Clove essential oil as a source of antitumoral compounds capable of crossing the blood brain barrier: a focus on the effects of β-Caryophyllene and Eugenol in a glioblastoma cell line.

This study aimed at investigating β-Caryophyllene (BCA) pharmacokinetics as well as the potential antitumor activity and mechanism of action of BCA and eugenol (EU), alone or in combination, in U87 glioblastoma (GB) cells. BCA pharmacokinetic was studied by evaluating its concentration profiles in rat blood and cerebrospinal fluid after oral and intravenous administration. EU and BCA antitumor mechanisms were assessed by comparing their effects in U87 GB cells and non-tumoral HMC3 cells. Cell death, cell cycle regulation and mitochondrial membrane potential (MMP) were evaluated using flow cytometry. mRNA levels of target genes were evaluated by qPCR. Secreted cytokines were measured by Luminex®. BCA, as well as EU, permeates the brain. EU and BCA affected viability and proliferation of U87 cells (up to 50%, p<0.001), but not HMC3 cells, and showed a synergistic effect. BCA and EU, induced G0/G1 cell cycle arrest, increasing apoptosis/necrosis. EU and BCA induced downregulation of mRNAs codifying for key proteins involved in GB angiogenesis (VEGFA decreased op to 60%, p<0.01), proliferation and progression and showed anti-inflammatory activity (IL-4 significantly decreased, p<0.001). EU and BCA demonstrated a strong and multitarget antitumor activity in U87 cells. Our results provide a strong rationale for the further evaluation of EU and BCA as possible therapeutic molecules in GB management.