Septic shock explained

Septic shock
Field:Infectious disease

Septic shock is a potentially fatal medical condition that occurs when sepsis, which is organ injury or damage in response to infection, leads to dangerously low blood pressure and abnormalities in cellular metabolism. The Third International Consensus Definitions for Sepsis and Septic Shock (Sepsis-3) defines septic shock as a subset of sepsis in which particularly profound circulatory, cellular, and metabolic abnormalities are associated with a greater risk of mortality than with sepsis alone. Patients with septic shock can be clinically identified by requiring a vasopressor to maintain a mean arterial pressure of 65 mm Hg or greater and having serum lactate level greater than 2 mmol/L (>18 mg/dL) in the absence of hypovolemia. This combination is associated with hospital mortality rates greater than 40%.[1]

The primary infection is most commonly caused by bacteria, but also may be by fungi, viruses or parasites. It may be located in any part of the body, but most commonly in the lungs, brain, urinary tract, skin or abdominal organs.[2] It can cause multiple organ dysfunction syndrome (formerly known as multiple organ failure) and death.

Frequently, people with septic shock are cared for in intensive care units. It most commonly affects children, immunocompromised individuals, and the elderly, as their immune systems cannot deal with infection as effectively as those of healthy adults. The mortality rate from septic shock is approximately 25–50%.[3]

Causes

Septic shock is a result of a systemic response to infection or multiple infectious causes. The precipitating infections that may lead to septic shock if severe enough include but are not limited to appendicitis, pneumonia, bacteremia, diverticulitis, pyelonephritis, meningitis, pancreatitis, necrotizing fasciitis, MRSA and mesenteric ischemia.[4] [5]

According to the earlier definitions of sepsis updated in 2001,[6] sepsis is a constellation of symptoms secondary to an infection that manifests as disruptions in heart rate, respiratory rate, temperature, and white blood cell count. If sepsis worsens to the point of end-organ dysfunction (kidney failure, liver dysfunction, altered mental status, or heart damage), then the condition is called severe sepsis. In septic shock, events within tissue capillaries induce distributive shock in which the recovery of blood pressure is not achieved upon the administration of additional intravenous fluids, and requires a vasoconstrictive agent such as noradrenaline and/or vasopressin.[7]

Pathophysiology

The pathophysiology of septic shock is not entirely understood, but it is known that a key role in the development of severe sepsis is played by an immune and coagulation response to an infection. Both pro-inflammatory and anti-inflammatory responses play a role in septic shock.[8] Septic shock involves a widespread inflammatory response that produces a hypermetabolic effect. This is manifested by increased cellular respiration, protein catabolism, and metabolic acidosis with a compensatory respiratory alkalosis.

Most cases of septic shock are caused by gram-positive bacteria,[9] followed by endotoxin-producing gram-negative bacteria, although fungal infections are an increasingly prevalent cause of septic shock.[10] Toxins produced by pathogens cause an immune response; in gram-negative bacteria these are endotoxins, which are bacterial membrane lipopolysaccharides (LPS).

Gram-positive

In gram-positive bacteria, these are exotoxins or enterotoxins, which may vary depending on the species of bacteria. These are divided into three types. Type I, cell surface-active toxins, disrupt cells without entering, and include superantigens and heat-stable enterotoxins. Type II, membrane-damaging toxins, destroy cell membranes in order to enter and include hemolysins and phospholipases. Type III, intracellular toxins or A/B toxins interfere with internal cell function and include shiga toxin, cholera toxin, and anthrax lethal toxin. (note that Shigella and Vibrio cholerae are Gram negative organisms).

Gram-negative

In gram-negative sepsis, free LPS attaches to a circulating LPS-binding protein, and the complex then binds to the CD14 receptor on monocytes, macrophages, and neutrophils. Engagement of CD14 (even at doses as minute as 10 pg/mL) results in intracellular signaling via an associated "Toll-like receptor" protein 4 (TLR-4). This signaling results in the activation of nuclear factor kappaB (NF-κB), which leads to transcription of a number of genes that trigger a proinflammatory response. It was the result of significant activation of mononuclear cells and synthesis of effector cytokines. It also results in profound activation of mononuclear cells and the production of potent effector cytokines such as IL-1, IL-6, and TNF-α. TLR-mediated activation helps to trigger the innate immune system to efficiently eradicate invading microbes, but the cytokines they produce also act on endothelial cells. There, they have a variety of effects, including reduced synthesis of anticoagulation factors such as tissue factor pathway inhibitor and thrombomodulin. The effects of the cytokines may be amplified by TLR-4 engagement on endothelial cells.

