Optimizations of Hydroxyl Terminated Polymerization of Mannose Tricyclic Orthoester Toward Ready-to-use Lipomannan Backbone

Optimizations of Hydroxyl Terminated Polymerization of Mannose Tricyclic Orthoester Toward Ready-to-use Lipomannan Backbone

Throughout the life cycle of mycobacterium tuberculosis (Mtb), its survival critically depends on its interactions with mammalian host cells. Therefore, in order to have better treatments for and preventions of tuberculosis (TB), it is important to understand the biological activity of the Mtb surfa...

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Main Authors: Harin Leelayuwapan, Somsak Ruchirawat, Siwarutt Boonyarattanakalin
Language:English
Published: Science Faculty of Chiang Mai University 2019
Subjects:
polymannan
carbohydrate
Mycobacterium tuberculosis (Mtb)
lipomannan (LM)
Online Access:http://it.science.cmu.ac.th/ejournal/dl.php?journal_id=6345
http://cmuir.cmu.ac.th/jspui/handle/6653943832/66066
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Institution: Chiang Mai University
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spelling th-cmuir.6653943832-660662019-08-21T09:18:20Z Optimizations of Hydroxyl Terminated Polymerization of Mannose Tricyclic Orthoester Toward Ready-to-use Lipomannan Backbone Harin Leelayuwapan Somsak Ruchirawat Siwarutt Boonyarattanakalin polymannan carbohydrate Mycobacterium tuberculosis (Mtb) lipomannan (LM) Throughout the life cycle of mycobacterium tuberculosis (Mtb), its survival critically depends on its interactions with mammalian host cells. Therefore, in order to have better treatments for and preventions of tuberculosis (TB), it is important to understand the biological activity of the Mtb surface components. a-1,6 Polymannan, the backbone of lipomannan (LM), is present abundantly on the surface of mycobacterium tuberculosis and interacts with mammalian hosts. Conjugation of polymannan with thiol linker comprises an essential biochemical tool to study the Mtb surface interactions with mammalian hosts. A short alkyl chain with hydroxyl head group is employed to attach to the reducing end of the polysaccharide via a glycosidic bond, and with a terminal thiol group to serve as a linker. The target - conjugated polymannan with thiol linker is achieved by a rapid synthetic route, relying on a ring-opening polymerization, using a tricyclic mannosyl orthoester as monomer. The ring-opening polymerization, triggered by a Lewis acid without the presence of the linker, was previously proposed to be terminated by water at the reducing end. However, in the present study, the results suggest that the polymerization may also be initiated from the reducing end by the attack of the hydroxyl head group of a short chain alkyl thiol linker. After that, an elongation of the growing polysaccharide may be achieved via the propagation to the non-reducing end. Optimizations for the polymerization and termination in a one-pot reaction were carried out. A half gram of the synthetic target molecule is attained in a single chemical step. The target synthetic bacterial surface molecule is in a ready-to-use form to be utilized further in several applications, such as immobilization on surfaces and conjugation to carrier proteins for biological and immunological studies. This biochemical tool may lead us to a better understanding on carbohydrate-based biointerfaces between the bacteria pathogen and the human immune system. 2019-08-21T09:18:20Z 2019-08-21T09:18:20Z 2016 Chiang Mai Journal of Science 43, 1 (Jan 2016), 138 - 146 0125-2526 http://it.science.cmu.ac.th/ejournal/dl.php?journal_id=6345 http://cmuir.cmu.ac.th/jspui/handle/6653943832/66066 Eng Science Faculty of Chiang Mai University
institution Chiang Mai University
building Chiang Mai University Library
country Thailand
collection CMU Intellectual Repository
language English
topic polymannan
carbohydrate
Mycobacterium tuberculosis (Mtb)
lipomannan (LM)
spellingShingle polymannan
carbohydrate
Mycobacterium tuberculosis (Mtb)
lipomannan (LM)
Harin Leelayuwapan
Somsak Ruchirawat
Siwarutt Boonyarattanakalin
Optimizations of Hydroxyl Terminated Polymerization of Mannose Tricyclic Orthoester Toward Ready-to-use Lipomannan Backbone
description Throughout the life cycle of mycobacterium tuberculosis (Mtb), its survival critically depends on its interactions with mammalian host cells. Therefore, in order to have better treatments for and preventions of tuberculosis (TB), it is important to understand the biological activity of the Mtb surface components. a-1,6 Polymannan, the backbone of lipomannan (LM), is present abundantly on the surface of mycobacterium tuberculosis and interacts with mammalian hosts. Conjugation of polymannan with thiol linker comprises an essential biochemical tool to study the Mtb surface interactions with mammalian hosts. A short alkyl chain with hydroxyl head group is employed to attach to the reducing end of the polysaccharide via a glycosidic bond, and with a terminal thiol group to serve as a linker. The target - conjugated polymannan with thiol linker is achieved by a rapid synthetic route, relying on a ring-opening polymerization, using a tricyclic mannosyl orthoester as monomer. The ring-opening polymerization, triggered by a Lewis acid without the presence of the linker, was previously proposed to be terminated by water at the reducing end. However, in the present study, the results suggest that the polymerization may also be initiated from the reducing end by the attack of the hydroxyl head group of a short chain alkyl thiol linker. After that, an elongation of the growing polysaccharide may be achieved via the propagation to the non-reducing end. Optimizations for the polymerization and termination in a one-pot reaction were carried out. A half gram of the synthetic target molecule is attained in a single chemical step. The target synthetic bacterial surface molecule is in a ready-to-use form to be utilized further in several applications, such as immobilization on surfaces and conjugation to carrier proteins for biological and immunological studies. This biochemical tool may lead us to a better understanding on carbohydrate-based biointerfaces between the bacteria pathogen and the human immune system.
author Harin Leelayuwapan
Somsak Ruchirawat
Siwarutt Boonyarattanakalin
author_facet Harin Leelayuwapan
Somsak Ruchirawat
Siwarutt Boonyarattanakalin
author_sort Harin Leelayuwapan
title Optimizations of Hydroxyl Terminated Polymerization of Mannose Tricyclic Orthoester Toward Ready-to-use Lipomannan Backbone
title_short Optimizations of Hydroxyl Terminated Polymerization of Mannose Tricyclic Orthoester Toward Ready-to-use Lipomannan Backbone
title_full Optimizations of Hydroxyl Terminated Polymerization of Mannose Tricyclic Orthoester Toward Ready-to-use Lipomannan Backbone
title_fullStr Optimizations of Hydroxyl Terminated Polymerization of Mannose Tricyclic Orthoester Toward Ready-to-use Lipomannan Backbone
title_full_unstemmed Optimizations of Hydroxyl Terminated Polymerization of Mannose Tricyclic Orthoester Toward Ready-to-use Lipomannan Backbone
title_sort optimizations of hydroxyl terminated polymerization of mannose tricyclic orthoester toward ready-to-use lipomannan backbone
publisher Science Faculty of Chiang Mai University
publishDate 2019
url http://it.science.cmu.ac.th/ejournal/dl.php?journal_id=6345
http://cmuir.cmu.ac.th/jspui/handle/6653943832/66066
_version_ 1681426385817567232

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