{"id":232,"date":"2025-10-08T13:49:00","date_gmt":"2025-10-08T08:19:00","guid":{"rendered":"https:\/\/www.najao.com\/learn\/?p=232"},"modified":"2026-01-26T04:28:14","modified_gmt":"2026-01-25T22:58:14","slug":"disease-modeling","status":"publish","type":"post","link":"https:\/\/www.najao.com\/learn\/disease-modeling\/","title":{"rendered":"Disease Modeling: Recreating Illness to Conquer It"},"content":{"rendered":"\n<p class=\"wp-block-paragraph\">Has it ever occurred to you how we can study diseases without endangering human lives? This question is also at the heart of modern biomedical science. Disease modeling provides the answer to this deceptively simple question. It involves recreating illnesses under controlled conditions\u2014whether in cells, animals, or computers, in order to understand what drives disease and how we might intervene in a better way.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">In the past, disease research used to rely on observational studies in patients and relatively crude animal models, which offered limited understanding of the mechanisms behind the diseases. However, the advent of molecular biology, advances in gene-editing technologies, and the explosive growth in computational power have revolutionized the field. This evolution has led to a paradigm shift towards the creation of more sophisticated, human-relevant, and often predictive models that can bridge the gap between basic scientific discovery and clinical application.<\/p>\n\n\n\n<h2 class=\"wp-block-heading\">From mechanisms to medicines<\/h2>\n\n\n\n<p class=\"wp-block-paragraph\">Disease models allow researchers to tweak a gene, remove a protein, or simulate a cellular interaction. This helps not only to investigate the root causes of illness, but also to identify new therapeutic targets\u2014proteins or pathways\u2014for drugs to target<strong><sup>1,2<\/sup><\/strong>. Disease models also enable the screening of hundreds or thousands of compounds, which makes them essential in the early stages of drug development for identifying promising candidates while eliminating ineffective or toxic ones<strong><sup>3<\/sup><\/strong>. The utility of disease models is not limited only to drug discovery. They also help to identify biomarkers and test novel approaches such as gene editing or stem cell therapies<strong><sup>4-6<\/sup><\/strong>. Computational models are highly valuable for simulating disease outbreaks and preparing more effective responses.<\/p>\n\n\n\n<h2 class=\"wp-block-heading\">Types of disease models<\/h2>\n\n\n\n<h3 class=\"wp-block-heading\"><em>In vitro<\/em> models<\/h3>\n\n\n\n<p class=\"wp-block-paragraph\"><em>In vitro<\/em> models, meaning those developed outside a living organism, are often the first line of inquiry in disease research. Traditionally, 2D cultures are the primary type of <em>in vitro<\/em> model, that utilize flat sheets of cells grown in petri dishes<strong><sup>7<\/sup><\/strong>. The simplicity and scalability of such cultures make them useful in early drug testing, although they fall short when it comes to replicating the complex interactions of real tissues.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">To address this, researchers now use 3D models such as organoids and spheroids. <a href=\"https:\/\/www.najao.com\/learn\/organoids\/\" target=\"_blank\" rel=\"noreferrer noopener\">Organoids<\/a> are miniaturized and simplified versions of organs grown from stem cells that mimic some of the functions of the human body<strong><sup>8<\/sup><\/strong>. Spheroids, on the other hand, are simple clusters of cells used for cancer research<strong><sup>9<\/sup><\/strong>.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">3D bioprinting has taken it one step ahead with its ability to construct tissue-like structures using layer-by-layer deposition of cells and biomaterials, producing an architecture that more closely resembles functional organs<strong><sup>10<\/sup><\/strong>.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">This progress brings ethical questions too. As models become more human-like\u2014particularly brain organoids\u2014new guidelines are needed to address issues of consciousness, consent, and moral status<strong><sup>11<\/sup><\/strong>.