In response to inflammation, a compensatory reaction of production of anti-inflammatory substances such as IL-4, IL-10 antagonists, IL-1 receptor, and cortisol occurs. This is called compensatory anti-inflammatory response syndrome (CARS).[11] Both the inflammatory and anti-inflammatory reactions are responsible for the course of sepsis and are described as MARS (Mixed Antagonist Response Syndrome). The aim of these processes is to keep inflammation at an appropriate level. CARS often leads to suppression of the immune system, which leaves patients vulnerable to secondary infection. It was once thought that SIRS or CARS could predominate in a septic individual, and it was proposed that CARS follows SIRS in a two-wave process. It is now believed that the systemic inflammatory response and the compensatory anti-inflammatory response occur simultaneously.[11]

At high levels of LPS, the syndrome of septic shock supervenes; the same cytokine and secondary mediators, now at high levels, result in systemic vasodilation (hypotension), diminished myocardial contractility, widespread endothelial injury, activation causing systemic leukocyte adhesion and diffuse alveolar capillary damage in the lung, and activation of the coagulation system culminating in disseminated intravascular coagulation (DIC).

The hypoperfusion from the combined effects of widespread vasodilation, myocardial pump failure, and DIC causes multiorgan system failure that affects the liver, kidneys, and central nervous system, among other organ systems. Recently, severe damage to liver ultrastructure has been noticed from treatment with cell-free toxins of Salmonella.[12] Unless the underlying infection (and LPS overload) is rapidly brought under control, the patient usually dies.

The ability of TLR4 to respond to a distinct LPS species are clinically important. Pathogenic bacteria may employ LPS with low biological activity to evade proper recognition by the TLR4/MD-2 system, dampening the host immune response and increasing the risk of bacterial dissemination. On the other hand, such LPS would not be able to induce septic shock in susceptible patients, rendering septic complications more manageable. Yet, defining and understanding how even the smallest structural differences between the very similar LPS species may affect the activation of the immune response may provide the mechanism for the fine tuning of the latter and new insights to immunomodulatory processes.[13]

Diagnosis

According to current guidelines, requirements for diagnosis with sepsis are "the presence (probable or documented) of infection together with systemic manifestations of infection".[10] These manifestations may include:

Documented evidence of infection may include positive blood culture, signs of pneumonia on chest x-ray, or other radiologic or laboratory evidence of infection. Signs of end-organ dysfunction are present in septic shock, including kidney failure, liver dysfunction, changes in mental status, or elevated serum lactate.

Septic shock is diagnosed if there is low blood pressure (BP) that does not respond to treatment. This means that intravenous fluid administration alone is not enough to maintain a patient's BP. Diagnosis of septic shock is made when systolic blood pressure is less than 90 mm Hg, a mean arterial pressure (MAP) is less than 70 mm Hg, or a systolic BP decrease of 40 mm Hg or more without other causes for low BP.[10]

Definition

Septic shock is a subclass of distributive shock, a condition in which abnormal distribution of blood flow in the smallest blood vessels results in inadequate blood supply to the body tissues, resulting in ischemia and organ dysfunction. Septic shock refers specifically to distributive shock due to sepsis as a result of infection.[14]

Septic shock may be defined as sepsis-induced low blood pressure that persists despite treatment with intravenous fluids.[10] Low blood pressure reduces tissue perfusion pressure, causing the tissue hypoxia that is characteristic of shock. Cytokines released in a large scale inflammatory response result in massive vasodilation, increased capillary permeability, decreased systemic vascular resistance, and low blood pressure. Finally, in an attempt to offset decreased blood pressure, ventricular dilatation and myocardial dysfunction occur.

