Multiple-Component Condensation Methods for Preparation of Combinatorial Libraries of β-Amino Carbonyl Derivatives

Multiple-Component Condensation Methods for the Preparation of Combinatorial Libraries of β-Amino Carbonyl Derivatives

ChemInform ◽

10.1002/chin.200640265 ◽

2006 ◽

Vol 37 (40) ◽

Author(s):

Jr. Adrian, James C.

Keyword(s):

Combinatorial Libraries ◽

Carbonyl Derivatives ◽

Multiple Component

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A stereoselective, multiple-component approach to $alpha;?$beta;-substituted-$beta;-amino carbonyl derivatives*1

Tetrahedron Letters ◽

10.1016/s0040-4039(04)01006-8 ◽

2004 ◽

Author(s):

A JOFFE

Keyword(s):

Carbonyl Derivatives ◽

Component Approach ◽

Multiple Component ◽

Alpha Beta

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A Stereoselective, Multiple-Component Approach to α,β-Substituted-β-amino Carbonyl Derivatives.

ChemInform ◽

10.1002/chin.200441093 ◽

2004 ◽

Vol 35 (41) ◽

Author(s):

Avrum L. Joffe ◽

Timothy M. Thomas ◽

James C. Jr. Adrian

Keyword(s):

Carbonyl Derivatives ◽

Component Approach ◽

Multiple Component

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A stereoselective, multiple-component approach to α–β-substituted-β-amino carbonyl derivatives

Tetrahedron Letters ◽

10.1016/j.tetlet.2004.04.170 ◽

2004 ◽

Vol 45 (26) ◽

pp. 5087-5090 ◽

Cited By ~ 13

Author(s):

Avrum L. Joffe ◽

Timothy M. Thomas ◽

James C. Adrian

Keyword(s):

Carbonyl Derivatives ◽

Component Approach ◽

Multiple Component

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Pollutant Identification by Selected Area Electron Diffraction

Proceedings, annual meeting, Electron Microscopy Society of America ◽

10.1017/s0424820100052675 ◽

1974 ◽

Vol 32 ◽

pp. 532-533

Author(s):

R. E. Ferrell ◽

G. G. Paulson ◽

C. W. Walker

Keyword(s):

Thermal Treatment ◽

Electron Diffraction ◽

Sample Preparation ◽

Crystal Structures ◽

Water Samples ◽

Environmental Samples ◽

Short Review ◽

Selected Area Electron Diffraction ◽

Multiple Component

Selected area electron diffraction (SAD) has been used successfully to determine crystal structures, identify traces of minerals in rocks, and characterize the phases formed during thermal treatment of micron-sized particles. There is an increased interest in the method because it has the potential capability of identifying micron-sized pollutants in air and water samples. This paper is a short review of the theory behind SAD and a discussion of the sample preparation employed for the analysis of multiple component environmental samples.

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Application of Combinatorial Libraries and Protein Engineering to the Discovery of Novel Anti-Thrombotic Drugs

Thrombosis and Haemostasis ◽

10.1055/s-0038-1642705 ◽

1995 ◽

Vol 74 (01) ◽

pp. 373-376 ◽

Cited By ~ 2

Author(s):

Lawrence L.K Leung

Keyword(s):

Protein Engineering ◽

Combinatorial Libraries

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Automated, Accurate, and Scalable Relative Protein-Ligand Binding Free Energy Calculations using Lambda Dynamics

10.26434/chemrxiv.12781310.v1 ◽

2020 ◽

Author(s):

E. Prabhu Raman ◽

Thomas J. Paul ◽

Ryan L. Hayes ◽

Charles L. Brooks III

Keyword(s):

Free Energy ◽

Ligand Binding ◽

Binding Affinity ◽

Binding Free Energy ◽

Computational Cost ◽

Combinatorial Libraries ◽

Free Energy Calculations ◽

Lead Optimization ◽

Efficient Estimation ◽

Lead Compound

<p>Accurate predictions of changes to protein-ligand binding affinity in response to chemical modifications are of utility in small molecule lead optimization. Relative free energy perturbation (FEP) approaches are one of the most widely utilized for this goal, but involve significant computational cost, thus limiting their application to small sets of compounds. Lambda dynamics, also rigorously based on the principles of statistical mechanics, provides a more efficient alternative. In this paper, we describe the development of a workflow to setup, execute, and analyze Multi-Site Lambda Dynamics (MSLD) calculations run on GPUs with CHARMm implemented in BIOVIA Discovery Studio and Pipeline Pilot. The workflow establishes a framework for setting up simulation systems for exploratory screening of modifications to a lead compound, enabling the calculation of relative binding affinities of combinatorial libraries. To validate the workflow, a diverse dataset of congeneric ligands for seven proteins with experimental binding affinity data is examined. A protocol to automatically tailor fit biasing potentials iteratively to flatten the free energy landscape of any MSLD system is developed that enhances sampling and allows for efficient estimation of free energy differences. The protocol is first validated on a large number of ligand subsets that model diverse substituents, which shows accurate and reliable performance. The scalability of the workflow is also tested to screen more than a hundred ligands modeled in a single system, which also resulted in accurate predictions. With a cumulative sampling time of 150ns or less, the method results in average unsigned errors of under 1 kcal/mol in most cases for both small and large combinatorial libraries. For the multi-site systems examined, the method is estimated to be more than an order of magnitude more efficient than contemporary FEP applications. The results thus demonstrate the utility of the presented MSLD workflow to efficiently screen combinatorial libraries and explore chemical space around a lead compound, and thus are of utility in lead optimization.</p>

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