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Research
Research in our laboratory consists of the
development and application of computational methods to diverse
systems of interest. The research projects are interdisciplinary
in nature, including subjects from organic chemistry, physical
chemistry, analytical chemistry, inorganic chemistry and
biochemistry. The group utilizes various computational tools
such as Gaussian 98/03, GAMESS, CHARMM, AMBER, MOE, CAChe,
UHBD, NAMD, and DL_POLY. Students in the group interact with faculty
members within the Department as well as faculty from Pitt
and PSC. Students also work with and visit scientists at IBM Almaden
and the Pittsburgh National Energy Technology Laboratory.
CdS
Project
 Description:
This project centers on the structure and electronic properties
of encapsulated cadmium sulfide nanoparticles. Our
interest is to understand the fundamental principles that lead
to stable, functionalized quantum dots. The
challenge of creating functionalized, robust quantum
confined group II-VI semiconductor nanoclusters (NC’s) involves
the ability to realize size-controlled and size-stable nanocrystallites.
The objective is to provide atomistic-level and fundamental insight
into the structure, stability and aqueous assembly of CdS NC’s
and of higher-order NC architectures with unique
physical properties.
Goals: The goals of
this project are to develop and apply computational protocols to
study organic and peptide encapsulated CdS nanoparticles. To achieve these goals we will make use of quantum mechanical
methods, molecular mechanical methods as well as Brownian dynamics
methods. Using these
computational methods we will explore the structure and electronic
properties of these nanoparticles. The broader impacts of the proposed
activity efforts focus upon the training and education of future
scientists in multidisciplinary sciences, and the impact of providing
a novel tool set that will assist scientists in quantum dot research
related to information technology.
Publications
- Nunes,
S.; Zhou, Z.; Evanseck, J. D.; Madura, J.
D. Computational analysis of Cadmium Sulfide (CdS)
Nanocrystals” Encyclopedia of
Nanoscience and Nanotechnology 2004, MarcelDekker Inc.
- Spreitzer,
G. et al. Peptide-encapsulated CdS Nanoclusters from a Combinatorial Ligand Library.
Chemical Communications (Cambridge).
(3), 209-210. 2000.
Oligosaccharide – Protein
Interactions
 Description:
A multi-disciplinary research project that is exploring
sugar – protein interactions
and is developing fundamental
scientific discoveries and advances
leading to a new understanding of biochemistry. This
project is a collaborative project
between a biochemistry group
at the University of South Alabama and here. The
computational component being
undertaken at Duquesne along
with some basic physical characterization
experiments.
Goals: The proposed goals of this project are to
elucidate the important interactions between oligosaccharides
and proteins. This is currently being accomplished
using computational methods, such as free energy
simulations and docking techniques. Additionally
these computations are being supported by isothermal
titration calorimetry and fluorescence experiments. This
research is trying to understand the role of these
proteins has in breast cancer.
Publications
- Aronson, N. N. Jr. et al. Homology Modeling of Glycosyl
Hydrolase Family 18 Enzymes and Proteins. Journal
of Chemical Information and Computer Sciences. 37(6),
999-1005. 1997.
- Dalal, P et al. Molecular Dynamics Simulations
of Oligosaccharide-Protein Interactions. Manuscript
in preparation, 2004
CO2 Sequestration in Brines and Coal
Description: The combustion of fossil fuels releases
large amounts of carbon dioxide into the atmosphere,
which is known to cause global warming. One idea
to get rid of the excess CO2 is to use brine aquifers
to sequester the gas by using mineral trapping in
brine aquifers, where the CO2 is introduced into
solution, converted to carbonate, and associates
ionically with metal ions to from insoluble metal
carbonates. Our interest is to understand how brines
can influence the sequestration of CO2 in brine aquifers.
This project is in collaboration with NETL of Pittsburgh
and Penn State University.
Goals: The goals of this project are to apply computational
techniques to determine the properties under which
CO2 may be best sequestered in brine aquifers. FEP/MC
simulations are used to determine the solubility
of CO2 in various brine solutions and hybrid QM/MM
dynamics simulations are performed to look at the
conversion of CO2 to carbonate in the presence of
high concentrations of ions. Together, these simulations
will provide a molecular explanation of the factors
that most influence the CO2 sequestration process
from a thermodynamic, kinetic, and structural aspect.
