Eight-week-old male Kunming mice (initially weighed 20–22 g on arrival) were purchased from Beijing Vital River Laboratory Animal Technology Co., Ltd. (Beijing, China). Mice were housed in groups of five in 320 × 215 × 170 mm cages at a constant temperature (23 ± 2°C) with a 12 h light/dark cycle (lights off from 8:00 a.m. to 8:00 p.m.), with free access to food and water. All behavioral experiments were conducted during the dark period and according to the guidelines of the National Institutes of Health Guide for the Care and Use of Laboratory Animals. The present study was reviewed and approved by the Laboratory Animal Ethical and Welfare Committee of Hebei Medical University.

LPS, CO-RM-3, and CO-RM-A1 were purchased from Sigma (Sigma-Aldrich, St. Louis, MO, United States). CO gas (purify >99.99%) was purchased from Wuhan Newradar Trade Company Limited (Wuhan, China). The dosages of CO-RM and CO-rich saline were prepared based on previous studies (Wang et al., 2018b; Chu et al., 2019; Li et al., 2019). The FITC Annexin V apoptosis Detection Kit I was purchased from BD Pharmingen^TM (BD Biosciences, China). HO-1 primary antibody (ab13243, United States) and β-actin primary antibody (ab8227, United States) were purchased from Abcam. The CellTiter96 AQueous One Solution Cell Proliferation Assay Kit was purchased from Promega Corporation (CAT3580, United States).

PC12 cells (from Prof. Di Wen, Hebei Medical University) were cultured in the high-glucose Dulbecco’s modified Eagle’s medium (DMEM) with 10% fetal bovine serum (FBS) at 37°C in a humidified incubator containing 5% of CO₂. According to our previous study (Wang et al., 2019), for the drug treatment, the cells were seeded onto a 96-well culture plate at 5 × 10⁷ cells/well until full confluence (70–80%). After the treatment with CO-RM or saline for 1h, cells were incubated with H₂O₂ (200 µΜ) for another 24 h in the culture medium.

The control plasmid (GFP-OE), recombinant HO-1 (NM_010442) overexpression plasmid (CMV bGlobin-MCS-EGFP-3FLAG-WPRE-hGH polyA, HO-1-GFP OE), and packaged AAV were purchased from Shanghai GeneChem Co. Ltd. (Shanghai, China). Mice were anesthetized with sodium pentobarbital (150 mg/kg, i.p.) and placed in a stereotaxic frame. Mice (n = 7–9) were infused bilaterally with 0.3 μl of purified and concentrated AAV (1.8E+13 v.g/ml) into the dorsal hippocampus region [anterior–posterior (Goldsmith et al., 2016): −2.1 mm, medial lateral (Fan et al., 2017): ±1.4 mm, dorsal ventral (DV): −1.5 mm] using an electric microinjection pump (RWD Life Science Co., Ltd., China) at a rate of 150 nl/min. Behavioral tests were performed 21 days after AAV microinfusion.

The MTS assay was conducted according to the kit’s protocol (Wang et al., 2019). Briefly, PC12 cells (5,000 cells/well) were seeded into 96-well microtiter plates. After incubation with 10–400 μM of CO-RM-3 or CO-RM-A1 for 1 h, the cells were co-incubated with 200 μM of H₂O₂ for another 24 h. Subsequently, 20 μl of MTS solution was added to each well, and the plates were incubated for 3 h at 37°C. Absorbance was measured at 470 nm and used to calculate the relative ratio of cell viability.

The FITC Annexin V Apoptosis Detection Kit (BD Pharmingen^TM, United States) was used for detecting the apoptosis (Wang et al., 2019). Annexin V binding and PI (propidium iodide) staining were determined by flow cytometry (EasycyteTm mini system). The cells were treated with 200 μM of CO-RM-3 for 1 h before incubation with 200 μM of H₂O₂ for 24 h, and washed with ice-cold PBS, and then double-stained for 20 min with FITC-coupled Annexin V protein and PI. Flow cytometry was carried out with a 488-nm laser coupled to a cell sorter (FACSCaliburTM; BD Biosciences). Cells stained with both PI and Annexin V were considered necrotic, and those stained only with Annexin V were considered apoptotic.

On the last day of behavioral testing, mice in each group were randomly selected and were anesthetized with sodium pentobarbital (150 mg/kg, i.p.), and slowly perfused with 4% paraformaldehyde (PFA). Their brains were removed and post-fixed with the same fixative overnight at 4°C followed by graded dehydration (Han et al., 2019). Paraffin-embedded brain slices (20 μm) were incubated with the primary polyclonal rabbit anti–HO-1 (1:500) antibody followed by the fluorescent-conjugated secondary antibody (goat anti-rabbit IgG, 1:200; Sigma-Aldrich). Images were acquired with the use of a scanning laser confocal microscope (LSM780, Carl Zeiss, Germany).

