Table 2.
Preclinical studies
| Study | Sample characteristics | Study design | Intervention | Donor | Measurement | Key findings and conclusions |
|---|---|---|---|---|---|---|
| Zhang et al. 2019 [28] | Chronic Stress Mice | Randomized Controlled Trial | FMT from wildtype (WT) and NLRP3 KO mice to chronic unpredictable stress (CUS) mice | WT and NLRP3 KO mice | SPT, FST, TST, and OFT | • Transplantation of the NLRP3 KO gut microbiota ameliorated CUS-induced depressive-like behaviors. |
| Li et al. 2019 [21] | Antibiotic treated 8 male WT and 8 male chronic unpredictable mild stress (CUMS) mice | Randomized Controlled Trial | Oral FMT for 2 weeks from WT and CUMS mice to antibiotic-treated WT and CUMS mice | 8 WT mice and 8 CUMS mice | SPT, OFT, EPM, FST | • FMT of CUMS microbiota induced anxiety-like and depression-like behavior in the recipient mice |
| Lv et al. 2019 [22] | Antibiotic treated Male rats with and without CUS | Randomized Controlled Trial | 3-day oral FMT from WT and CUMS mice to antibiotic-treated rats with and without CUS | WT and CUMS mice | SPT, OFT, EPM, FST | • Transplantation of CUMS Microbiome Induces Depression-Like Behaviors in Antibiotic-Treated Rats as shown via a decrease in time spent in the central area in the OFT and increased immobility in the TST |
| Xiao et al. 2018 [29] | 6–8 week male C57BL/6 mice | Randomized Controlled Trial | 14 days of saline or oral FMT from alcohol or water exposed mice to healthy control mice | Alcohol-exposed and water-exposed mice | FST and TST | • FMT from alcohol-exposed mice induced depressive behavior in the recipients, shown by significant results in FST and TST |
| • Alcohol withdrawal induced symptoms were transmitted to healthy controls | ||||||
| Yang et al. 2019 [68] | Antibiotic treated two-month-old male C57BL/6 mice | Randomized Controlled Trial | 14 days of FMT from rats to antibiotic treated C57BL/6 mice | Two-month old | Mechanical withdrawal test (MWT), Tail flick test (TFT), SPT, locomotion, TST, and FST | • Antibiotic administration significantly aggravated the MWT scores, latency of TFT, and depression-like behaviors. |
| Sprague Dawley rats with and without anhedonia | ||||||
| • FMT from rats with anhedonia significantly aggravated behavioral abnormalities, pain, depression-like, and anhedonia-like behaviors in recipient mice | ||||||
| • Antibiotics-treated pseudogerm-free mice showed depression-like and anhedonia-like phenotype compared to control group, which were improved by FMT from mice without anhedonia. | ||||||
| Tillmann et al. 2019 [32] | 24 adult male Flinders sensitive line (FSL) and 24 Flinders resistant line | Randomized Controlled Trial | FMT from FRL, saline, or FSL rats to FRL and FSL rats administered every third day over a 16-day period | FSL, FRL, or saline rats | OFT and FST | • Rats receiving FRL feces struggled less than saline-treated ones while there was no difference between FSL feces and saline or FSL and FRL feces. |
| • Rats receiving FSL feces had significantly increased immobility compared with saline, whereas FRL feces did not differ from saline. | ||||||
| • No difference in immobility between FSL and FRL feces. | ||||||
| Langgartner et al. 2018 [25] | Male C57BL/6 N chronically stressed mice via chronic subordinate colony (CSC) | Randomized Controlled Trial | Repeated FMT from non-stressed single-housed control (SHC) mice | Non-stressed, SHC Male C57BL/6 N mice | OFT and open-field/novel object (OF/NO) test | • SHC feces transplantation had mild stress-protective effects as shown by an improvement of CSC-induced thymus atrophy, anxiety, systemic low-grade inflammation, and alterations in bone homeostasis. |
| • CSC feces transplantation slightly aggravated CSC-induced systemic low-grade inflammation and alterations in bone homeostasis in SHC and/or CSC animals. | ||||||
| Jiang et al. 2020 [30] | 18, 7-weeek old, antibiotic treated C57BL/6 J mice | Randomized Controlled Trial | FMT from 6 control, 6 alcohol-induced depression, and 6 alcohol-induced depression nicotinamide riboside (NR) treated mice after 3 weeks of antibiotic treatment | Control, alcohol-induced depression model, and alcohol-induced depression model NR-treated C57BL/6 J mice | SPT, FST, EPM, and Y-Maze | • Mice receiving FMT from alcohol induced depression model exhibited depression-like behaviour |
| • Mice receiving FMT from control or NR mice did not exhibit depression-like behaviour. | ||||||
| Schmidt et al. 2020 [33] | Adult female Lewis rats | Randomized Double-Blind Sham Controlled Trial | FMT from healthy rats is given to rats with spinal cord injury (SCI) | Healthy, uninjured, adult female Lewis rats | Light-dark box, Cylinder test, SPT, EPM, OFT | • FMT from healthy rats significantly reduced depression and anxiety-like behaviour resulting from SCI in the elevated plus maze and light-dark box (significantly more time in open arms of the maze and light box) |
| Siopi et al. 2020 [23] | 8-week old, antibiotic-treated, GF C57BL/6 J mice | Randomized Controlled Trial | Antibiotic-treated GF mice receive FMT from 10 control, or 10 unpredictable chronic mild stress (USMS) mice | Control or UCMS mice | TST, FST, OFT, EPM, Light-dark Box | • FMT from UCMS mice resulted in despair-like behaviour in the TST and FST (increased immobility time in both) |
| Pearson-Leary et al. 2019 [24] | Experimental Intruders: Singly housed male Sprague–Dawley rats | FMT from vulnerable, resilient, and control rats delivered via oral gavage to naïve recipient rats once daily for 5 days. | SL/vulnerable, LL/resilient rats, or control rats | FST and SIT | • FMT from SL/vulnerable rats to naïve, non-stresses rats promotes some stress vulnerability | |
| • No differences in time spent interacting in SIT between recipient groups suggesting no difference in anxiety-like behavior | ||||||
| Residents: Male Long–Evans (LE) retired breeders (600–800 g) were used as residents. | ||||||
| • Rats treated with vulnerable microbiota had increased passive depression-like behaviours (decreased latency to immobility, less time swimming, and increased time spent immobile) | ||||||
| • SL/vulnerable microbiota treated rats also spent less time climbing, but this was not significant |