Use of vasopressin in the treatment of refractory septic shock

Kny, Katiuce Tomazi; Ferreira, Maria Angélica Pires; Pizzol, Tatiane da Silva Dal

doi:10.5935/0103-507X.20180060

ABSTRACT

Objective:

To evaluate the short-term evolution of patients with septic shock refractory to norepinephrine treated with vasopressin in an intensive care unit of a university hospital.

Methods:

An unmatched retrospective study (case series) was performed. Clinical, laboratory, and anthropometric data were collected from patients who received vasopressin infusion for treatment of catecholamine-refractory shock from December 2014 to June 2016. For the assessment of severity, APACHE II and SOFA scores were used. The main outcome was mortality at 3 and 30 days.

Results:

A total of 80 patients were included, of which 60% were male. In 86.3% of the cases, APACHE II was observed in the highest ranges (> 20). The 30-day mortality was 86.2%, and 75% of the patients died within 72 hours after starting vasopressin.

Conclusion:

The series evaluated had high mortality in the first 72 hours of treatment with vasopressin. The use of vasopressin in patients who are refractory to norepinephrine had little or no impact on mortality. It was not possible to exclude the possibility that the high mortality in the present study was linked to the relatively late onset (after established refractoriness of norepinephrine) of vasopressin; this hypothesis should be further evaluated in a randomized study.

Keywords:
Sepsis; Mortality; Hypotension; Vasopressin; Norepinephrine

RESUMO

Objetivo:

Avaliar a evolução em curto prazo de pacientes com choque séptico refratário à norepinefrina tratados com vasopressina em uma unidade de terapia intensiva de um hospital universitário.

Métodos:

Foi realizado estudo retrospectivo não comparado (série de casos). Foram coletados dados clínicos, laboratoriais e antropométricos de pacientes que receberam infusão de vasopressina para tratamento de choque refratário a catecolaminas no período de dezembro de 2014 a junho de 2016. Para a avaliação de gravidade, foram utilizados o APACHE II e o SOFA. O desfecho principal foi mortalidade em 3 e em 30 dias.

Resultados:

Foram incluídos 80 pacientes, sendo 60% do sexo masculino. Em 86,3% dos casos, verificou-se APACHE II nas faixas mais altas (> 20). A mortalidade em 30 dias foi de 86,2%, sendo que 75% dos pacientes foram a óbito dentro de 72 horas após início do uso da vasopressina.

Conclusão:

A série avaliada apresentou alta mortalidade nas primeiras 72 horas de tratamento com vasopressina. O uso de vasopressina em pacientes refratários à norepinefrina teve pouco ou nenhum impacto na mortalidade. Não é possível excluir que a alta mortalidade no presente estudo esteja vinculada ao início relativamente tardio (após estabelecida refratariedade à norepinefrina) da vasopressina, devendo essa hipótese ser melhor avaliada por estudo randomizado.

Descritores:
Sepse; Mortalidade; Hipotensão; Vasopressina; Norepinefrina

INTRODUCTION

Septic shock, defined by the need to use vasopressor to maintain mean blood pressure above 65mmHg after adequate infusion of fluids, associated with a serum lactate level above 2mmol/L, is the most common type of shock among hospitalized patients and an important cause of morbidity and mortality in Brazil and worldwide.⁽¹1 Instituto Latino Americano para Estudos da Sepse (ILAS). Sepse: um problema de saúde pública [Internet]. Brasília (DF): Conselho Federal de Medicina; 2015 [citado 2017 Maio 7]. Disponível em: http://www.ilas.org.br/assets/arquivos/upload/Livro-ILAS(Sepse-CFM-ILAS).pdf
http://www.ilas.org.br/assets/arquivos/u... ^,²2 Rocha LL, Pessoa CM, Corrêa TD, Pereira AJ, de Assunção MS, Silva E. Current concepts on hemodynamic support and therapy in septic shock. Braz J Anesthesiol. 2015;65(5):395-402.⁾ In Brazil, the incidence of septic shock has increased in recent years; the 28-day mortality rate has reached approximately 50%, with an incidence density of 30 cases per thousand patients/day. According to the PROGRESS study, the overall lethality rate of septic shock is 49.6%; in Brazil, it is estimated that this rate reaches approximately 67%, with even higher rates in public hospitals.⁽¹1 Instituto Latino Americano para Estudos da Sepse (ILAS). Sepse: um problema de saúde pública [Internet]. Brasília (DF): Conselho Federal de Medicina; 2015 [citado 2017 Maio 7]. Disponível em: http://www.ilas.org.br/assets/arquivos/upload/Livro-ILAS(Sepse-CFM-ILAS).pdf
http://www.ilas.org.br/assets/arquivos/u...

