Scientists reveal detailed maps of DNA's 3D structure

Researchers have produced the most detailed maps yet of how human DNA folds and reorganizes in three dimensions and over time. This work, led by scientists at Northwestern University as part of the 4D Nucleome Project, highlights how genome architecture influences gene activity and disease risk. The findings, published in Nature, could accelerate the discovery of genetic mutations linked to illnesses like cancer.

In a significant advance for genetics, scientists at Northwestern University, collaborating on the 4D Nucleome Project, have created comprehensive maps of the human genome's three-dimensional organization and its changes over time. The research utilized human embryonic stem cells and fibroblasts to capture how DNA interacts, folds, and shifts during cell growth, function, and division. Published in the journal Nature in 2025, the study provides fresh insights into the physical arrangements that control gene expression.

DNA does not remain as a linear strand inside cells; it forms loops and compartments within the nucleus, which determine which genes activate or deactivate. This affects development, cell identity, and susceptibility to diseases. The team integrated multiple genomic techniques to generate a detailed dataset, revealing more than 140,000 chromatin loops per cell type, along with anchoring elements that regulate genes. They also classified chromosomal domains and produced high-resolution 3D models at the single-cell level, showing variations in structure tied to processes like transcription and DNA replication.

Co-corresponding author Feng Yue, the Duane and Susan Burnham Professor of Molecular Medicine at Northwestern's department of biochemistry and molecular genetics, emphasized the importance of this work. "Understanding how the genome folds and reorganizes in three dimensions is essential to understanding how cells function," Yue said. "These maps give us an unprecedented view of how genome structure helps regulate gene activity in space and time."

The researchers benchmarked various technologies to assess their effectiveness in detecting loops, domain boundaries, and positional changes. They further developed computational tools to predict genome folding from DNA sequences alone, enabling estimates of how genetic variants might alter 3D structures without lab experiments.

These advances hold promise for medicine, particularly since many disease-linked variants occur in non-coding regions. "The 3D genome organization provides a powerful framework for predicting which genes are likely to be affected by these pathogenic variants," Yue noted. Future applications may include targeting structural errors in cancers like leukemia through drugs such as epigenetic inhibitors, potentially leading to new diagnostics and therapies.

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Photorealistic lab scene depicting DoriVac DNA origami vaccine triggering strong immune responses in mouse and organ chip models, as an advance over mRNA vaccines.
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DNA origami “DoriVac” shows strong immune activation in early tests, offering a potential complement to mRNA vaccines

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Researchers at Harvard’s Wyss Institute and Dana-Farber Cancer Institute report that a DNA origami-based vaccine platform called DoriVac generated robust immune responses in mice and in a human lymph node “Organ Chip” model. The team says the approach could be easier to store and manufacture than lipid nanoparticle–delivered mRNA vaccines, though the work remains preclinical. The results were published in Nature Biomedical Engineering.

Researchers have discovered that DNA in newly fertilized eggs forms a structured 3D scaffold before the genome activates, challenging long-held assumptions. Using a new technique called Pico-C, scientists mapped this organization in fruit fly embryos. A related study shows that disrupting this structure in human cells triggers an immune response as if under viral attack.

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Researchers have developed a genomic mapping technique that reveals how thousands of genes work together to influence disease risk, helping to bridge gaps left by traditional genetic studies. The approach, described in a Nature paper led by Gladstone Institutes and Stanford University scientists, combines large-scale cell experiments with population genetics data to highlight promising targets for future therapies and deepen understanding of conditions such as blood disorders and immune-mediated diseases.

Scientists have used human cells fused with plant DNA to test the purpose of non-coding DNA in the human genome. The experiment shows that activity in this so-called 'dark DNA' is largely random noise, supporting the idea that much of it is junk. The findings challenge claims that high activity implies function.

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Researchers have created the first complete map of mutations in the CTNNB1 gene that influence tumor development. By testing all possible changes in a critical hotspot, they revealed varying effects on cancer signals. The findings align with patient data and suggest implications for immunotherapy.

In 2025, scientists revived the cassette tape using DNA to store vast amounts of data, far surpassing traditional versions. The innovation, developed in China, can hold every song ever recorded on just 100 meters of tape. Researchers aim to bring the technology to market within five years.

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Researchers at Cold Spring Harbor Laboratory have identified key proteins and protein complexes that help certain carcinomas shift their cellular identity and potentially evade treatment. Two new studies, focusing on pancreatic cancer and tuft cell lung cancer, highlight molecular structures that could become targets for more precise and selective therapies.

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