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">The rapid advancement in this space has been possible particularly due to the use of induced pluripotent stem cells (iPSCs)<strong><sup>3<\/sup><\/strong>. They help to address the ethical concerns associated with the use of embryonic stem cells, as they are basically adult cells, reprogrammed into a stem-cell-like state and then induced to develop into any desired cell type.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">The use of iPSCs has also enabled the development of highly <a href=\"https:\/\/www.najao.com\/learn\/precision-medicine\/\" target=\"_blank\" rel=\"noreferrer noopener\">personalized<\/a> disease modeling, as for example, it allows researchers to collect cells from a person with Parkinson\u2019s disease, turn them into neurons, and study what\u2019s going wrong inside those neurons. Such \u201cdisease-in-a-dish\u201d approach offers unparalleled insight into the genetic and cellular mechanisms of any disease<strong><sup>12<\/sup><\/strong>.<\/p>\n\n\n\n<h3 class=\"wp-block-heading\"><em>In vivo<\/em> models<\/h3>\n\n\n\n<p class=\"wp-block-paragraph\">Despite all the advancements in the field of <em>in vitro<\/em> models, they may never replicate the complexity of a living organism. Mice and rats are the most widely used <em>in vivo<\/em> models due to their genetic similarity to humans and can thus be bred to naturally develop human-like diseases. Also, due to the ease with which their genomes can be manipulated, these animals can be genetically engineered to carry specific mutations.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">Transgenic mice, for example, may be made to overexpress a disease-related protein, which helps scientists understand its role<strong><sup>13<\/sup><\/strong>. Knockout models, where a gene is entirely deleted, enable us to investigate what happens when certain proteins are missing<strong><sup>14<\/sup><\/strong>. Conditional inducible models even allow researchers to control when and where these genetic changes take place within the body<strong><sup>15<\/sup><\/strong>.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">However, rodent models do not have identical physiology to ours and so results often fail to translate perfectly to human outcomes. To bridge this gap, researchers also use \u201chumanized\u201d mice that carry elements of the human immune system or express human genes<strong><sup>16<\/sup><\/strong>.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">Nevertheless, ethical concerns loom large in animal research<strong><sup>17<\/sup><\/strong>. There has been an ongoing debate about how to balance scientific progress with animal welfare, although guidelines promoting replacement, reduction, and refinement (the 3Rs) are in place to address some of the concerns.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">Other animals like zebrafish and frogs offer unique advantages<strong><sup>18,19<\/sup><\/strong>. For example: zebrafish embryos are transparent, and this makes them excellent for observing development and drug responses in real time.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">Smaller organisms such as the nematode <em>C. elegans<\/em> and the fruit fly <em>Drosophila melanogaster<\/em> are also invaluable for genetic studies, despite their simplicity<strong><sup>20,21<\/sup><\/strong>. These creatures share many basic biological pathways with humans, and their short lifespans and genetic manipulability make them ideal for studying aging, <a href=\"https:\/\/www.najao.com\/learn\/neurodegeneration\/\" target=\"_blank\" rel=\"noreferrer noopener\">neurodegeneration<\/a>, and other complex traits.<\/p>\n\n\n\n<h3 class=\"wp-block-heading\"><em>In silico<\/em> models<\/h3>\n\n\n\n<p class=\"wp-block-paragraph\"><em>In silico<\/em> models are the various computational models that have emerged as powerful tools to manage the explosive growth of biological data. They use various algorithms and mathematical frameworks to analyze the large biological datasets, in order to simulate disease processes. <a href=\"https:\/\/www.najao.com\/learn\/artificial-intelligence-applications-in-healthcare\/\" target=\"_blank\" rel=\"noreferrer noopener\">Artificial intelligence<\/a> has made these models more efficient, allowing them to sift through complex datasets to predict disease risk or uncover new drug targets<strong><sup>22<\/sup><\/strong>.