2 Rocha LL, Pessoa CM, Corrêa TD, Pereira AJ, de Assunção MS, Silva E. Current concepts on hemodynamic support and therapy in septic shock. Braz J Anesthesiol. 2015;65(5):395-402.

3 Silva E, Pinheiro C, Michels Júnior V. Consenso Brasileiro de Sepse. Epidemiologia. Rev Bras Ter Intensiva. 2004;16(2):97-101.

4 Singer M, Deutschman CS, Seymour CW, Shankar-Hari M, Annane D, Bauer M, et al. The Third International Consensus Definitions for Sepsis and Septic Shock (Sepsis-3). JAMA. 2016;315(8):801-10.

5 Kaukonen KM, Bailey M, Suzuki S, Pilcher D, Bellomo R. Mortality related to severe sepsis and septic shock among critically ill patients in Australia and New Zealand, 2000-2012. JAMA. 2014;311(13):1308-16.

6 Harrison DA, Welch CA, Eddleston JM. The epidemiology of severe sepsis in England, Wales and Northern Ireland, 1996 to 2004: secondary analysis of a high quality clinical database, the ICNARC Case Mix Programme Database. Crit Care. 2006;10(2):R42.

7 Silva E, Pedro MA, Sogayar AC, Mohovic T, Silva CL, Janiszewski M, Cal RG, de Sousa EF, Abe TP, de Andrade J, de Matos JD, Rezende E, Assunção M, Avezum A, Rocha PC, de Matos GF, Bento AM, Corrêa AD, Vieira PC, Knobel E; Brazilian Sepsis Epidemiological Study. Brazilian Sepsis Epidemiological Study (BASES study). Crit Care. 2004;8(4):R251-60.

8 Noritomi DT, Ranzani OT, Monteiro MB, Ferreira EM, Santos SR, Leibel F, et al. Implementation of a multifaceted sepsis education program in an emerging country setting: clinical outcomes and cost-effectiveness in a long-term follow-up study. Intensive Care Med. 2014;40(2):182-91.^-⁹9 Rede Brasileira de Avaliação de Tecnologias em Saúde (REBRATS). Alfadrotrecogina para o tratamento de sepse grave. Bol Bras Aval Tecnol Saúde (BRATS). 2006;1(2):1-5.⁾

A prevalence study in 230 Brazilian intensive care units (ICUs) found that 30% of ICU beds in Brazil were occupied by patients with severe sepsis or septic shock.⁽¹1 Instituto Latino Americano para Estudos da Sepse (ILAS). Sepse: um problema de saúde pública [Internet]. Brasília (DF): Conselho Federal de Medicina; 2015 [citado 2017 Maio 7]. Disponível em: http://www.ilas.org.br/assets/arquivos/upload/Livro-ILAS(Sepse-CFM-ILAS).pdf
http://www.ilas.org.br/assets/arquivos/u... ^,⁹9 Rede Brasileira de Avaliação de Tecnologias em Saúde (REBRATS). Alfadrotrecogina para o tratamento de sepse grave. Bol Bras Aval Tecnol Saúde (BRATS). 2006;1(2):1-5.⁾ According to a report by the Instituto Latino Americano da Sepse (ILAS), 42.2% of patients hospitalized in public and private Brazilian hospitals in July 2015 died of complications and severity of sepsis.⁽¹⁰10 Instituto Latino Americano de Sepse (ILAS). Relatório Nacional. Protocolos Gerenciados de sepse: sepse grave e choque séptico 2005-2015. [Internet]. São Paulo: ILAS; 2005 [citado 2017 Maio 23]. Disponível em: http://www.ilas.org.br/assets/arquivos/relatorio-nacional/relatorio-nacional.pdf
http://www.ilas.org.br/assets/arquivos/r... ^,¹¹11 Rhodes A, Evans LE, Alhazzani W, Levy MM, Antonelli M, Ferrer R, et al. Surviving Sepsis Campaign: International Guidelines for Management of Sepsis and Septic Shock: 2016. Intensive Care Med. 2017;43(3):304-77.⁾ The mortality rate for septic shock with usual treatment (catecholamine use) varies in the range from 40 - 60%.⁽¹²12 Angus DC, Linde-Zwirble WT, Lidicker J, Clermont G, Carcillo J, Pinsky MR. Epidemiology of severe sepsis in the United States: analysis of incidence, outcome, and associated costs of care. Crit Care Med. 2001;29(7):1303-10.⁾

