Abstract

Programmed cell death plays an important role during animal development, and defects in this process result in a variety of human disorders including cancer and autoimmunity. A family of cysteine proteases, called Caspases, are conserved throughout animals and function to dismantle cells during programmed cell death by proteolysis. The goal of this project is to develop, optimize, and apply new multidimensional microfluidics technology for the rapid profiling of protein modifications based on changes in isoelectric point (pi) and molecular weight (MW) during programmed cell death, and identification of modified proteins via mass spectrometry. By using the fruit fly Drosophila melanogaster as a model system, these studies will explore pathways and identify biomarkers associated with Caspase activation during cell death in developing animals which will provide important insight into human cell death pathways. This challenge will be addressed through the development and application of a microfluidic platform capable of ultra-high-throughput multidimensional protein separation, followed by extremely sensitive protein quantification and identification, enabling effective screening of protein modifications. By offering significant reductions in sample requirements, the platforms will also serve to greatly improve the efficiency of Drosophila proteomic studies, and provide important benefits for downstream clinical applications of the technology. The proposed research will couple our team's expertise in programmed cell death studies and bioinformatics with experience in the development of capillary electrophoresis, microfluidic, and mass spectrometry proteomic instrumentation. Dr. DeVoe (Univ. of Maryland) will lead the project as PI, and take responsibility for overall coordination between the personnel and organizations involved in the research. He will be the leader for all activities involving microfabrication, micro and nanofluidics, and system engineering. Dr. Lee (Univ. of Maryland) will direct the activities in protein separation development and mass spectrometry analysis. Dr. Baehrecke (Univ. of Maryland Biotechnology Institute) will lead the investigation of the programmed cell death studies, and analysis of the resulting protein profiling data. Dr. Rudnick (Calibrant Biosystems) will work in concert with Drs. Baehrecke and Lee to develop and apply bioinformatics tools relevant to the programmed cell death studies. Dr. English (Univ. of Maryland) will collaborate with Drs. DeVoe and Lee on the development and implementation of ultrasensitive confocal microscopy systems for nanofluidic separation platforms. Dr. Ivory (Washington State Univ.) will work with Dr. DeVoe to develop electrokinetic simulations to be employed in optimizing the microfluidic separation systems in order to meet the stated performance goals for ultra-high-throughput protein profiling.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
1R01GM072512-01A1
Application #
6943690
Study Section
Special Emphasis Panel (ZRG1-SSS-U (90))
Program Officer
Edmonds, Charles G
Project Start
2005-09-15
Project End
2009-08-31
Budget Start
2005-09-15
Budget End
2006-08-31
Support Year
1
Fiscal Year
2005
Total Cost
$291,565
Indirect Cost

  Institution

Name
University of Maryland College Park
Department
Engineering (All Types)
Type
Schools of Engineering
DUNS #
790934285
City
College Park
State
MD
Country
United States
Zip Code
20742

  Publications

Shao, Chenren; Sun, Bing; Colombini, Marco et al. (2011) Rapid microfluidic perfusion enabling kinetic studies of lipid ion channels in a bilayer lipid membrane chip. Ann Biomed Eng 39:2242-51
Liu, Jikun; White, Ian; DeVoe, Don L (2011) Nanoparticle-functionalized porous polymer monolith detection elements for surface-enhanced Raman scattering. Anal Chem 83:2119-24
Tsao, Chia-Wen; Devoe, Don L (2011) Nanofilament silicon for matrix-free laser desorption/ionization mass spectrometry. Methods Mol Biol 790:183-9
Liu, Jikun; Chen, Chien-Fu; Yang, Shuang et al. (2010) Mixed-mode electrokinetic and chromatographic peptide separations in a microvalve-integrated polymer chip. Lab Chip 10:2122-9
Liu, Jikun; Chen, Chien-Fu; Chang, Chih-Wei et al. (2010) Flow-through immunosensors using antibody-immobilized polymer monoliths. Biosens Bioelectron 26:182-8
Chen, C F; Liu, J; Hromada, L P et al. (2009) High-pressure needle interface for thermoplastic microfluidics. Lab Chip 9:50-5
Liu, Jikun; Chen, Chien-Fu; Tsao, Chia-Wen et al. (2009) Polymer microchips integrating solid-phase extraction and high-performance liquid chromatography using reversed-phase polymethacrylate monoliths. Anal Chem 81:2545-54
Chen, Chien-Fu; Liu, Jikun; Chang, Chien-Cheng et al. (2009) High-pressure on-chip mechanical valves for thermoplastic microfluidic devices. Lab Chip 9:3511-6
Yang, Shuang; Liu, Jikun; Lee, Cheng S et al. (2009) Microfluidic 2-D PAGE using multifunctional in situ polyacrylamide gels and discontinuous buffers. Lab Chip 9:592-9
Hromada, Louis P; Nablo, Brian J; Kasianowicz, John J et al. (2008) Single molecule measurements within individual membrane-bound ion channels using a polymer-based bilayer lipid membrane chip. Lab Chip 8:602-8

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