Expedient synthesis of E-hydrazone esters and 1H-indazole scaffolds through heterogeneous single-atom platinum catalysis

Cuibo Liu; Zhongxin Chen; Huan Yan; Shibo Xi; Kah Meng Yam; Jiajian Gao; Yonghua Du; Jing Li; Xiaoxu Zhao; Keyu Xie; Haisen Xu; Xing Li; Kai Leng; Stephen J. Pennycook; Bin Liu; Chun Zhang; Ming Joo Koh; Kian Ping Loh

doi:10.1126/sciadv.aay1537

Expedient synthesis of E-hydrazone esters and 1H-indazole scaffolds through heterogeneous single-atom platinum catalysis

Cuibo Liu
, Zhongxin Chen
, Huan Yan
, Shibo Xi
, Kah Meng Yam
, Jiajian Gao
, Yonghua Du
, Jing Li
, Xiaoxu Zhao
, Keyu Xie
, Haisen Xu
, Xing Li
, Kai Leng
, Stephen J. Pennycook
, Bin Liu
, Chun Zhang
, Ming Joo Koh
, Kian Ping Loh

材料学院

National University of Singapore
Agency for Science, Technology and Research, Singapore
Nanyang Technological University
Brookhaven National Laboratory

科研成果: 期刊稿件 › 文章 › 同行评审

36 引用（Scopus）

摘要

Unprotected E-hydrazone esters are prized building blocks for the preparation of 1H-indazoles and countless other N-containing biologically active molecules. Despite previous advances, efficient and stereoselective synthesis of these compounds remains nontrivial. Here, we show that Pt single atoms anchored on defect-rich CeO₂ nanorods (Pt₁/CeO₂), in conjunction with the alcoholysis of ammonia borane, promotes exceptionally E-selective hydrogenation of α-diazoesters to afford a wide assortment of N-H hydrazone esters with an overall turnover frequency of up to 566 hours⁻¹ upon reaction completion. The α-diazoester substrates could be generated in situ from readily available carboxylic esters in one-pot hydrogenation reaction. Utility is demonstrated through concise, scalable synthesis of 1H-indazole–derived pharmaceuticals and their ¹⁵N-labeled analogs. The present protocol highlights a key mechanistic nuance wherein simultaneous coordination of a Pt site with the diazo N=N and ester carbonyl motifs plays a central role in controlling stereoselectivity, which is supported by density functional theory calculations.

源语言	英语
文章编号	eaay1537
期刊	Science Advances
卷	5
期	12
DOI	https://doi.org/10.1126/sciadv.aay1537
出版状态	已出版 - 6 12月 2019

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Liu, C., Chen, Z., Yan, H., Xi, S., Yam, K. M., Gao, J., Du, Y., Li, J., Zhao, X., Xie, K., Xu, H., Li, X., Leng, K., Pennycook, S. J., Liu, B., Zhang, C., Koh, M. J., & Loh, K. P. (2019). Expedient synthesis of E-hydrazone esters and 1H-indazole scaffolds through heterogeneous single-atom platinum catalysis. Science Advances, 5(12), 文章 eaay1537. https://doi.org/10.1126/sciadv.aay1537

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title = "Expedient synthesis of E-hydrazone esters and 1H-indazole scaffolds through heterogeneous single-atom platinum catalysis",

abstract = "Unprotected E-hydrazone esters are prized building blocks for the preparation of 1H-indazoles and countless other N-containing biologically active molecules. Despite previous advances, efficient and stereoselective synthesis of these compounds remains nontrivial. Here, we show that Pt single atoms anchored on defect-rich CeO2 nanorods (Pt1/CeO2), in conjunction with the alcoholysis of ammonia borane, promotes exceptionally E-selective hydrogenation of α-diazoesters to afford a wide assortment of N-H hydrazone esters with an overall turnover frequency of up to 566 hours−1 upon reaction completion. The α-diazoester substrates could be generated in situ from readily available carboxylic esters in one-pot hydrogenation reaction. Utility is demonstrated through concise, scalable synthesis of 1H-indazole–derived pharmaceuticals and their 15N-labeled analogs. The present protocol highlights a key mechanistic nuance wherein simultaneous coordination of a Pt site with the diazo N=N and ester carbonyl motifs plays a central role in controlling stereoselectivity, which is supported by density functional theory calculations.",