To detect the expression of HO-1 in the dorsal hippocampus region of mice (n = 4), on the last day of behavioral testing, mice were anesthetized with sodium pentobarbital (150 mg/kg, i.p.) and were decapitated for collection of dorsal hippocampus tissue. Protein samples were prepared and analyzed by Western blot. The polyclonal rabbit anti–HO-1 (1:1,000) and anti–β-actin (1:8,000) were used in the present study. Protein band densities were quantified using ImageJ software and were normalized to β-actin (Shi et al., 2012).

CO-RM or saline was administered before H₂O₂/saline treatment (in Exp. 2; n = 6–9 per group) or prior to behavioral testing (in Exp. 3; n = 8–9 per group). CO gas or saline was administered prior to behavioral testing in the absence (Exp. 4; n = 8–9 per group) or presence (Exp. 5; n = 8–9 per group) of LPS-induced depression. Mice were randomly assigned to experimental conditions.

Based on previous studies, LPS was diluted in saline at a constant dose of 0.83 mg/kg and administered intraperitoneally for 3 days. Twenty-four hours after LPS or saline administration in Exp. 5, behavioral tests were conducted in the presence or absence of CO pretreatment. Mice were randomly assigned to one of the following conditions: sal+sal; sal+LPS; saline, 0.1 ml CO+LPS, or 0.3 ml CO+LPS condition (n = 8–9 per group).

The sample size per experimental condition is that each experiment was determined based on a power analysis indicating that n = 7–9 is sufficient to achieve significant results. All data were expressed as mean ± SEM. One-way analyses of variance (ANOVAs) (Basuroy et al.) were used for all data analyses followed by Dunnett’s post hoc tests for multiple group comparisons through SPSS 21.0 statistical software. We ensured that the assumption of parametric statistics was met before using ANOVAs. Levene’s tests of homogeneity indicated equal variance across groups in all experiments (p > 0.05) and the Shapiro–Wilk test confirmed that the data were normally distributed in all experiments (p > 0.05). The values of p < 0.05 were considered statistically significant.

First, we investigated the effect of HO-1 overexpression in the dorsal hippocampus on depressive- and anxiety-like behaviors. The AAV-HO-1 or AAV-GFP control virus was constructed and infused bilaterally into the dorsal hippocampus region of mice (Figure 1A). Immunofluorescence staining results showed that both GFP (Yabluchanskiy et al., 2012) and HO-1 (Sindermann et al., 2021) were expressed in the mouse dorsal hippocampus region (Figure 1Bi). A one-way ANOVA revealed that there were significant differences in the HO-1 protein level (F_(2,11) = 18.419, p < 0.001, Figure 1Bi) between groups. A post hoc analysis revealed that HO-1 protein levels were significantly increased in the dorsal hippocampus area of mice microinfused with AAV-HO-1 virus as compared to those of NAV (naïve) (p = 0.001) or AAV-GFP–treated groups (p < 0.001).

We then conducted a series of behavioral testing to determine whether chemogenetic overexpression of HO-1 produces antidepressant-like responses. In the OFT, no significant difference was observed in time spent in the center (F_(2,24) = 0.063, p = 0.939; Figure 1C) and in the total distance (F_(2,24) = 0.379, p = 0.689; Figure 1D) traveled by naïve, AAV-GFP-OE, and AAV-HO-1-GFP-OE groups. In the NSF, HO-1 overexpression had no significant effect on latency to feeding (F_(2,24) = 1.640, p = 0.215; Figure 1E) and on total food intake (F_(2,24) = 0.286, p = 0.754; Figure 1F). In the SPT, HO-1 overexpression within the dorsal hippocampus showed no significant effect on sucrose preference (F_(2,24) = 0.481, p = 0.624; Figure 1G) and total water intake (F_(2,24) = 0.858, p = 0.437; Figure 1H). However, significant differences between groups were revealed in the FST and TST. One-way ANOVAs on floating time in the FST (F_(2,24) = 11.237, p < 0.001, Figure 1I) and immobility time in the TST (F_(2,24) = 7.715, p = 0.003, Figure 1K) revealed significant differences between groups. A post hoc analysis showed that overexpression of HO-1 within the dorsal hippocampus led to significant antidepressant activities, as indicated by decreased floating time (p < 0.001) and immobility time (p = 0.003), but did not affect the latency to floating (Figure 1J) and latency to immobility (Figure 1L), as compared to mice receiving an AAV-vector control injection and naïve mice. These results indicated that the dorsal hippocampus HO-1 overexpression induced antidepressant-like activities in mice that were evident in the FST and TST.

