| Germ-free and Specific-pathogen free rats |
Presence of auto-Abs against appetite-regulating neuropeptides found in both groups Levels differed (lower levels observed in Germ-free rats) Conclusion: Gut microbiota modulates auto-Ab levels against appetite-regulating neuropeptides, but not necessary for auto-Ab production |
n = 6/group |
Fetissov et al. (2008a) |
| Healthy female participants |
|
n = 15 |
| Male C57Bl/6 mice |
Anti-ClpB auto-Abs cross-reactive with α-MSH lead to reduced MC4R signaling and influenced food intake, body weight, and anxiety behavior Conclusion: Anti-ClpB auto-Abs influence ED-related behaviors via reduced sensitivity to anorexigenic effects of α-MSH |
n = 8/group |
Tennoune et al. (2014) |
| Female patients with AN, BN, or BED |
Anti-ClpB auto-Abs against α-MSH elevated in ED patients and correlated with ED-related behaviors Conclusion: ClpB protein can alter auto-Ab production and impact feeding and emotion in humans with EDs |
AN n = 27 BN n = 32 BED n = 14 Control n = 65 |
| Adult Wistar rats |
Sex-related differences in male and female rat food and water intake in response to E. coli K12 gavage Conclusion: Sex-related differences in gut microbiota contribute to differences in satiety, feeding, and emotion and may represent a risk factor for ED development |
n = 48 |
Tennoune et al. (2015) |
| Female patients with AN or BN |
Auto-Abs present in both ED and control participants; elevated levels in EDs; differences in auto-Ab levels between AN and BN Auto-Abs correlate with of ED-related behaviors Conclusion: ED-related psychobehavioral outcomes correlate with auto-Ab levels against α-MSH |
AN n = 12 BN n = 42 Control n = 41 |
Fetissov et al. (2005) |
| Female patients with AN or BN and male Sprague-Dawley rats |
Human sera (from ED and control participants) applied to rat brains and adsorbed with appetite-regulating neuropeptides; reduced staining observed for α-MSH and ACTH Conclusion: Plasma auto-Abs from ED participants have the potential to cross-react with administered peptides |
AN n = 12 BN n = 42 Control n = 41 |
Fetissov et al. (2005) |
| Female patients with AN, BN or BED |
ClpB present in all groups, but higher in EDs ClpB positively correlated with α-MSH auto-Abs and ED-related behaviors Conclusion: ED-related psychobehavioral outcomes are correlated with gut microbial factors |
AN n = 24 BN n = 29 BED n = 13 Control n = 29 |
Breton et al. (2016a) |
| Female patients with AN |
AN patients demonstrated lower microbial diversity than healthy controls; diversity correlated with ED-related clinical assessments Slight improvements in diversity occurred during AN treatment Conclusion: Intestinal dysbiosis is associated with altered mood and ED symptoms in patients with AN |
T1 n = 16 T2 n = 19 Control n = 12 |
Kleiman et al. (2015b) |
| Female patients with AN and/or BN and Sprague-Dawley rats |
Human sera applied to rat brains and adsorbed with melanotropes and/or corticotropes; reduced staining observed for α-MSH and ACTH Conclusion: A significant subpopulation of ED patients has auto-Abs with the potential to cross react with administered peptides |
AN n = 28 BN n = 22 AN/BN n = 7 Control n = 13 |
Fetissov et al. (2002) |
