Tunable Strategy for the Asymmetric Synthesis of Sulfoglycolipids from Mycobacterium tuberculosis To Elucidate the Structure and Immunomodulatory Property Relationships

Soumik Mondal; Chieh Jen Tseng; Janet Jia Yin Tan; Ding Yuan Lin; Hsien Ya Lin; Jui–Hsia H. Weng; Chun Hung Lin; Kwok Kong Tony Mong

doi:10.1002/anie.202212514

Tunable Strategy for the Asymmetric Synthesis of Sulfoglycolipids from Mycobacterium tuberculosis To Elucidate the Structure and Immunomodulatory Property Relationships

Soumik Mondal, Chieh Jen Tseng, Janet Jia Yin Tan, Ding Yuan Lin, Hsien Ya Lin, Jui–Hsia H. Weng, Chun Hung Lin^*, Kwok Kong Tony Mong^*

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摘要

We developed a versatile asymmetric strategy to synthesize different classes of sulfoglycolipids (SGLs) from Mycobacterium tuberculosis. The strategy features the use of asymmetrically protected trehaloses, which were acquired from the glycosylation of TMS α-glucosyl acceptors with benzylidene-protected thioglucosyl donors. The positions of the protecting groups at the donors and acceptors can be fine-tuned to obtain different protecting-group patterns, which is crucial for regioselective acylation and sulfation. In addition, a chemoenzymatic strategy was established to prepare the polymethylated fatty acid building blocks. The strategy employs inexpensive lipase as a desymmetrization agent in the preparation of the starting substrate and readily available chiral oxazolidinone as a chirality-controlling agent in the construction of the polymethylated fatty acids. A subsequent investigation on the immunomodulatory properties of each class of SGLs showed how the structures of SGLs impact the host innate immunity response.

原文	English
文章編號	e202212514
期刊	Angewandte Chemie - International Edition
卷	62
發行號	1
DOIs	https://doi.org/10.1002/anie.202212514
出版狀態	Published - 2 1月 2023

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10.1002/anie.202212514

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Mondal, S., Tseng, C. J., Tan, J. J. Y., Lin, D. Y., Lin, H. Y., Weng, JH. H., Lin, C. H., & Mong, K. K. T. (2023). Tunable Strategy for the Asymmetric Synthesis of Sulfoglycolipids from Mycobacterium tuberculosis To Elucidate the Structure and Immunomodulatory Property Relationships. Angewandte Chemie - International Edition, 62(1), 文章 e202212514. https://doi.org/10.1002/anie.202212514

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abstract = "We developed a versatile asymmetric strategy to synthesize different classes of sulfoglycolipids (SGLs) from Mycobacterium tuberculosis. The strategy features the use of asymmetrically protected trehaloses, which were acquired from the glycosylation of TMS α-glucosyl acceptors with benzylidene-protected thioglucosyl donors. The positions of the protecting groups at the donors and acceptors can be fine-tuned to obtain different protecting-group patterns, which is crucial for regioselective acylation and sulfation. In addition, a chemoenzymatic strategy was established to prepare the polymethylated fatty acid building blocks. The strategy employs inexpensive lipase as a desymmetrization agent in the preparation of the starting substrate and readily available chiral oxazolidinone as a chirality-controlling agent in the construction of the polymethylated fatty acids. A subsequent investigation on the immunomodulatory properties of each class of SGLs showed how the structures of SGLs impact the host innate immunity response.",

keywords = "1,1′-Glycosylation, Asymmetric Trehaloses, Deoxypropionates, Oxazolidinones, Sulfoglycolipids",

author = "Soumik Mondal and Tseng, {Chieh Jen} and Tan, {Janet Jia Yin} and Lin, {Ding Yuan} and Lin, {Hsien Ya} and Weng, {Jui–Hsia H.} and Lin, {Chun Hung} and Mong, {Kwok Kong Tony}",

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doi = "10.1002/anie.202212514",

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Mondal, S, Tseng, CJ, Tan, JJY, Lin, DY, Lin, HY, Weng, JHH, Lin, CH & Mong, KKT 2023, 'Tunable Strategy for the Asymmetric Synthesis of Sulfoglycolipids from Mycobacterium tuberculosis To Elucidate the Structure and Immunomodulatory Property Relationships', Angewandte Chemie - International Edition, 卷 62, 編號 1, e202212514. https://doi.org/10.1002/anie.202212514

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T1 - Tunable Strategy for the Asymmetric Synthesis of Sulfoglycolipids from Mycobacterium tuberculosis To Elucidate the Structure and Immunomodulatory Property Relationships

AU - Mondal, Soumik

AU - Tseng, Chieh Jen

AU - Tan, Janet Jia Yin

AU - Lin, Ding Yuan

AU - Lin, Hsien Ya

AU - Weng, Jui–Hsia H.

AU - Lin, Chun Hung

AU - Mong, Kwok Kong Tony

PY - 2023/1/2

Y1 - 2023/1/2

N2 - We developed a versatile asymmetric strategy to synthesize different classes of sulfoglycolipids (SGLs) from Mycobacterium tuberculosis. The strategy features the use of asymmetrically protected trehaloses, which were acquired from the glycosylation of TMS α-glucosyl acceptors with benzylidene-protected thioglucosyl donors. The positions of the protecting groups at the donors and acceptors can be fine-tuned to obtain different protecting-group patterns, which is crucial for regioselective acylation and sulfation. In addition, a chemoenzymatic strategy was established to prepare the polymethylated fatty acid building blocks. The strategy employs inexpensive lipase as a desymmetrization agent in the preparation of the starting substrate and readily available chiral oxazolidinone as a chirality-controlling agent in the construction of the polymethylated fatty acids. A subsequent investigation on the immunomodulatory properties of each class of SGLs showed how the structures of SGLs impact the host innate immunity response.

AB - We developed a versatile asymmetric strategy to synthesize different classes of sulfoglycolipids (SGLs) from Mycobacterium tuberculosis. The strategy features the use of asymmetrically protected trehaloses, which were acquired from the glycosylation of TMS α-glucosyl acceptors with benzylidene-protected thioglucosyl donors. The positions of the protecting groups at the donors and acceptors can be fine-tuned to obtain different protecting-group patterns, which is crucial for regioselective acylation and sulfation. In addition, a chemoenzymatic strategy was established to prepare the polymethylated fatty acid building blocks. The strategy employs inexpensive lipase as a desymmetrization agent in the preparation of the starting substrate and readily available chiral oxazolidinone as a chirality-controlling agent in the construction of the polymethylated fatty acids. A subsequent investigation on the immunomodulatory properties of each class of SGLs showed how the structures of SGLs impact the host innate immunity response.

KW - 1,1′-Glycosylation

KW - Asymmetric Trehaloses

KW - Deoxypropionates

KW - Oxazolidinones

KW - Sulfoglycolipids

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U2 - 10.1002/anie.202212514

DO - 10.1002/anie.202212514

M3 - Article

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AN - SCOPUS:85143291570

SN - 1433-7851

VL - 62

JO - Angewandte Chemie - International Edition

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IS - 1

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ER -

Tunable Strategy for the Asymmetric Synthesis of Sulfoglycolipids from Mycobacterium tuberculosis To Elucidate the Structure and Immunomodulatory Property Relationships

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