July 27, 2016, Filed Under: 2016, cancer, reflections, researchFinding a Cure for Cancer Together I cannot believe it is week 8. I have grown tremendously from nearly starting at the beginning of cell culturing. I knew that researchers worked as a team, though they still had their individual projects. There are constant communication and collaboration efforts even in their individualized projects. The research community is constantly interacting with one another. Photo source: Carabiner Communications The question is, do different areas of science and engineering communicate together? Cancer is a fight that is different for each person it affects, but the fight against cancer is a united front of various routes. The research paths lead to the same end in the fight against cancer, but the team effort is what keeps the fight alive and growing. Cancer is a fight that is different for each person, and individualized treatments are needed for each battle. There is more than one way to fight cancer. The cure itself is not just one method but several combined methods that take out cancer on all the possible fronts. During this summer, I have been around different types of engineering from biomedical to mechanical to material science and biology. I have learned that collaboration is endless because everyone has different ideas and knowledge, and different viewpoints are necessary. I have learned so much not only about cancer and how the cancer cells interact with their microenvironment, but also how biomaterials can be used to mimic the cancer microenvironment. – Alston-Lauren Feggins, Florida Institute of Technology
July 25, 2016, Filed Under: 2016, cancer, texas4000Letter to Texas 4000 Rider: Geena May Photo of Lady Bird Lake in Austin by Dylan Beam Dear Geena, As I read your profile on the Texas 4000 page, I found you to be very relatable. I never lived outside of Oregon until I decided to go to Ohio State to study Biological Engineering, but it didn’t take me long to start bleeding Scarlet and Grey. My girlfriend likes to tease me about how I’m more of an Ohioan than she is despite the fact that I haven’t even lived there for a full year and she has lived there her whole life. I grew up loving the outdoors and I know how beautiful the Sierras are. Seeing how much I could relate to you made it even harder to read about how cancer has affected your life. Your drive to ride in honor of your cousin and become an engineer to honor your high school teacher inspires me. Cancer affects us all, and we need strong people like you to lead the fight. Stay strong, and I hope you enjoy the rest of your ride. Sincerely, Dylan Beam, The Ohio State University Geena May is a UT Austin sophomore studying Mechanical Engineering, and is currently riding to Alaska on the Texas 4000 Sierra 2016 team!
July 22, 2016, Filed Under: 2016, cancer, researchResearch Updates! It is crazy to think we are on week 7 out of our 10 weeks here at the UT Austin BME department! Research is a notoriously slow process, but many of us REU students are finally starting to get some meaningful data. Across the board, all of us have vastly improved our skills and knowledge in the lab and are enjoying are heightened independence within our individual projects. Now faced with the daunting task of reporting our results in an abstract and poster, we are all beginning to consolidate our work and practice those scientific communication skills we have been working on! 🙂 The REU students report their research progress and accomplishments so far: Alston: I have seeded fibroblast cells and invasive breast cancer 231s cells onto my electrospun aligned and nonaligned fibers. I’m doing data analysis on the fibroblast cells to see the rate they proliferated. Adiel: I have been examining the effects that stiffening has on macrophages in order to better understand how macrophages behave within the tumor microenvironment. This is being done by placing macrophages into alginate gels of different degrees of stiffness, and examining their behavior. Hannah: I’ve been developing a new MATLAB algorithm to quantify inward movement and hopefully endocytosis. Right now we’re applying it to a cell line that’s drug resistant and treated with a certain kind of inhibitor, and we’re trying to test if the treated cells will show less inward movement in the trajectories we collect. Dylan: I am developing a low-cost imaging system primarily using 3D printed parts. This system will utilize the Laser Speckle Contrast Imaging (LSCI) technique to track relative blood flow in the brain. This technique is used by physicians and researchers to observe how blood flow returns to damaged parts of the brain after the removal of tumors. Nyrobi’s phantom gels Emilio’s smart glasses Dylan’s early model Adiel’s macrophage gels Rachel: I have been exploring how the changes in the stiffness of the microenvironment of breast cancer cells affects the cancer cells resistance to doxorubicin. So far this summer, I have seeded 3 experiments of the hydrogel based cell cultures in which I varied the dosages, acclimation times, and stiffness of the gels. Currently, I am performing Live/Dead assays to quantify the cancer cells response to doxorubucin. Grant: I’ve been working on creating liposomal nanoparticles to create a better binding site between the two membranes that fuses them together. We achieve this fusion by mixing the lipids that make up the membrane with this one specific lipid called DOTAP which due to its charge is attracted to the cell membrane and causes the fusion. Over my experiments so far in the lab, our results have found that lipids composed of 8% DOTAP deliver the best out of any variety of concentrations. We were able to determine this by dying one of the lipids and then scanning the cells and seeing how many cells were determined to fluoresce. Nyrobi: I am creating a tissue phantom to see how light can be manipulated in order to detect cancer noninvasively. I am using an imaging technique that is sensitive to scattering and absorption, and will allow us to accurately identify the boundaries of tumors. The first seven phantoms I made had bubbles that were too close to the phantom holes where the fluorescent dye will be. The last phantom made had very few, very small bubbles not close to the holes that would affect the results. Currently I’m making a new phantom with less scattering components in order to possibly see the fluorescent dye easier in the shorter phantom holes. Daniel: I am working on how physical environment forces such as strain (stretch) affects the behavior of cancer cells. So far we have seen mix results, with some knockout and knockdown cancer cell lines exhibit more cell adhesion while others resemble more metastatic behavior. Sydney: I compiled data about the interaction of PO4, cAMP and cGMP with different proteins then used that data to determine their most common interacting residues and atoms. I am using that data to isolate ligand residue interactions via Pymol then am running energy decomposition analysis to quantify the dominate forces in the interaction. Compiled by Sydney Hutton, Stanford
