Morphine worsens the severity and prevents pancreatic regeneration in mouse models of acute pancreatitis

Usman Barlass; Raini Dutta; Hassam Cheema; John George; Archana Sareen; Ajay Dixit; Zuobiao Yuan; Bhuwan Giri; Jingjing Meng; Santanu Banerjee; Sulagna Banerjee; Vikas Dudeja; Rajinder K. Dawra; Sabita Roy; Ashok K. Saluja

doi:10.1136/gutjnl-2017-313717

Morphine worsens the severity and prevents pancreatic regeneration in mouse models of acute pancreatitis

Usman Barlass, Raini Dutta, Hassam Cheema, John George, Archana Sareen, Ajay Dixit, Zuobiao Yuan, Bhuwan Giri, Jingjing Meng, Santanu Banerjee, Sulagna Banerjee, Vikas Dudeja, Rajinder K. Dawra, Sabita Roy, Ashok K. Saluja

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Abstract

Background Opioids such as morphine are widely used for the management of pain associated with acute pancreatitis. Interestingly, opioids are also known to affect the immune system and modulate inflammatory pathways in non-pancreatic diseases. However, the impact of morphine on the progression of acute pancreatitis has never been evaluated. In the current study, we evaluated the impact of morphine on the progression and severity of acute pancreatitis. Methods Effect of morphine treatment on acute pancreatitis in caerulein, L-arginine and ethanol-palmitoleic acid models was evaluated after induction of the disease. Inflammatory response, gut permeability and bacterial translocation were compared. Experiments were repeated in mu (μ) opioid receptor knockout mice (MORKO) and in wild-type mice in the presence of opioid receptor antagonist naltrexone to evaluate the role of μ-opioid receptors in morphine's effect on acute pancreatitis. Effect of morphine treatment on pathways activated during pancreatic regeneration like sonic Hedgehog and activation of embryonic transcription factors like pdx-1 and ptf-1 were measured by immunofluorescence and quantitative PCR. Results Histological data show that treatment with morphine after induction of acute pancreatitis exacerbates the disease with increased pancreatic neutrophilic infiltration and necrosis in all three models of acute pancreatitis. Morphine also exacerbated acute pancreatitis-induced gut permeabilisation and bacteraemia. These effects were antagonised in the MORKO mice or in the presence of naltrexone suggesting that morphine's effect on severity of acute pancreatitis are mediated through the μ-opioid receptors. Morphine treatment delayed macrophage infiltration, sonic Hedgehog pathway activation and expression of pdx-1 and ptf-1. Conclusion Morphine treatment worsens the severity of acute pancreatitis and delays resolution and regeneration. Considering our results, the safety of morphine for analgesia during acute pancreatitis should be re-evaluated in future human studies.

Original language	English (US)
Pages (from-to)	719-727
Number of pages	9
Journal	Gut
Volume	67
Issue number	4
DOIs	https://doi.org/10.1136/gutjnl-2017-313717
State	Published - Apr 2018

Bibliographical note

Funding Information:
This work was supported, in whole or in part, by National Institutes of Health DK058694, DK093047, and DK092145 (to AKS), DA034582, K05DA033881 (to SR) and intramural support from Department of Surgery, University of Minnesota.

Funding Information:
Funding this work was supported, in whole or in part, by national institutes of Health DK058694, DK093047, and DK092145 (to aKS), Da034582, K05Da033881 (to Sr) and intramural support from Department of Surgery, University of Minnesota.

Publisher Copyright:
© 2018 Article author(s).

