Presentation is loading. Please wait.

Presentation is loading. Please wait.

Chemical Genomics – Biol503 Lecture 4 Other Applications of Chemical Genomics.

Published by Modified over 9 years ago

Similar presentations

Presentation on theme: "Chemical Genomics – Biol503 Lecture 4 Other Applications of Chemical Genomics."— Presentation transcript:

1 Chemical Genomics – Biol503 Lecture 4 Other Applications of Chemical Genomics

2 Chemical Screening by Mass Spectrometry

3 Chemical Screen Assays Many chemical screening assays rely on fluorescent strategies to report on enzymatic activities However, the need for labels may be a detriment due to: Labels can compromise activity of substrates Some enzymatic assays can not be adapted to fluorescent labels Fluorescent properties of small molecules in the libraries can lead to false positive signals

4 MS Methods Mass Spectrometry based methods avoid the need for labels in analyzing the products of enzymatic reactions because they report on the mass of the substrate, an intrinsic property of every molecule Min et al. described a class of surfaces that both simplifies sample preparation and gives clear and easily interpretable peaks in MS They combine self-assembled monolayers (SAMs) with MALDI-TOF mass spectrometry to discover inhibitors of anthrax lethal factor

5 Anthrax virulence factors Bacillus anthracis secrete three major virulence factors: Protective antigen, it binds to a TEM-8 cell- surface receptor of the host cell and mediates delivery of edema factor and lethal factor into the cytosol Edema factor, an ademylate cyclase that causes edema Lethal factor, a protease that cleaves N terminus of mitogen-activated protein kinase kinase (MAPKK or MEK1)

6 Anthrax lethal factor Lethal factor Source: Min et al Nat Biotech 2004

7 Strategy and Results

8 Dose response curve for compound DS-998 Source: Min et al Nat Biotech 2004

9 Chemical Genomics coupled with MS Source: Min et al Nat Biotech 2004 Cellular Protection Of DS-998

10 Chemical Screening using Microfluidics

11 Microfluidics Microfluidics deals with the behavior, precise control and manipulation of fluids that are geometrically constrained to a small, typically sub-millimeter, scale. Quake Group at Stanford developed a microfluidic platform for measuring binding constants by using mechanical trapping of molecular interactions (MITOMI)

12 Microfluidics The Quake Group studied RNA binding by the HCV transmembrane protein NS4B It was shown that NS4B binds RNA and that this binding is specific for the 3’ terminus of the negative strand of the viral genome with a dissociation constant (K d ) of 3.4 nM. A high throughput microfluidic screen of a compound library identified 18 inhibitors of binding of RNA by NS4B.

13 Maekkl and Quaje, Science 2007 MITOMI (Mechanical Trapping of Molecular Interactions)

14 Chemical Genomics coupled with microfluidics Source: Einav et al Nat Biotech 2008

15 Chemical Genomics coupled with microfluidics Source: Einav et al Nat Biotech 2008

Download ppt "Chemical Genomics – Biol503 Lecture 4 Other Applications of Chemical Genomics."

Similar presentations

ANTHRAX BACTERIUM Protective antigen (PA) Edema factor (EF) Lethal factor (LF) PA+LF combine to produce lethal activity EF+PA produce.

ANTHRAX BACTERIUM Protective antigen (PA) Edema factor (EF) Lethal factor (LF) PA+LF combine to produce lethal activity EF+PA produce.
Cell Communication Cells need to communicate with one another, whether they are located close to each other or far apart. Extracellular signaling molecules.

Cell Communication Cells need to communicate with one another, whether they are located close to each other or far apart. Extracellular signaling molecules.
Molecular Biomedical Informatics Machine Learning and Bioinformatics Machine Learning & Bioinformatics 1.

Molecular Biomedical Informatics Machine Learning and Bioinformatics Machine Learning & Bioinformatics 1.
Professor Robin Leatherbarrow Head of Biological Chemistry Department of Chemistry.

Professor Robin Leatherbarrow Head of Biological Chemistry Department of Chemistry.
Pathogenesis. Fig. 1-15 KOCH’S POSTULATES Tools: Diseased animal Healthy animal Red blood cell Observe blood/tissue under the microscope Red blood cell.

