Removal of luminal content protects the small intestine during hemorrhagic shock but is not sufficient to prevent lung injury

Altshuler, Angelina E.; Richter, Michael; Modestino, Augusta; Penn, Alexander H.; Heller, Michael; Schmid‐Schönbein, Geert W.

doi:10.1002/phy2.109

Cited by 14 publications

(17 citation statements)

References 62 publications

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“…D’Alessandro and coworkers [22] reported that the upregulation of such proteins is accompanied by an impaired homeostasis of the balance between proteases and anti-proteases, especially serine proteases and MMPs, and that this could entail an activation of neutrophils following extracellular matrix metalloproteinase involvement. These observations are consistent with the evidence that digestive enzymes can promote “autodigestion” [2–5]. Hence, we took the next step in this investigation, the analysis of peptides in plasma, with the goal of looking for evidence of proteolytic processes in shock, which could prove impactful in future clinical studies.…”

Section: Discussionsupporting

confidence: 75%

“…The intestinal mucosal barrier may become severely damaged due to hypoperfusion in hemorrhage and sepsis. As a consequence, its function as a barrier between the intestinal lumen and the interstitial tissue and vasculature may become compromised, and digestive enzymes, such as proteases and lipases may exit the intestinal lumen and reach the systemic circulation, resulting in global cellular and organ dysfunction [2–5]. Digestive proteases contribute to malfunction of important transmembrane receptors, such as the insulin receptor, possibly through cleavage [4], but they are also known to activate matrix metalloproteinases (MMPs) in vivo , and could therefore act as mediators of secondary cell and tissue injury.…”

Section: Introductionmentioning

confidence: 99%

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Peptidomic Analysis of Rat Plasma

Aletti

Maffioli

Negri

et al. 2016

Shock

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It has been previously shown that intestinal proteases translocate into the circulation during hemorrhagic shock and contribute to proteolysis in distal organs. However, consequences of this phenomenon have not previously been investigated using high-throughput approaches. Here, a shotgun label-free quantitative proteomic approach was utilized to compare the peptidome of plasma samples from healthy and hemorrhagic shock rats to verify the possible role of uncontrolled proteolytic activity in shock. Plasma was collected from rats after hemorrhagic shock (HS) consisting of two-hour hypovolemia followed by two-hour reperfusion, and from healthy control (CTRL) rats. A new two-step enrichment method was applied to selectively extract peptides and low molecular weight proteins from plasma, and directly analyze these samples by tandem mass spectrometry. 126 circulating peptides were identified in CTRL and 295 in HS animals. 96 peptides were present in both conditions; of these, 57 increased and 30 decreased in shock. In total, 256 peptides were increased or present only in HS confirming a general increase in proteolytic activity in shock. Analysis of the proteases that potentially generated the identified peptides suggests that the larger relative contribution of to the proteolytic activity in shock is due to chymotryptic-like proteases. These results provide quantitative confirmation that extensive, system-wide proteolysis is part of the complex pathologic phenomena occurring in hemorrhagic shock.

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Section: Discussionsupporting

confidence: 75%

Section: Introductionmentioning

confidence: 99%

Peptidomic Analysis of Rat Plasma

Aletti

Maffioli

Negri

et al. 2016

Shock

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View full text Add to dashboard Cite

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“…Aside from its barrier function, the gut contains growth factors, adenosine and hormones, which are potential mediators of the modulation of intestinal inflammation and repair, due to their roles in cellular proliferation, differentiation, migration, apoptosis and autophagy [18][19][20][21][22]. Physiologically, the gut could initiate and propagate sepsis due to the ability of bacteria, endotoxins, and other antigens to translocate, along with the production of pro-inflammatory cytokines and toxins [11].…”

Section: Multistep Pathophysiologymentioning

confidence: 99%

“…The action of these enzymes would involve degradation of inter-enterocytic tight junction's proteins such as E-cadherin. Moreover, these enzymes would also induce a cleavage of the prometalloproteinases into active metalloproteinases [22].…”

Section: Intestinal Autodigestionmentioning

confidence: 99%

Diagnosis biomarkers in acute intestinal ischemic injury: so close, yet so far

Peoc’h

Nuzzo

Guedj

et al. 2017

Clinical Chemistry and Laboratory Medicine (CCLM)

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Acute intestinal ischemic injury (i3) is a lifethreatening condition with disastrous prognosis, which is currently difficult to diagnose at the early stages of the disease; a rapid diagnosis is mandatory to avoid irreversible ischemia, extensive bowel resection, sepsis and death. The overlapping protein expression of liver and gut related to the complex physiopathology of the disease, the heterogeneity of the disease and its relative rarity could explain the lack of a useful early biochemical marker of i3. Apart from non-specific biological markers of thrombosis, hypoxia inflammation, and infection, several more specific biomarkers in relation with the gut barrier dysfunction, the villi injury and the enterocyte mass have been used in the diagnosis of acute i3. It includes particularly D-lactate, intestinal fatty acid-binding protein (FABP) and citrulline. Herein, we will discuss leading publications concerning these historical markers that point out the main limitations reagrding their use in routine clinical practice. We will also introduce the first and limited results arising from omic studies, underlying the remaining effort that needs to be done in the field of acute i3 biological diagnosis, which remains a challenge.

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“…A typical cecal slurry consists of a mixture of fully or partially digested food items, the powerful digestive enzymes, enteral bacteria and viruses, each needs to be contained in the cecum and the intestine to avoid peritoneal cell injuries and inflammation. The containment of these cytotoxic and proinflammatory materials in the cecum or in the lumen of the intestine requires an intact mucosal epithelial barrier (5) and therefore there is a possibility that MMP-8 may be involved in the maintenance of barrier properties.…”

mentioning

confidence: 99%

Removal of luminal content protects the small intestine during hemorrhagic shock but is not sufficient to prevent lung injury

Cited by 14 publications

References 62 publications

Peptidomic Analysis of Rat Plasma

Peptidomic Analysis of Rat Plasma

Diagnosis biomarkers in acute intestinal ischemic injury: so close, yet so far

Is Matrix Metalloproteinase-8 Activity in the Mucosal Barrier a Requirement for Leakage of Cecal Material in Peritonitis?*

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