Keywords

Morphine
PDX-1
PTF-1
hedgehog
macrophages
pancreatitis
regeneration
severity

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title = "Morphine worsens the severity and prevents pancreatic regeneration in mouse models of acute pancreatitis",

abstract = "Background Opioids such as morphine are widely used for the management of pain associated with acute pancreatitis. Interestingly, opioids are also known to affect the immune system and modulate inflammatory pathways in non-pancreatic diseases. However, the impact of morphine on the progression of acute pancreatitis has never been evaluated. In the current study, we evaluated the impact of morphine on the progression and severity of acute pancreatitis. Methods Effect of morphine treatment on acute pancreatitis in caerulein, L-arginine and ethanol-palmitoleic acid models was evaluated after induction of the disease. Inflammatory response, gut permeability and bacterial translocation were compared. Experiments were repeated in mu (μ) opioid receptor knockout mice (MORKO) and in wild-type mice in the presence of opioid receptor antagonist naltrexone to evaluate the role of μ-opioid receptors in morphine's effect on acute pancreatitis. Effect of morphine treatment on pathways activated during pancreatic regeneration like sonic Hedgehog and activation of embryonic transcription factors like pdx-1 and ptf-1 were measured by immunofluorescence and quantitative PCR. Results Histological data show that treatment with morphine after induction of acute pancreatitis exacerbates the disease with increased pancreatic neutrophilic infiltration and necrosis in all three models of acute pancreatitis. Morphine also exacerbated acute pancreatitis-induced gut permeabilisation and bacteraemia. These effects were antagonised in the MORKO mice or in the presence of naltrexone suggesting that morphine's effect on severity of acute pancreatitis are mediated through the μ-opioid receptors. Morphine treatment delayed macrophage infiltration, sonic Hedgehog pathway activation and expression of pdx-1 and ptf-1. Conclusion Morphine treatment worsens the severity of acute pancreatitis and delays resolution and regeneration. Considering our results, the safety of morphine for analgesia during acute pancreatitis should be re-evaluated in future human studies.",

keywords = "Morphine, PDX-1, PTF-1, hedgehog, macrophages, pancreatitis, regeneration, severity",

author = "Usman Barlass and Raini Dutta and Hassam Cheema and John George and Archana Sareen and Ajay Dixit and Zuobiao Yuan and Bhuwan Giri and Jingjing Meng and Santanu Banerjee and Sulagna Banerjee and Vikas Dudeja and Dawra, {Rajinder K.} and Sabita Roy and Saluja, {Ashok K.}",

note = "Funding Information: This work was supported, in whole or in part, by National Institutes of Health DK058694, DK093047, and DK092145 (to AKS), DA034582, K05DA033881 (to SR) and intramural support from Department of Surgery, University of Minnesota. Funding Information: Funding this work was supported, in whole or in part, by national institutes of Health DK058694, DK093047, and DK092145 (to aKS), Da034582, K05Da033881 (to Sr) and intramural support from Department of Surgery, University of Minnesota. Publisher Copyright: {\textcopyright} 2018 Article author(s).",

year = "2018",

month = apr,

doi = "10.1136/gutjnl-2017-313717",

language = "English (US)",

volume = "67",

pages = "719--727",

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T1 - Morphine worsens the severity and prevents pancreatic regeneration in mouse models of acute pancreatitis

AU - Barlass, Usman

AU - Dutta, Raini

AU - Cheema, Hassam

AU - George, John

AU - Sareen, Archana

AU - Dixit, Ajay

AU - Yuan, Zuobiao

AU - Giri, Bhuwan

AU - Meng, Jingjing

AU - Banerjee, Santanu

AU - Banerjee, Sulagna

AU - Dudeja, Vikas

AU - Dawra, Rajinder K.

AU - Roy, Sabita

AU - Saluja, Ashok K.

N1 - Funding Information: This work was supported, in whole or in part, by National Institutes of Health DK058694, DK093047, and DK092145 (to AKS), DA034582, K05DA033881 (to SR) and intramural support from Department of Surgery, University of Minnesota. Funding Information: Funding this work was supported, in whole or in part, by national institutes of Health DK058694, DK093047, and DK092145 (to aKS), Da034582, K05Da033881 (to Sr) and intramural support from Department of Surgery, University of Minnesota. Publisher Copyright: © 2018 Article author(s).

