Bryophyllum pinnatum enhances the inhibitory effect of atosiban and nifedipine on human myometrial contractility: an in vitro study

B. pinnatum leaves were harvested on the 25 March 2014 from B. pinnatum plants cultivated at the Medical Plants Garden located in S. Roque, Brazil, and that descend from seedlings brought from Weleda AG, Arlesheim, Switzerland, in the past. Plant collection did not affect Brazilian biodiversity and was done in accordance to Brazilian Environmental and Biodiversity laws, mainly Provisional Measure 2186–16 from 23 August 2001 that rules access to genetic resources and traditional knowledge. The Medical Plants Garden from S. Roque belongs to Weleda Brazil and the harvested B. pinnatum plants were identified by the Weleda employees Moacyr Copani and Paulo Copani. A voucher specimen ZSS 29717 was deposited at the Zurich Succulent Plant Collection. Leaves were sent by airmail to Weleda Arlesheim, Switzerland, in a refrigerated box. BPJ was obtained by mechanical pressing in a roller, the procedure used in the first step of the production of the active ingredient of Weleda Bryophyllum 50% chewable tablets (Weleda AG, Arlesheim). Unfiltered press juice was kept at − 80 °C until use.

Atosiban (Tractocile®, 7.5 mg/mL injectable solution), was purchased from Ferring Pharmaceuticals, Baar, Switzerland. Nifedipine was obtained from Sigma-Aldrich (purity ≥98%, N7634-1G); a 3.7 μg/mL stock solution was prepared in DMSO.

The ethics committee of canton Zurich approved the study with human myometrium biopsies (KEK-ZH-Nr. 2014–0717, approval date 12.05.2015). Patients were asked prior to elective caesarean sections to donate a myometrium biopsy if the following inclusion criteria were fulfilled: single pregnancy, planned first caesarean section, negative HIV test, age > 18 years, and no tocolysis within 2 weeks before caesarean section.

A myometrial biopsy of approx. 5 g was taken from each study participant at the cranial margin of the uterotomy. The myometrial biopsy was immediately stored in Ringer solution and transported to the lab. Longitudinal strips of muscle of about 15 × 2 × 1 mm were cut and mounted in a myograph bath chamber. Each of the four myograph chambers contained 6 mL of Krebs solution (in mM: NaCl 118, NaHCO₃ 24.9, KCl 4.7, KH₂PO₄ 1.24, CaCl₂ 2.48, MgSO₄ 1.21, Glucose 10, EDTA 0.034; pH = 7.4), with temperature regulated at 37 °C and bubbled with 95% O₂ and 5% CO₂ (PanGas, Dagmersellen, Switzerland). Contractions were recorded with a DMT800MS myograph (Danish Mayo Technology, Denmark) and transferred to a personal computer via a transducer (ADInstruments PowerLab 4/30). Myometrial strips were allowed to contract spontaneously (which took in most cases approximately 2 h). During this time, the Krebs solution was replaced every 30 min.

In preliminary experiments, concentrations of atosiban, nifedipine and BPJ were determined that would lead to moderate lowering (by 20–30%) of contraction strength. These concentrations were used in the main combination experiments, performed as described below. In preliminary experiments, two slightly different experimental protocols appeared equally promising. We used both protocols, one for the experiments with atosiban, and the second for nifedipine, to find out whether one of the protocols would result in lower standard error of the means (SEM) values.

In all cases, regular spontaneous myometrial contractions in amplitude and frequency were recorded for 30 min.

When the effects of the combination of BPJ with atosiban were being studied, each one of four strips was treated with one test substance, and contractility was recorded for additional 30 min. Test substances were: Krebs solution, 5 μL (control; n = 11); BPJ, 15 μL (0.25% final concentration, corresponding to 2.5 μg/mL; n = 13); atosiban, 4.3 μL of 375 μg/mL (0.27 μg/mL final concentration; n = 11); and BPJ and atosiban combined (same concentrations, n = 12). Temporal and vehicle controls were run in parallel in each experiment to access the decay in contractility of the myometrium with time.

