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BioWorld - Thursday, February 19, 2026
Home » Authors » Xavier Bofill Bruna

Xavier Bofill Bruna

Articles

ARTICLES

Lung cancer illustration
Cancer

GUK1 is metabolic gate in ALK-driven lung cancer

Feb. 19, 2025
By Xavier Bofill Bruna
Using ALK+ lung cancer patient-derived cell lines, researchers have performed phosphoproteomic screening and identified guanylate kinase 1 (GUK1) as a TKI sensitive metabolic molecule in ALK-driven lung cancer. They reported their results online in Cell on Feb. 6, 2025.
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Illustration of lungs in the night sky with molecular structures as stars
Cardiovascular

Lysosomes, NCOA7 on the scene of pulmonary arterial hypertension

Jan. 24, 2025
By Xavier Bofill Bruna
Researchers from the University of Pittsburgh School of Medicine have linked pulmonary arterial hypertension (PAH), a progressive disease characterized by blood vessel remodeling, with lysosomal dysfunction and sterol metabolism. They reported their results on Jan. 23, 2025, in Science.
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Pain illustration
Neurology/psychiatric

NRP1 is NGF/TrkA partner in crime in pain signaling

Dec. 20, 2024
By Xavier Bofill Bruna
Chronic pain affects about 20% of the population worldwide. It is – inadequately – treated with nonsteroidal anti-inflammatory compounds and opioids that lack efficacy and that are associated with serious side effects. The signaling axis composed of nerve growth factor (NGF) and the receptor tropomyosin-related kinase A (TrkA) is one of the few nonopioid targets that have been validated for treating chronic pain in patients.
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Сross-section of the small intestine under the microscope
Gastrointestinal

LXR dissociates gut tissue regeneration from tumorigenesis, study shows

Nov. 28, 2024
By Xavier Bofill Bruna
By comparing the transcriptomic profile of tissue regeneration after induced damage in the small intestine and colon with their transcriptomic landscape in their steady state, researchers have identified a pathway that unlinks tissue regeneration from tumorigenesis.
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Illustration of human body composed of molecules
Cancer

Using black hole study methods, digital twins take aim at the patient black box

Oct. 29, 2024
By Xavier Bofill Bruna
Currently, cancer therapy trial-and-error methodology is inefficient and unsustainable. Oncology is the worst therapeutic area for drug trial success; only 3.4% of drugs that enter phase I end up being FDA approved, and 57% fail due to poor drug efficacy in trials. Building tools that may aid in predicting an individual’s response to a specific therapy may help in reducing costs, guesswork, and importantly improve the outcome of patients and accelerate new drug development.
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Illustration of human body composed of molecules
Cancer

Using black hole study methods, digital twins take aim at the patient black box

Oct. 25, 2024
By Xavier Bofill Bruna
Currently, cancer therapy trial-and-error methodology is inefficient and unsustainable. Oncology is the worst therapeutic area for drug trial success; only 3.4% of drugs that enter phase I end up being FDA approved, and 57% fail due to poor drug efficacy in trials. Building tools that may aid in predicting an individual’s response to a specific therapy may help in reducing costs, guesswork, and importantly improve the outcome of patients and accelerate new drug development.
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AI-generated image for cancer cells observed under a microscope

Lung macrophages put invasive breast cancer cells to sleep

Oct. 15, 2024
By Xavier Bofill Bruna
Breast cancer cells, when disseminated to other secondary organs such as the lungs, may stay in a dormant state for years, even decades. But the mechanisms that limit their expansion are not well understood. This is what researchers call a dormant mesenchymal-like phenotype before metastasis to the lungs. Now, scientists have shown in a study published Oct. 7, 2024, in Cell, that the limiting of disseminated breast cancer cells (DCCs) to metastasize in the lungs is due to alveolar macrophages, which activate signals that make DCCs stay dormant.
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AI-generated image for cancer cells observed under a microscope
Cancer

Lung macrophages put invasive breast cancer cells to sleep

Oct. 14, 2024
By Xavier Bofill Bruna
Breast cancer cells, when disseminated to other secondary organs such as the lungs, may stay in a dormant state for years, even decades. But the mechanisms that limit their expansion are not well understood. This is what researchers call a dormant mesenchymal-like phenotype (M-like) before metastasis to the lungs. Now, scientists have shown in a study published Oct. 7, 2024, in Cell, that the limiting of disseminated breast cancer cells (DCCs) to metastasize in the lungs is due to alveolar macrophages (AMs), which activate signals that make DCCs stay dormant.
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Illustration of bacteriophage landing on rod-shaped bacteria

Phylogeographics, phage typing combo fights antibiotic resistance

Oct. 1, 2024
By Xavier Bofill Bruna
The spread of drug-resistant bacteria is a global health concern and could once again become a leading cause of mortality. The World Health Organization has flagged carbapenem-resistant Acinetobacter baumannii as a top priority pathogen requiring innovative therapies for its management, which has a mortality rate of 25%-60% and caused more than 100,000 deaths worldwide in 2019. Therapy based on the use of bacteriophages (phages) to fight antibiotic-resistant bacteria is one such innovative strategy.
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Illustration of bacteriophage landing on rod-shaped bacteria
Infection

Phylogeographics, phage typing combo fights antibiotic resistance

Sep. 30, 2024
By Xavier Bofill Bruna
The spread of drug-resistant bacteria is a global health concern and could once again become a leading cause of mortality. The World Health Organization has flagged carbapenem-resistant Acinetobacter baumannii (CRAB), which has a mortality rate of 25%-60%, as a top priority pathogen requiring innovative therapies for its management. Researchers from the HUN-REN Biological Research Centre in Hungary have published a paper in Cell in which they describe designing and developing phage cocktails that target the most prevalent CRAB strains within specific geographic regions by using phylogeographic analysis and mapping the pathogen’s genetic diversity.
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