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	<title>Ride for Dad &#8211; Porter Lab</title>
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		<title>Groundbreaking Prostate Cancer Research at the University of Windsor</title>
		<link>https://porterlab.com/groundbreaking-prostate-cancer-research-at-the-university-of-windsor/</link>
					<comments>https://porterlab.com/groundbreaking-prostate-cancer-research-at-the-university-of-windsor/#respond</comments>
		
		<dc:creator><![CDATA[fidalgo]]></dc:creator>
		<pubDate>Mon, 22 Sep 2025 14:07:34 +0000</pubDate>
				<category><![CDATA[Graduate Student]]></category>
		<category><![CDATA[In the spotlight]]></category>
		<category><![CDATA[CCS]]></category>
		<category><![CDATA[CRS]]></category>
		<category><![CDATA[Lisa Porter]]></category>
		<category><![CDATA[NSERC]]></category>
		<category><![CDATA[Porter Lab]]></category>
		<category><![CDATA[Prostate Cancer]]></category>
		<category><![CDATA[Ride for Dad]]></category>
		<category><![CDATA[University of Windsor]]></category>
		<category><![CDATA[WeSpark]]></category>
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					<description><![CDATA[My name is Jeffery Martin, and I am a second-year Master’s student working on the prostate cancer project in Dr. Porter’s lab in the Biomedical Science Department at the University of Windsor. In honour of Prostate Cancer Awareness Month, I would like to share some of the exciting prostate cancer research happening at the University [&#8230;]]]></description>
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									<p>My name is Jeffery Martin, and I am a second-year Master’s student working on the prostate cancer project in Dr. Porter’s lab in the Biomedical Science Department at the University of Windsor. In honour of Prostate Cancer Awareness Month, I would like to share some of the exciting prostate cancer research happening at the University of Windsor! Prostate cancer is the second most common cancer in men worldwide, affecting 76 men daily in Canada (<a href="https://cancer.ca/en/cancer-information/cancer-types/prostate/statistics" target="_blank" rel="noopener">Canadian Cancer Society</a>). Disease management and overall patient outcomes have improved as treatment options continue to evolve, and while effective in many cases, these treatments can sometimes pressure prostate cancer cells to change into a more aggressive type of cancer, known as Neuroendocrine Prostate Cancer (NEPC). NEPC can metastasize to other parts of the body, making the current treatments available for prostate cancer much more challenging. Our research focuses on studying the progression of early-stage prostate cancer adenocarcinoma to advanced NEPC and understanding the mechanism of the cell cycle’s regulation in this process.</p>								</div>
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									<p>We believe that through better understanding prostate cancer progression and the cell cycle’s role in this process, we will become more informed on potential treatment options. As a result of our findings, we are now testing selected drugs on prostate cancer cells to try to develop novel therapeutics that can treat and prevent the progression of prostate cancer.</p>								</div>
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										<img fetchpriority="high" decoding="async" width="1020" height="402" src="https://porterlab.com/wp-content/uploads/2025/09/Brief-Overview-of-NEPC-scaled-e1758400127333-1020x402.png" class="attachment-large size-large wp-image-4591" alt="" srcset="https://porterlab.com/wp-content/uploads/2025/09/Brief-Overview-of-NEPC-scaled-e1758400127333-1020x402.png 1020w, https://porterlab.com/wp-content/uploads/2025/09/Brief-Overview-of-NEPC-scaled-e1758400127333-500x197.png 500w, https://porterlab.com/wp-content/uploads/2025/09/Brief-Overview-of-NEPC-scaled-e1758400127333-480x189.png 480w, https://porterlab.com/wp-content/uploads/2025/09/Brief-Overview-of-NEPC-scaled-e1758400127333-768x303.png 768w, https://porterlab.com/wp-content/uploads/2025/09/Brief-Overview-of-NEPC-scaled-e1758400127333-1536x606.png 1536w, https://porterlab.com/wp-content/uploads/2025/09/Brief-Overview-of-NEPC-scaled-e1758400127333-2048x808.png 2048w" sizes="(max-width: 1020px) 100vw, 1020px" />											<figcaption class="widget-image-caption wp-caption-text">Progression of Prostate Cancer and treatment options at different stages</figcaption>
