Crystal Structure of 2-(1-Benzoylazetidin-3-yl)thio-1,3-thiazoline

IF 0.1 Q4 CRYSTALLOGRAPHY

X-ray Structure Analysis Online Pub Date : 2021-09-10 DOI:10.2116/xraystruct.37.57

K. Sugiura, Yoshimi Ichimaru, Koichi Kato, Masanori Imai, H. Kurosaki, Kazuhiko Hayashi

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Abstract

Tebipenem pivoxil is an oral 1β-methylcarbapenem antibiotic with a broad spectrum and potent antibacterial activity against various bacteria, except for Pseudomonas aeruginosa, which has the [1-(1,3-thiazolin-2-yl)azetidin-3-yl]thio moiety as the pendant at the C-2 position.1 The pendant moiety of Tebipenem pivoxil was introduced using 1-(1,3-thiazolin-2-yl)azetidine-3thiol, and was also introduced into the antibiotic T405 under development.2 However, no chrystallographic studies of 1-(1,3-thiazolin-2-yl)azetidine-3-thiol and its synthetic precursors have been reported, except for Tebipenem pivoxil, which has the thio group.3 In this paper, we describe the X-ray crystal structure of 2-(1-benzoylazetidin-3-yl)thio-1,3-thiazoline (Fig. 1), which is a synthetic precursor of 1-(1,3-thiazolin-2-yl)azetidine-3-thiol. The title compound was synthesized by reacting 1-azabicyclo[1.1.0] butane and 3-benzoyl-1,3-thiazolidine-2-thione in the presence of a Lewis acid, such as Mg(OTf )2. Then, the crude compound was purified using column chromatography, followed by recrystallization from diethyl ether. Crystal data were collected on a Rigaku XtaLAB Synergy-i diffractometer (Rigaku Co., Tokyo, Japan) using the graphitemonochromated Cu-Kα radiation at 93.15 K, which are provided in Table 1. The initial structure was solved using an intrinsic phasing method with SHELXT-2018.5 All non-hydrogen atoms were refined using the full-matrix least-squares method on F2 by utilizing SHELXL-2018.6 All calculations were performed using Olex2 crystallographic software.7 Crystallographic data have been deposited to the Cambridge Crystallographic Data Center (CCDC-2075942). The absolute structure of this crystal was determined by X-ray diffraction method (Flack’s parameter: 0.006(11)). The ORTEP drawing is shown in Fig. 2, and selected bond lengths and angles are listed in Table 2. The S1– C4 bond length is 1.778(3)Å as a reasonable single-bond. The N2–C4 bond length of 1.256(4)Å is shorter than the N2–C6 bond length [1.472(4)Å] and is considered to form a double-bond. The thiazoline ring, defined by S1–C4–N2–C6–C5, forms a distorted five-membered ring from the ring strain (C4–S1–C5, 2021 © The Japan Society for Analytical Chemistry

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2-（1-苯甲酰基氮杂环丁烷-3-基）硫代-1,3-噻唑啉的晶体结构

替比芬酯是一种口服1β-甲基碳青霉烯类抗生素，具有广谱和强效抗菌活性，对各种细菌具有抗菌活性，但铜绿假单胞菌除外，它在C-2位具有[1-（1,3-噻唑啉-2-基）氮杂环丁烷-3-基]硫基部分作为侧链，并且也被引入到正在开发的抗生素T405中。2然而，除了具有硫基的替比苯新酯外，还没有对1-（1,3-噻唑啉-2-基）氮杂环丁烷-3-硫醇及其合成前体的晶体结构研究的报道。3在本文中，我们描述了2-（1-苯甲酰基氮杂环丁烷-2-基）硫-1,3-噻唑啉的X射线晶体结构（图1），其是1-（1,3-噻唑啉-2-基）氮杂环丁烷-3-硫醇的合成前体。标题化合物是通过1-氮杂双环[1.1.0]丁烷和3-苯甲酰基-1,3-噻唑烷-2-硫酮在路易斯酸如Mg（OTf）2存在下反应合成的。然后，使用柱色谱法纯化粗化合物，然后从乙醚中重结晶。在Rigaku XtaLAB Synergy-i衍射仪（Rigaku Co.，Tokyo，Japan）上使用93.15K的图形单铬酸盐Cu-Kα辐射收集晶体数据，如表1所示。初始结构使用SHELXT-2018.5所有非氢原子都使用SHELXL-2018.6所有计算都使用Olex2晶体学软件进行。7晶体学数据已存入剑桥晶体学数据中心（CCDC-2075942）。该晶体的绝对结构通过X射线衍射法测定（Flack参数：0.006（11））。ORTEP图如图所示。表2中列出了所选的键长和角度。作为一个合理的单键，S1–C4键长为1.778（3）Å。1.256（4）Å的N2–C4键长比N2–C6键长[1.472（4）å]短，并且被认为形成双键。由S1–C4–N2–C6–C5定义的噻唑啉环由环应变形成扭曲的五元环（C4–S1–C5，2021©日本分析化学学会

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X-ray Structure Analysis Online CRYSTALLOGRAPHY-

CiteScore

0.60

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50.00%

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