Babao Dan improves neurocognitive function by inhibiting inflammation in clinical minimal hepatic encephalopathy - 03/03/21
, Chao Wu a, b, 1 , Nisma Lena Bahaji Azami a, b , Dong Xie a, b , Changqing Zhao a , Wan Xu a, b , Dengcheng Hui a, b , Xi Chen c , Runfei Sun a , Jingru Song a, b , Yongtong An d , Kun Li e , Huijun Wang e , Guan Ye d, ⁎ , Mingyu Sun a, b, ⁎ Benvenuto su EM|consulte, il riferimento dei professionisti della salute.
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Graphical abstract |
Highlights |
• | Inhibition of inflammation is beneficial to the treatment of MHE. |
• | BBD plus lactulose inhibited systemic inflammation and improved MHE clinically. |
• | BBD inhibited inflammation in BMDMs/PMs/microglia/astrocytes through TLR4 pathway. |
• | BBD improved neurocognitive dysfunction in mice with endotoxin shock/endotoxemia. |
• | BBD inhibited inflammation via TLR4 pathway to improve neurocognitive function. |
Abstract |
Background and purpose |
Inflammation has been considered a precipitating event that contributes to neurocognitive dysfunction in minimal hepatic encephalopathy (MHE). Inhibition TLR-4 related inflammation can effectively improve neurocognitive dysfunction of MHE. Our previous study showed that Babao Dan (BBD) effectively inhibited inflammation and ameliorated neurocognitive function in rats with acute hepatic encephalopathy (HE) and chronic HE. The mechanism may lie in the regulation of TLR4 signaling pathway. Therefore, this study aimed to evaluate the role of BBD in the treatment of MHE patients with cirrhosis and to elucidate the underlying mechanism by which BBD regulated TLR4 pathway to alleviate inflammation.
Methods |
A randomized controlled trial (n = 62) was conducted to evaluate the clinical efficacy between BBD plus lactulose (n = 31) and lactulose alone (n = 31) in MHE patients by testing neurocognitive function (NCT-A and DST), blood ammonia, liver function (ALT, AST and TBIL) and blood inflammation (IL-1β, IL-6 and TNF-α). Afterward, we detected NO, inflammatory cytokines (IL-1β, IL-6 and TNF-α) and the phosphorylation of P65, JNK, ERK as well as P38 in LPS-activated rat primary bone marrow-derived macrophages (BMDMs), peritoneal macrophages (PMs), and mouse primary BMDMs/PMs/microglia/astrocytes, to investigate the underlying mechanism of BBD inhibiting inflammation through TLR4 pathway. Also, the survival rate of mice, liver function (ALT, AST), blood inflammation (IL-1β, IL-6 and TNF-α), inflammatory cytokines (IL-1β, IL-6 and TNF-α) and histopathological changes in the liver, brain and lung were measured to assess the anti-inflammatory effect of BBD on neurocognitive function in endotoxin shock/endotoxemia mice.
Results |
BBD combined with lactulose significantly ameliorated neurocognitive function by decreasing NCT-A ( p <0.001) and increasing DST ( p <0.001); inhibited systemic inflammation by decreasing IL-1β ( p <0.001), IL-6( p <0.001) and TNF-α ( p <0.001); reduced ammonia level ( p = 0.005), and improved liver function by decreasing ALT( p = 0.043), AST( p = 0.003) and TBIL ( p = 0.026) in MHE patients. Furthermore, BBD inhibited gene and protein expression of IL-1β, IL-6 and TNF-α as well as NO in rat primary BMDMs/PMs, and mouse primary BMDMs/PMs/microglia/astrocytes in a dose-dependent manner. BBD inhibited the activation of mouse primary BMDMs/PMs/microglia/astrocytes by regulating TLR4 pathway involving the phosphorylation of P65, JNK, ERK and P38. Also, BBD reduced the mortality of mice with endotoxin shock/endotoxemia; serum levels of ALT, AST, IL-1β, IL-6 and TNF-α; gene expression of IL-1β, IL-6 and TNF-α in the liver, brain and lung, and tissue damage in the liver and lung.
Conclusion |
Our study provided for the first time clinical and experimental evidence supporting the use of BBD in MHE, and revealed that BBD could play a crucial role in targeting and regulating TLR4 inflammatory pathway to improve neurocognitive function in MHE patients.
Il testo completo di questo articolo è disponibile in PDF.Abbreviation : BBD, HE, MHE, OHE, BMDMs, PMs, LPS, TLR4
Chemical compounds studied in this article : Dimethyl sulfoxide (DMSO) (PubChem CID: 679), Ethanol (PubChem CID: 702) chloroform (PubChem CID: 6212), Methanol (PubChem CID: 887), Acrylamide (PubChem CID: 6579), Ammonium persulfate (PubChem CID: 62648), Glycine (PubChem CID: 750), Sodium chloride (PubChem CID: 5234), Formaldehyde (PubChem CID: 712), Potassium chloride (PubChem CID: 4873), Disodium hydrogen phosphate (PubChem CID:24203), Potassium dihydrogen phosphate (PubChem CID: 516951), Xylene (PubChem CID: 6850715), Carbon tetrachloride (PubChem CID: 5943), Thioacetamide (PubChem CID: 2723949), Sodium dihydrogen phosphate (PubChem CID:23672064), Sodium dodecyl sulfate (PubChem CID: 3423265), Tris (PubChem CID: 6503)
Keywords : BBD, MHE, Neurocognitive function, Neuroinflammation, Systemic inflammation, TLR4 pathway
Mappa
Vol 135
Articolo 111084- marzo 2021 Ritorno al numero
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