author = "Cuibo Liu and Zhongxin Chen and Huan Yan and Shibo Xi and Yam, \{Kah Meng\} and Jiajian Gao and Yonghua Du and Jing Li and Xiaoxu Zhao and Keyu Xie and Haisen Xu and Xing Li and Kai Leng and Pennycook, \{Stephen J.\} and Bin Liu and Chun Zhang and Koh, \{Ming Joo\} and Loh, \{Kian Ping\}",

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doi = "10.1126/sciadv.aay1537",

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T1 - Expedient synthesis of E-hydrazone esters and 1H-indazole scaffolds through heterogeneous single-atom platinum catalysis

AU - Liu, Cuibo

AU - Chen, Zhongxin

AU - Yan, Huan

AU - Xi, Shibo

AU - Yam, Kah Meng

AU - Gao, Jiajian

AU - Du, Yonghua

AU - Li, Jing

AU - Zhao, Xiaoxu

AU - Xie, Keyu

AU - Xu, Haisen

AU - Li, Xing

AU - Leng, Kai

AU - Pennycook, Stephen J.

AU - Liu, Bin

AU - Zhang, Chun

AU - Koh, Ming Joo

AU - Loh, Kian Ping

PY - 2019/12/6

Y1 - 2019/12/6

N2 - Unprotected E-hydrazone esters are prized building blocks for the preparation of 1H-indazoles and countless other N-containing biologically active molecules. Despite previous advances, efficient and stereoselective synthesis of these compounds remains nontrivial. Here, we show that Pt single atoms anchored on defect-rich CeO2 nanorods (Pt1/CeO2), in conjunction with the alcoholysis of ammonia borane, promotes exceptionally E-selective hydrogenation of α-diazoesters to afford a wide assortment of N-H hydrazone esters with an overall turnover frequency of up to 566 hours−1 upon reaction completion. The α-diazoester substrates could be generated in situ from readily available carboxylic esters in one-pot hydrogenation reaction. Utility is demonstrated through concise, scalable synthesis of 1H-indazole–derived pharmaceuticals and their 15N-labeled analogs. The present protocol highlights a key mechanistic nuance wherein simultaneous coordination of a Pt site with the diazo N=N and ester carbonyl motifs plays a central role in controlling stereoselectivity, which is supported by density functional theory calculations.

AB - Unprotected E-hydrazone esters are prized building blocks for the preparation of 1H-indazoles and countless other N-containing biologically active molecules. Despite previous advances, efficient and stereoselective synthesis of these compounds remains nontrivial. Here, we show that Pt single atoms anchored on defect-rich CeO2 nanorods (Pt1/CeO2), in conjunction with the alcoholysis of ammonia borane, promotes exceptionally E-selective hydrogenation of α-diazoesters to afford a wide assortment of N-H hydrazone esters with an overall turnover frequency of up to 566 hours−1 upon reaction completion. The α-diazoester substrates could be generated in situ from readily available carboxylic esters in one-pot hydrogenation reaction. Utility is demonstrated through concise, scalable synthesis of 1H-indazole–derived pharmaceuticals and their 15N-labeled analogs. The present protocol highlights a key mechanistic nuance wherein simultaneous coordination of a Pt site with the diazo N=N and ester carbonyl motifs plays a central role in controlling stereoselectivity, which is supported by density functional theory calculations.

UR - https://www.scopus.com/pages/publications/85076535464

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DO - 10.1126/sciadv.aay1537

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AN - SCOPUS:85076535464

SN - 2375-2548

VL - 5

JO - Science Advances

JF - Science Advances

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ER -

Expedient synthesis of E-hydrazone esters and 1H-indazole scaffolds through heterogeneous single-atom platinum catalysis

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