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Neoantigen Prediction Pipeline

Description
Cells become cancerous due to changes in their genetic makeup. In cancers, an altered amino acid due to a tumor mutation can result in proteins that are identified as "foreign" by the immune system. An MHC molecule will bind to these "foreign" peptide fragments, also called neoantigens. There are 2

Cells become cancerous due to changes in their genetic makeup. In cancers, an altered amino acid due to a tumor mutation can result in proteins that are identified as "foreign" by the immune system. An MHC molecule will bind to these "foreign" peptide fragments, also called neoantigens. There are 2 classes of MHC molecules. While the MHC I complex is found in all cells with a nucleus, MHC II complexes are mostly found in antigen presenting cells (APCs), such as macrophages, B cells, and dendritic cells. The MHC molecule then presents the neoantigen on the cell's surface. If an immune cell, such as a T-cell, is able to bind to the neoantigen, it can then destroy the tumor cell. However, there are molecules that act as checkpoints on certain immune cells that have to be activated or inactivated to start an immune response. This ensures that healthy cells are not being killed. However, sometimes cancer cells can find ways to use these checkpoints to avoid being attacked. An example of immunotherapy which has had clinical successes is checkpoint blockade inhibition, which means blocking the activity of immune checkpoint proteins in order to release the "brakes" on the immune system to increase its ability to destroy cancer cells. Studies have found that there is a correlation between mutational load and response to immunotherapy. The goal of this project is to create a pipeline that identifies tumor neoantigens. This involved researching various softwares and implementing them to work together. This project involved developing a neoantigen prediction pipeline, which works with TGen's genomics pipeline, to help understand a patient's immune response. The neoantigen prediction pipeline first creates two protein fastas from the high quality non-synonymous mutations, frameshifts, codon insertions, and codon deletions from vcfmerger. One of the protein fastas includes the mutations, while the other one does not representing the wildtype protein. The pipeline then predicts both classes of HLA genotypes of the MHC molecules using DNA or RNA expression in the form of fastqs. The protein fastas and each HLA are fed into IEDB to obtain peptide-MHC binding predictions. Wildtype peptides and neoantigens with low binding affinities are then removed. RNA expression information is then added into the final text file from dseq and sailfish files from TGen's genomics pipeline.
ContributorsNaveed, Fatima (Author) / Craig, David (Thesis director) / Halperin, Rebecca (Committee member) / Computer Science and Engineering Program (Contributor, Contributor) / Barrett, The Honors College (Contributor)
Created2017-05

Scaled Formulations of Succinate based Polymeric particles for Eventual Testing in Clinical Settings

Description

With an estimated 19.3 million cases and nearly 10 million deaths from cancer in a year worldwide, immunotherapies, which stimulate the immune system so that it can attack and kill cancer cells, are of interest. Tumors are produced from the uncontrolled and rapid proliferation of cells in the body. Cancer

With an estimated 19.3 million cases and nearly 10 million deaths from cancer in a year worldwide, immunotherapies, which stimulate the immune system so that it can attack and kill cancer cells, are of interest. Tumors are produced from the uncontrolled and rapid proliferation of cells in the body. Cancer cells rely heavily on glutamine for proliferation due to its contribution of nitrogen for nucleotides and amino acids. Glutamine enters the tricarboxylic acid (TCA) cycle as α-ketoglutarate via glutaminolysis, in which glutamine is converted into glutamate by the enzyme glutaminase (GLS). Cancer cell proliferation may be limited by using glutaminase inhibitor CB-839. However, immune cells also rely on these metabolic pathways. Thus, a method for restarting the metabolic pathways in the presence of inhibitors is attractive. Succinate, a key metabolite in the TCA cycle, has been shown to stimulate the immune system despite the presence of metabolic inhibitors, such as CB-839. A delivery method of succinate is through microparticles (MPs) or nanoparticles (NPs) which may be coated in polyethylene glycol (PEG) for improved hydrophilicity. Polyethylene glycol succinate (PEGS) MPs were generated and tested in vivo and were shown to reduce tumor growth and prolong mouse survival. With the success in stimulating the immune system with MPs, NPs were investigated for an improved immune response due to their smaller size. These PES NPs were generated in this study. For clinical settings, it is necessary to scale-up the production of particles. Two methods of scale-up were proposed: (1) a combination of multiple small batches into a mixed batch, and (2) a singular, big batch. Size and release properties were compared to a small batch of PES NPs, and it was concluded that the big batch more closely resembled the small batch compared to the mixed batch. Thus, it was concluded that batch-to-batch variability plays a larger role than volume changes when scaling-up. In clinical settings, it is recommended to produce the particles in a big batch rather than a mixed batch.
ContributorsSundem, Alison (Author) / Acharya, Abhinav (Thesis director) / Inamdar, Sahil (Committee member) / Barrett, The Honors College (Contributor) / School of Molecular Sciences (Contributor) / Chemical Engineering Program (Contributor)
Created2023-05