲氧基-6-(deca-1',3',5'-三烯基)哌啶]的明确1 H NMR数据,Microcos中发现的一种生物碱paniculata,据报道。该化合物的(2 S,3 R,6 S)-和(2 S,3 S,6 S)-立体异构体形式的不对称合成[在C(3)上的异构体]允许相对相对的2,天然产物的3-顺-3,6-顺-构型。合成使用对映体纯锂(S)-N-苄基-的共轭加成N-(α-甲基苄基)酰胺至巴豆酸叔丁酯,并随后与(+)-樟脑磺酰基恶二丙啶进行烯醇氧化,以生成在目标物中发现的必需C(2)和C(3)立体中心。详细阐述后,使用分子内还原胺化作用形成哌啶环,并伴随形成C(6)立体异构中心。特定旋转数据的比较与具有绝对(2 R,3 R,6 R)-构型的生物碱一致。
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Microcosamine A, Microgrewiapine A and Microgrewiapine B: three homochiral alkaloids?作者:Stephen G. Davies、Ai M. Fletcher、Paul M. Roberts、Cameron E. Taylor、James E. ThomsonDOI:10.1016/j.tet.2021.132056日期:2021.6nOe analyses allow unambiguous assignment of relative configuration of the alkaloids. Comparison of specific rotation data for microcosamine A and microgrewiapine B is consistent with both possessing the absolute (2S,3R,6S)-configuration. For microgrewiapine A, conflicting data regarding the absolute configuration are revealed: in the isolation study a Mosher’s analysis concludes a (2S,3R,6S)-configuration报道了microcosamine A、microgrewiapine A 和 microgrewiapine B(Microcos paniculata生物碱)的不对称合成。将锂 ( S ) -N-苄基-N- (α-甲基苄基)酰胺与巴豆酸叔丁酯共轭加成,然后烯醇氧化生成靶标的 C(2) 和 C(3) 立体中心,随后非对映选择性分子内还原胺化用于形成哌啶环,同时产生 C(6) 立体中心。1 H NMR 3 J耦合常数和 nOe 分析允许明确分配生物碱的相对构型。microcosamine A 和 microgrewiapine B 的比旋光度数据的比较与两者都具有绝对 (2 S ,3 R ,6 S )-构型一致。对于 microgrewiapine A,揭示了关于绝对构型的相互矛盾的数据:在隔离研究中,Mosher 的分析得出 (2 S ,3 R ,6 S )-构型的结论,但比旋光度数据的比较表明
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Asymmetric synthesis of N,O-diacetyl-3-epi-xestoaminol C: structure and absolute configuration confirmation of 3-epi-xestoaminol C作者:Susanna G. Archer、Kristína Csatayová、Stephen G. Davies、Ai M. Fletcher、Paul M. Roberts、James E. ThomsonDOI:10.1016/j.tetlet.2016.02.021日期:2016.3The asymmetric synthesis of N,O-diacetyl-3-epi-xestoaminol C is reported. The synthesis employs diastereoselective aminohydroxylation of tert-butyl crotonate [conjugate addition of lithium (S)-N-benzyl-N-(α-methylbenzyl)amide, then in situ enolate oxidation with (+)-camphorsulfonyloxaziridine (CSO)] and a diastereoselective reduction protocol as the key stereodefining steps. The synthetic sample of
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