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. 2021 Dec 31;23(1):426. doi: 10.3390/ijms23010426

Table 6.

Treatments targeting dysbiosis in liver cirrhosis.

Conditions Treatment Main Results Ref.
Human Double blind trial, LC with an episode of HC during the previous month Probiotic preparation (VSL #3) (n = 66)
6 months or placebo (n = 64)
↓ The risk of hospitalization for HE
↓ CTP and MELD score
[157]
Human LC with MHE
: randomized LGG
or placebo group
Probiotic group, 8 weeks
or placebo
↓ Endotoxemia, TNF-α [158]
Alteration in gut microbiome
-↓ Enterobacteriaceae,Clostridiales Incertae Sedis XIV, ↑ Lachnospiraceae
Rat CCl4-induced
cirrhotic rats
LI01: L. salivarius
LI05: P. pentosaceus
L. rhamnosus GG,
C. butyricum MIYAIRI and Bacillus,
13 weeks
LI01 or LI05 [154]
-prevent liver fibrosis, ↓ hepatic expression of profibrogenic genes
Alteration in gut microbiome
-↓ Enterobacteriaceae, ↑ Clostridiales Incertae Sedis XIV and Lachnospiraceae
C57BL/6J mice Bile-duct ligation
CCl4-induced cirrhosis
FXR-agonists oral gavage
: fexaramine (100 mg/kg/day)
obeticholic acid (30 mg/kg/day)
FXR-agonists treatment group
- ameliorate pathological translocation of GFP-E. coli from the ileal lumen to the liver in cirrhotic mice
Obeticholic acid treatment group
-significantly increases ileal TJ protein expression (ZO1, claudin-1,-2, and occludin), upregulating them to the level of healthy control mice
[159]

LC, liver cirrhosis; HC, hepatic encephalopathy; CTP, Child–Turcotte–Pugh; MELD, model for end-stage liver disease; MHE, minimal hepatic encephalopathy; CCl4, carbon tetrachloride; TNF, tumor necrosis factor; FXR, farnesoid X receptor; TJ, tight junction; GFP-E. coli, green fluorescent protein, Escherichia coli.