Literature DB >> 16521271

Granulocyte colony-stimulating factor prophylaxis improves survival and inflammation in a two-hit model of hemorrhage and sepsis.

Artur Bauhofer1, Wilfried Lorenz, Frank Kohlert, Alexander Torossian.   

Abstract

OBJECTIVE: We evaluated the effects of a granulocyte-colony stimulating factor (G-CSF) prophylaxis in two clinically relevant situations, hemorrhage on the day before infection (e.g., trauma) and acute hemorrhage followed subsequently by infection (e.g., operative complication). A two-hit model of hemorrhage and polymicrobial peritoneal contamination and infection (PCI) was used to assess the influence of G-CSF on the outcome, bacterial clearance, and cytokine pattern.
DESIGN: Clinic modeling randomized laboratory trial.
SETTING: University laboratory.
SUBJECTS: One hundred thirty-two male rats.
INTERVENTIONS: In trial 1 we compared a) preoperative PCI only; b) preoperative hemorrhage plus PCI; and c) hemorrhage plus PCI plus G-CSF prophylaxis (n=18 rats/group). In trial 2, intraoperative hemorrhage was assessed with the same trial design. Primary end point was survival at 120 hrs. In trial 2 additionally, six rats per group and six naive control rats were used for secondary end point analysis.
MEASUREMENTS AND MAIN RESULTS: Primary end point was mortality at 120 hrs. Secondary end points were granulocyte counts, bacterial clearance, and local cytokine levels. In trial 1 survival rate was 56% after PCI only, 17% after hemorrhage plus PCI, and 61% after hemorrhage plus PCI plus G-CSF (p<.01). In trial 2 survival rate was 33% after PCI only, 17% after hemorrhage plus PCI, and 50% after hemorrhage plus PCI plus G-CSF (p<.05). In trial 2, neutrophil counts were doubled to 66% 1 hr after hemorrhage (p<.05), colony-forming units of microbes in the lung and liver were halved to 166+/-56 and 134+/-28 colony-forming units (p<.05 for liver), and the macrophage inflammatory protein-2 expression in the lung was halved to 0.88+/-0.06 pg of complementary DNA (p<.05) by G-CSF prophylaxis compared with hemorrhage and PCI.
CONCLUSIONS: Hemorrhage (first hit) sensitized the host for a second hit of polymicrobial PCI independent of the timing. G-CSF prophylaxis improved survival and clearance of microbes and reduced the proinflammatory chemokine macrophage inflammatory protein-2 in the lung.

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Year:  2006        PMID: 16521271     DOI: 10.1097/01.ccm.0000201900.01000.6b

Source DB:  PubMed          Journal:  Crit Care Med        ISSN: 0090-3493            Impact factor:   7.598


  6 in total

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Review 2.  Intramedullary nailing as a 'second hit' phenomenon in experimental research: lessons learned and future directions.

Authors:  Nikolaos G Lasanianos; Nikolaos K Kanakaris; Peter V Giannoudis
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3.  Pre-existing renal disease promotes sepsis-induced acute kidney injury and worsens outcome.

Authors:  Kent Doi; Asada Leelahavanichkul; Xuzhen Hu; Karen L Sidransky; Hua Zhou; Yan Qin; Christoph Eisner; Jürgen Schnermann; Peter S T Yuen; Robert A Star
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4.  Modulation of Innate Immunity by G-CSF and Inflammatory Response by LBPK95A Improves the Outcome of Sepsis in a Rat Model.

Authors:  Haoshu Fang; Chuanfeng Hua; Stefanie Weiss; Anding Liu; Wenhui Cheng; Ralf Claus; Jürgen Rödel; Olaf Dirsch; Uta Dahmen
Journal:  J Immunol Res       Date:  2018-11-07       Impact factor: 4.818

Review 5.  Of mice and men: Laboratory murine models for recapitulating the immunosuppression of human sepsis.

Authors:  Ning Wang; Yongling Lu; Jiang Zheng; Xin Liu
Journal:  Front Immunol       Date:  2022-08-05       Impact factor: 8.786

6.  Differential effects of antibiotics in combination with G-CSF on survival and polymorphonuclear granulocyte cell functions in septic rats.

Authors:  Artur Bauhofer; Markus Huttel; Wilfried Lorenz; Daniel I Sessler; Alexander Torossian
Journal:  BMC Infect Dis       Date:  2008-04-30       Impact factor: 3.090

  6 in total

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