Infusion of vasopressors in septic patients should be instituted whenever volume expansion is not sufficient to restore blood pressure and reverse organ dysfunction.⁽⁶6 Harrison DA, Welch CA, Eddleston JM. The epidemiology of severe sepsis in England, Wales and Northern Ireland, 1996 to 2004: secondary analysis of a high quality clinical database, the ICNARC Case Mix Programme Database. Crit Care. 2006;10(2):R42.⁾ According to international guidelines, the use of norepinephrine is recommended as the first choice vasopressor (recommended dose of 0.05 to 2µg/kg/min). A significant proportion of patients, however, do not achieve an adequate clinical response. Observational randomized clinical studies have shown that the administration of low doses of vasopressin in septic shock patients who are refractory to fluid replacement and the use of catecholamines may raise blood pressure and reduce the use of catecholamines; other potential physiological benefits are highlighted, such as a reduced risk of renal failure and arrhythmias.⁽¹³13 Westphal GA, Silva E, Salomão R, Bernardo WM, Machado FR. Diretrizes para tratamento da sepse grave/choque séptico: ressuscitação hemodinâmica. Rev Bras Ter Intensiva. 2011;23(1):13-23.

14 Malay MB, Ashton RC Jr, Landry DW, Townsend RN. Low-dose vasopressin in the treatment of vasodilatory septic shock. J Trauma. 1999;47(4):699-703; discussion 703-5.^-¹⁵15 Patel BM, Chittock DR, Russell JA, Walley KR. Beneficial effects of short-term vasopressin infusion during severe septic shock. Anesthesiology. 2002;96(3):576-82.⁾

Thus, despite lacking high quality evidence showing a benefit in mortality, septic shock treatment guidelines recommend the addition of low dose vasopressin, corresponding to 0.03 - 0.04 International Units (IU)/minute, to norepinephrine as a therapeutic alternative in refractory cases, with the intention of increasing the mean arterial pressure (MAP) and decreasing the dose of norepinephrine.⁽¹⁶16 Polito A, Parisini E, Ricci Z, Picardo S, Annane D. Vasopressin for treatment of vasodilatory shock: an ESICM systematic review and meta-analysis. Intensive Care Med. 2012;38(1):9-19.⁾ However, the effect of vasopressin on mortality remains controversial.⁽¹⁷17 Russell JA, Walley KR, Singer J, Gordon AC, Hébert PC, Cooper DJ, Holmes CL, Mehta S, Granton JT, Storms MM, Cook DJ, Presneill JJ, Ayers D; VASST Investigators. Vasopressin versus norepinephrine infusion in patients with septic shock. N Engl J Med. 2008;358(9):877-87.⁾ More studies are needed to determine the best treatment strategy as well as which groups of patients would benefit most from the association of vasopressor with different mechanisms of action in this situation.

The present study aimed to evaluate the short-term evolution of patients with septic shock refractory to norepinephrine treated with vasopressin, in terms of mortality and length of stay in the ICU. The secondary objective was to describe the clinical characteristics of a series of cases with shock refractory to the first line of treatment.

METHODS

An observational study of an unmatched retrospective design was performed. Data from patients who were hospitalized in the period from December 2014 to June 2016 were analyzed. Patients aged 18 years and older who were hospitalized in any hospital unit and started using vasopressin for the treatment of septic shock were included in the study. According to hospital policy, vasopressin in only released for the treatment of septic shock in cases that are refractory to norepinephrine, as defined by the attending physician. The patients were identified through a computerized prescription report, and those with a registry of dispensing and administration of vasopressin infusion were included. Data were collected on anthropometric measurements, baseline disease, duration of vasopressor use, presence of organ dysfunction, and complications. Patient data were collected directly from the electronic medical record, and evolution data were recorded until hospital outcome (discharge or death) or for up to 30 days after starting treatment with vasopressin.⁽¹⁸18 Hospital de Clínicas de Porto Alegre (HCPA). Institucional do Hospital de Clínicas de Porto Alegre. [Internet]. 2017 [citado 2017 Maio 17]. Disponível em: https://www.hcpa.edu.br/institucional
https://www.hcpa.edu.br/institucional... ⁾

For the assessment of severity and likelihood of complications, the Acute Physiology and Chronic Health Evaluation II (APACHE II, obtained at the time of initiation of vasopressin therapy) and Sequential Organ Failure Assessment (SOFA) scores were recorded.⁽¹⁹19 Knaus WA, Zimmerman JE, Wagner DP, Draper EA, Lawrence DE. APACHE-acute physiology and chronic health evaluation: a physiologically based classification system. Crit Care Med. 1981;9(8):591-7.