Septic shock may be regarded as a stage of SIRS (Systemic Inflammatory Response Syndrome), in which sepsis, severe sepsis and multiple organ dysfunction syndrome (MODS) represent different stages of a pathophysiological process. If an organism cannot cope with an infection, it may lead to a systemic response - sepsis, which may further progress to severe sepsis, septic shock, organ failure, and eventually, result in death.

Treatment

Treatment primarily consists of the following:

  1. Giving intravenous fluids[15]
  2. Early antibiotic administration [15]
  3. Early goal directed therapy[15]
  4. Rapid source identification and control
  5. Support of major organ dysfunction

Fluids

Because lowered blood pressure in septic shock contributes to poor perfusion, fluid resuscitation is an initial treatment to increase blood volume. Patients demonstrating sepsis-induced hypoperfusion should be initially resuscitated with at least 30 ml/kg of intravenous crystalloid within the first three hours. Crystalloids such as normal saline and lactated Ringer's solution are recommended as the initial fluid of choice, while the use of colloid solutions such as hydroxyethyl starch have not shown any advantage or decrease in mortality. When large quantities of fluids are given, administering albumin has shown some benefit.[9] However, too high of a rate of fluid infusion can be more risky; the particular type of fluid's flow rate must be closely monitored, along with the patient's condition and vital signs.[16]

Antibiotics

Treatment guidelines call for the administration of broad-spectrum antibiotics within the first hour following recognition of septic shock. Prompt antimicrobial therapy is important, as risk of dying increases by approximately 10% for every hour of delay in receiving antibiotics.[9] Time constraints do not allow the culture, identification, and testing for antibiotic sensitivity of the specific microorganism responsible for the infection. Therefore, combination antimicrobial therapy, which covers a wide range of potential causative organisms, is tied to better outcomes.[9] Antibiotics should be continued for 7–10 days in most patients, though treatment duration may be shorter or longer depending on clinical response.

Vasopressors

Among the choices for vasopressors, norepinephrine is superior to dopamine in septic shock.[17] Norepinephrine is the preferred vasopressor, while epinephrine may be added to norepinephrine when needed. Low-dose vasopressin also may be used as an addition to norepinephrine, but is not recommended as a first-line treatment. Dopamine may cause rapid heart rate and arrhythmias, and is only recommended in combination with norepinephrine in those with slow heart rate and low risk of arrhythmia. In the initial treatment of low blood pressure in septic shock, the goal of vasopressor treatment is a mean arterial pressure (MAP) of 65 mm Hg.[9] In 2017, the FDA approved angiotensin II injection for intravenous infusion to increase blood pressure in adults with septic or other distributive shock.[18]

Methylene blue

Methylene blue has been found to be useful for this condition.[19] [20] [21] [22] Although use of methylene blue has mostly been in adults it has also been shown to work in children.[23] [24] Its mechanism of action is thought to be via the inhibition of the nitric oxide-cyclic guanosine monophosphate pathway.[25] This pathway is excessively activated in septic shock. Methylene blue has been found to work in cases resistant to the usual agents.[26] This effect was first reported in the early 1990s.[27] [28]

Other

While there is tentative evidence for β-Blocker therapy to help control heart rate, evidence is not significant enough for its routine use.[29] [30] There is tentative evidence that steroids may be useful in improving outcomes.[31]

Tentative evidence exists that Polymyxin B-immobilized fiber column hemoperfusion may be beneficial in treatment of septic shock.[32] Trials are ongoing and it is currently being used in Japan and Western Europe.[33]

Recombinant activated protein C (drotrecogin alpha) in a 2011 Cochrane review was found not to decrease mortality and to increase bleeding, and thus, was not recommended for use.[34] Drotrecogin alfa (Xigris), was withdrawn from the market in October 2011.

Epidemiology

Sepsis has a worldwide incidence of more than 20 million cases a year, with mortality due to septic shock reaching up to 50 percent even in industrialized countries.[35]

According to the U.S. Centers for Disease Control, septic shock is the thirteenth leading cause of death in the United States and the most frequent cause of death in intensive care units. There has been an increase in the rate of septic shock deaths in recent decades, which is attributed to an increase in invasive medical devices and procedures, increases in immunocompromised patients, and an overall increase in elderly patients.