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											<a href="https://pubmed.ncbi.nlm.nih.gov/37575217/">
							<img decoding="async" width="792" height="570" src="https://porterlab.com/wp-content/uploads/2025/09/Liquid-vs-Traditional-Biopsy.png" class="attachment-large size-large wp-image-4595" alt="" srcset="https://porterlab.com/wp-content/uploads/2025/09/Liquid-vs-Traditional-Biopsy.png 792w, https://porterlab.com/wp-content/uploads/2025/09/Liquid-vs-Traditional-Biopsy-500x360.png 500w, https://porterlab.com/wp-content/uploads/2025/09/Liquid-vs-Traditional-Biopsy-389x280.png 389w, https://porterlab.com/wp-content/uploads/2025/09/Liquid-vs-Traditional-Biopsy-768x553.png 768w" sizes="(max-width: 792px) 100vw, 792px" />								</a>
											<figcaption class="widget-image-caption wp-caption-text">Liquid Bioppsies vs. Traditional Biopsies (Adapted from https://doi.org/10.1016/j.omto.2023.07.004)  </figcaption>
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									<p> Additionally, we are also looking for novel biomarkers that can detect prostate cancer progression, and we are using non-invasive liquid biopsies to do so! Biomarkers are measurable indicators, like genes or proteins found within the body, that reveal a biological process or disease within the body. Common biomarkers for prostate cancer include PSA (prostate-specific antigen), PSMA (prostate-specific membrane antigen), and AR (androgen receptor). Although these markers are very effective at detecting early stages of cancer, unfortunately, as the disease progresses, these markers are often lost. This leads to the need for the development of new biomarkers to track disease progression. </p>								</div>
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									<p>Further, we hope to find biomarkers that can be detected in early stages of prostate cancer and indicate whether or not disease progression is expected. This would help to guide treatment plans and create a more personalized medicine approach going forward. As mentioned, we plan to use non-invasive liquid biopsies instead of traditional biopsies to detect these biomarkers.  Although they are effective, traditional biopsies are invasive, painful for patients, and can lead to potential risks down the road. With liquid biopsies, we can detect these biomarkers in a less invasive way by using a blood, urine, or saliva sample. Through a collaboration with Dr. Kanjeekal at Windsor Regional Hospital, we will be searching for these new biomarkers with liquid biopsies collected from prostate cancer patients.</p>								</div>
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										<img decoding="async" width="1020" height="1107" src="https://porterlab.com/wp-content/uploads/2025/09/IMG_7691-e1758401687643-1020x1107.jpg" class="attachment-large size-large wp-image-4592" alt="" srcset="https://porterlab.com/wp-content/uploads/2025/09/IMG_7691-e1758401687643-1020x1107.jpg 1020w, https://porterlab.com/wp-content/uploads/2025/09/IMG_7691-e1758401687643-500x543.jpg 500w, https://porterlab.com/wp-content/uploads/2025/09/IMG_7691-e1758401687643-258x280.jpg 258w, https://porterlab.com/wp-content/uploads/2025/09/IMG_7691-e1758401687643-768x834.jpg 768w, https://porterlab.com/wp-content/uploads/2025/09/IMG_7691-e1758401687643.jpg 1179w" sizes="(max-width: 1020px) 100vw, 1020px" />											<figcaption class="widget-image-caption wp-caption-text">A photo of myself culturing cells</figcaption>
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									<p>The research we conduct is mainly done<em> in vitro</em>, which means it&#8217;s done in a controlled environment, like in a test tube, instead of a living organism. Specifically, we work in a cell culture room for a lot of our experiments. At the moment, I’m working with 4 different prostate cancer cell lines, which are all derived from prostate cancer patients. We use these cell lines to mimic the progression of disease, and also for drug testing to see how the cells respond to treatment.</p>								</div>