20 Kress JP, Hall JB. Approach to the patient with critical illness. In: Kasper D, Fauci A, Hauser S, Longo D, Jameson JL, Loscalzo J, editors. Harrison's principles of internal medicine. 19th ed. New York: McGraw Hill; 2015.^-²¹21 Bihari D, Prakash S, Bersten A. Low-dose vasopressin in addition to noradrenaline may lead to faster resolution of organ failure in patients with severe sepsis/septic shock. Anaesth Intensive Care. 2014;42(5):671-4.⁾ To evaluate the correlation of mortality with SOFA, the Mann-Whitney test was used for independent samples.

The main outcomes were mortality at 3 and 30 days and length of ICU stay.

Data were collected using a standardized form, included in an Excel^® database, and analyzed quantitatively through the Statistical Package for Social Sciences (SPSS) software. The study was approved by the Research Ethics Committee of the Hospital de Clínicas de Porto Alegre (project: 150592; CAAE 51721915700005327).

RESULTS

A total of 80 patients were included with a mean age of 55 years, and there was a predominance of the age group 61 years or older (42.5%), most of whom were men (60%). The clinical and demographic data of the sample are described in table 1. Most patients (86.3%) presented an APACHE score above 20 points; the median SOFA score obtained on the day of determined norepinephrine refractoriness was 11 points (25% percentile: 9; 75%: 13).

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Table 1
Demographic and clinical characteristics of the analyzed patients (n = 80)

In all cases, the use of vasopressin followed the use of norepinephrine, which was used as the first option, in the usual dosage of 1µg/kg/minute.

The mean duration of norepinephrine treatment prior to initiation of vasopressin was 5 days. Vasopressin was used, on average, for 3 days, and the use was interrupted by death in most cases. At the time vasopressin was started, hemodialysis was performed in 26.3% of cases, and ventilatory failure was observed in 92.5% of cases.

Sixty patients (75%) died within 72 hours of initiation of vasopressin infusion. The 30-day mortality rate was 86.2% (Tables 2 and 3). There was no association between APACHE II score in relation to the incidence of death, with a lethality rate of 81.8% in the range of zero to 19 points and 78.3% in the range of >20 points. The same was observed using the SOFA score;⁽²²22 Singer M, Deutschman CS, Seymour CW, Shankar-Hari M, Annane D, Bauer M, et al. The Third International Consensus Definitions for Sepsis and Septic Shock (Sepsis-3). JAMA. 2016;315(8):801-10.^,²³23 Ferreira FL, Bota DP, Bross A, Mélot C, Vincent JL. Serial evaluation of the SOFA score to predict outcome in critically ill patients. JAMA. 2001;286(14):1754-8.⁾ a median of 11 (25% percentile: 9% and 75: 13) was observed in the group that died within 72 hours, and a median of 10 (25% percentile: 8 and 75%: 12.75) was observed in the group that survived (p = 0.238).

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Table 2
Results (n = 80)

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Table 3
Clinical evolution of patients who survived after 72 hours (n = 19)

DISCUSSION

Vasopressin was incorporated into the hospital's drug list in 2014 at the request of the Heart Transplant Service. Its use was approved for cases of shock associated with vasoplegia in the postoperative period of cardiac surgery. After inclusion on the list, however, vasopressin has also been prescribed in refractory cases of septic shock, especially in adults. In this way, the Pharmacy and Therapeutics Commission decided to evaluate the standard of use of the drug and its effectiveness when it was used outside the initially approved indication.