Publications
- Dick, T. et al. Molecular basis for carbon dioxide
sequestration in coal.
Preprints of Symposia - American Chemical Society,
Division of Fuel Chemistry, 47(1), 14-16, 2002.
- Dick, Thomas J., et al. Advancements in CO2 Sequestration:
Development and Testing
of Aqueous Parameters for Carbon Dioxide. Manuscript
in preparation.
- Dick, Thomas J., et al. Advancements in CO2 Sequestration:
Solubility of CO2 in
Brines using FEP/MC Simulations,. Manuscript in
preparation.
Metals
in Biology
Description: Recent studies have shown that cells
use proteins called “metallochaperones” to
perform the routing of metal ions to protect the
cell and to ensure delivery to nascent enzymes. However,
the mechanism of binding and relese of metals by
these metallochaperones is not well understood. The
largest protein of the copper chaperone family has
a common structure known as an “open-faced
b-sandwich”, consisting of two a-helices
overlaying four b-strands. An exposed –cys-x-x-cys-
metal binding motif is positioned in a loop near
one end of the protein. A similar motif is seen in
the Thioredoxin family of proteins.The cysteinyl
thiolates in the Thioredoxin family, with markedly
altered pKa’s, serve a catalytic function.
Goals: We are proposing that, as in the Thioredoxin,
the thiolates have perturbed pKa’s and these
differences are important in the release of the metal
ions. A new procedure has been developed to calculate
the pKa value of the cysteines in both Thioredoxin
and metallochaperones proteins. We use state-of-the
art computational chemistry to make such calculations.
Publications
- Esposito, E. X. et al. Docking Substrates To
Metalloenzymes. Molecular Simulation. 24(4-6),
293-306. 2001
- R. R. Radwan et al. Determination of Cysteine
pKas in a Copper Chaperone Protein. Manuscript
in preparation, 2004.
- R. R. Radwan et al., pKa of metalloproteins ligand,
Manuscript in preparation,
2004.
Nitrile Anion Structure and Reactivity
Description: The nitrile functional group is a small,
under-utilized unit in organic synthesis. However,
it has been demonstrated that this functional group
can be used in the synthesis of complex organic compounds. In
particular the stereochemistry of cis/trans decalin
systems. Fundamental insight on how nitrile
anions operate is not fully realized. Computational
methods are being applied to study these systems
Goals: The goal is to use ab initio methods to elucidate
the role solvent and counter-ions have on the structure
and reactivity of nitrile anions and how the solvent
and counter-ions can be used to direct the stereochemistry
of specific reactions involving nitrile anions.
Publications
- Carlier, P. R. et al. Effective Computational Modeling
of Constitutional Isomerism and Aggregation States
of Explicit Solvates of Lithiated Phenylacetonitrile.
Journal of Organic Chemistry, 67 (11), 3832-3840.
2002
Proteins
at Ice/Water Interfaces
 Description: Antifreeze Proteins (AFPs) found
in fish, plants and insects help the organisms to
survive cold temperatures. Various applications
of such molecules are in agricultural (grain preservation
and transgenic plants), medicine
(organ preservation and cryosurgery), aerospace (wing
de-icers) and other industries.
Goals: The goal of this project is to apply various
computational techniques such as MM, MD and QSAR
to elucidate the molecular mechanism of these proteins. As
an outcome of this research a more potent antifreeze
molecule will be proposed for industrial use.
Publications
- Dalal, P., et al., Hydrogen bond analysis of type
1 antifreeze protein in water and the ice/water interface.
PhysChemComm,: Paper No. 7. 2001
- Dalal, P., et al., "Antifreeze" Proteins
at the Ice/Water Interface:
Three calculated discriminating properties for
orientation of Type I proteins. Manuscript in Preparation,
2004.
Proteins
and Inorganic Crystals at Lipid/Water Interfaces
Description: This project investigates a) the mechanism
of inflammatory diseases such as arthritis and pseudogout
and b) the mechanism of protection of lipid membrane
by antifreeze proteins. Our interest is to understand
the mechanism of interaction of different molecules
with lipid membranes.