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										<img loading="lazy" decoding="async" width="1020" height="762" src="https://porterlab.com/wp-content/uploads/2025/09/JM-FBS-Stock-Jan-27-2025-1020x762.jpg" class="attachment-large size-large wp-image-4605" alt="" srcset="https://porterlab.com/wp-content/uploads/2025/09/JM-FBS-Stock-Jan-27-2025-1020x762.jpg 1020w, https://porterlab.com/wp-content/uploads/2025/09/JM-FBS-Stock-Jan-27-2025-500x374.jpg 500w, https://porterlab.com/wp-content/uploads/2025/09/JM-FBS-Stock-Jan-27-2025-375x280.jpg 375w, https://porterlab.com/wp-content/uploads/2025/09/JM-FBS-Stock-Jan-27-2025-768x574.jpg 768w, https://porterlab.com/wp-content/uploads/2025/09/JM-FBS-Stock-Jan-27-2025.jpg 1392w" sizes="(max-width: 1020px) 100vw, 1020px" />											<figcaption class="widget-image-caption wp-caption-text">Microscope image of the prostate cancer cells I work with.</figcaption>
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									<p>We also do some <em>in vivo</em> experiments, which means using living organisms. We specifically use zebrafish as a model system for testing the drugs! Using Zebrafish is becoming increasingly common around the world for drug testing and there are many benefits of this model system. First, Zebrafish are genetically similar to humans, and they are a cost-effective model that requires easy maintenance. Next, they develop quite rapidly, which is great for experimentation, and they have a transparent embryo, allowing for easy visualization. Finally, and most importantly, Zebrafish lack a functional immune system for the first 10 days of their life! This allows us to transplant human cells directly into zebrafish and then observe how these prostate cancer cells behave in a living system. From there, we can test various drugs in the Zebrafish with the prostate cancer cells and see how the cells respond to treatments in this environment. This will also help the results from our studies translate more easily and rapidly to use in humans.</p>								</div>
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										<img loading="lazy" decoding="async" width="350" height="144" src="https://porterlab.com/wp-content/uploads/2025/09/Zfish2.jpeg" class="attachment-large size-large wp-image-4603" alt="" />											<figcaption class="widget-image-caption wp-caption-text">Zebrafish imaged with a fluorescent microscope</figcaption>
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									<p>This fundamental work has been supported by grants from Cancer Research Society (CRS), Ride for Dad and WE-SPARK Health Institute. Through this funding, we have made some excellent progress so far, and I look forward to the progress that we will continue to make in the upcoming years! Additionally, through submitting my project proposal to various organizations, I have been lucky enough to receive funding from NSERC (Natural Sciences and Engineering Research Council of Canada), the Windsor Prostate Cancer Scholarship, the Dr. Michael L. Petras Memorial Scholarship, and the Doctor Family Health Research Student Support Award. Each of these awards has helped fund my education and allowed me to spend more time working in the lab. Further, another Master’s student working on this project, Christian Kassa, was recently awarded a Canadian Cancer Society Research Training Award. This is a very prestigious award with only 6 recipients across all of Canada. Christian just started his graduate studies this year and will be helping advance this project over the next 2 years!</p>								</div>
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												<figure class="wp-caption">
