Impact of endothelial nitric oxide synthase activation on accelerated liver regeneration in a rat ALPPS model

Although the associating liver partition and portal vein ligation for staged hepatectomy (ALPPS) induces more rapid liver regeneration than portal vein embolization, the mechanism remains unclear. To assess the influence of inflammatory cytokines and endothelial nitric oxide synthase (eNOS) activati...

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Published in:World journal of gastroenterology : WJG 2023-02, Vol.29 (5), p.867-878
Main Authors: Masuo, Hitoshi, Shimizu, Akira, Motoyama, Hiroaki, Kubota, Koji, Notake, Tsuyoshi, Yoshizawa, Takahiro, Hosoda, Kiyotaka, Yasukawa, Koya, Kobayashi, Akira, Soejima, Yuji
Format: Article
Language:English
Subjects:
Animals
Basic Study
Cytokines
Focal Nodular Hyperplasia
Hepatectomy
Ki-67 Antigen
Ligation
Liver - surgery
Liver Neoplasms - surgery
Liver Regeneration - physiology
Molsidomine
NG-Nitroarginine Methyl Ester
Nitric Oxide Synthase Type III
Portal Vein - surgery
Proto-Oncogene Proteins c-akt
Rats
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container_title World journal of gastroenterology : WJG
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creator Masuo, Hitoshi
Shimizu, Akira
Motoyama, Hiroaki
Kubota, Koji
Notake, Tsuyoshi
Yoshizawa, Takahiro
Hosoda, Kiyotaka
Yasukawa, Koya
Kobayashi, Akira
Soejima, Yuji
description Although the associating liver partition and portal vein ligation for staged hepatectomy (ALPPS) induces more rapid liver regeneration than portal vein embolization, the mechanism remains unclear. To assess the influence of inflammatory cytokines and endothelial nitric oxide synthase (eNOS) activation on liver regeneration in ALPPS. The future liver remnant/body weight (FLR/BW) ratio, hepatocyte proliferation, inflammatory cytokine expression, and activation of the Akt-eNOS pathway were evaluated in rat ALPPS and portal vein ligation (PVL) models. Hepatocyte proliferation was assessed based on Ki-67 expression, which was confirmed using immunohistochemistry. The serum concentrations of inflammatory cytokines were measured using enzyme linked immune-solvent assays. The Akt-eNOS pathway was assessed using western blotting. To explore the role of inflammatory cytokines and NO, Kupffer cell inhibitor gadolinium chloride (GdCl ), NOS inhibitor N-nitro-arginine methyl ester (L-NAME), and NO enhancer molsidomine were administered intraperitoneally. The ALPPS group showed significant FLR regeneration (FLR/BW: 1.60% ± 0.08%, < 0.05) compared with that observed in the PVL group (1.33% ± 0.11%) 48 h after surgery. In the ALPPS group, serum interleukin-6 expression was suppressed using GdCl to the same extent as that in the PVL group. However, the FLR/BW ratio and Ki-67 labeling index were significantly higher in the ALPPS group administered GdCl (1.72% ± 0.19%, < 0.05; 22.25% ± 1.30%, < 0.05) than in the PVL group (1.33% ± 0.11% and 12.78% ± 1.55%, respectively). Phospho-Akt Ser and phospho-eNOS Ser levels were enhanced in the ALPPS group compared with those in the PVL group. There was no difference between the ALPPS group treated with L-NAME and the PVL group in the FLR/BW ratio and Ki-67 labeling index. In the PVL group treated with molsidomine, the FLR/BW ratio and Ki-67 labeling index increased to the same level as in the ALPPS group. Early induction of inflammatory cytokines may not be pivotal for accelerated FLR regeneration after ALPPS, whereas Akt-eNOS pathway activation may contribute to accelerated regeneration of the FLR.
