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Multiple organ dysfunction syndrome, Inflammatory cytokines and intraabdominal hypertension

Intraabdominal hypertension contributes to MODS in two ways:

Intra-abdominal hypertension leads to organ dysfunction via two distinct and separate pathways. First, early on in the disease process there is a purely mechanical effects that cause significant and measurable organ dysfunction largely related to the effect of the elevated pressure on organ function and organ perfusion (see figure below, please also see individual organ system discussions for further detail).

Click here for high resolution PDF of this process

Click here for higher resolution of the poster on the right

As time progresses, untreated IAH also causes immune and inflammatory effects that can result in progressive organ failure –known as multiple organ dysfunction syndrome or MODS. Multiple organ dysfunction syndrome (MODS) is well recognized as a potentially fatal final complication in patients who suffer from hypovolemic or septic shock. MODS is felt to be due to excessive systemic inflammation (SIRS) that causes massive cytokine production.[1, 2] This systemic response, when overly active leads activation of multiple pathways resulting in acute capillary permeability syndrome, cellular metabolic alterations, cellular apoptosis and necrosis.[2, 3]  An important factor in the development of MODS is exposure of the patient to a second insult or “hit” and that there is an underlying driving force or “motor” that leads to the development of MODS.[1, 3]

Two Hit model of MODS and how IAH is related

An emerging body of experimental and clinical evidence suggests that untreated intra-abdominal hypertension (IAH) acts as this second insult in the two-event model of multiple organ failure (MOF). [3-12] The two-event model of multiple organ failure postulates that an initial insult causing cellular ischemia primes the patients immune system for an exaggerated response to any secondary insult.[1, 13, 14] This "priming" occurs for a limited time - about 3-16 hours following the initial insult - at which point the hyperresponsiveness of the immune system begins to taper.[15, 16] Interestingly, the most common time for IAH to develop is within an 8-16 hour time range following an initial tissue insult - the exact period of maximal immune responsiveness. [4, 15, 16] Rezende-Neto el al found that IAH causes elevated levels of pro-inflammatory cytokines (tumor necrosis factor, and interleukins IL-6 and IL-1) as well a lung myeloperoxidase (MPO) in an animal model.[6] They also found that the presence of IAH during the 8-16 hour "critical" time period resulted in a 3-fold increase in inflammatory neutrophil expression.[5] However, animals subjected to IAH insults < 2 hours or > 18 hours after initial insult fared much better. These authors conclude that a vulnerable period exists following ischemic injury and a second insult such as IAH causes a hyper-inflammatory immune response leading to a high incidence of MOF and death.[5] Other investigators have also found increases in inflammatory mediators as well as bacterial translocation across the bowel wall during the ischemic insult that occurs during from intra-abdominal pressure.[8, 17-20] These data suggest that abdominal compartment syndrome is not the terminal event caused by refractory shock/multiple organ failure. Instead, elevated intra-abdominal pressure acts as a "secondary insult" in the two-event model of multiple organ failure, leading to an overly aggressive immune response with inflammatory cytokine release.[4-9] The end result of this undetected and untreated "secondary insult" is multiple organ failure.

From an etiologic perspective it is likely that the gut is the initial motor of MODS and that ischemic injury to the gut due to intra-abdominal hypertension is the “second-hit” that drives the production of the inflammatory cascade leading to MODS.[3] Microcirculation of the gut is disrupted during shock.[21, 22] This can lead to tissue hypoxia and inflammation and loss of endothelial and epithelial function. This loss of barrier function leads to capillary permeability, intestinal edema and ascites formation. Intraabdominal hypertension then develops leading to increases in intestinal ischemia and a self perpetuating cycle of ischemia and inflammation.[10] The damaged gut then acts as a continual source of inflammatory mediators propagating SIRS and eventually MODS. [10, 23]

Interventions that can attenuate the cytokine induced organ injury:

Kubiak and others provide some very interesting data to suggest that a therapeutic intervention exists that may attenuate this cascade of events – the removal of inflammatory cytokines from the gut and peritoneal cavity.[22-24] By implementing such therapy they were able to markedly reduce circulating cytokine resulting in a dramatic improvement in organ function and tissue histopathology (see figures below). They used negative pressure suction on an open abdomen as their method of cytokine removal, however there is little reason to believe that the same therapy instituted at an earlier phase – before the onset of ACS - could not also remove cytokines via a percutaneous method as has been demonstrated in multiple case series and is being investigated right now.[25-30]

 

Figures: These Figures from Kubiak et al note the dramatic decrease in both peritoneal and circulating cytokines once negative pressure therapy is applied to the gut and excess fluid is removed. The tissue slides show the dramatic effect this therapy has on organ tissue histopathology.

Summary:

Intra-abdominal hypertension leads to organ dysfunction via two distinct and separate pathways. Early on IAH causes mechanical obstruction of blood flow and tissue perfusion, which directly impact organ function. Later IAH induced ischemia and edema contribute significantly to gut inflammation and the production of inflammatory cytokines that act locally and remotely - leading to multiple organ dysfunction. The inflammation that occurs in the gut leads to massive increases in gut cytokines – both in the bowel wall as well as in any surround ascites. This insight may result in a new way of attenuating MODS in the critically ill patient – by local removal of gut cytokine via either percutaneous drainage or suction, or perhaps peritoneal dialysis. It is already being employed in the clinical setting during open abdominal interventions with negative pressure therapy.

References:

1.            Garrison, R.N., et al., Microvascular changes explain the "two-hit" theory of multiple organ failure. Ann Surg, 1998. 227(6): p. 851-60.

2.            Marshall, J.C., Inflammation, coagulopathy, and the pathogenesis of multiple organ dysfunction syndrome. Crit Care Med, 2001. 29(7 Suppl): p. S99-106.

