Administration of human recombinant activated protein C is not associated with pancreatic parenchymal haemorrhage in L-arginine-induced experimental acute pancreatitis

Saurabh Jamdar; Benoy I. Babu; Mahesh Nirmalan; Maria Jeziorska; Raymond F T Mcmahon; Ajith K. Siriwardena

doi:10.6092/1590-8577/1328

Administration of human recombinant activated protein C is not associated with pancreatic parenchymal haemorrhage in L-arginine-induced experimental acute pancreatitis

Saurabh Jamdar, Benoy I. Babu, Mahesh Nirmalan, Maria Jeziorska, Raymond F T Mcmahon, Ajith K. Siriwardena

Research output: Contribution to journal › Article › peer-review

Abstract

Context Microvascular thrombosis is a critical event in severe acute pancreatitis. Human recombinant activated protein C (Xigris®, Eli Lilly, Indianapolis, IN, USA) modulates the interplay between pro-inflammatory and pro-coagulant pathways and maintains microvascular patency. However, the anticoagulant properties of Xigris® may precipitate bleeding from the inflamed pancreas. This study tests the hypothesis that Xigris® can ameliorate experimental acute pancreatitis without causing pancreatic haemorrhage. Methods Sprague Dawley rats were allocated as follows: Group 1: control (n=7); Group 2: acute pancreatitis (n=6); Group 3: administration of Xigris® 500 μg/kg body weight before induction of acute pancreatitis (n=6); and Group 4: Administration of Xigris® 500 μg/kg body weight 30 minutes after induction of acute pancreatitis (n=6). Acute pancreatitis was induced by intraperitoneal administration of L-arginine 300 mg/100 g body weight. Animals were sacrificed at 48 hours and biochemical, haematological, and histological markers of pancreatic haemorrhage and inflammation assessed. Results Median lipase in animals with acute pancreatitis was 10 U/mL (range: 7-16 U/mL) compared to 5.5 (range: 3-8 U/mL) in controls (P=0.028). Lipase was also elevated in animals given Xigris® both before (12 U/mL, range: 8-22 U/mL; P=0.031 vs. control group) and after (46 U/mL, range: 9-71 U/mL; P=0.015 vs. control group) induction of acute pancreatitis). Haemoglobin levels were similar among all groups (P=0.323). There was no histological evidence of pancreatic haemorrhage in animals treated with Xigris®. Pre-treatment with Xigris® was associated with a significant reduction in pancreatic injury. This effect was absent when Xigris® was administered after induction of acute pancreatitis. Conclusion Xigris® did not lead to pancreatic haemorrhage in experimental acute pancreatitis. Administration of Xigris® prior to induction of acute pancreatitis was associated with amelioration of injury. This effect was not seen with administration of Xigris® after induction of acute pancreatitis.

Original language	English
Pages (from-to)	610-617
Number of pages	7
Journal	Journal of the Pancreas
Volume	14
Issue number	6
DOIs	https://doi.org/10.6092/1590-8577/1328
Publication status	Published - 10 Nov 2013

Keywords

Arginine
Drotrecogin alfa activated
Pancreatitis, Acute necrotizing
Protein c
Recombinant proteins

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10.6092/1590-8577/1328

http://www.serena.unina.it/index.php/jop/article/Download/1328/1974

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@article{d5cdb731ec4a4d86af266b0d3e19f035,

title = "Administration of human recombinant activated protein C is not associated with pancreatic parenchymal haemorrhage in L-arginine-induced experimental acute pancreatitis",

abstract = "Context Microvascular thrombosis is a critical event in severe acute pancreatitis. Human recombinant activated protein C (Xigris{\textregistered}, Eli Lilly, Indianapolis, IN, USA) modulates the interplay between pro-inflammatory and pro-coagulant pathways and maintains microvascular patency. However, the anticoagulant properties of Xigris{\textregistered} may precipitate bleeding from the inflamed pancreas. This study tests the hypothesis that Xigris{\textregistered} can ameliorate experimental acute pancreatitis without causing pancreatic haemorrhage. Methods Sprague Dawley rats were allocated as follows: Group 1: control (n=7); Group 2: acute pancreatitis (n=6); Group 3: administration of Xigris{\textregistered} 500 μg/kg body weight before induction of acute pancreatitis (n=6); and Group 4: Administration of Xigris{\textregistered} 500 μg/kg body weight 30 minutes after induction of acute pancreatitis (n=6). Acute pancreatitis was induced by intraperitoneal administration of L-arginine 300 mg/100 g body weight. Animals were sacrificed at 48 hours and biochemical, haematological, and histological markers of pancreatic haemorrhage and inflammation assessed. Results Median lipase in animals with acute pancreatitis was 10 U/mL (range: 7-16 U/mL) compared to 5.5 (range: 3-8 U/mL) in controls (P=0.028). Lipase was also elevated in animals given Xigris{\textregistered} both before (12 U/mL, range: 8-22 U/mL; P=0.031 vs. control group) and after (46 U/mL, range: 9-71 U/mL; P=0.015 vs. control group) induction of acute pancreatitis). Haemoglobin levels were similar among all groups (P=0.323). There was no histological evidence of pancreatic haemorrhage in animals treated with Xigris{\textregistered}. Pre-treatment with Xigris{\textregistered} was associated with a significant reduction in pancreatic injury. This effect was absent when Xigris{\textregistered} was administered after induction of acute pancreatitis. Conclusion Xigris{\textregistered} did not lead to pancreatic haemorrhage in experimental acute pancreatitis. Administration of Xigris{\textregistered} prior to induction of acute pancreatitis was associated with amelioration of injury. This effect was not seen with administration of Xigris{\textregistered} after induction of acute pancreatitis.",

keywords = "Arginine, Drotrecogin alfa activated, Pancreatitis, Acute necrotizing, Protein c, Recombinant proteins",

author = "Saurabh Jamdar and Babu, {Benoy I.} and Mahesh Nirmalan and Maria Jeziorska and Mcmahon, {Raymond F T} and Siriwardena, {Ajith K.}",

year = "2013",

month = nov,

day = "10",

doi = "10.6092/1590-8577/1328",

language = "English",

volume = "14",

pages = "610--617",

journal = "Journal of the Pancreas",

issn = "1590-8577",

publisher = "E.S. Burioni Ricerche Bibliografiche",

number = "6",

}

TY - JOUR

T1 - Administration of human recombinant activated protein C is not associated with pancreatic parenchymal haemorrhage in L-arginine-induced experimental acute pancreatitis

AU - Jamdar, Saurabh

AU - Babu, Benoy I.

