職員瀏覽: Structure and dynamics of cutinase encapsulated in isoreticular metal organic framework-74-VI

Structure and dynamics of cutinase encapsulated in isoreticular metal organic framework-74-VI

Cutinase is a serine hydrolases enzyme that is widely used as a biocatalyst to produce industrially important chemicals ranging from pharmaceuticals to biological and food additives. However, low thermal stability and lack of efficient recovery are the limitation of cutinase. Enzyme immobilizatio...

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主要作者:	Tuan Kob @ Yaakub, Nurul Azura
格式:	Thesis
語言:	English
出版:	2019
主題:	Hydrolases Metal-organic frameworks
在線閱讀:	http://psasir.upm.edu.my/id/eprint/104348/1/TUAN%20NURUL%20AZURA%20-%20IR.pdf http://psasir.upm.edu.my/id/eprint/104348/
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spelling	my.upm.eprints.1043482023-08-08T02:15:08Z http://psasir.upm.edu.my/id/eprint/104348/ Structure and dynamics of cutinase encapsulated in isoreticular metal organic framework-74-VI Tuan Kob @ Yaakub, Nurul Azura Cutinase is a serine hydrolases enzyme that is widely used as a biocatalyst to produce industrially important chemicals ranging from pharmaceuticals to biological and food additives. However, low thermal stability and lack of efficient recovery are the limitation of cutinase. Enzyme immobilization is one of the techniques used to improve enzyme stability and activity. Recently, immobilization with porous materials such as metalorganic frameworks (MOFs) have shown to improve the thermostability of enzymes even in extreme conditions. Here, quantum mechanics (QM) calculations and molecular dynamics (MD) simulations were performed in order to investigate the structural stability of cutinase when encapsulated within an IRMOF-74-VI. Ab initio calculations were performed on the crystal structure of IRMOF-74-VI to obtain partial atomic charges for IRMOF-74-VI atoms. Then, MD simulations of cutinase and cutinase-IRMOF-74-VI in water were performed at different temperatures (300, 350, 400, 450 and 500 K) and 1 atm pressure. The encapsulated cutinase showed greater stability than the free enzyme. Although the average root mean square deviation (RMSD) value increased for both systems with temperature, the cutinase-IRMOF-74-VI exhibited lower RMSD values when compared to free-cutinase especially at 500 K. IRMOF-74-VI was able to control the strong fluctuations at higher temperatures and thereby, helped retain the cutinase structure. The key interactions that maintained the stability of cutinase were identified, such as hydrophobic interactions between amino acid residues of Pro193 and Thr45 with aromatic ring of IRMOF-74-VI. In addition, ion pair interactions between Arg96 residue and carboxylate group of IRMOF-74-VI was found to have a distance of 4.53 Å and was classified as a strong salt bridge. MD simulations also have been employed to study the effect of encapsulation towards stability and flexibility of cutinase in different solvents (water, ethanol and hexane) at room temperature. Cutinase-IRMOF-74-VI in water and ethanol produced lower RMSD values (0.14 ± 0.006 and 0.17 ± 0.017 nm respectively) compared to cutinase-IRMOF-74-VI in hexane (0.24 ± 0.015 nm). Further analysis also showed that cutinase-IRMOF74-VI complex was more stable in polar solvent. Cutinase- IRMOF-74-VI exhibited the highest number of intermolecular interactions with hexane compared to water and ethanol, leading to the least stable conformation between the three solvents. These findings demonstrate the potential for cutinase-encapsulation applications in cage-like pore frameworks by showing that encapsulation of cutinase with IRMOF-74- VI helps to retain the structural integrity at high temperature. However, IRMOF-74-VI destabilized cutinase in hexane compared to higher polarity solvents which are ethanol and water. This information can be used to optimize cutinase-MOF applications and develop new cutinase-specific MOF for biocatalysis and biosensing purposes. The interactions between cutinase and IRMOF-74-VI under different temperatures and solvents would be beneficial as guideline for future rational design of enzyme-MOF biocatalysts. 2019-12 Thesis NonPeerReviewed text en http://psasir.upm.edu.my/id/eprint/104348/1/TUAN%20NURUL%20AZURA%20-%20IR.pdf Tuan Kob @ Yaakub, Nurul Azura (2019) Structure and dynamics of cutinase encapsulated in isoreticular metal organic framework-74-VI. Masters thesis, Universiti Putra Malaysia. Hydrolases Metal-organic frameworks
institution	Universiti Putra Malaysia
building	UPM Library
collection	Institutional Repository
continent	Asia