										<img loading="lazy" decoding="async" width="1020" height="1349" src="https://porterlab.com/wp-content/uploads/2025/09/Jeffery-Christian-at-Conference-1020x1349.jpg" class="attachment-large size-large wp-image-4593" alt="" srcset="https://porterlab.com/wp-content/uploads/2025/09/Jeffery-Christian-at-Conference-1020x1349.jpg 1020w, https://porterlab.com/wp-content/uploads/2025/09/Jeffery-Christian-at-Conference-500x661.jpg 500w, https://porterlab.com/wp-content/uploads/2025/09/Jeffery-Christian-at-Conference-212x280.jpg 212w, https://porterlab.com/wp-content/uploads/2025/09/Jeffery-Christian-at-Conference-768x1016.jpg 768w, https://porterlab.com/wp-content/uploads/2025/09/Jeffery-Christian-at-Conference-1162x1536.jpg 1162w, https://porterlab.com/wp-content/uploads/2025/09/Jeffery-Christian-at-Conference.jpg 1179w" sizes="(max-width: 1020px) 100vw, 1020px" />											<figcaption class="widget-image-caption wp-caption-text">Me and Christian at the 2025 WE-SPARK Conference</figcaption>
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									<p>A highlight of my project has been the various connections I have made with the community and other researchers at various conferences and local events. At the <a href="https://wesparkconference.com/previous-conferences-2025/" target="_blank" rel="noopener">WE-SPARK Health Research Conference</a>, I had the privilege of being a LEARN program host, which stands for Lived Experience Accelerating Research Knowledge. As a LEARN host, I was paired up with two local prostate cancer survivors who were able to share their lived experiences with me and give insight into the patient perspective. Oftentimes, when working in the lab, I forget about the direct impact my work can have, and these connections remind me of the importance of research. Further, the two patient participants that I was paired with are both members of Windsor’s local Prostate Cancer Support Group, and through making a connection with them, I was invited to speak to their group this upcoming November! Presenting our important work at various conferences has attracted the interest of other researchers and physicians for possible collaborations.</p>								</div>
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									<p>It’s important to recognize everyone involved in this project as none of this work would be possible without the help of our multi-disciplinary team. This project is supervised by Principal Investigator, Dr. Lisa Porter, and Research Associates, Dr. Elizabeth Fidalgo and Dr. Bre-Anne Fifield. Our clinical collaborator is Dr. Sindu Kanjeekal, the Chief of the Department of Oncology at the Windsor Regional Cancer Centre. In-lab experiments are carried out by myself, Jeffery Martin, fellow graduate student, Christian Kassa, and undergraduate student, Kaitlin Ferraro. Previous lab work was completed by Dr. Martin Bakht while a PhD student in our lab, and undergraduate thesis student, Maria Badalova. Knowledge translation work is completed by our Clinical RA, MSc Samavia Ahmad, and Masters of Translational Health Science student, Hannah Ferasol. Finally, none of this project’s advancements would be possible without the help of everyone else in Porter lab who help to provide meaningful feedback and insights that help drive this research further.</p>								</div>
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										<img loading="lazy" decoding="async" width="1020" height="566" src="https://porterlab.com/wp-content/uploads/2025/09/Porter-Lab-Photo-1020x566.png" class="attachment-large size-large wp-image-4596" alt="" srcset="https://porterlab.com/wp-content/uploads/2025/09/Porter-Lab-Photo-1020x566.png 1020w, https://porterlab.com/wp-content/uploads/2025/09/Porter-Lab-Photo-500x277.png 500w, https://porterlab.com/wp-content/uploads/2025/09/Porter-Lab-Photo-480x266.png 480w, https://porterlab.com/wp-content/uploads/2025/09/Porter-Lab-Photo-768x426.png 768w, https://porterlab.com/wp-content/uploads/2025/09/Porter-Lab-Photo.png 1414w" sizes="(max-width: 1020px) 100vw, 1020px" />											<figcaption class="widget-image-caption wp-caption-text">Porter Lab photo at the 2025 WE-SPARK Health Research Conference</figcaption>
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									<p>I hope you enjoyed learning a little bit more about the prostate cancer research taking place at the University of Windsor. Feel free to watch the video <a href="https://drive.google.com/file/d/1gjpOyJiVPiMab_ayRdMOebzNBa024G2v/view?pli=1" target="_blank" rel="noopener">here</a> if you want to see more of the work we do. If you have any questions, please leave a comment below, and I will get back to you! And if you enjoy reading it, please share it below! <em>Jeffery </em></p>								</div>