In the present study, a high mortality within 30 days was observed in patients who used vasopressin for the treatment of septic shock refractory to the use of norepinephrine. In fact, in several localized studies, mortality was lower than that observed in the present series. In the meta-analysis performed by Polito et al.,⁽¹⁶16 Polito A, Parisini E, Ricci Z, Picardo S, Annane D. Vasopressin for treatment of vasodilatory shock: an ESICM systematic review and meta-analysis. Intensive Care Med. 2012;38(1):9-19.⁾ 40.6% mortality was verified in 512 septic patients who used vasopressin. However, that meta-analysis included studies in which vasopressin was used as a first-line therapy, while the present series evaluated its use in a situation of refractoriness to norepinephrine.

In a meta-analysis of randomized trials (32 studies, 3,544 patients) conducted by Avni et al.,⁽²⁴24 Avni T, Lador A, Lev S, Leibovici L, Paul M, Grossman A. Vasopressors for the treatment of septic shock: systematic review and meta-analysis. PLoS One. 2015;10(8):e0129305.⁾ the effect of different vasopressors on the total mortality of adult patients with septic shock was evaluated. With the exception of norepinephrine, which was associated with decreased mortality from all causes compared with dopamine (relative risk - RR 0.89; 95% confidence interval - 95%CI 0.81 - 0.98), no differences were observed in mortality among the different treatments. Hemodynamic outcomes were similar among the various vasopressors, with some superiority of norepinephrine in central venous pressure in urinary output and in lactate levels.

In a meta-analysis of randomized trials (9 studies, n = 998), Serpa Neto et al.⁽²⁵25 Serpa Neto A, Nassar AP, Cardoso SO, Manetta JA, Pereira VG, Espósito DC, et al. Vasopressin and terlipressin in adult vasodilatory shock: a systematic review and meta-analysis of nine randomized controlled trials. Crit Care. 2012;16(4):R154.⁾ observed a decrease in the need for norepinephrine among patients receiving vasopressin or terlipressin compared with controls (standard mean difference 1.58, 95%CI -1.73 - -1.44); p < 0.0001). In that study, the effect estimates are provided in combination for users of vasopressin and terlipressin.

Despite the limitations of APACHE II for predicting death, its use was approved given its widespread application in clinical practice as a parameter for severity and prognosis.⁽¹⁹19 Knaus WA, Zimmerman JE, Wagner DP, Draper EA, Lawrence DE. APACHE-acute physiology and chronic health evaluation: a physiologically based classification system. Crit Care Med. 1981;9(8):591-7.^,²⁶26 Hissa PN, Hissa MR, Araújo PS. Análise comparativa entre dois escores na previsão de mortalidade em unidade de terapia intensiva. Rev Soc Bras Clin Med. 2013;11(1):21-6.⁾ The APACHE II score obtained after the analysis of cases showed that the highest incidence of death was in the range of > 20 points (69 patients), while the incidence of death in the range from zero to 19 points included 11 patients.

The follow-up of the individual evolution of patients through the medical records of the hospital occurred until the hospital outcome (discharge or death) or for a maximum period of 30 days after starting treatment with vasopressin.⁽²⁷27 Mehta S, Granton J, Gordon AC, Cook DJ, Lapinsky S, Newton G, Bandayrel K, Little A, Siau C, Ayers D, Singer J, Lee TC, Walley KR, Storms M, Cooper DJ, Holmes CL, Hebert P, Presneill J, Russell JA; Vasopressin and Septic Shock Trial (VASST) Investigators. Cardiac ischemia in patients with septic shock randomized to vasopressin or norepinephrine. Crit Care. 2013;17(3):R117.^,²⁸28 Gordon AC, Mason AJ, Thirunavukkarasu N, Perkins GD, Cecconi M, Cepkova M, Pogson DG, Aya HD, Anjum A, Frazier GJ, Santhakumaran S, Ashby D, Brett SJ; VANISH Investigators. Effect of Early Vasopressin vs Norepinephrine on Kidney Failure in Patients with Septic Shock: The VANISH Randomized Clinical Trial. JAMA. 2016;316(5):509-18.⁾ Therefore, for the patients who survived for a period of more than 30 days, the final outcome is not known, which may be considered as a limitation of the study. Among patients who survived more than 72 hours, only 18.8% showed improvement. This finding provide an explanation for why randomized clinical trials usually have a short follow-up time, as in the case of the studies by Malay et al.⁽¹⁴14 Malay MB, Ashton RC Jr, Landry DW, Townsend RN. Low-dose vasopressin in the treatment of vasodilatory septic shock. J Trauma. 1999;47(4):699-703; discussion 703-5.⁾ and Patel et al.,⁽¹⁵15 Patel BM, Chittock DR, Russell JA, Walley KR. Beneficial effects of short-term vasopressin infusion during severe septic shock. Anesthesiology. 2002;96(3):576-82.⁾ with follow-up times of 4 and 24 hours, respectively. However, there are other cases with a prolonged follow-up, such as in the study by Russell et al.⁽¹⁷17 Russell JA, Walley KR, Singer J, Gordon AC, Hébert PC, Cooper DJ, Holmes CL, Mehta S, Granton JT, Storms MM, Cook DJ, Presneill JJ, Ayers D; VASST Investigators. Vasopressin versus norepinephrine infusion in patients with septic shock. N Engl J Med. 2008;358(9):877-87.⁾ in which mortality was assessed at 28 and 90 days.

