Abstract

We introduce the second generation theranostic devices that integrate multiple targeting moieties (e.g., antibody- or aptamer-based) with two additional molecular components: (1) molecular computing in order to analyze obtained disease signatures;and (2) specific drug delivery triggered by the outcome of this computing. These devices will be capable of specific targeting of cells based on multiple disease markers, resulting in elimination of narrow subpopulations of cells, and improved treatment of malignancies. Over the next two years we will accomplished goals described in two aims:
Aim 1. Demonstration and optimization of molecular computing cascades on the surface of the lymphocytes targeted with antibody- or aptamer-oligonucleotide conjugates. Molecular computing on cell surfaces will be based on cascades of chemical reactions that occur only if all required components of these cascades are present on the cell surface (cascaded AND gates) or protective factors are absent (cascaded NOT gates).
Aim 2. Demonstration of drug delivery to the cells on the surface of which molecular cascades have been completed. Cells targeted for elimination with molecular computing will at the end of cascades display specific oligonucleotides, while non-target cells will not. We will construct various toxic agents integrated with an oligonucleotide complementary to the displayed one, and we will study their effects on cells treated with molecular computing cascades. The large multidisciplinary team ensures that at the end of the second year, we will have demonstrated all the components of cascades, putting us in a position to start optimization process needed for the first animal studies.

Public Health Relevance

We propose that complex diseases and traits, such as many cancers, autoimmune diseases, or obesity, can be addressed through interactions with matching multi-input molecular networks or molecular automata. The successful completion of our project will lead to the following vision of personalized therapy: A physician determines the unique surface immunophenotype of a cell type that he/she would like to target for elimination from a patient. Guided by the comparison with the phenotypes of healthy cells, the physician combines off-the- shelf reagents, creating and administering automata to the patient, specifically killing the targeted cell types, while protecting non-target cells.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
High Impact Research and Research Infrastructure Programs (RC2)
Project #
1RC2CA147925-01
Application #
7852629
Study Section
Special Emphasis Panel (ZCA1-SRLB-R (O9))
Program Officer
Forry, Suzanne L
Project Start
2009-09-30
Project End
2011-08-31
Budget Start
2009-09-30
Budget End
2010-08-31
Support Year
1
Fiscal Year
2009
Total Cost
$902,220
Indirect Cost

  Institution

Name
Columbia University (N.Y.)
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
621889815
City
New York
State
NY
Country
United States
Zip Code
10032

  Publications

Palla, Mirkó; Bosco, Filippo G; Yang, Jaeyoung et al. (2015) Mathematical Model for Biomolecular Quantification Using Large-Area Surface-Enhanced Raman Spectroscopy Mapping. RSC Adv 5:85845-85853
Zhu, Jing; Shang, Junyi; Jia, Yuan et al. (2014) Spatially selective release of aptamer-captured cells by temperature mediation. IET Nanobiotechnol 8:2-9
Zhu, Jing; Shang, Junyi; Olsen, Timothy et al. (2014) A Mechanically Tunable Microfluidic Cell-Trapping Device. Sens Actuators A Phys 215:197-203
Wang, Bin; Huang, Fengliang; Nguyen, Thaihuu et al. (2013) Microcantilever-Based Label-Free Characterization of Temperature-Dependent Biomolecular Affinity Binding. Sens Actuators B Chem 176:653-659
Yang, Jaeyoung; Palla, Mirko; Bosco, Filippo Giacomo et al. (2013) Surface-enhanced Raman spectroscopy based quantitative bioassay on aptamer-functionalized nanopillars using large-area Raman mapping. ACS Nano 7:5350-9
Kim, Jinho; Hilton, John P; Yang, Kyung A et al. (2013) Nucleic Acid Isolation and Enrichment on a Microchip. Sens Actuators A Phys 195:183-190
Fong, Erika J; Sharma, Yasha; Fallica, Brian et al. (2013) Decoupling directed and passive motion in dynamic systems: particle tracking microrheology of sputum. Ann Biomed Eng 41:837-46
Zhu, Jing; Palla, Mirkó; Ronca, Stefano et al. (2013) A MEMS-Based Approach to Single Nucleotide Polymorphism Genotyping. Sens Actuators A Phys 195:175-182
Rudchenko, Maria; Taylor, Steven; Pallavi, Payal et al. (2013) Autonomous molecular cascades for evaluation of cell surfaces. Nat Nanotechnol 8:580-6
Lepzelter, David; Zaman, Muhammad (2012) Subdiffusion of proteins and oligomers on membranes. J Chem Phys 137:175102

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