Scientists develop molecule to target aggressive breast cancer

Scientists at Oregon State University say they have engineered an iron-based nanomaterial that exploits acidic, peroxide-rich conditions inside tumors to generate two types of reactive oxygen species and kill cancer cells while largely sparing healthy cells. In mouse tests using human breast-cancer tumors, the team reports complete tumor regression without observable adverse effects, though the work remains preclinical.

January 15, 2026 Iniulat ng AI

Scientists at Northwestern Medicine have developed an antibody that counters pancreatic cancer's sugar-based disguise, enabling the immune system to attack tumors more effectively. In mouse studies, the therapy slowed tumor growth by restoring immune activity. The team is preparing the antibody for human trials.

Researchers at the University of California San Diego have discovered the enzyme N4BP2, which triggers chromothripsis, a chaotic genetic event in cancer cells. This process allows tumors to rapidly evolve and resist treatments. The findings, published in Science, suggest blocking N4BP2 could limit cancer's genomic instability.

January 05, 2026 Iniulat ng AI

Researchers at the University of Technology Sydney have created experimental compounds that prompt mitochondria to burn more calories safely. These mild mitochondrial uncouplers could offer a new approach to treating obesity without the deadly risks of past chemicals. The findings, published in Chemical Science, highlight potential benefits for metabolic health and aging.

Scientists have created innovative nanoparticles designed to destroy harmful proteins linked to dementia and cancer. These particles can access difficult tissues like the brain and precisely eliminate problematic proteins without broad side effects. The technology shows early promise for precision medicine.

January 10, 2026 Iniulat ng AI Fact checked

Researchers at Cold Spring Harbor Laboratory report they have identified a three-part molecular circuit involving SRSF1, Aurora kinase A (AURKA) and MYC that helps drive aggressive pancreatic ductal adenocarcinoma. In laboratory models, a splice-switching antisense oligonucleotide designed to alter AURKA splicing disrupted the circuit, reducing tumor-cell viability and triggering programmed cell death.