Genetic variants heighten Epstein-Barr virus risks for some

A large-scale study reveals that about one in ten people carry genetic variants making them more vulnerable to severe effects from the Epstein-Barr virus, which infects over 90 percent of the population. These variants are linked to higher viral persistence and increased risks of autoimmune diseases like multiple sclerosis and lupus. The findings, based on over 735,000 genomes, suggest pathways for targeted treatments and vaccines.

The Epstein-Barr virus (EBV), first identified in 1964 in connection with Burkitt’s lymphoma, infects more than 90 percent of people worldwide, often causing infectious mononucleosis that resolves in weeks. However, it has been increasingly tied to long-term autoimmune conditions. A 2022 study provided strong evidence linking EBV to multiple sclerosis, where nerve sheaths are damaged, impairing mobility. Similar connections exist with lupus and rheumatoid arthritis.

Researchers, led by Caleb Lareau at Memorial Sloan Kettering Cancer Center in New York, analyzed genomes from 735,000 participants in the UK Biobank and the US All of Us cohort. Using blood samples, they detected EBV DNA persistence: 9.7 percent of participants (47,452 individuals) retained more than 1.2 complete EBV genomes per 10,000 cells, indicating incomplete viral clearance.

The team identified 22 genomic regions associated with elevated EBV levels, many previously linked to immune diseases. The strongest ties involved variants in major histocompatibility complex (MHC) genes, which help distinguish self from pathogens. These variants impair EBV detection, allowing persistent infection that may trigger immune attacks on the body.

"This virus does something to our immune system, and it does something persistent and permanent to our immune system in some people," says Ruth Dobson at Queen Mary University of London. The variants also correlated with higher risks of autoimmune disorders and fatigue, potentially relating to chronic fatigue syndrome, though the exact link remains unclear.

Chris Wincup at King’s College London, not involved in the study, notes: "Almost everyone is exposed to EBV... How come everyone is exposed to the same virus and that virus causes autoimmunity, yet the majority of people don’t end up with an autoimmune condition?" The results highlight immune components for targeted therapies and underscore the need for EBV vaccines, despite the virus often seeming benign.

Published in Nature, the study offers hope for mitigating EBV's severe impacts on a subset of the population.

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Illustration of a woman with depression symptoms overlaid with microscopic view of aging monocytes in blood, linking to study on women with and without HIV.
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Study links monocyte “biological aging” in blood to emotional depression symptoms in women with and without HIV

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A study of 440 participants from the Women’s Interagency HIV Study found that accelerated epigenetic aging in monocytes—an immune cell type—tracked more closely with emotional and cognitive depression symptoms such as hopelessness and loss of pleasure than with physical symptoms like fatigue. The work, published in The Journals of Gerontology: Series A, adds evidence that cell-type-specific aging measures could contribute to future biological tools to complement symptom-based depression screening, though researchers say more validation is needed before clinical use.

Researchers at Fred Hutch Cancer Center have created human-like monoclonal antibodies that prevent Epstein-Barr virus (EBV) from infecting immune cells. Using mice engineered with human antibody genes, the team identified antibodies targeting viral proteins gp350 and gp42, with one fully blocking infection in lab models. The findings, published in Cell Reports Medicine, could lead to therapies for transplant patients at risk of EBV-related complications.

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Researchers at the Salk Institute have developed a detailed epigenetic catalog of human immune cells, showing how genetics and life experiences influence immune responses differently. The study, published in Nature Genetics, analyzed samples from 110 diverse individuals to distinguish inherited from environmental epigenetic changes. This work could lead to personalized treatments for infectious diseases.

Researchers found that infecting mice with respiratory syncytial virus (RSV) reduced breast cancer cells' ability to form tumors in the lungs by 65 to 70 percent. The effect stems from type I interferons, proteins that fight viral replication and hinder cancer cell seeding. The study raises hopes for drugs mimicking this mechanism.

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Scientists in Japan have discovered a giant virus called ushikuvirus that infects amoebae and provides evidence for the theory that viruses contributed to the evolution of complex cells. Isolated from Lake Ushiku, the virus exhibits unique structural and replication traits linking it to other giant DNA viruses. This finding, published in the Journal of Virology, deepens understanding of viral roles in eukaryotic evolution.

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