To find out whether the effect of the combination treatments would further increase at higher concentrations, a previously described approach was followed [24]. In brief, when spontaneous contractions were regular for 20 min, Krebs solution was added (addition 0), and contractility was recorded for 20 min. Then, each strip was treated with one test substance by adding 4 times, at time intervals of 20 min, the same volume of a stock solution. Test solutions included: control, 5 μL Krebs solution; BPJ, 15 μL; combination of BPJ (15 μL) plus atosiban (4.3 μL of 375 μg/mL) or BPJ (15 μL) plus nifedipine (5 μL of 3.7 μg/mL). For each substance tested, 5 different biopsies were used (n = 5).

The exposure to the different test substances was followed by a 30-min washing period where Krebs solution was changed several times (at 5, 10, 20 and 30 min). Vitality of the strips was determined at the end of the experiment (30 min after washing) by observation of spontaneous contractions. In all cases, strips were contracting and data were included in the present analysis.

Myometrium contractions were recorded by LabChart Pro 8.0.6 (ADInstruments, Germany) and analysed with the peak analysis module. For each contraction, the area under the curve (AUC) and the amplitude were analysed. Depending on the type of experiments, for each 20 or 30 min interval, the average AUC and average amplitude were calculated, and the number of contractions was noted (frequency). Initial values of AUC, amplitude and frequency of spontaneous contractions (before any addition) were set at 100%. Effects after addition of test substances were expressed as percentage of initial. When studying the combination of BPJ and atosiban and in all dose-dependency experiments, the values obtained in one strip per biopsy were used for further statistical analyses. When investigating the combination of BPJ and nifedipine, two strips per biopsy were used to determine the effect of each substance (BPJ, nifedipine, BPJ plus nifedipine, and control). In this case, average values of the two determinations were calculated and used for further statistical analyses.

Human myometrial telomerase reverse transcriptase cell line (hTERT-C3) [25, 26], provided by M. Grãos (University of Coimbra, Portugal), was cultured in an 1:1 mixture of DMEM and F-12 supplemented with antibiotics (100 U/mL penicillin and 100 μg/mL streptomycin) and 10% (v/v) heat-inactivated foetal bovine serum (FBS) (all from Gibco, Paisley, UK). Human uterine myometrium smooth muscle cells (PHM1–41), obtained from American Type Culture Collection (ATCC® CRL-3046™) were maintained in ATCC-formulated DMEM (ATCC® No. 30–2002) supplemented with 0.1 mg/mL G-418 (Carl Roth, Zurich, Switzerland), 2 mM glutamine and 10% (v/v) heat-inactivated FBS.

hTERT-C3 cells were seeded at a density of 5 × 10⁴ cells/mL (5 × 10³ cells per well) and PHM1–41 cells at a density of 8 × 10⁴ cells/mL (8 × 10³ cells per well) into transparent 96-well microplates. 1 day after seeding, cells were exposed to BPJ (2.5–10.0 μg/mL), atosiban (0.27–1.08 μg/mL), nifedipine (3.0–12.0 ng/mL) or the combinations BPJ plus atosiban or BPJ plus nifedipine for 24 h. After exposure, resazurin (Alamar Blue, Invitrogen, Illkirch Cedex, France) was added to cells (final concentration 1.0 mg/mL), and the plate incubated at 37 °C for 4 h. The extent of resazurin reduction was measured in a microplate reader (SpectraMax Paradigm, Molecular Devices, Berkshire, UK) at 570 and 600 nm. For each substance tested, 4 independent experiments were carried out in quadruplicate. Ethyl methanesulfonate (30 mM) [27] and Triton X-100 (1%) were used as a positive control. In each experiment, wells with no test substance added to the culture medium served as untreated control (100% viability). Cell viability was determined according to the following equation: \documentclass[12pt]{minimal} \usepackage{amsmath} \usepackage{wasysym} \usepackage{amsfonts} \usepackage{amssymb} \usepackage{amsbsy} \usepackage{mathrsfs} \usepackage{upgreek} \setlength{\oddsidemargin}{-69pt} \begin{document}$$ \mathrm{Viability}=\frac{\left({\mathrm{A}}_{570}-{\mathrm{A}}_{600}\right)\mathrm{sample}-\left({\mathrm{A}}_{570}-{\mathrm{A}}_{600}\right)\mathrm{blank}}{\left({\mathrm{A}}_{570}-{\mathrm{A}}_{600}\right)\mathrm{control}-\left({\mathrm{A}}_{570}-{\mathrm{A}}_{600}\right)\mathrm{blank}} $$\end{document}Viability=A570−A600sample−A570−A600blankA570−A600control−A570−A600blank