To determine the potential effects of CO, two commonly used CO-RMs, CO-RM-3 and CO-RM-A1, were used in the H₂O₂-induced cell injury experiment. Four concentrations of each CO-RM were used for subsequent experiments: CO-RM-3 (10, 50, 100, and 200 μM) and CO-RM-A1 (50, 100, 200, and 400 μM). One-way ANOVAs of the MTS test showed there were significant differences in the survival rates (F_(5,24) = 20.765, p < 0.001, Figure 2B; F_(5,24) = 7.795, p < 0.001, Figure 2C) between groups. A post hoc analysis revealed that H₂O₂ treatment significantly reduced the cell survival ratio (p < 0.001, Figure 2B; p < 0.001, Figure 2C), which was blocked by 200 μM CO-RM-3 (p = 0.001) and 400 μM CO-RM-A1 (p = 0.004) pretreatments for 1h, indicating a dose-dependent protection of CO-RMs against H₂O₂-induced PC12 cell injury. One-way ANOVAs on the flow cytometry data revealed significant differences in the cell survival ratio (F_(3,11) = 25.383, p < 0.001, Figure 2D) and cell death ratio (F_(3,11) = 25.242, p < 0.001, Figure 2E) between groups. The post hoc analysis showed that the H₂O₂ treatment significantly reduced the cell survival ratio (p < 0.001) and increased the cell death ratio (p < 0.001), which was all prevented by pretreatment with 200 μM CO-RM-3 (p = 0.001; p = 0.001). These results confirmed that CO-RMs protect PC12 cells from H₂O₂-induced apoptosis, exerting significant protective effects in a dose-dependent manner.

In the next experiment, to determine whether CO produces antidepressant- and anxiolytic-like effects in mice, we conducted a battery of behavioral tests after mice were repeatedly treated with different doses of CO-RM-A1 and CO-RM-3. After a 3-day adaptation period, mice received injections of CO-RM-A1 (3, 10 mg/kg, i.p) or CO-RM-3 (3, 10 mg/kg, i.p) interperitoneally 30 min before behavioral tests (Figure 2F). CO-RM-A1 and CO-RM-3 administration had no effect on time spent in the central zone (F_(4,36) = 0.905, p = 0.472; Figure 2G) and total distance traveled (F_(4,36) = 1.854, p = 0.14; Figure 2H) in the OFT. CO-RM-A1 and CO-RM-3 administration did not affect the latency to feeding (F_(4,36) = 1.538, p = 0.212; Figure 2I) and total intake of food (F_(4,36) = 0.893, p = 0.478; Figure 2J) in the NSF test. However, significant differences between groups were observed in the FST.

One-way ANOVAs on floating time (F_(4,36) = 6.272, p = 0.001, Figure 2K) and latency to floating (F_(4,36) = 4.492, p = 0.005, Figure 2L) revealed significant differences between groups. A post hoc analysis showed that 3 mg/kg (p = 0.031) and 10 mg/kg (p = 0.031) CO-RM-3 treatment decreased floating time, while 10 mg/kg CO-RM-3 increased latency to floating (p = 0.002) of mice as compared to the vehicle group. Thus, these data suggest that CO-RMs produce antidepressant-like effects.

CO-rich saline (0.1, 0.3 ml, i.p.) was used to explore whether direct administration of CO has antidepressant- and anxiolytic-like effects (Figure 3A). A one-way ANOVA on the OFT data revealed that CO-rich saline had an effect on time spent in the center (F_(2,24) = 3.463, p = 0.049; Figure 3B) without influencing the total movement distance (F_(2,24) = 0.987, p = 0.387; Figure 3C). A post hoc analysis showed that CO-rich saline increased the time spent in the center (p = 0.034). The one-way ANOVA on the NSF data revealed that CO-rich saline had a significant effect on latency to feeding (F_(2,28) = 8.892, p = 0.001; Figure 3D) without influencing the total intake (F_(2,28) = 2.391, p = 0.11; Figure 3E). The post hoc analysis showed that both 0.1 ml (p = 0.001) and 0.3 ml (p = 0.003) of CO-rich saline significantly decreased the latency to feeding. In the FST, CO-rich saline treatment had a significant effect on floating time (F_(2,20) = 4.274, p = 0.030; Figure 3F) without influencing the latency to floating (F_(2,20) = 2.817, p = 0.084; Figure 3G). The post hoc analysis showed that both 0.1 ml (p = 0.049) and 0.3 ml (p = 0.030) of CO-rich saline significantly decreased floating time. These behavioral results suggest that CO-rich saline produces rapid antidepressant- and anxiolytic-like effects.