Tertiary care centers (such as hospice care facilities) have 2-4 times the rate of bacteremia than primary care centers, 75% of which are hospital-acquired infections.

The process of infection by bacteria or fungi may result in systemic signs and symptoms that are variously described. Approximately 70% of septic shock cases were once traceable to gram-negative bacteria that produce endotoxins, however, with the emergence of MRSA and the increased use of arterial and venous catheters, gram-positive bacteria are implicated approximately as commonly as bacilli. In rough order of increasing severity these are, bacteremia or fungemia; sepsis, severe sepsis or sepsis syndrome; septic shock, refractory septic shock, multiple organ dysfunction syndrome, and death.

35% of septic shock cases derive from urinary tract infections, 15% from the respiratory tract, 15% from skin catheters (such as IVs), and more than 30% of all cases are idiopathic in origin.

The mortality rate from sepsis, especially if it is not treated rapidly with the needed medications in a hospital, is approximately 40% in adults and 25% in children. It is significantly greater when sepsis is left untreated for more than seven days.[36]

Notes and References

  1. Singer M, Deutschman CS, Seymour CW, Shankar-Hari M, Annane D, Bauer M, Bellomo R, Bernard GR, Chiche JD, Coopersmith CM, Hotchkiss RS, Levy MM, Marshall JC, Martin GS, Opal SM, Rubenfeld GD, van der Poll T, Vincent JL, Angus DC . 6. The Third International Consensus Definitions for Sepsis and Septic Shock (Sepsis-3) . JAMA . 315 . 8 . 801–10 . February 2016 . 26903338 . 4968574 . 10.1001/jama.2016.0287 .
  2. Book: Jui, Jonathan . Ch. 146: Septic Shock . Tintinalli . Judith E. . Stapczynski . J. Stephan . Cline . David M. . Ma . O. John . Cydulka . Rita K. . Meckler . Garth D. . American College of Emergency Physicians . 4 . Tintinalli's Emergency Medicine: A Comprehensive Study Guide . 7th . New York . . 1003–14. 2011 . http://www.accessmedicine.com/content.aspx?aID=6364928 . December 11, 2012 . AccessMedicine . subscription .
  3. Book: Kumar . V. . Abbas . A.K. . Fausto . N. . 3 . Mitchell . R.N. . 2007 . Robbins Basic Pathology . 8th . . 102–3 . 9781416029731.
  4. Melis M, Fichera A, Ferguson MK . Bowel necrosis associated with early jejunal tube feeding: A complication of postoperative enteral nutrition . Arch Surg . 141 . 7 . 701–4 . July 2006 . 16847244 . 10.1001/archsurg.141.7.701 . free .
  5. Gwon JG, Lee YJ, Kyoung KH, Kim YH, Hong SK . Enteral nutrition associated non-occlusive bowel ischemia . J Korean Surg Soc . 83 . 3 . 171–4 . September 2012 . 22977764 . 3433554 . 10.4174/jkss.2012.83.3.171 .
  6. for the International Sepsis Definitions Conference. Levy. Mitchell M.. Fink. Mitchell P.. Marshall. John C.. Abraham. Edward. Angus. Derek. Cook. Deborah. Cohen. Jonathan. Opal. Steven M.. 2003. 2001 SCCM/ESICM/ACCP/ATS/SIS International Sepsis Definitions Conference. Intensive Care Medicine. en. 29. 4. 530–538. 10.1007/s00134-003-1662-x. 12664219. 11214199. 0342-4642.
  7. Hotchkiss . Richard S. . Moldawer . Lyle L. . Opal . Steven M. . Reinhart . Konrad . Turnbull . Isaiah R. . Vincent . Jean-Louis . 2016-06-30 . Sepsis and septic shock . Nature Reviews. Disease Primers . 2 . 16045 . 10.1038/nrdp.2016.45 . 2056-676X . 5538252 . 28117397.