Myometrium hTERT-C3 cells and PHM1–41 cells were stained with fluorescent probes for nuclei (double-stranded DNA) and cytoplasm (F-actin), as follows. After treatment with test substances, alone or combined, for 24 h, cells were washed with phosphate buffered saline (PBS; Gibco, Paisley, UK) and fixed with 4% paraformaldehyde (PFA; from Artechemis, Zoffingen, Switzerland) in PBS for 20 min. Cells were then permeabilised with 0.3% Triton X-100 (Sigma, St. Louis, USA) in 1% bovine serum albumin (BSA; Sigma, St. Louis, USA) for 30 min. Then, cells were incubated with a 1:10000 dilution of 4′,6-diamidino-2-phenylindole (DAPI; Sigma, St. Louis, USA) and 1:400 rhodamine phalloidin (Invitrogen, Illkirch Cedex, France) prepared in 0.1% Triton X-100 (Sigma, St. Louis, USA) in 1% BSA, for 4 h, in the dark. Cells were rinsed with PBS and examined with the Leica CTR 6000 microscope (Leica microsystems, Heerbrugg, Switzerland). The entire procedure was performed at room temperature.

Statistical analyses were performed using GraphPad Prism 7 (GraphPad Software, Inc., CA, USA). In all cases, a significance level of p < 0.05 was considered statistically significant.

Because of the slightly different experimental set-ups used to investigate the combinations of BPJ with atosiban and of BPJ with nifedipine in the myograph model, different tests were used in the two cases. Data from the combination of BPJ and atosiban measurements were analysed with the Kruskal Wallis test followed by Dunn’s multiple comparisons test. Data from the combination of BPJ and nifedipine were analysed with the Wilcoxon test to compare control with BPJ and nifedipine with the combination (determinations in the same strips, paired test), and with the Mann-Whitney to compare control with nifedipine and with combination (determinations in different strips, unpaired test). Effects of combination treatments on myometrial contractility are expressed in scatter dot plots as mean values ± SEM.

For each test substance, dose-dependency data obtained in the myograph model and cell viability data was analysed with the paired, non-parametric Friedman test. Statistical analyses of cell viability data was followed by Dunn’s multiple comparisons test. In the case of the single concentrations of positive controls used in cell viability assays, the paired t-test was used to compare their effects with untreated control. Myograph measurements on dose-dependency and cell viability data are given as mean ± SEM.

BPJ decreased the amplitude to 91.0 ± 4.6% of initial, and atosiban to 93.4 ± 4.6% of initial, but the decreases were not statistically significant. The combination of BPJ and atosiban led to a significantly stronger decrease of amplitude (80.1 ± 7.4% of initial, p = 0.01; Fig. 2b) relative to control.

The frequency of myometrial contractions increased with the addition of BPJ to 204.7 ± 27.8% of initial, which was significantly higher than with atosiban (81.0 ± 10.1% of initial; p = 0.03). Also, the combination of BPJ and atosiban led to a significant increase of frequency (345.4 ± 73.0% of initial) relative to control and atosiban alone (p = 0.010 and p < 0.001, respectively; Fig. 2c) that per se did not increase frequency.

The amplitude of myometrial contractions decreased with BPJ (91.7 ± 4.7%), nifedipine (86.4 ± 4.4%), and the combination (65.4 ± 5.3%). Compared to control, the effect of nifedipine (p < 0.001) and the combination of BPJ with nifedipine (p = 0.003) was significant. The combination of BPJ and nifedipine also significantly decreased the amplitude when compared to nifedipine alone (p = 0.002; Fig. 4b).

As shown in Fig. 4c, BPJ strongly increased the frequency of myometrial contractions to 257.1 ± 40.6% of initial (p < 0.001). In contrast, nifedipine alone had no effect on frequency when compared to control. However, the combination of BPJ and nifedipine led to an increase of 190.1 ± 22.2% of initial, which was significantly different from control (p < 0.0001) and from nifedipine alone (p < 0.001; Fig. 4c).

Exposing the strips to successively higher concentrations of the combination of BPJ and nifedipine led to stepwise increases of the inhibitory effects on myometrial contractility (Fig. 3a and b, data on BPJ + Nifedipine).