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		<title>UNDERGRADS 2025</title>
		<link>https://porterlab.com/undergrads-2025/</link>
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		<dc:creator><![CDATA[fidalgo]]></dc:creator>
		<pubDate>Wed, 14 May 2025 14:53:46 +0000</pubDate>
				<category><![CDATA[News & Events]]></category>
		<category><![CDATA[Cancer research]]></category>
		<category><![CDATA[CIHR]]></category>
		<category><![CDATA[Faculty of Science]]></category>
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		<category><![CDATA[NSERC]]></category>
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		<category><![CDATA[University of Windsor]]></category>
		<category><![CDATA[Windsor Cancer Research]]></category>
		<guid isPermaLink="false">https://porterlab.com/?p=4447</guid>

					<description><![CDATA[Christopher Jaworski Christopher Jaworski Glioblastoma (GBM) stands as one of the most lethal and aggressive brain cancers, often defying current treatment strategies. The outlook for patients remains grim, with average survival hovering around just 14 months after diagnosis. A major reason for this is the tumor’s ability to resist therapy and recur, often driven by [&#8230;]]]></description>
										<content:encoded><![CDATA[		<div data-elementor-type="wp-post" data-elementor-id="4447" class="elementor elementor-4447" data-elementor-post-type="post">
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										<img loading="lazy" decoding="async" width="1020" height="765" src="https://porterlab.com/wp-content/uploads/2021/10/Christopher_-1020x765.jpg" class="attachment-large size-large wp-image-4388" alt="" srcset="https://porterlab.com/wp-content/uploads/2021/10/Christopher_-1020x765.jpg 1020w, https://porterlab.com/wp-content/uploads/2021/10/Christopher_-500x375.jpg 500w, https://porterlab.com/wp-content/uploads/2021/10/Christopher_-373x280.jpg 373w, https://porterlab.com/wp-content/uploads/2021/10/Christopher_-768x576.jpg 768w, https://porterlab.com/wp-content/uploads/2021/10/Christopher_-1536x1152.jpg 1536w, https://porterlab.com/wp-content/uploads/2021/10/Christopher_-2048x1536.jpg 2048w" sizes="(max-width: 1020px) 100vw, 1020px" />											<figcaption class="widget-image-caption wp-caption-text">Christopher Jaworski</figcaption>
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									<h3 class="primaryText-698" title="Christopher Jaworski" data-log-name="DisplayName">Christopher Jaworski</h3><div data-olk-copy-source="MessageBody">Glioblastoma (GBM) stands as one of the most lethal and aggressive brain cancers, often defying current treatment strategies. The outlook for patients remains grim, with average survival hovering around just 14 months after diagnosis. A major reason for this is the tumor’s ability to resist therapy and recur, often driven by a complex network of cellular interactions within the tumor microenvironment. My research focuses on understanding the relationship between glioblastoma and a group of cells known as cancer-associated fibroblasts (CAFs). CAFs play a critical role in shaping the tumor environment by promoting tumor growth, supporting resistance to therapies, and enhancing invasive behavior. A protein of particular interest in our studies is YKL-40—a glycoprotein that is highly expressed in the mesenchymal subtype of GBM. This subtype is known for its aggressive nature and poor response to conventional treatments. By investigating how CAFs and tumor-initiating cells communicate through YKL-40, we aim to identify vulnerabilities that could lead to more effective treatment strategies. We’re also working with brain tumor organoids to model these interactions more realistically, and using techniques like shRNA knockdowns to probe the role of YKL-40 more precisely.