country	Malaysia
content_provider	Universiti Putra Malaysia
content_source	UPM Institutional Repository
url_provider	http://psasir.upm.edu.my/
language	English
topic	Hydrolases Metal-organic frameworks
spellingShingle	Hydrolases Metal-organic frameworks Tuan Kob @ Yaakub, Nurul Azura Structure and dynamics of cutinase encapsulated in isoreticular metal organic framework-74-VI
description	Cutinase is a serine hydrolases enzyme that is widely used as a biocatalyst to produce industrially important chemicals ranging from pharmaceuticals to biological and food additives. However, low thermal stability and lack of efficient recovery are the limitation of cutinase. Enzyme immobilization is one of the techniques used to improve enzyme stability and activity. Recently, immobilization with porous materials such as metalorganic frameworks (MOFs) have shown to improve the thermostability of enzymes even in extreme conditions. Here, quantum mechanics (QM) calculations and molecular dynamics (MD) simulations were performed in order to investigate the structural stability of cutinase when encapsulated within an IRMOF-74-VI. Ab initio calculations were performed on the crystal structure of IRMOF-74-VI to obtain partial atomic charges for IRMOF-74-VI atoms. Then, MD simulations of cutinase and cutinase-IRMOF-74-VI in water were performed at different temperatures (300, 350, 400, 450 and 500 K) and 1 atm pressure. The encapsulated cutinase showed greater stability than the free enzyme. Although the average root mean square deviation (RMSD) value increased for both systems with temperature, the cutinase-IRMOF-74-VI exhibited lower RMSD values when compared to free-cutinase especially at 500 K. IRMOF-74-VI was able to control the strong fluctuations at higher temperatures and thereby, helped retain the cutinase structure. The key interactions that maintained the stability of cutinase were identified, such as hydrophobic interactions between amino acid residues of Pro193 and Thr45 with aromatic ring of IRMOF-74-VI. In addition, ion pair interactions between Arg96 residue and carboxylate group of IRMOF-74-VI was found to have a distance of 4.53 Å and was classified as a strong salt bridge. MD simulations also have been employed to study the effect of encapsulation towards stability and flexibility of cutinase in different solvents (water, ethanol and hexane) at room temperature. Cutinase-IRMOF-74-VI in water and ethanol produced lower RMSD values (0.14 ± 0.006 and 0.17 ± 0.017 nm respectively) compared to cutinase-IRMOF-74-VI in hexane (0.24 ± 0.015 nm). Further analysis also showed that cutinase-IRMOF74-VI complex was more stable in polar solvent. Cutinase- IRMOF-74-VI exhibited the highest number of intermolecular interactions with hexane compared to water and ethanol, leading to the least stable conformation between the three solvents. These findings demonstrate the potential for cutinase-encapsulation applications in cage-like pore frameworks by showing that encapsulation of cutinase with IRMOF-74- VI helps to retain the structural integrity at high temperature. However, IRMOF-74-VI destabilized cutinase in hexane compared to higher polarity solvents which are ethanol and water. This information can be used to optimize cutinase-MOF applications and develop new cutinase-specific MOF for biocatalysis and biosensing purposes. The interactions between cutinase and IRMOF-74-VI under different temperatures and solvents would be beneficial as guideline for future rational design of enzyme-MOF biocatalysts.
format	Thesis
author	Tuan Kob @ Yaakub, Nurul Azura
author_facet	Tuan Kob @ Yaakub, Nurul Azura
author_sort	Tuan Kob @ Yaakub, Nurul Azura
title	Structure and dynamics of cutinase encapsulated in isoreticular metal organic framework-74-VI
title_short	Structure and dynamics of cutinase encapsulated in isoreticular metal organic framework-74-VI
title_full	Structure and dynamics of cutinase encapsulated in isoreticular metal organic framework-74-VI
title_fullStr	Structure and dynamics of cutinase encapsulated in isoreticular metal organic framework-74-VI
title_full_unstemmed	Structure and dynamics of cutinase encapsulated in isoreticular metal organic framework-74-VI
title_sort	structure and dynamics of cutinase encapsulated in isoreticular metal organic framework-74-vi
publishDate	2019
url	http://psasir.upm.edu.my/id/eprint/104348/1/TUAN%20NURUL%20AZURA%20-%20IR.pdf http://psasir.upm.edu.my/id/eprint/104348/
_version_	1775624539370160128
score	13.149126

Structure and dynamics of cutinase encapsulated in isoreticular metal organic framework-74-VI

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