Goals: The goals of this project are to apply computational
techniques to determine the mechanisms of interaction. Specifically,
we will use molecular mechanics and molecular dynamics
methods to model the interaction between lipid and
inorganic crystal such as Calcium Pyrophosphate
Dihydrate (CPPD) in order to determine the molecular
mechanism of pseudogout. On the other hand similar
models involving lipid membranes will be developed
to understand the protection offered by such proteins
onto the membranes during thermal stress.
Publications
- Wierzbicki, A. et al. Molecular dynamics simulations
of crystal induced membranolysis.
J. Phys. Chem. B 107, 12346-12351, 2003.
- Dalal, P., et al. Molecular dynamics simulations
of inhibition of crystal
induced membranolysis. Manuscript in Preparation,
2004.
Melatonin
Receptors
 Description: This project involves creating
structures of G-Protein Coupled Receptors (GPCRs)
through a technique called “comparative modeling.” The
GPCRs of interest are the melatonin receptors (MT1
and MT2), which belong to the rhodopsin family. Specific,
highly conserved motifs of these models that contain
key mutations are being analyzed in order to elucidate
their function. Currently, there is collaboration
between the computational chemistry group and pharmacy
group at Duquesne in hopes that this family of receptors
can be better understood.
Goals: The goals of this project are to use programs
like MOE and Modeller to create structures for the
melatonin receptors using rhodopsin as a template
model. At the moment rhodopsin is the only GPCR
whose structure has been solved through X-Ray Diffraction
and NMR methods. Once sufficient models have
been created and evaluated through programs such
as PROCHECK or 3D-Profiler different motifs will
be analyzed using MOE and BioCAChe. Specifically,
different ligands will be docked into the models
using Grid-based methods.
HIV-RT
Inhibitors
Description: HIV-1 reverse transcriptase (RT) is
an important target for drugs used in the treatment
of AIDS. Drugs known as non-nucleoside RT inhibitors
(NNRTI) appear to alter the structural and dynamical
properties of RT which in turn inhibit RTs ability
to transcribe. Molecular dynamics, principal component
analysis and binding free energy simulations are
employed to explore the dynamics of RT and its interaction
with a bound NNRTI, for both wild type and mutant
RT. We show that a bound NNRTI hinders the motion
of RT subdomains. Mutations in the non-nucleoside
RT inhibitor binding pocket partially restore RT
flexibility.
Goals: The goal of this project is to understand
the impact of protein dynamics plays in the activity
of this enzyme. In addition we are trying to
elucidate the mutations play in drug resistance by
potentially restoring the required dynamical motion
of the enzyme.
Publications
- Zhou, Z. et al. Docking of Non-nucleoside Inhibitors:
Neotripterifordin and
its Derivatives to HIV-1 Reverse Transcriptase,
Proteins: Structure, Function, and Genetics. 49(4),
529-542. 2002
- Zhou, Z. and J.D. Madura Relative Free Energy
of Binding and Binding Mode Calculations of HIV-1
RT Inhibitors Based on Dock-MM-PB/GS. In press,
Proteins, 2004.
- Zhou, Z., and J.D. Madura, 3D-QSAR CoMFA and
Docking Study on HIV-1 RT Non-nuclesodie inhibitors,
TIBO derivatives. Submitted JCICS, 2004.
- Zhou, Z., Madrid, M., Evanseck, J., Madura, J.
Effect of a bound non-nucleoside RT inhibitor on
the dynamics of HIV-1 Reverse Transcriptase, In
preparation, Proteins, 2004.
Methane
Hydrates
Description: Gas clathrates are viable energy resources.
Methane stored in naturally occurring clathrates
potentially hold enough methane to ensure supply
for many years; methane clathrates are also known
to cause blockage in the natural gas pipelines. Clathrates
have also been discussed as possible storage sites
in CO2 sequestration. Although these have been known
about for over a century, there is little known about
the clusters on an atomistic scale and what structural
properties are critical in the formation and dissipation
of gas clathrates.
Goals: The goals of this project are to apply computational
techniques to determine the properties under which
clathrates may be utilized as effective energy sources.
QM calculations are used to determine stable clathrate
structures and to calculate the interaction energy
between the gas and the clathrate shell. MC simulations
map out the phase diagram of the clathrate and provide
structural information on the average configurations
of the clathrates under their naturally occurring
conditions. Together, these simulations will provide
an understanding of the formation, dissipation, and
gas exchange of clathrates from a thermodynamic and
structural viewpoint.
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