</div><div data-olk-copy-source="MessageBody"> </div><div>My journey in research began in my second year of university when I joined the Porter Lab. I entered as a volunteer, initially gaining exposure to the fundamentals of cancer biology. Through the Peer Mentor Network, I was mentored by upper-year students who helped me develop a foundational understanding of lab techniques and experimental design. As I grew more confident and capable, I began contributing more directly to ongoing experiments and even helped identify gaps in existing research that informed new directions for study. By the time I reached my upper years, I had the privilege of having my own project, from hypothesis formation to troubleshooting complex protocols. This experience has sharpened my analytical thinking and strengthened my collaborative skills, especially through interdisciplinary discussions with researchers across different fields. Being part of such a dynamic lab has deepened my appreciation for the intricacies of cancer research and sparked a commitment to lifelong learning and scientific inquiry. I’m incredibly thankful to Dr. Porter and the entire lab team for their mentorship, support, and trust in my development. This journey has not only shaped my academic path but also inspired me to continue contributing to the broader fight against cancer.</div>								</div>
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									<div data-olk-copy-source="MessageBody">Glioblastoma (GBM) is the most aggressive type of brain tumour, characterized by its highly infiltrative and heterogeneous nature, which poses significant challenges to standard therapies. The presence of therapy-resistant Glioma Stem Cells (GSCs) contributes to GBM heterogeneity. Cancer cells (including GBM) are characterized by uncontrolled cell proliferation, which is linked to cell cycle dysregulation. SPY1 (SPDYA/RingoA) is an atypical cell cycle regulator that overrides cell cycle checkpoints, aiding in uncontrolled cell proliferation and survival through unique activation of CDKs. In GBM, elevated levels of SPY1 regulate CDK2 activity and drive clonal expansion of CD133+ GSCs. SPY1-CDK2 can also activate RNA-binding protein, Musashi-1 (MSI1), which plays a critical role in GSC maintenance through post-transcriptional regulation of NUMB and Notch pathway. MSI1 supports GSC populations to drive tumor</div><div>initiation and resistance to differentiation. This study aims to understand the role of MSI1 in maintaining GSC properties and its potential correlation with specific subgroups, and how MSI1 influences GSC self-renewal, proliferation, and response to therapies, with the goal of identifying novel therapeutic strategies to overcome treatment resistance in GBM. To demonstrate this, established GBM cell lines were infected with short hairpin (sh) MSI1 lentivirus, which resulted in reduced proliferation and self-renewal. The Zebrafish PDX platform was used to further validate the effects, confirming the impact of the MSI1 knockdown<br /><br />Being part of the Porter Lab family was one of the most amazing and rewarding experiences of my undergraduate studies. It offered far more than experimental training &#8211; it provided a supportive, intellectually stimulating environment where I learned to think critically, troubleshoot experiments, and develop my intrapersonal skills, which will help me in the real world. From the beginning, I was welcomed into a community that values both scientific excellence and personal growth. Whether it was executing the experiment, analyzing data, or collaborating with your lab peers, every task contributed to my development as a researcher. The most important thing I&#8217;ve learned during the whole experience is the value of perseverance. You are bound to experimental errors that may alter your results, but you have to see these setbacks as opportunities to rethink and improve, not as failures.</div>								</div>
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										<img loading="lazy" decoding="async" width="743" height="954" src="https://porterlab.com/wp-content/uploads/2025/05/Jagdeep-poster.jpg" class="attachment-large size-large wp-image-4449" alt="" srcset="https://porterlab.com/wp-content/uploads/2025/05/Jagdeep-poster.jpg 743w, https://porterlab.com/wp-content/uploads/2025/05/Jagdeep-poster-500x642.jpg 500w, https://porterlab.com/wp-content/uploads/2025/05/Jagdeep-poster-218x280.jpg 218w" sizes="(max-width: 743px) 100vw, 743px" />											<figcaption class="widget-image-caption wp-caption-text">Jagdeep Singh</figcaption>
