Scientists in a lab discovering the 'Big Bang' of immune escape in bowel cancer evolution, with microscopic tumor cell visuals.
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Scientists pinpoint early 'Big Bang' of immune escape in bowel cancer evolution

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An international team has identified an early 'Big Bang' moment in colorectal (bowel) cancer when tumor cells first evade immune surveillance, a finding that could refine who benefits from immunotherapy. The work, funded by Cancer Research UK and the Wellcome Trust, analyzed samples from 29 patients and was published in Nature Genetics on November 5, 2025.

Researchers from The Institute of Cancer Research in London, Fondazione Human Technopole in Milan, and Chalmers University of Technology in Sweden report that colorectal cancer undergoes a decisive early event—immune escape—that sets the tumor’s future course. Once this immune-evasive state is established, the tumor’s interaction with the immune system changes little as the cancer grows, the team found.

Professor Trevor A. Graham, Professor of Genomics and Evolution and Director of the Centre for Evolution and Cancer at The Institute of Cancer Research, said: "Some bowel cancers are 'born to be bad.' How they interact with the immune system is set early on. Immunotherapy and bowel cancer vaccines hold enormous promise for treating the disease. Our research suggests that a bowel cancer's relationship with the immune system doesn't change very much as it grows. If we can target that relationship early on, treatment should have a stronger chance of success."

The study examined tumor and immune cells from 29 patients, sequencing DNA and RNA and profiling chromatin accessibility. The authors conclude that epigenetic alterations—not just genetic mutations—reduce expression of antigen‑presenting machinery and silence neoantigens, making cancer cells harder for immune cells to detect. These changes appear early and are shared across the tumor, consistent with a "Big Bang" model of evolution.

Colorectal cancer is a major public health burden in the UK, where it is the fourth most common cancer with about 44,100 new cases each year—roughly 120 per day, according to Cancer Research UK.

The findings also help explain why only a subset of patients benefit from current immunotherapies. About 15% of colorectal cancers are mismatch repair–deficient (MMRd), a group that generally responds to immune checkpoint inhibitors, though not all do; checkpoint blockade is typically ineffective in mismatch repair–proficient tumors. The researchers suggest that combining immunotherapy with drugs that modify the epigenome could enhance antigen display and improve responses, a strategy that will require further testing.

Study lead author Eszter Lakatos, a mathematical biologist at Chalmers University of Technology and the University of Gothenburg, said: "Our research group has investigated and found answers to how cancer cells render themselves invisible to the immune system. Our hope is that these insights will eventually lead to more targeted, effective and early treatments, in addition to surgery."

Cancer Research UK’s Director of Research, Dr. Catherine Elliott, added: "To beat bowel cancer for everyone, we need to understand what happens at the very earliest stages of the disease. No matter how different bowel cancer tumors can look, one defining moment at the start makes a big difference to how the cancer grows."

The paper, "Epigenetically driven and early immune evasion in colorectal cancer evolution," appeared in Nature Genetics on November 5, 2025.

관련 기사

Illustration of worried young adults viewing news on rising global colorectal cancer rates in under-50s, featuring trend graphs, lifestyle factors, and screening tests.
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Colorectal cancer rates rising among younger adults worldwide

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Cases of colorectal cancer in people under 50 are increasing in many countries, alarming health experts. A recent international study found rising incidence in 27 of 50 countries through 2017, while researchers point to lifestyle factors, obesity and inherited genetic risks, and highlight new non‑invasive tests that could help close screening gaps.

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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A new study reveals that chemotherapy's damage to the gut lining unexpectedly rewires the microbiota, producing a compound that strengthens immune defenses against cancer spread. This process reduces immunosuppressive cells and enhances resistance to metastasis, particularly in the liver. Patient data links higher levels of this compound to improved survival in colorectal cancer cases.

Cold Spring Harbor Laboratory researchers report that engineered anti-uPAR CAR T cells cleared senescence-linked cells in mice, improving intestinal regeneration, reducing inflammation and strengthening gut barrier function. The approach also aided recovery from radiation-related intestinal injury and showed regenerative signals in experiments using human intestinal and colorectal cells, raising the possibility of future clinical trials.

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A small clinical trial shows that faecal microbiota transplants can improve outcomes for kidney cancer patients on immunotherapy drugs. Participants receiving transplants experienced longer cancer stability and greater tumor shrinkage compared to those given placebos. The approach targets the gut microbiome to boost immune responses against tumors.

Researchers at The Rockefeller University and Memorial Sloan Kettering Cancer Center have revealed a hidden spring‑like motion in the T cell receptor that helps trigger immune responses. Observed with cryo‑electron microscopy in a native‑like membrane environment, the mechanism may help explain why some T cell–based immunotherapies succeed while others fall short, and could inform efforts to make such treatments work for more patients.

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절강대학교 연구원들이 일반적으로 알레르기에 관여하는 비만세포를 재프로그래밍하여 암 싸움 바이러스를 종양에 직접 전달하는 새로운 방법을 개발했다. 최근 《셀》 저널 연구에서 상세히 설명된 이 접근법은 면역 반응을 강화하고 동물 모델에서 유망한 결과를 보인다. 이는 개인화된 암 치료를 위한 길을 열어준다.

 

 

 

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