skip to main content
US FlagAn official website of the United States government
dot gov icon
Official websites use .gov
A .gov website belongs to an official government organization in the United States.
https lock icon
Secure .gov websites use HTTPS
A lock ( lock ) or https:// means you've safely connected to the .gov website. Share sensitive information only on official, secure websites.

Explore Research Products in the PAR
It may take a few hours for recently added research products to appear in PAR search results.


Title: Synthetic glycosidases for the precise hydrolysis of oligosaccharides and polysaccharides
Glycosidases are an important class of enzymes for performing the selective hydrolysis of glycans. Although glycans can be hydrolyzed in principle by acidic water, hydrolysis with high selectivity using nonenzymatic catalysts is an unachieved goal. Molecular imprinting in cross-linked micelles afforded water-soluble polymeric nanoparticles with a sugar-binding boroxole in the imprinted site. Post-modification installed an acidic group near the oxygen of the targeted glycosidic bond, with the acidity and distance of the acid varied systematically. The resulting synthetic glycosidase hydrolyzed oligosaccharides and polysaccharides in a highly controlled fashion simply in hot water. These catalysts not only broke down amylose with similar selectivities to those of natural enzymes, but they also could be designed to possess selectivity not available with biocatalysts. Substrate selectivity was mainly determined by the sugar residues bound within the active site, including their spatial orientations. Separation of the product was accomplished through in situ dialysis, and the catalysts left behind could be used multiple times with no signs of degradation. This work illustrates a general method to construct synthetic glycosidases from readily available building blocks via self-assembly, covalent capture, and post-modification. In addition, controlled, precise, one-step hydrolysis is an attractive way to prepare complex glycans from naturally available carbohydrate sources.  more » « less
Award ID(s):
1708526
PAR ID:
10218663
Author(s) / Creator(s):
;
Date Published:
Journal Name:
Chemical Science
Volume:
12
Issue:
1
ISSN:
2041-6520
Page Range / eLocation ID:
374 to 383
Format(s):
Medium: X
Sponsoring Org:
National Science Foundation
More Like this
  1. ; (, Organic & Biomolecular Chemistry)
    Rational design of synthetic catalysts that mimic enzymes in catalysis and substrate selectivity is a long-standing goal of chemists. We report bottom-up synthesis of artificial acetal hydrolase that hydrolyzes its substrate with high selectivity under otherwise impossible neutral and basic conditions. Our synthetic method allows facile modification of the active site, including introduction of a local water pool near the acetal group of the bound substrate to alter the catalytic mechanism, or installment of a secondary catalytic group to enhance the catalytic activity. 
    more » « less
  2. ; ; ; ; ; ; ; ; (, Chemical Science)
    The challenge of site-selectivity must be overcome in many chemical research contexts, including selective functionalization in complex natural products and labeling of one biomolecule in a living system. Synthetic catalysts incorporating molecular recognition domains can mimic naturally-occurring enzymes to direct a chemical reaction to a particular instance of a functional group. We propose that DNA-conjugated small molecule catalysts (DCats), prepared by tethering a small molecule catalyst to a DNA aptamer, are a promising class of reagents for site-selective transformations. Specifically, a DNA-imidazole conjugate able to increase the rate of ester hydrolysis in a target ester by >100-fold compared with equimolar untethered imidazole was developed. Other esters are unaffected. Furthermore, DCat-catalyzed hydrolysis follows enzyme-like kinetics and a stimuli-responsive variant of the DCat enables programmable “turn on” of the desired reaction. 
    more » « less
  3. ; (, Nanomaterials)
    Aliphatic polycarbonate (PC) can be readily hydrolyzed by lipase, but bisphenol A-derived PC (i.e., BPA-PC) lacks enzyme catalysts for their efficient hydrolysis due to the high hydrophobicity and rigidity of its polymer backbone. This study aims to develop an artificial nanozyme for the selective hydrolysis of small-molecule aromatic carbonates as model substrates for BPA-PC. The catalyst is prepared through molecular imprinting of cross-linkable micelles in a one-pot reaction using a thiourea template and a zinc-containing functional monomer. The resulting water-soluble nanoparticle resembles a hydrolytic metalloenzyme to bind the appropriately shaped aromatic carbonate substrate in the active site, with the nearby zinc acting as a cofactor to activate a water molecule for the nucleophilic attack on the carbonate. Catalytic hydrolysis is observed at room temperature and pH 7, with a rate acceleration of 1,000,000 for diphenyl carbonate. 
    more » « less
  4. ; ; (, ACS Sustainable Chemistry & Engineering)
    Post-consumer polyethylene terephthalate (PET) was hydrolyzed in pure water over a wide range of temperatures (190−400 °C) and pressures (1−35 MPa) to produce terephthalic acid (TPA). Solid or molten PET was subjected to water as a saturated vapor, superheated vapor, saturated liquid, compressed liquid, and supercritical fluid. The highest TPA yields were observed for the hydrolysis of molten PET in saturated liquid water. Isothermal and non-isothermal hydrolysis of PET was also explored. Rapidly heating the reactor contents at about 5−10 °C/s (“fast” hydrolysis) led to high TPA yields, as did isothermal PET hydrolysis, but within 1 min instead of 30 min. Notably, these conditions resulted in the lowest environmental energy impact metric observed to date for uncatalyzed hydrolysis. 
    more » « less
  5. ; ; ; ; ; (, WIREs Computational Molecular Science)
    Abstract The hydrolysis of extremely stable peptide and phosphoester bonds by metalloenzymes is of great interest in biotechnology and industry. However, due to various shortcomings only a handful of these enzymes have been used for industrial applications. Therefore, in the last two decades intensive scientific efforts have been made in rational development of small molecules to imitate the activities of natural enzymes. Despite these efforts, their currently available synthetic analogues are inferior in terms of selectivity, catalytic rate, and turnover and the designing of efficient artificial metalloenzymes remains a distant goal. This is a challenging area of research that necessitates a rigorous integration between experiments and theory. The realization of this goal requires knowledge of the catalytic activities of both enzymes and their existing analogues and an effective fusion of that knowledge. This article reviews several studies in which a plethora of computational techniques have been successfully employed to investigate the functioning of two chemically promiscuous mono‐ and binuclear metalloenzymes (insulin degrading enzyme and glycerophosphodiesterase) and two synthetic analogues. These studies will help us derive fundamental principles of peptide and phosphoester hydrolysis and pave the way to design efficient small molecule catalysts for these reactions. This article is categorized under:Structure and Mechanism > Reaction Mechanisms and Catalysis 
    more » « less
  • Citation Formats
  • MLA
  • APA
  • Chicago
  • BibTeX
  • Save / Share this Record
  • Send to Email