Another limitation is that during the study, detailed measurements of important hemodynamic and metabolic outcomes, such as blood levels of lactate, cytokines, and troponins, were not performed; thus, there is the need for further studies to evaluate these variables. It was chosen not to evaluate these parameters in detail but instead to evaluate a "difficult" outcome (mortality). The clinical response to the vasopressor effect was evaluated through MAP.⁽¹⁵15 Patel BM, Chittock DR, Russell JA, Walley KR. Beneficial effects of short-term vasopressin infusion during severe septic shock. Anesthesiology. 2002;96(3):576-82.⁾

Given the uncontrolled design, this study can be considered to be predominantly exploratory and hypothesis-generating in nature; in fact, based on these data, it is not possible to establish the efficacy of vasopressin for reducing mortality. The study is, however, considered useful for reflections on clinical practice, given the frequent use of vasopressin in this context, despite the lack of good quality evidence in situations of refractoriness.

CONCLUSION

Early mortality was elevated in septic patients with refractory shock treated with vasopressin. The high rate of therapeutic failure may have been due to the severity profile of the baseline disease; another possibility could be the relatively late introduction of vasopressin. However, the association of vasopressin with first-line catecholamines has not been shown to be effective in clinical studies.

REFERÊNCIAS

¹
Instituto Latino Americano para Estudos da Sepse (ILAS). Sepse: um problema de saúde pública [Internet]. Brasília (DF): Conselho Federal de Medicina; 2015 [citado 2017 Maio 7]. Disponível em: http://www.ilas.org.br/assets/arquivos/upload/Livro-ILAS(Sepse-CFM-ILAS).pdf
» http://www.ilas.org.br/assets/arquivos/upload/Livro-ILAS(Sepse-CFM-ILAS).pdf
²
Rocha LL, Pessoa CM, Corrêa TD, Pereira AJ, de Assunção MS, Silva E. Current concepts on hemodynamic support and therapy in septic shock. Braz J Anesthesiol. 2015;65(5):395-402.
³
Silva E, Pinheiro C, Michels Júnior V. Consenso Brasileiro de Sepse. Epidemiologia. Rev Bras Ter Intensiva. 2004;16(2):97-101.
⁴
Singer M, Deutschman CS, Seymour CW, Shankar-Hari M, Annane D, Bauer M, et al. The Third International Consensus Definitions for Sepsis and Septic Shock (Sepsis-3). JAMA. 2016;315(8):801-10.
⁵
Kaukonen KM, Bailey M, Suzuki S, Pilcher D, Bellomo R. Mortality related to severe sepsis and septic shock among critically ill patients in Australia and New Zealand, 2000-2012. JAMA. 2014;311(13):1308-16.
⁶
Harrison DA, Welch CA, Eddleston JM. The epidemiology of severe sepsis in England, Wales and Northern Ireland, 1996 to 2004: secondary analysis of a high quality clinical database, the ICNARC Case Mix Programme Database. Crit Care. 2006;10(2):R42.
⁷
Silva E, Pedro MA, Sogayar AC, Mohovic T, Silva CL, Janiszewski M, Cal RG, de Sousa EF, Abe TP, de Andrade J, de Matos JD, Rezende E, Assunção M, Avezum A, Rocha PC, de Matos GF, Bento AM, Corrêa AD, Vieira PC, Knobel E; Brazilian Sepsis Epidemiological Study. Brazilian Sepsis Epidemiological Study (BASES study). Crit Care. 2004;8(4):R251-60.
⁸
Noritomi DT, Ranzani OT, Monteiro MB, Ferreira EM, Santos SR, Leibel F, et al. Implementation of a multifaceted sepsis education program in an emerging country setting: clinical outcomes and cost-effectiveness in a long-term follow-up study. Intensive Care Med. 2014;40(2):182-91.