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">There are various kinds of <em>in silico<\/em> models:<\/p>\n\n\n\n<ul class=\"wp-block-list\">\n<li>Systems biology models track how changes in molecular pathways affect cell behavior<strong><sup>23<\/sup><\/strong>.<\/li>\n\n\n\n<li>Agent-based models simulate interactions between individual cells. This enables researchers to study tumor growth or immune responses <em>in silico<\/em><strong><sup>24,25<\/sup><\/strong>.<\/li>\n\n\n\n<li>Pharmacokinetic and pharmacodynamic models help predict how a drug will behave in the body and what effects it will have over time<strong><sup>26<\/sup><\/strong>.<\/li>\n\n\n\n<li>Epidemiological models, like the widely known SIR (Susceptible-Infected-Recovered) framework, <a href=\"https:\/\/www.britannica.com\/science\/epidemiology\/Basic-concepts-and-tools\" target=\"_blank\" rel=\"noreferrer noopener\">help predict<\/a> the spread of infectious diseases and evaluate how successful will the impact of interventions like vaccines or lockdowns be<strong><sup>27<\/sup><\/strong>.<\/li>\n<\/ul>\n\n\n\n<p class=\"wp-block-paragraph\">However, these models are only as good as the data they rely on. Poor-quality or incomplete datasets can lead to misleading predictions<strong><sup>28<\/sup><\/strong>. Computational models also suffer from challenges like model transparency and generalizability across populations<strong><sup>29,30<\/sup><\/strong>. Therefore, most simulations must eventually be validated through experimental or clinical research.<\/p>\n\n\n\n<h2 class=\"wp-block-heading\">Building a reliable model<\/h2>\n\n\n\n<p class=\"wp-block-paragraph\">The process of building a model starts with a clear research question, which determines the selection of the appropriate platform: cellular, animal, or computational. The model is then developed, rigorously validated, and used to generate data. The model is then refined iteratively using constant feedback from the experimental results.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">The following are the key criteria to determine the utility and reliability of a disease model:<\/p>\n\n\n\n<ul class=\"wp-block-list\">\n<li><strong>Face validity:<\/strong> The model should resemble the human disease in symptoms<strong><sup>31<\/sup><\/strong>.<\/li>\n\n\n\n<li><strong>Construct validity:<\/strong> The underlying mechanisms that cause the disease in the model should be similar to those in the human condition<strong><sup>32<\/sup><\/strong>.<\/li>\n\n\n\n<li><strong>Predictive validity:<\/strong> A good model should respond to treatments in ways that match human outcomes<strong><sup>33<\/sup><\/strong>.<\/li>\n\n\n\n<li><strong>Reproducibility and robustness:<\/strong> The model should consistently produce similar results across different laboratories and under varying conditions<strong><sup>23<\/sup><\/strong>.<\/li>\n<\/ul>\n\n\n\n<p class=\"wp-block-paragraph\">Ultimately, a reliable model should enable confident extrapolation of findings from the model to human disease for successful clinical application.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">While acute diseases are easier to model and observe, chronic conditions like <a href=\"https:\/\/www.najao.com\/learn\/alzheimers-disease\/\" target=\"_blank\" rel=\"noreferrer noopener\">Alzheimer&#8217;s<\/a>, diabetes, and autoimmune disorders are particularly difficult to replicate in the lab<strong><sup>34<\/sup><\/strong>. This is because their long-term nature requires extended study periods, as well as the involvement of multiple organs in such conditions and the environmental influences require intricate model designs, which are both costly and time-consuming.<\/p>\n\n\n\n<h2 class=\"wp-block-heading\">Conclusion<\/h2>\n\n\n\n<p class=\"wp-block-paragraph\">Disease modeling is invaluable in modern medicine. These models let us study illnesses in controlled settings and bridge the gap between discovery and clinical application. Each model type\u2014<em>in vitro<\/em>, <em>in vivo<\/em>, and <em>in silico<\/em>\u2014offers unique advantages and presents specific challenges. However, future progress depends on integrating these diverse approaches. Only by combining methods, balancing simplicity with complexity, and leveraging both data and biological insights can we advance our understanding and improve our ability to tackle human disease.