In animal tests, nanoparticles containing substances already approved for human use reduced inflammation in the biological microenvironment where such cancers develop, facilitating the action of the immune system.

April 25, 2024 – Published 1 month ago

Text: Ricardo Muniz
Art: Diego Facundini

A recently published article in the Journal of Controlled Release details the results of an international scientific collaboration that developed an alternative treatment for solid tumors by inhibiting the so-called inflammatory tumor microenvironment (TME).

Solid tumors are among the most challenging types of cancer to treat due to the difficulty of drug penetration. The inflammatory tumor microenvironment, where the tumors are located, contains various cells and substances from the patient that prevent the immune cells from combating the tumor. “Often these cells and molecules help the tumor grow, and that’s why we say it escapes the immune system’s surveillance,” explains Lúcia Helena Faccioli, a full professor at the School of Pharmaceutical Sciences of Ribeirão Preto (FCFRP) at USP and coordinator of the Lipid Quantification and Identification Center (Ceqil), established with support from Fapesp through the Multi-User Equipment Program.

Lucia Helena Faccioli – Photo: Marcos Santos/USP Images.

“There is always a tug-of-war between tumor-promoting and tumor-inhibiting immune cells in the TME, where metabolites, lipid mediators, cytokines, and chemokines play an important role in dominating the immunosuppressive nature,” write the authors of the article, which include researcher Viviani Nardini from the Department of Clinical, Toxicological, and Bromatological Analysis at FCFRP-USP and scientists from Indian institutions led by Avinash Bajaj, head of the Nanotechnology and Biological Chemistry Laboratory at the Regional Centre for Biotechnology in Faridabad, Haryana, India.

The team developed nanomicelles—very small particles, measuring between 1 and 100 nanometers—composed of different substances, hence called chimeras. The chimeric nanomicelles produced are composed of phospholipids (NMs), docetaxel (DTX), a substance used to kill tumor cells, and dexamethasone (DEX), an anti-inflammatory widely used to reduce the production of various inflammatory substances, such as prostaglandin E2 (PGE2).

Laboratory animal studies showed that these particles (NMs+DTX+DEX), administered intravenously, were very efficient, reducing tumor size and increasing the animals’ survival: untreated animals always die around 28-30 days, but treated animals survive up to 44-50 days, explains Faccioli.

The chimeric nanomicelles are composed of phospholipids (NMs), docetaxel (DTX), a substance used to kill tumor cells, and the anti-inflammatory dexamethasone (DEX) – Photo: researchers’ archive.