The Inhibitory Effect of Extra Virgin Olive Oil and Its Active Compound Oleocanthal on Prostaglandin-Induced Uterine Hypercontraction and Pain—Ex Vivo and In Vivo Study

The drugs and solutions used in this work were as follows: dimethyl sulfoxide (DMSO) (Sigma-Aldrich, St. Louis, MO, USA), oleocanthal (PhytoLab), acetonitrile, hexane, electrochemiluminescence (ECL) immunoassay (Thermo), oxytocin (Sigma-Aldrich, St. Louis, MO, USA, O3251) (Sigma-Aldrich, St. Louis, MO, USA, O6379), carbachol (Sigma-Aldrich, St. Louis, MO, USA, C4382), PGF2α (Cayman, Ann Arbor, MI, USA, 16010), acetylcholine (Sigma-Aldrich, St. Louis, MO, USA, A2661), Bay K 8644 (TOCRIS, Taiwan, 1544), potassium chloride (KCl) (SHOWA, Saitama, Japan, 1630-5150), calcium chloride dehydrate (CaCl₂) (Wako, TX, USA, 038-00445), acetic acid (LAB-SCAN, Bangkok, Thailand, A8401E), β-Estradiol 3-benzoate (EB) (Sigma-Aldrich, St. Louis, MO, USA, E8515), ibuprofen (Sigma-Aldrich, St. Louis, MO, USA, I4883).

The experiment of uterine contraction used female Sprague Dawley rats (200–300 g), and the writhing test experiment used female Institute of Cancer Research (ICR) mice that were housed in a temperature-controlled room (22 ± 2 °C) with artificial illumination for 12 h, with food and water provided ad libitum. The study was approved by the Experimental Animal Care and Use Committee of Taipei Medical University (NO. LAC-2018-0210/NO. LAC-2018-0297). All animals received humane care in compliance with the Principles of Laboratory Animal Care and the Guide for the Care and Use of Laboratory Animals, published by the National Science Council, Taiwan.

The extra virgin olive oil (LAUDEMIO, L8057) was mixed with acetonitrile (ACN) and n-hexane (HEX) at a ratio of 1:2:3. After mixing, the solution was separated into ACN and HEX layers using a separator funnel. The ACN layer extracts after liquid separation were weighted and concentrated by a vacuum condenser. The ACN layer extract was concentrated to a small amount of liquid and transferred to a vial. It was then concentrated to a paste through continued rotation for 1 h for further experiments. after the layer forming the paste, the remaining liquid was aspirated. Finally, DMSO was used to dissolve the paste.

A photodiode array (PDA) detector set to 223 nm was used for the identification of compound oleocanthal (OC), based on the retention time (Rt) and ultraviolet (UV) characteristics. A BEH Shieid RP18 column (Waters Acquity, 2.1 mm × 100 mm, 1.7 μm) was used for the analysis, and the flow rate was set to 0.5 mL/min. The mobile phase consisted of solvents A: acetonitrile (ACN) and B: water with 0.1% formic acid. The gradient method was used for the quantification of the compounds of interest for 0–5 min: 100% A; 0% B. The column temperature was kept at 40 °C throughout all experiments, and the injection volume was 10 μL.

Rats were sacrificed by carbon dioxide and the uterus was removed and placed in an organ bath. The tissue water bath contained Krebs’ solution (113 mM NaCl, 4.8 mM KCl, 2.5 mM CaCl₂, 18 mM NaHCO₃, 1.2 mM KH₂PO₄, 1.2 mM MgSO₄, 5.5 mM glucose, 30 mM mannitol, and pH 7.4). We removed the uterine fat and cut it into segments of equal length. The segments were placed in isolated organ baths containing Krebs’ solution at 37 °C with a 95% O₂ and 5% CO₂ supply. Each organ bath was equilibrated using 1 g of weight for at least 60 min. Uterine contractions were recorded with force-displacement transducers by using the LabScribe software [12].

Molecular docking was performed by a PyMOL plug-in—NRGsuite [22]—under the PyMOL version 1.8 environment. This included the detection of surface cavities in protein and was used as a target binding site for docking simulations. The structures of COX-2 bound with ibuprofen were downloaded from the protein data bank (PDB) database [23], and ibuprofen was separated from COX-2 in PyMOL for further docking analysis.