<\/p>\n\n\n\n<!--nextpage-->\n\n\n\n<h2 class=\"wp-block-heading\">FAQs<\/h2>\n\n\n\n<h4 class=\"wp-block-heading\">1. How long does it typically take to develop a new disease model?<\/h4>\n\n\n\n<p class=\"wp-block-paragraph\">The time required to develop a new disease model varies widely depending on the disease&#8217;s complexity and the specific research question. Simpler <em>in vitro<\/em> or <em>in silico<\/em> models may take a few months, while complex <em>in vivo<\/em> animal models can take several years, especially if genetic engineering or extensive validation is involved.<\/p>\n\n\n\n<h4 class=\"wp-block-heading\">2. How do regulatory bodies view data from disease models in the drug approval process?<\/h4>\n\n\n\n<p class=\"wp-block-paragraph\">Regulatory bodies, like the FDA, are increasingly recognizing the value of advanced disease models, especially human-relevant <em>in vitro<\/em> and <em>in silico<\/em> models, as they can reduce reliance on animal testing and accelerate drug development. However, these models typically serve as supporting evidence rather than replacing human clinical trials.<\/p>\n\n\n\n<h4 class=\"wp-block-heading\">3. Can disease models predict rare diseases, and what are the challenges?<\/h4>\n\n\n\n<p class=\"wp-block-paragraph\">Yes, disease models can be developed for rare diseases, but it&#8217;s often more challenging, primarily due to the scarcity of patient data and biological samples, which are crucial for developing and validating robust models. Collaboration and shared resources are key to progress in this field.<\/p>\n\n\n\n<h2 class=\"wp-block-heading\">Reference<\/h2>\n\n\n\n<p class=\"wp-block-paragraph\">1. Lauretti, E., &amp; Pratic\u00f2, D. (2020). Alzheimer\u2019s disease: Phenotypic approaches using disease models and the targeting of tau protein.&nbsp;<em>Expert opinion on therapeutic targets<\/em>,&nbsp;<em>24<\/em>(4), 319-330.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">2. Sebastian-Leon, P., Vidal, E., Minguez, P., <em>et al<\/em>. (2014). Understanding disease mechanisms with models of signaling pathway activities.&nbsp;<em>BMC systems biology<\/em>,&nbsp;<em>8<\/em>(1), 121.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">3. Marei, H. E., Khan, M. U. A., &amp; Hasan, A. (2023). Potential use of iPSCs for disease modeling, drug screening, and cell-based therapy for Alzheimer\u2019s disease.&nbsp;<em>Cellular &amp; Molecular Biology Letters<\/em>,&nbsp;<em>28<\/em>(1), 98.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">4. Jack, C. R., &amp; Holtzman, D. M. (2013). Biomarker modeling of Alzheimer\u2019s disease.&nbsp;<em>Neuron<\/em>,&nbsp;<em>80<\/em>(6), 1347-1358.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">5. Hoes, M. F., Bomer, N., &amp; Meer, P. (2019). Concise review: the current state of human in vitro cardiac disease modeling: a focus on gene editing and tissue engineering.&nbsp;<em>Stem cells translational medicine<\/em>,&nbsp;<em>8<\/em>(1), 66-74.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">6. Stoddard-Bennett, T., &amp; Pera, R. R. (2020). Stem cell therapy for Parkinson\u2019s disease: safety and modeling.&nbsp;<em>Neural Regeneration Research<\/em>,&nbsp;<em>15<\/em>(1), 36-40.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">7. Centeno, E. G., Cimarosti, H., &amp; Bithell, A. (2018). 2D versus 3D human induced pluripotent stem cell-derived cultures for neurodegenerative disease modelling.&nbsp;<em>Molecular neurodegeneration<\/em>,&nbsp;<em>13<\/em>(1), 27.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">8. Dutta, D., Heo, I., &amp; Clevers, H. (2017). Disease modeling in stem cell-derived 3D organoid systems.&nbsp;<em>Trends in molecular medicine<\/em>,&nbsp;<em>23<\/em>(5), 393-410.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">9. Griffin, K. H., Fok, S. W., &amp; Kent Leach, J. (2022). Strategies to capitalize on cell spheroid therapeutic potential for tissue repair and disease modeling.