PY - 2018/4

Y1 - 2018/4

N2 - Background Opioids such as morphine are widely used for the management of pain associated with acute pancreatitis. Interestingly, opioids are also known to affect the immune system and modulate inflammatory pathways in non-pancreatic diseases. However, the impact of morphine on the progression of acute pancreatitis has never been evaluated. In the current study, we evaluated the impact of morphine on the progression and severity of acute pancreatitis. Methods Effect of morphine treatment on acute pancreatitis in caerulein, L-arginine and ethanol-palmitoleic acid models was evaluated after induction of the disease. Inflammatory response, gut permeability and bacterial translocation were compared. Experiments were repeated in mu (μ) opioid receptor knockout mice (MORKO) and in wild-type mice in the presence of opioid receptor antagonist naltrexone to evaluate the role of μ-opioid receptors in morphine's effect on acute pancreatitis. Effect of morphine treatment on pathways activated during pancreatic regeneration like sonic Hedgehog and activation of embryonic transcription factors like pdx-1 and ptf-1 were measured by immunofluorescence and quantitative PCR. Results Histological data show that treatment with morphine after induction of acute pancreatitis exacerbates the disease with increased pancreatic neutrophilic infiltration and necrosis in all three models of acute pancreatitis. Morphine also exacerbated acute pancreatitis-induced gut permeabilisation and bacteraemia. These effects were antagonised in the MORKO mice or in the presence of naltrexone suggesting that morphine's effect on severity of acute pancreatitis are mediated through the μ-opioid receptors. Morphine treatment delayed macrophage infiltration, sonic Hedgehog pathway activation and expression of pdx-1 and ptf-1. Conclusion Morphine treatment worsens the severity of acute pancreatitis and delays resolution and regeneration. Considering our results, the safety of morphine for analgesia during acute pancreatitis should be re-evaluated in future human studies.

AB - Background Opioids such as morphine are widely used for the management of pain associated with acute pancreatitis. Interestingly, opioids are also known to affect the immune system and modulate inflammatory pathways in non-pancreatic diseases. However, the impact of morphine on the progression of acute pancreatitis has never been evaluated. In the current study, we evaluated the impact of morphine on the progression and severity of acute pancreatitis. Methods Effect of morphine treatment on acute pancreatitis in caerulein, L-arginine and ethanol-palmitoleic acid models was evaluated after induction of the disease. Inflammatory response, gut permeability and bacterial translocation were compared. Experiments were repeated in mu (μ) opioid receptor knockout mice (MORKO) and in wild-type mice in the presence of opioid receptor antagonist naltrexone to evaluate the role of μ-opioid receptors in morphine's effect on acute pancreatitis. Effect of morphine treatment on pathways activated during pancreatic regeneration like sonic Hedgehog and activation of embryonic transcription factors like pdx-1 and ptf-1 were measured by immunofluorescence and quantitative PCR. Results Histological data show that treatment with morphine after induction of acute pancreatitis exacerbates the disease with increased pancreatic neutrophilic infiltration and necrosis in all three models of acute pancreatitis. Morphine also exacerbated acute pancreatitis-induced gut permeabilisation and bacteraemia. These effects were antagonised in the MORKO mice or in the presence of naltrexone suggesting that morphine's effect on severity of acute pancreatitis are mediated through the μ-opioid receptors. Morphine treatment delayed macrophage infiltration, sonic Hedgehog pathway activation and expression of pdx-1 and ptf-1. Conclusion Morphine treatment worsens the severity of acute pancreatitis and delays resolution and regeneration. Considering our results, the safety of morphine for analgesia during acute pancreatitis should be re-evaluated in future human studies.

KW - Morphine

KW - PDX-1

KW - PTF-1

KW - hedgehog

KW - macrophages

KW - pancreatitis

KW - regeneration

KW - severity

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Morphine worsens the severity and prevents pancreatic regeneration in mouse models of acute pancreatitis

Abstract

Bibliographical note

Keywords

UN SDGs

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