  8. Angus DC, van der Poll T . Severe sepsis and septic shock . N. Engl. J. Med. . 369 . 9 . 840–51 . August 2013 . 23984731 . 10.1056/NEJMra1208623 . free .
  9. Martin GS . Sepsis, severe sepsis and septic shock: changes in incidence, pathogens and outcomes . Expert Rev Anti Infect Ther . 10 . 6 . 701–6 . June 2012 . 22734959 . 3488423 . 10.1586/eri.12.50 .
  10. Dellinger RP, Levy MM, Rhodes A, Annane D, Gerlach H, Opal SM, Sevransky JE, Sprung CL, Douglas IS, Jaeschke R, Osborn TM, Nunnally ME, Townsend SR, Reinhart K, Kleinpell RM, Angus DC, Deutschman CS, Machado FR, Rubenfeld GD, Webb SA, Beale RJ, Vincent JL, Moreno R . 6. Surviving sepsis campaign: international guidelines for management of severe sepsis and septic shock: 2012 . Crit. Care Med. . 41 . 2 . 580–637 . February 2013 . 23353941 . 10.1097/CCM.0b013e31827e83af . 34855187. free .
  11. Adib-Conquy M, Cavaillon JM . Compensatory anti-inflammatory response syndrome . Thromb. Haemost. . 101 . 1 . 36–47 . January 2009 . 19132187 . 10.1160/TH08-07-0421. 11156883 . 0340-6245.
  12. YashRoy . R.C. . June 1994 . Liver damage by intra-ileal treatment with Salmonella 3,10:r:- extract as studied by light and electron microscopy . Indian Journal of Animal Sciences . 64 . 6 . 597–99 . ResearchGate. (animal study).
  13. Korneev KV, Arbatsky NP, Molinaro A, Palmigiano A, Shaikhutdinova RZ, Shneider MM, Pier GB, Kondakova AN, Sviriaeva EN, Sturiale L, Garozzo D, Kruglov AA, Nedospasov SA, Drutskaya MS, Knirel YA, Kuprash DV. 6 . Structural Relationship of the Lipid A Acyl Groups to Activation of Murine Toll-Like Receptor 4 by Lipopolysaccharides from Pathogenic Strains of Burkholderia mallei, Acinetobacter baumannii, and Pseudomonas aeruginosa . Front Immunol . 6 . 595 . 2015 . 26635809 . 4655328 . 10.3389/fimmu.2015.00595 . free .
  14. 2024-06-26 . Septic Shock: Practice Essentials, Background, Pathophysiology .
  15. Levinson . A.T. . Casserly . B.P. . Levy . M.M. . Reducing mortality in severe sepsis and septic shock . Seminars in Respiratory and Critical Care Medicine . April 2011 . 32 . 2 . 195–205 . 21506056 . 10.1055/s-0031-1275532. 20763016 .
  16. 10.1056/NEJMoa2202707 . Restriction of Intravenous Fluid in ICU Patients with Septic Shock . 2022 . Meyhoff . Tine S. . Hjortrup . Peter B. . Wetterslev . Jørn . Sivapalan . Praleene . Laake . Jon H. . Cronhjort . Maria . Jakob . Stephan M. . Cecconi . Maurizio . Nalos . Marek . Ostermann . Marlies . Malbrain . Manu . Pettilä . Ville . Møller . Morten H. . Kjær . Maj-Brit N. . Lange . Theis . Overgaard-Steensen . Christian . Brand . Björn A. . Winther-Olesen . Marie . White . Jonathan O. . Quist . Lars . Westergaard . Bo . Jonsson . Andreas B. . Hjortsø . Carl J.S. . Meier . Nick . Jensen . Thomas S. . Engstrøm . Janus . Nebrich . Lars . Andersen-Ranberg . Nina C. . Jensen . Jacob V. . Joseph . Neeliya A. . New England Journal of Medicine . 386 . 26 . 2459–2470 . 35709019 . 249711011 . 1 . free .
  17. Vasu TS, Cavallazzi R, Hirani A, Kaplan G, Leiby B, Marik PE . Norepinephrine or dopamine for septic shock: systematic review of randomized clinical trials . J Intensive Care Med . 27 . 3 . 172–8 . 2012 . 21436167 . 10.1177/0885066610396312 . free .
  18. Web site: Press Announcements - FDA approves drug to treat dangerously low blood pressure. Commissioner. Office of the. www.fda.gov. en. 2017-12-22.