AU - Nirmalan, Mahesh

AU - Jeziorska, Maria

AU - Mcmahon, Raymond F T

AU - Siriwardena, Ajith K.

PY - 2013/11/10

Y1 - 2013/11/10

N2 - Context Microvascular thrombosis is a critical event in severe acute pancreatitis. Human recombinant activated protein C (Xigris®, Eli Lilly, Indianapolis, IN, USA) modulates the interplay between pro-inflammatory and pro-coagulant pathways and maintains microvascular patency. However, the anticoagulant properties of Xigris® may precipitate bleeding from the inflamed pancreas. This study tests the hypothesis that Xigris® can ameliorate experimental acute pancreatitis without causing pancreatic haemorrhage. Methods Sprague Dawley rats were allocated as follows: Group 1: control (n=7); Group 2: acute pancreatitis (n=6); Group 3: administration of Xigris® 500 μg/kg body weight before induction of acute pancreatitis (n=6); and Group 4: Administration of Xigris® 500 μg/kg body weight 30 minutes after induction of acute pancreatitis (n=6). Acute pancreatitis was induced by intraperitoneal administration of L-arginine 300 mg/100 g body weight. Animals were sacrificed at 48 hours and biochemical, haematological, and histological markers of pancreatic haemorrhage and inflammation assessed. Results Median lipase in animals with acute pancreatitis was 10 U/mL (range: 7-16 U/mL) compared to 5.5 (range: 3-8 U/mL) in controls (P=0.028). Lipase was also elevated in animals given Xigris® both before (12 U/mL, range: 8-22 U/mL; P=0.031 vs. control group) and after (46 U/mL, range: 9-71 U/mL; P=0.015 vs. control group) induction of acute pancreatitis). Haemoglobin levels were similar among all groups (P=0.323). There was no histological evidence of pancreatic haemorrhage in animals treated with Xigris®. Pre-treatment with Xigris® was associated with a significant reduction in pancreatic injury. This effect was absent when Xigris® was administered after induction of acute pancreatitis. Conclusion Xigris® did not lead to pancreatic haemorrhage in experimental acute pancreatitis. Administration of Xigris® prior to induction of acute pancreatitis was associated with amelioration of injury. This effect was not seen with administration of Xigris® after induction of acute pancreatitis.

AB - Context Microvascular thrombosis is a critical event in severe acute pancreatitis. Human recombinant activated protein C (Xigris®, Eli Lilly, Indianapolis, IN, USA) modulates the interplay between pro-inflammatory and pro-coagulant pathways and maintains microvascular patency. However, the anticoagulant properties of Xigris® may precipitate bleeding from the inflamed pancreas. This study tests the hypothesis that Xigris® can ameliorate experimental acute pancreatitis without causing pancreatic haemorrhage. Methods Sprague Dawley rats were allocated as follows: Group 1: control (n=7); Group 2: acute pancreatitis (n=6); Group 3: administration of Xigris® 500 μg/kg body weight before induction of acute pancreatitis (n=6); and Group 4: Administration of Xigris® 500 μg/kg body weight 30 minutes after induction of acute pancreatitis (n=6). Acute pancreatitis was induced by intraperitoneal administration of L-arginine 300 mg/100 g body weight. Animals were sacrificed at 48 hours and biochemical, haematological, and histological markers of pancreatic haemorrhage and inflammation assessed. Results Median lipase in animals with acute pancreatitis was 10 U/mL (range: 7-16 U/mL) compared to 5.5 (range: 3-8 U/mL) in controls (P=0.028). Lipase was also elevated in animals given Xigris® both before (12 U/mL, range: 8-22 U/mL; P=0.031 vs. control group) and after (46 U/mL, range: 9-71 U/mL; P=0.015 vs. control group) induction of acute pancreatitis). Haemoglobin levels were similar among all groups (P=0.323). There was no histological evidence of pancreatic haemorrhage in animals treated with Xigris®. Pre-treatment with Xigris® was associated with a significant reduction in pancreatic injury. This effect was absent when Xigris® was administered after induction of acute pancreatitis. Conclusion Xigris® did not lead to pancreatic haemorrhage in experimental acute pancreatitis. Administration of Xigris® prior to induction of acute pancreatitis was associated with amelioration of injury. This effect was not seen with administration of Xigris® after induction of acute pancreatitis.

KW - Arginine

KW - Drotrecogin alfa activated

KW - Pancreatitis, Acute necrotizing

KW - Protein c

KW - Recombinant proteins

U2 - 10.6092/1590-8577/1328

DO - 10.6092/1590-8577/1328

M3 - Article

C2 - 24216546

SN - 1590-8577

VL - 14

SP - 610

EP - 617

JO - Journal of the Pancreas

JF - Journal of the Pancreas

IS - 6

ER -

Administration of human recombinant activated protein C is not associated with pancreatic parenchymal haemorrhage in L-arginine-induced experimental acute pancreatitis

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Keywords

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