To investigate whether exogenous CO gas could also exert antidepressant- and anxiolytic-like effects, mice were administered with saline (0.3 ml, i.p.) or CO gas (0.1, 0.3 ml, i.p.) 30 min before behavioral testing (Figure 4A). There was no significant effect of CO gas on time spent in the center (F_(2,24) = 0.491, p = 0.618; Figure 4B) and total distance traveled (F_(2,24) = 1.07, p = 0.359; Figure 4C) in the OFT. A one-way ANOVA on the NSF data showed that CO gas had a significant effect on latency to feeding (F_(2,24) = 4.282, p = 0.027; Figure 4D) without influencing the total intake (F_(2,24) = 0.124, p = 0.884; Figure 4E). A post hoc analysis showed that 0.3 ml CO gas injection significantly decreased mice’s latency to feeding (p = 0.017). In the SPT, CO gas injection had no effect on sucrose preference (F_(2,24) = 2.294, p = 0.123; Figure 4F) and total intake (F_(2,24) = 0.772, p = 0.473; Figure 4G). In the FST, CO gas treatment had a significant effect on floating time (F_(2,24) = 9.051, p = 0.001; Figure 4H) without influencing the latency to floating (F_(2,24) = 1.615, p = 0.22; Figure 4I). The post hoc analysis showed that both 0.1 ml (p = 0.017) and 0.3 ml (p = 0.001) CO gas administration significantly reduced the floating time. CO gas treatment had a significant effect on immobility time (F_(2,24) = 4.145, p = 0.030; Figure 4J) without influencing the latency to immobility (F_(2,24) = 1.487, p = 0.246; Figure 4K) in the TST. The post hoc analysis showed that 0.3 ml CO gas administration significantly reduced floating time (p = 0.017). These results suggest that treatment with CO gas can produce significant antidepressant- and anxiolytic-like effects in mice.

To provide additional evidence for the antidepressant- and anxiolytic-like effects of CO, a LPS-induced depression mice model was used (Figure 5A). The mice were randomly divided into four groups: 1) Sal + Sal group, untreated group neither with LPS or CO gas; 2) Sal + LPS group, treated with LPS once and 0.1 ml saline injection daily; 3) CO gas + LPS group, treated with LPS once and 0.1 ml CO gas injection daily; and 4) 0.3 ml CO gas + LPS group, treated with LPS once and 0.3 ml CO gas injection daily. LPS (0.83 mg/kg, 0.2 ml, i.p.) was administered for 3 days. After twenty-four hours, saline and CO gas (0.1 ml, 0.3 ml, i.p.) were administered 30 min before each behavioral experiment.

One-way ANOVAs on the OFT data revealed that there were differences in time spent in the center (F_(3,30) = 5.653, p = 0.004; Figure 5B) and total distance (F_(3,30) = 3.513, p = 0.029; Figure 5C) between groups. A post hoc analysis showed that both 0.1 ml (p = 0.001) and 0.3 ml (p = 0.018) CO gas treatments significantly increased time spent in the center, and that 0.1 ml CO gas treatment significantly increased total distance traveled (p = 0.012), as compared to the Sal + LPS group. In the NSF test, there was a significant difference in the latency to feeding between three groups (F_(3,30) = 4.080, p = 0.016; Figure 5D), while no difference was observed in total food intake (F_(3,30) = 0.094, p = 0.963; Figure 5E). Post hoc analyses showed that LPS prolonged the latency to feeding of mice (p = 0.036), which was not reversed by the CO gas treatment. In the SPT, there was a significant difference in the sucrose preference between groups (F_(3,30) = 4.080, p = 0.016; Figure 5F), while no difference was observed in total intake (F_(3,30) = 1.761, p = 0.176; Figure 5G). Post hoc analyses showed that LPS injection led to a significant decrease in sucrose preference (p = 0.003), which was reversed by 0.1 (p = 0.016) or 0.3 ml (p = 0.001) CO gas treatment. One-way ANOVAs on the FST data revealed that there were significant differences in floating time (F_(3,30) = 10.610, p < 0.001; Figure 5H) and latency to floating (F_(3,30) = 5.314, p = 0.005; Figure 5I). Post hoc analyses showed that LPS significantly prolonged the floating time (p = 0.019), which was reversed by 0.1 ml (p < 0.001) or 0.3 ml (p < 0.001) CO gas treatment, and that both 0.1 ml (p = 0.003) and 0.3 ml (p = 0.018) CO gas treatment increased the latency to floating, as compared to the Sal + LPS group. One-way ANOVAs on the TST data showed that there were significant differences in immobility time (F_(3,30) = 10.330, p < 0.001; Figure 5J) between groups, while no differences were observed in latency to immobility (F_(3,30) = 1.603, p = 0.209; Figure 5K). Post hoc analyses showed that LPS caused prolongation of immobility time (p = 0.034), which was reversed by 0.1 ml (p < 0.001) or 0.3 ml (p < 0.001) CO gas treatment.

These data suggest that CO gas reverses LPS-induced and anxiety-like behaviors in mice.