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To assess the influence of inflammatory cytokines and endothelial nitric oxide synthase (eNOS) activation on liver regeneration in ALPPS. The future liver remnant/body weight (FLR/BW) ratio, hepatocyte proliferation, inflammatory cytokine expression, and activation of the Akt-eNOS pathway were evaluated in rat ALPPS and portal vein ligation (PVL) models. Hepatocyte proliferation was assessed based on Ki-67 expression, which was confirmed using immunohistochemistry. The serum concentrations of inflammatory cytokines were measured using enzyme linked immune-solvent assays. The Akt-eNOS pathway was assessed using western blotting. To explore the role of inflammatory cytokines and NO, Kupffer cell inhibitor gadolinium chloride (GdCl ), NOS inhibitor N-nitro-arginine methyl ester (L-NAME), and NO enhancer molsidomine were administered intraperitoneally. The ALPPS group showed significant FLR regeneration (FLR/BW: 1.60% ± 0.08%, &lt; 0.05) compared with that observed in the PVL group (1.33% ± 0.11%) 48 h after surgery. In the ALPPS group, serum interleukin-6 expression was suppressed using GdCl to the same extent as that in the PVL group. However, the FLR/BW ratio and Ki-67 labeling index were significantly higher in the ALPPS group administered GdCl (1.72% ± 0.19%, &lt; 0.05; 22.25% ± 1.30%, &lt; 0.05) than in the PVL group (1.33% ± 0.11% and 12.78% ± 1.55%, respectively). Phospho-Akt Ser and phospho-eNOS Ser levels were enhanced in the ALPPS group compared with those in the PVL group. There was no difference between the ALPPS group treated with L-NAME and the PVL group in the FLR/BW ratio and Ki-67 labeling index. In the PVL group treated with molsidomine, the FLR/BW ratio and Ki-67 labeling index increased to the same level as in the ALPPS group. 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To assess the influence of inflammatory cytokines and endothelial nitric oxide synthase (eNOS) activation on liver regeneration in ALPPS. The future liver remnant/body weight (FLR/BW) ratio, hepatocyte proliferation, inflammatory cytokine expression, and activation of the Akt-eNOS pathway were evaluated in rat ALPPS and portal vein ligation (PVL) models. Hepatocyte proliferation was assessed based on Ki-67 expression, which was confirmed using immunohistochemistry. The serum concentrations of inflammatory cytokines were measured using enzyme linked immune-solvent assays. The Akt-eNOS pathway was assessed using western blotting. To explore the role of inflammatory cytokines and NO, Kupffer cell inhibitor gadolinium chloride (GdCl ), NOS inhibitor N-nitro-arginine methyl ester (L-NAME), and NO enhancer molsidomine were administered intraperitoneally. The ALPPS group showed significant FLR regeneration (FLR/BW: 1.60% ± 0.08%, &lt; 0.05) compared with that observed in the PVL group (1.33% ± 0.11%) 48 h after surgery. In the ALPPS group, serum interleukin-6 expression was suppressed using GdCl to the same extent as that in the PVL group. However, the FLR/BW ratio and Ki-67 labeling index were significantly higher in the ALPPS group administered GdCl (1.72% ± 0.19%, &lt; 0.05; 22.25% ± 1.30%, &lt; 0.05) than in the PVL group (1.33% ± 0.11% and 12.78% ± 1.55%, respectively). Phospho-Akt Ser and phospho-eNOS Ser levels were enhanced in the ALPPS group compared with those in the PVL group. There was no difference between the ALPPS group treated with L-NAME and the PVL group in the FLR/BW ratio and Ki-67 labeling index. In the PVL group treated with molsidomine, the FLR/BW ratio and Ki-67 labeling index increased to the same level as in the ALPPS group. 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subjects Animals
Basic Study
Cytokines
Focal Nodular Hyperplasia
Hepatectomy
Ki-67 Antigen
Ligation
Liver - surgery
Liver Neoplasms - surgery
Liver Regeneration - physiology
Molsidomine
NG-Nitroarginine Methyl Ester
Nitric Oxide Synthase Type III
Portal Vein - surgery
Proto-Oncogene Proteins c-akt
Rats
title Impact of endothelial nitric oxide synthase activation on accelerated liver regeneration in a rat ALPPS model
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