&nbsp;<em>NPJ Regenerative Medicine<\/em>,&nbsp;<em>7<\/em>(1), 70.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">10. Ma, X., Liu, J., Zhu, W., <em>et al<\/em>. (2018). 3D bioprinting of functional tissue models for personalized drug screening and in vitro disease modeling.&nbsp;<em>Advanced drug delivery reviews<\/em>,&nbsp;<em>132<\/em>, 235-251.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">11. Jeziorski, J., Brandt, R., Evans, J. H., <em>et al<\/em>. (2023, July). Brain organoids, consciousness, ethics and moral status. In&nbsp;<em>Seminars in cell &amp; developmental biology<\/em>&nbsp;(Vol. 144, pp. 97-102). Academic Press.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">12. Davaapil, H., Shetty, D. K., &amp; Sinha, S. (2020). Aortic \u201cdisease-in-a-dish\u201d: mechanistic insights and drug development using iPSC-based disease modeling.&nbsp;<em>Frontiers in Cell and Developmental Biology<\/em>,&nbsp;<em>8<\/em>, 550504.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">13. Myers, A., &amp; McGonigle, P. (2019). Overview of transgenic mouse models for Alzheimer&#8217;s disease.&nbsp;<em>Current protocols in neuroscience<\/em>,&nbsp;<em>89<\/em>(1), e81.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">14. da Silva-Buttkus, P., Spielmann, N., Klein-Rodewald, T., <em>et al<\/em>. (2023). Knockout mouse models as a resource for the study of rare diseases.&nbsp;<em>Mammalian Genome<\/em>,&nbsp;<em>34<\/em>(2), 244-261.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">15. Chapeau, E. A., Mandon, E., Gill, J., <em>et al<\/em>. (2019). A conditional inducible JAK2V617F transgenic mouse model reveals myeloproliferative disease that is reversible upon switching off transgene expression.&nbsp;<em>PLoS One<\/em>,&nbsp;<em>14<\/em>(10), e0221635.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">16. Chuprin, J., Buettner, H., Seedhom, M. O., <em>et al<\/em>. (2023). Humanized mouse models for immuno-oncology research.&nbsp;<em>Nature Reviews Clinical Oncology<\/em>,&nbsp;<em>20<\/em>(3), 192-206.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">17. Liguori, G. R., Jeronimus, B. F., de Aquinas Liguori, T. T., <em>et al<\/em>. (2017). Ethical issues in the use of animal models for tissue engineering: reflections on legal aspects, moral theory, three rs strategies, and harm\u2013benefit analysis.&nbsp;<em>Tissue Engineering Part C: Methods<\/em>,&nbsp;<em>23<\/em>(12), 850-862.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">18. Patton, E. E., Zon, L. I., &amp; Langenau, D. M. (2021). Zebrafish disease models in drug discovery: from preclinical modelling to clinical trials.&nbsp;<em>Nature reviews Drug discovery<\/em>,&nbsp;<em>20<\/em>(8), 611-628.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">19. Drawert, B., Griesemer, M., Petzold, L. R., <em>et al<\/em>. (2017). Using stochastic epidemiological models to evaluate conservation strategies for endangered amphibians.&nbsp;<em>Journal of the Royal Society Interface<\/em>,&nbsp;<em>14<\/em>(133), 20170480.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">20. Caldwell, K. A., Willicott, C. W., &amp; Caldwell, G. A. (2020). Modeling neurodegeneration in Caenorhabditis elegans.&nbsp;<em>Disease Models &amp; Mechanisms<\/em>,&nbsp;<em>13<\/em>(10), dmm046110.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">21. Aryal, B., &amp; Lee, Y. (2019). Disease model organism for Parkinson disease: Drosophila melanogaster.&nbsp;<em>BMB reports<\/em>,&nbsp;<em>52<\/em>(4), 250.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">22. Sanchez de la Nava, A. M., Arenal, \u00c1., Fern\u00e1ndez-Avil\u00e9s, F., <em>et al<\/em>. (2021). Artificial intelligence-driven algorithm for drug effect prediction on atrial fibrillation: An in silico population of models approach.&nbsp;<em>Frontiers in physiology<\/em>,&nbsp;<em>12<\/em>, 768468.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">23. Tiwari, K., Kananathan, S., Roberts, M. G., <em>et al<\/em>. (2021). Reproducibility in systems biology modelling.&nbsp;<em>Molecular systems biology<\/em>,&nbsp;<em>17<\/em>(2), e9982.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">24. Wang, Z., Butner, J. D., Kerketta, R., <em>et al<\/em>. (2015, February). Simulating cancer growth with multiscale agent-based modeling. In&nbsp;<em>Seminars in cancer biology<\/em>&nbsp;(Vol. 30, pp. 70-78). Academic Press.