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										<img loading="lazy" decoding="async" width="1020" height="1360" src="https://porterlab.com/wp-content/uploads/2025/05/Vanessa-poster-1020x1360.jpeg" class="attachment-large size-large wp-image-4453" alt="" srcset="https://porterlab.com/wp-content/uploads/2025/05/Vanessa-poster-1020x1360.jpeg 1020w, https://porterlab.com/wp-content/uploads/2025/05/Vanessa-poster-500x667.jpeg 500w, https://porterlab.com/wp-content/uploads/2025/05/Vanessa-poster-210x280.jpeg 210w, https://porterlab.com/wp-content/uploads/2025/05/Vanessa-poster-768x1024.jpeg 768w, https://porterlab.com/wp-content/uploads/2025/05/Vanessa-poster-1152x1536.jpeg 1152w, https://porterlab.com/wp-content/uploads/2025/05/Vanessa-poster-1536x2048.jpeg 1536w, https://porterlab.com/wp-content/uploads/2025/05/Vanessa-poster-scaled.jpeg 1920w" sizes="(max-width: 1020px) 100vw, 1020px" />											<figcaption class="widget-image-caption wp-caption-text">Vanessa Riolo</figcaption>
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									<div data-olk-copy-source="MessageBody">Glioblastoma (GBM) is the most lethal and aggressive primary brain tumour affecting the central nervous system. Despite standard treatments, prognosis remains poor due to several barriers that limit successful treatment such as the presence of the blood-brain barrier, tumour heterogeneity, and glioma stem cells (GSCs). GSCs are known to increase aggressiveness and hinder therapy response. A notable GSC marker is the CD44 receptor, which is activated by its primary ligand, hyaluronic acid (HA), to promote cancer progression. High CD44 expression in GBM is correlated to increased aggressiveness, stemness, proliferation and, ultimately, poorer prognosis. Nanoparticle therapies are an emerging field of cancer research that allow for selective targeting of GSC populations. Our lab has shown that HA-Conjugated Nanoparticles (HA-CPNs) can selectively target CD44+ cells, eliciting anti-tumour effects both <i>in vitro</i> and<i> in vivo</i>. Within my project, I utilize HA-CPNs to target GSC populations within a biologically relevant model known as glioblastoma organoids. Organoids mimic real 3D tumour tissues making them a suitable model to study the effects of HA-CPNs on GSC regulation.</div><div> </div><div>My journey within Porter Lab, starting in my second year of undergraduate studies, has provided me with some of the most rewarding experiences of my entire undergraduate career. I have been extremely fortunate to work alongside a team of talented students and RAs that I view as incredible role models and mentors. My time in lab has expanded my ability to problem solve, think critically, and above all has made me a more resilient person, appreciative of the intricacies of scientific discovery. I am extremely grateful for all of the opportunities, support, and guidance I have received from Dr. Porter, Dr. Lubanska, and the whole Porter Lab team this past year!</div><div> </div>								</div>
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									<p>My project focuses on determining the potential of the CDK1/2 inhibitor Dinaciclib as a therapeutic direction for prostate cancer (PC). Adenocarcinoma prostate cancer (AdPC) represents 95% of all PC cases and has several treatment options available, such as surgery, chemotherapy, and hormone therapy, like androgen deprivation therapy (ADT). ADT works by blocking the production of androgens in the body, such as testosterone, to reduce the proliferation of prostate cancer cells. However, some patients do become resistant to ADT, leading to treatment-resistant populations of PC to emerge, called castration-resistant prostate cancer (CRPC). CRPC has a median-survival rate of 1-2 years and is much more aggressive than AdPC. A common treatment method used for CRPC is AR inhibitors, which block the activity of the androgen receptor (AR) outright to slow the proliferation of the prostate cancer