  19. Jang DH, Nelson LS, Hoffman RS (2013) Methylene blue for distributive shock: a potential new use of an old antidote. J Med Toxicol 9(3):242-249
  20. Baldo CF, Silva LM, Arcencio L, Albuquerque AAS, Celotto AC, Basile-Filho A, Evora PRB (2018) Why Methylene Blue have to be always present in the tocking of emergency antidotes. Curr Drug Targets 19(13):1550-1559
  21. McCartney SL, Duce L, Ghadimi K (2018) Intraoperative vasoplegia: methylene blue to the rescue! Curr Opin Anaesthesiol. 31(1):43-49
  22. Booth AT, Melmer PD, Tribble B, Mehaffey JH, Tribble C (2017) Methylene blue for vasoplegic syndrome. Heart Surg Forum 20(5):E234-E238
  23. Rutledge C, Brown B, Benner K, Prabhakaran P, Hayes L (2015) A novel use of methylene blue in the pediatric ICU. Pediatrics 136(4):e1030-4
  24. Volpon LC, Evora PRB, Teixeira GD, Godinho M, Scarpelini S, Carmona F, Carlotti APCP (2018) Methylene blue for refractory shock in polytraumatized patient: A case report. J Emerg Med 55(4):553-558
  25. Da Silva PS, Furtado P (2018) Methylene blue to treat refractory latex-induced anaphylactic shock: a case report. A A Pract 10(3):57-60
  26. Lo JC, Darracq MA, Clark RF (2014) A review of methylene blue treatment for cardiovascular collapse. J Emerg Med 46(5):670-679
  27. Schneider F, Lutun P, Hasselmann M, Stoclet JC, Tempé JD (1992) Methylene blue increases systemic vascular resistance in human septic shock. Preliminary observations. Intensive Care Med 18(5):309-11
  28. Preiser JC, Lejeune P, Roman A, Carlier E, De Backer D, Leeman M, Kahn RJ, Vincent JL (1995) Methylene blue administration in septic shock: a clinical trial. Crit Care Med 23(2):259-264
  29. Chacko CJ, Gopal S . Systematic review of use of β-blockers in sepsis . J Anaesthesiol Clin Pharmacol . 31 . 4 . 460–5 . 2015 . 26702201 . 4676233 . 10.4103/0970-9185.169063 . free .
  30. Sanfilippo F, Santonocito C, Morelli A, Foex P . Beta-blocker use in severe sepsis and septic shock: a systematic review . Curr Med Res Opin . 31 . 10 . 1817–25 . 2015 . 26121122 . 10.1185/03007995.2015.1062357 . 22393745 .
  31. Annane. Djillali. Bellissant. Eric. Bollaert. Pierre Edouard. Briegel. Josef. Keh. Didier. Kupfer. Yizhak. Pirracchio. Romain. Rochwerg. Bram. 6 December 2019. Corticosteroids for treating sepsis in children and adults. The Cochrane Database of Systematic Reviews. 2019. 12. CD002243. 10.1002/14651858.CD002243.pub4. 1469-493X. 6953403. 31808551.
  32. Mitaka C, Tomita M . Polymyxin B-immobilized fiber column hemoperfusion therapy for septic shock . Shock . 36 . 4 . 332–8 . October 2011 . 21654557 . 10.1097/SHK.0b013e318225f839 . 28404720 . free .
  33. Ronco C, Klein DJ . Polymyxin B hemoperfusion: a mechanistic perspective . Crit Care . 18 . 3 . 309 . June 2014 . 25043934 . 4077196 . 10.1186/cc13912 . free .
  34. Martí-Carvajal AJ, Solà I, Gluud C, Lathyris D, Cardona AF . Human recombinant protein C for severe sepsis and septic shock in adult and paediatric patients . Cochrane Database Syst Rev . 2018 . CD004388 . December 2012 . 12 . 23235609 . 10.1002/14651858.CD004388.pub6 . 6464614 .
  35. Web site: Researchers make blood poisoning breakthrough . June 4, 2010 . Phys.org.
  36. Book: Huether . S.E. . McCance . K.L. . 2008 . Understanding Pathophysiology . Mosby/Elsevier . 4th . 9780323049900 . registration .