Pathogenesis. Fig KOCH’S POSTULATES Tools: Diseased animal Healthy animal Red blood cell Observe blood/tissue under the microscope Red blood cell.
Exploiting Protein Cage Dynamics to Engineer Active Nanostructures Brian Bothner, Ives U Idzerda, Mark J Young, and Trevor Douglas 2007 NIRT Montana State.

Exploiting Protein Cage Dynamics to Engineer Active Nanostructures Brian Bothner, Ives U Idzerda, Mark J Young, and Trevor Douglas 2007 NIRT Montana State.
Chemical Biology 1 – Pharmacology 10-17-14. Methods for studying protein function – Loss of Function 1. Gene knockouts 2. Conditional knockouts 3. RNAi.

Chemical Biology 1 – Pharmacology Methods for studying protein function – Loss of Function 1. Gene knockouts 2. Conditional knockouts 3. RNAi.
Anthrax Another Reason to Fear Your Mailman By Stefko Waschuk R.C. Liddington, Nature, 415 : 373-374 (2002)

Anthrax Another Reason to Fear Your Mailman By Stefko Waschuk R.C. Liddington, Nature, 415 : (2002)
Cell signaling: responding to the outside world Cells interact with their environment by interpreting extracellular signals via proteins that span their.

Cell signaling: responding to the outside world Cells interact with their environment by interpreting extracellular signals via proteins that span their.
Endocrinology Introduction Lecture 3.

Endocrinology Introduction Lecture 3.
Why tethered-ligand technology? It is easy to bind targets to microarrays, but in order to detect interactions, the fluorescence of a spot must either.

Why tethered-ligand technology? It is easy to bind targets to microarrays, but in order to detect interactions, the fluorescence of a spot must either.
Antigen presentation to T lymphocytes Chapter 5. Objectives Explain and illustrate the mechanisms of antigen processing for presentation on –MHC I –MHC.

Antigen presentation to T lymphocytes Chapter 5. Objectives Explain and illustrate the mechanisms of antigen processing for presentation on –MHC I –MHC.
Chemical Genomics – Biol503 Lecture 2 Chemical Genomics and cancer/cardiovascular diseases.

Chemical Genomics – Biol503 Lecture 2 Chemical Genomics and cancer/cardiovascular diseases.
Chemical Genetics – Biol503

Chemical Genetics – Biol503
Cytokine Subversion —and inducible transient organogenesis— by Bacillus anthracis Tom Kepler Center for Bioinformatics & Computational Biology Duke University.

Cytokine Subversion —and inducible transient organogenesis— by Bacillus anthracis Tom Kepler Center for Bioinformatics & Computational Biology Duke University.
POSTER TEMPLATE BY: www.PosterPresentations.com Developing Novel Supported Membrane Interfaces for SPR Study of Transmembrane Proteins Heather Ferguson*,

POSTER TEMPLATE BY: Developing Novel Supported Membrane Interfaces for SPR Study of Transmembrane Proteins Heather Ferguson*,
Vaccines and Antivirals. Clinical Use of Interferon Therefore they have been used in the treatment of cancers of various types. Therefore they have been.

Vaccines and Antivirals. Clinical Use of Interferon Therefore they have been used in the treatment of cancers of various types. Therefore they have been.
02.07.11 Lecture 9: Cell Communication I. Multicellular organisms need to coordinate cellular functions in different tissues Cell-to-cell communication.

Lecture 9: Cell Communication I. Multicellular organisms need to coordinate cellular functions in different tissues Cell-to-cell communication.
Channel-linked Receptors aka: ligand-gated channels a receptor type seen in synaptic transmission rapid response (ms) limited response –depolarization.

Channel-linked Receptors aka: ligand-gated channels a receptor type seen in synaptic transmission rapid response (ms) limited response –depolarization.
Chem 509 Signal Transduction Winter 2012 Lecture 5.

Chem 509 Signal Transduction Winter 2012 Lecture 5.

Similar presentations

Ads by Google