cells. However, patients can also become resistant to this form of therapy, and differentiate into a treatment-resistant form called neuroendocrine prostate cancer (NEPC). NEPC is the most aggressive and deadly subtype of prostate cancer, and has a 7-month median survival rate. Furthermore, the downregulation of prostate-specific membrane antigen (PSMA), an important detection target, and AR in the transdifferentiation to NEPC further contribute to the poor prognosis of this type of cancer. Our lab proposes targeting the cell cycle to slow the proliferation of prostate cancer, using a CDK1/2 inhibitor named Dinaciclib. My project uses three prostate cancer cell lines to test the efficacy of Dinaciclib in vitro in stopping the proliferation of prostate cancer cells: LNCaP-FBS, an AdPC cell line, LNCaP-CSS, a CRPC cell line, and NCI-H660, an NEPC cell line. My project also uses zebrafish as an in vivo model to test Dinaciclib’s effect on tumour burden, where zebrafish have been injected with prostate cancer cell lines and treated with Dinaciclib. Zebrafish are a viable model for prostate cancer because they develop rapidly, have transparent embryos, which makes them easy to see under a microscope, and also lack an immune system within their first 10 days of life, decreasing the chance of rejection if they were to be given human cells.</p><p>My time in Porter Lab has been one of the most important and fulfilling experiences of my life because it has allowed me to grow not only as a scientist but also as a learner. I would like to express my sincere gratitude to my supervisors Dr. Lisa Porter and Dr. Elizabeth Fidalgo da Silva, as well as PhD and master’s students for their mentorship, encouragement, and guidance in developing my research ability. I wish the best of luck to the next group of thesis undergraduates!</p>								</div>
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										<img loading="lazy" decoding="async" width="468" height="505" src="https://porterlab.com/wp-content/uploads/2025/05/Christian-poster.jpg" class="attachment-large size-large wp-image-4457" alt="" srcset="https://porterlab.com/wp-content/uploads/2025/05/Christian-poster.jpg 468w, https://porterlab.com/wp-content/uploads/2025/05/Christian-poster-259x280.jpg 259w" sizes="(max-width: 468px) 100vw, 468px" />											<figcaption class="widget-image-caption wp-caption-text">Christian Kassa</figcaption>
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										<img loading="lazy" decoding="async" width="1020" height="656" src="https://porterlab.com/wp-content/uploads/2025/05/thumbnail_IMG_8209-1020x656.jpg" class="attachment-large size-large wp-image-4465" alt="" srcset="https://porterlab.com/wp-content/uploads/2025/05/thumbnail_IMG_8209-1020x656.jpg 1020w, https://porterlab.com/wp-content/uploads/2025/05/thumbnail_IMG_8209-500x322.jpg 500w, https://porterlab.com/wp-content/uploads/2025/05/thumbnail_IMG_8209-435x280.jpg 435w, https://porterlab.com/wp-content/uploads/2025/05/thumbnail_IMG_8209-768x494.jpg 768w, https://porterlab.com/wp-content/uploads/2025/05/thumbnail_IMG_8209.jpg 1318w" sizes="(max-width: 1020px) 100vw, 1020px" />											<figcaption class="widget-image-caption wp-caption-text">Christian - First place best presentation</figcaption>
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										<img loading="lazy" decoding="async" width="1020" height="656" src="https://porterlab.com/wp-content/uploads/2025/05/thumbnail_IMG_8210-1020x656.jpg" class="attachment-large size-large wp-image-4466" alt="" srcset="https://porterlab.com/wp-content/uploads/2025/05/thumbnail_IMG_8210-1020x656.jpg 1020w, https://porterlab.com/wp-content/uploads/2025/05/thumbnail_IMG_8210-500x322.jpg 500w, https://porterlab.com/wp-content/uploads/2025/05/thumbnail_IMG_8210-435x280.jpg 435w, https://porterlab.com/wp-content/uploads/2025/05/thumbnail_IMG_8210-768x494.jpg 768w, https://porterlab.com/wp-content/uploads/2025/05/thumbnail_IMG_8210.jpg 1318w" sizes="(max-width: 1020px) 100vw, 1020px" />											<figcaption class="widget-image-caption wp-caption-text">Lauren - Third place best presentation</figcaption>
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