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">25. Chiacchio, F., Pennisi, M., Russo, G., <em>et al<\/em>. (2014). Agent\u2010based modeling of the immune system: NetLogo, a promising framework.&nbsp;<em>BioMed research international<\/em>,&nbsp;<em>2014<\/em>(1), 907171.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">26. Sung, J. H., Esch, M. B., &amp; Shuler, M. L. (2010). Integration of in silico and in vitro platforms for pharmacokinetic\u2013pharmacodynamic modeling.&nbsp;<em>Expert opinion on drug metabolism &amp; toxicology<\/em>,&nbsp;<em>6<\/em>(9), 1063-1081.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">27. McMahon, A., &amp; Robb, N. C. (2020). Reinfection with SARS-CoV-2: Discrete SIR (susceptible, infected, recovered) modeling using empirical infection data.&nbsp;<em>JMIR public health and surveillance<\/em>,&nbsp;<em>6<\/em>(4), e21168.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">28. Robertson, J., Yoshida, C., Kruczkiewicz, P., <em>et al<\/em>. (2018). Comprehensive assessment of the quality of Salmonella whole genome sequence data available in public sequence databases using the Salmonella in silico Typing Resource (SISTR).&nbsp;<em>Microbial genomics<\/em>,&nbsp;<em>4<\/em>(2), e000151.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">29. Johansson, U., S\u00f6nstr\u00f6d, C., Norinder, U., <em>et al<\/em>. (2011). Trade-off between accuracy and interpretability for predictive in silico modeling.&nbsp;<em>Future medicinal chemistry<\/em>,&nbsp;<em>3<\/em>(6), 647-663.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">30. Richter, M., Emden, D., Leenings, R., <em>et al<\/em>. (2025). Generalizability of clinical prediction models in mental health.&nbsp;<em>Molecular Psychiatry<\/em>, <em>30<\/em>, 3632\u20133639.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">31. Tapper, E. B., &amp; Chhatwal, J. (2024). The need to revise the model for face validity.&nbsp;<em>Official journal of the American College of Gastroenterology| ACG<\/em>,&nbsp;<em>119<\/em>(6), 1205.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">32. L Burrows, E., &amp; J Hannan, A. (2013). Towards environmental construct validity in animal models of CNS disorders: optimizing translation of preclinical studies.&nbsp;<em>CNS &amp; Neurological Disorders-Drug Targets (Formerly Current Drug Targets-CNS &amp; Neurological Disorders)<\/em>,&nbsp;<em>12<\/em>(5), 587-592.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">33. Scannell, J. W., Bosley, J., Hickman, J. A., <em>et al<\/em>. (2022). Predictive validity in drug discovery: what it is, why it matters and how to improve it.&nbsp;<em>Nature Reviews Drug Discovery<\/em>,&nbsp;<em>21<\/em>(12), 915-931.<\/p>\n\n\n\n<p class=\"wp-block-paragraph\">34. Golriz Khatami, S., Robinson, C., Birkenbihl, C., <em>et al<\/em>. (2020). Challenges of integrative disease modeling in Alzheimer&#8217;s disease.&nbsp;<em>Frontiers in molecular biosciences<\/em>,&nbsp;<em>6<\/em>, 158.<\/p>\n","protected":false},"excerpt":{"rendered":"<p>Has it ever occurred to you how we can study diseases without endangering human lives? Disease modeling makes this possible by recreating illnesses under controlled conditions\u2014whether in cells, animals, or computers\u2014to understand what drives disease and how we might intervene more effectively.<\/p>\n","protected":false},"author":3,"featured_media":234,"comment_status":"closed","ping_status":"closed","sticky":false,"template":"","format":"standard","meta":{"footnotes":""},"categories":[17,16,8],"tags":[],"coauthors":[10],"class_list":["post-232","post","type-post","status-publish","format-standard","has-post-thumbnail","hentry","category-biomedical-engineering","category-biotechnology","category-healthcare"],"yoast_head":"<!-- This site is optimized with the Yoast SEO plugin v27.6 - https:\/\/yoast.com\/product\/yoast-seo-wordpress\/ -->\n<title>Disease Modeling: Recreating Illness to Conquer It<\/title>\n<meta name=\"description\" content=\"Disease modeling involves recreating illnesses under controlled conditions to understand what drives disease and how we 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