The test was carried out using a previously described technique [24]. Mice were treated with three different doses (28, 70, and 140 mg/kg) of extra virgin olive oil (EVOO) extracts and ibuprofen (120 mg/kg, P group) as a positive control. A total of 60 min after oral administration, writhing was induced by 0.6% acetic acid (10 mL/kg i.p., V group). Each mouse was placed in a transparent observation box, and the amount of writhing was recorded for 30 min after the acetic acid administration.

This test was performed using the modified method described by a previous study [25]. During the experiment, the female mice were injected intraperitoneally with 1 mg/kg body weight estradiol benzoate and administration of EVOO extracts (28, 70, and 140 mg/kg) or ibuprofen (100 mg/kg, P group) every day, except for the control group, by an oral gavage. Mice were induced to writhe by an intraperitoneal injection with 67 IU/kg oxytocin solution in DMSO at day 7, and we recorded the number of writhing responses that occurred 30 min after oxytocin injection. Uterine samples were collected for protein expression analysis.

We used a commercial kit (Dojindo, Japan) and followed the instructions to evaluate the antioxidant ability. The scavenging activity was detected using 100 μL 2,2-Diphenyl-1-Picrylhydrazyl (DPPH) solution mixed with the sample in a 96-well microplate and incubated at room temperature for 30 min. The absorbance was measured at 517 nm using a VERSA Max microplate reader (Molecular Devices, San Jose, CA, USA) and using the following formula: Scavenging activity (%) = [control − sample/control] × 100.

The IC₅₀ DPPH values were obtained through extrapolation from regression analysis.

The levels of malondialdehyde (MDA) in plasma followed the manufacturer’s instructions (TBARS Assay Kit Cayman, USA). Results were measured on a 532 nm plate using a VERSA Max microplate reader (Molecular Devices, San Jose, CA, USA).

To investigate whether OC affects the expression of PGF2α receptor (FP) protein in the uterus ex vivo, OC was added 10 min after the stimulation of the uterus with PGF2α, and the uterus was taken at 10, 30, and 60 min after the addition of OC for analysis.

Samples were lysed in radioimmunoprecipitation assay (RIPA) lysis buffer containing protease and phosphatase inhibitors (Roche, Mannheim, Baden-Württemberg, Germany). Protein was quantitated by the bicinchoninic acid assay (BCA) and then resolved using sodium dodecyl sulfate polyacrylamide gel electrophoresis (SDS-PAGE). After transfer to a polyvinylidene fluoride (PVDF) membrane, 5% bovine serum albumin (BSA) solution was used to block the empty space of the membrane. Subsequently, membranes were incubated with primary antibodies—PGF2α receptor (FP) (Cayman, 101802), COX-2 (Cayman, 160106), oxytocin receptor (OTR) (Santa Cruz, CA, USA, sc-8109), p-ERK (Cell Signaling, 9101), ERK (Cell Signaling, 9102), p-MLC20 (Cell Signaling, 3675), MLC20 (Santa Cruz, CA, USAsc-28329), Protein kinase C (PKC-δ) (BD Bio, 610397), α-actin (Santa Cruz, CA, USA, sc-32251)—at 4 °C overnight and then with a horseradish peroxidase (HRP)-conjugated secondary antibody (1:10,000) for 1 to 2 h. The visual signal was captured by an image analysis system (UVP BioChemi, Analytik Jena US, Upland, CA, USA). The band densities were determined as arbitrary absorption units using the Image-J software program version 1.52 t (NIH, Bethesda, MD, USA). The expression level of these target proteins was analyzed by three individual experiments.

All data are presented as the mean ± standard error of the mean (SEM). The statistical significance of differences between the groups was analyzed by using Graphpad Prism (version 6.0). The statistically significant difference from the respective controls for each experiment was determined using a one-way analysis of variance (ANOVA) for all groups. A Student’s unpaired t-test was used for comparison between two groups. A value of p < 0.05 was considered to be statistically significant.