3.            Kubiak, B.D., et al., Peritoneal negative pressure therapy prevents multiple organ injury in a chronic porcine sepsis and ischemia/reperfusion model. Shock, 2010. 34(5): p. 525-34.

4.            Balogh, Z., et al., Both primary and secondary abdominal compartment syndrome can be predicted early and are harbingers of multiple organ failure. J Trauma, 2003. 54(5): p. 848-59.

5.            Rezende-Neto, J.B., et al., The abdominal compartment syndrome as a second insult during systemic neutrophil priming provokes multiple organ injury. Shock, 2003. 20(4): p. 303-8.

6.            Rezende-Neto, J.B., et al., Systemic inflammatory response secondary to abdominal compartment syndrome: stage for multiple organ failure. J Trauma, 2002. 53(6): p. 1121-8.

7.            Kacmaz, A., et al., Octreotide: a new approach to the management of acute abdominal hypertension. Peptides, 2003. 24(9): p. 1381-6.

8.         Sener, G., et al., Melatonin ameliorates oxidative organ damage induced by acute intra-abdominal compartment syndrome in rats. J Pineal Res, 2003. 35(3): p. 163-8.

9.         Bathe, O.F., A.W. Chow, and P.T. Phang, Splanchnic origin of cytokines in a porcine model of mesenteric ischemia-reperfusion. Surgery, 1998. 123(1): p. 79-88.

10.            Balogh, Z., et al., Abdominal compartment syndrome: the cause or effect of postinjury multiple organ failure. Shock, 2003. 20(6): p. 483-92.

11.            Duchesne, J.C., et al., Recurrent abdominal compartment syndrome: an inciting factor of the second hit phenomenon. Am Surg, 2009. 75(12): p. 1193-8.

12.       Oda, J., et al., Acute lung injury and multiple organ dysfunction syndrome secondary to intra-abdominal hypertension and abdominal decompression in extensively burned patients. J Trauma, 2007. 62(6): p. 1365-9.

13.       Moore, F.A., E.E. Moore, and R.A. Read, Postinjury multiple organ failure: role of extrathoracic injury and sepsis in adult respiratory distress syndrome. New Horizons, 1993. 1(4): p. 538-49.

14.       Butt, I. and B.M. Shrestha, Two-hit hypothesis and multiple organ dysfunction syndrome. JNMA J Nepal Med Assoc, 2008. 47(170): p. 82-5.

15.       Botha, A.J., et al., Postinjury neutrophil priming and activation: an early vulnerable window. Surgery, 1995. 118(2): p. 358-64; discussion 364-5.

16.       Zallen, G., et al., Circulating postinjury neutrophils are primed for the release of proinflammatory cytokines. J Trauma, 1999. 46(1): p. 42-8.

17.            Kacmaz, A., et al., Octreotide improves reperfusion-induced oxidative injury in acute abdominal hypertension in rats. J Gastrointest Surg, 2004. 8(1): p. 113-9.

18.       Diebel, L.N., S.A. Dulchavsky, and W.J. Brown, Splanchnic ischemia and bacterial translocation in the abdominal compartment syndrome. J Trauma, 1997. 43(5): p. 852-5.

19.            Eleftheriadis, E., et al., Gut ischemia, oxidative stress, and bacterial translocation in elevated abdominal pressure in rats. World J Surg, 1996. 20(1): p. 11-6.

20.            Gargiulo, N.J., 3rd, et al., Hemorrhage exacerbates bacterial translocation at low levels of intra-abdominal pressure. Arch Surg, 1998. 133(12): p. 1351-5.

21.       Ince, C., The microcirculation is the motor of sepsis. Crit Care, 2005. 9 Suppl 4: p. S13-9.

22.       Zakaria el, R., N. Li, and R.N. Garrison, Mechanisms of direct peritoneal resuscitation-mediated splanchnic hyperperfusion following hemorrhagic shock. Shock, 2007. 27(4): p. 436-42.

23.            Kubiak, B.D., et al., Peritoneal negative pressure therapy reduces both peritoneal and systemic inflammation and prevents abdominal compartment syndrome. Acta Clinica Belgica, 2009. 64(3): p. 260 (Abstract 43).

24.       Zaletel, C.L., Factors affecting fluid resuscitation in the burn patient: the collaborative role of the APN. Adv Emerg Nurs J, 2009. 31(4): p. 309-20; quiz 321-2.

25.            Corcos, A.C. and H.F. Sherman, Percutaneous treatment of secondary abdominal compartment syndrome. J Trauma, 2001. 51(6): p. 1062-4.

26.            Dambrauskas, Z., et al., Interventional and surgical management of abdominal compartment syndrome in severe acute pancreatitis. Medicina (Kaunas), 2010. 46(4): p. 249-55.

27.            Latenser, B.A., et al., A pilot study comparing percutaneous decompression with decompressive laparotomy for acute abdominal compartment syndrome in thermal injury. J Burn Care Rehabil, 2002. 23(3): p. 190-5.

28.            Radenkovic, D.V., et al., Decompressive laparotomy with temporary abdominal closure versus percutaneous puncture with placement of abdominal catheter in patients with abdominal compartment syndrome during acute pancreatitis: background and design of multicenter, randomised, controlled study. BMC Surg, 2010. 10: p. 22.

29.            Reckard, J.M., et al., Management of intraabdominal hypertension by percutaneous catheter drainage. J Vasc Interv Radiol, 2005. 16(7): p. 1019-21.

30.            Vikrama, K.S., et al., Percutaneous catheter drainage in the treatment of abdominal compartment syndrome. Can J Surg, 2009. 52(1): p. E19-20.