A pure compound of OC was used for ex vivo experiments. After the steady spontaneous contraction, PGF2α was used to induced hypercontraction. We also used PGF2α (10⁻⁶ M) to induce uterine contractions, and the uterus was treated with OC (10–100 μM). The results show that OC dose-dependently inhibited the PGF2α-induced contraction amplitude (Figure 1a, IC₅₀ = 55.20 μM). The results demonstrate that OC has an effect on the inhibition of PGF2α-induced uterine hypercontraction. Oxytocin is a hormone that increases uterine and mammary gland contractions. OC (10–100 μM) was administered after oxytocin (10⁻⁷ M)-induced uterine contraction. The results show that OC can significantly inhibit oxytocin-induced uterine contractions (Figure 1b, IC₅₀ = 91.35 μM). To investigate the effect of OC on the inhibition of acetylcholine or carbachol-induced uterine contraction, OC (10–100 μM) was added after acetylcholine or carbachol (10⁻⁶ M)-induced uterine contraction. OC can significantly inhibit acetylcholine (Figure 1c, IC₅₀ = 85.63 μM) and carbachol (Figure 1d)-induced uterine contraction. Further analysis shows that the frequency had the identical effect in the uterine contract inhibition (Figure S1). To examine the OC’s cytotoxicity, it was treated with OC at the beginning and the organ bath was washed to exclude the OC’s effect, then it was treated with PGF2α. The results show that the organ can recover the contraction and that there is no cytotoxicity effect on the OC treatment. (Figure S2).

Previous studies have reported that high K⁺ concentrations and Ca²⁺ activator can induce uterine contractions [26]. The results show that OC (50–100 μM) can inhibit Bay K 8644 (10⁻⁶ M), a Ca²⁺ channel activator, and KCl (50 mM)-induced uterine contraction (Figure 2a,b). In order to investigate the role of calcium, the following experiment used calcium to induce uterine contractions. When the solution without calcium was used, spontaneous uterine contractions were not present; after adding calcium (0.05–5 mM) into the solution, the spontaneous uterine contractions were restored (Figure 2c). However, when adding OC (50 μM) before adding calcium, the spontaneous uterine contractions were inhibited. This indicates that OC inhibits uterine contraction by blocking calcium channels. After removing OC and using PGF2α stimulant, the spontaneous contraction recovered by no more than 50% (Figure 2c). The results showed that, after treatment with OC, the intracellular calcium influx cannot effectively trigger uterine contractions. Therefore, we used a western blot to analyze the mechanism of OC in terms of the inhibition of uterine contraction. The results also show that OC inhibits the FP receptor to reduce uterine hypercontraction (Figure 2d). To examine the solvent effect, the solvent DMSO was treated after PGF2α oxytocin-induced contraction. Results found there are no effect on PGF2α, oxytocin, or calcium-induced uterine contraction inhibition (Figure S3). The inhibition effect of OC was not from the DMSO effect, and 0.04–0.4% DMSO shows no toxicity to the uterine.

We proposed a hypothetical binding mode for oleocanthal and ibuprofen to the possible active site of human COX-2 (PDB ID: 4ph9), based on a computational docking program. Oleocanthal has been reported as a “natural ibuprofen”, which is a homolog of ibuprofen [17]. The docking results revealed that both oleocanthal and ibuprofen bind to Ser531 through hydrogen bonds and occupy the same as of COX-2 (Figure 3). This suggests that both compounds may have a similar effect to the COX-2 protein.

The previous results of this study show that OC effectively inhibits the effects of uterine contractions. Pain is the most common symptom of dysmenorrhea, so we investigated the effect of extra virgin olive oil extracts on female ICR mice to inhibit the writhing reaction induced by acetic acid (Figure 5a) or oxytocin (Figure 5b). In both models, the amounts of writhing in the EVOO ACN layer extract groups were significantly lower than the control group, indicating that the EVOO ACN layer extracts had an analgesic effect. The EVOO ACN layer also showed an antioxidant ability by receiving a hydrogen ion from the ACN layer, turning the violet DPPH to yellow DPPH [27] (Figure 5c, IC₅₀: 1.54 mg/mL). The plasma also showed that the treatment of OC can significantly reduce the MDA concentration (Figure 5d). Moreover, OC can significantly decrease oxytocin-induced COX-2 protein expression by decreasing OTR and transient receptor potential ankyrin 1 (TRPA1). Furthermore, it decreases OTR-modulated signaling transduction by decreasing the PKC-δ and ERK phosphorylation. Simultaneously, OC decreased the TRPA1-modulated calcium influx signal by decreasing the TRPA1, and the decreased calcium influx induced phosphorylation-MLC20 protein expression (Figure 6).