⁹
Rede Brasileira de Avaliação de Tecnologias em Saúde (REBRATS). Alfadrotrecogina para o tratamento de sepse grave. Bol Bras Aval Tecnol Saúde (BRATS). 2006;1(2):1-5.
¹⁰
Instituto Latino Americano de Sepse (ILAS). Relatório Nacional. Protocolos Gerenciados de sepse: sepse grave e choque séptico 2005-2015. [Internet]. São Paulo: ILAS; 2005 [citado 2017 Maio 23]. Disponível em: http://www.ilas.org.br/assets/arquivos/relatorio-nacional/relatorio-nacional.pdf
» http://www.ilas.org.br/assets/arquivos/relatorio-nacional/relatorio-nacional.pdf
¹¹
Rhodes A, Evans LE, Alhazzani W, Levy MM, Antonelli M, Ferrer R, et al. Surviving Sepsis Campaign: International Guidelines for Management of Sepsis and Septic Shock: 2016. Intensive Care Med. 2017;43(3):304-77.
¹²
Angus DC, Linde-Zwirble WT, Lidicker J, Clermont G, Carcillo J, Pinsky MR. Epidemiology of severe sepsis in the United States: analysis of incidence, outcome, and associated costs of care. Crit Care Med. 2001;29(7):1303-10.
¹³
Westphal GA, Silva E, Salomão R, Bernardo WM, Machado FR. Diretrizes para tratamento da sepse grave/choque séptico: ressuscitação hemodinâmica. Rev Bras Ter Intensiva. 2011;23(1):13-23.
¹⁴
Malay MB, Ashton RC Jr, Landry DW, Townsend RN. Low-dose vasopressin in the treatment of vasodilatory septic shock. J Trauma. 1999;47(4):699-703; discussion 703-5.
¹⁵
Patel BM, Chittock DR, Russell JA, Walley KR. Beneficial effects of short-term vasopressin infusion during severe septic shock. Anesthesiology. 2002;96(3):576-82.
¹⁶
Polito A, Parisini E, Ricci Z, Picardo S, Annane D. Vasopressin for treatment of vasodilatory shock: an ESICM systematic review and meta-analysis. Intensive Care Med. 2012;38(1):9-19.
¹⁷
Russell JA, Walley KR, Singer J, Gordon AC, Hébert PC, Cooper DJ, Holmes CL, Mehta S, Granton JT, Storms MM, Cook DJ, Presneill JJ, Ayers D; VASST Investigators. Vasopressin versus norepinephrine infusion in patients with septic shock. N Engl J Med. 2008;358(9):877-87.
¹⁸
Hospital de Clínicas de Porto Alegre (HCPA). Institucional do Hospital de Clínicas de Porto Alegre. [Internet]. 2017 [citado 2017 Maio 17]. Disponível em: https://www.hcpa.edu.br/institucional
» https://www.hcpa.edu.br/institucional
¹⁹
Knaus WA, Zimmerman JE, Wagner DP, Draper EA, Lawrence DE. APACHE-acute physiology and chronic health evaluation: a physiologically based classification system. Crit Care Med. 1981;9(8):591-7.
²⁰
Kress JP, Hall JB. Approach to the patient with critical illness. In: Kasper D, Fauci A, Hauser S, Longo D, Jameson JL, Loscalzo J, editors. Harrison's principles of internal medicine. 19th ed. New York: McGraw Hill; 2015.
²¹
Bihari D, Prakash S, Bersten A. Low-dose vasopressin in addition to noradrenaline may lead to faster resolution of organ failure in patients with severe sepsis/septic shock. Anaesth Intensive Care. 2014;42(5):671-4.
²²
Singer M, Deutschman CS, Seymour CW, Shankar-Hari M, Annane D, Bauer M, et al. The Third International Consensus Definitions for Sepsis and Septic Shock (Sepsis-3). JAMA. 2016;315(8):801-10.
²³
Ferreira FL, Bota DP, Bross A, Mélot C, Vincent JL. Serial evaluation of the SOFA score to predict outcome in critically ill patients. JAMA. 2001;286(14):1754-8.
²⁴
Avni T, Lador A, Lev S, Leibovici L, Paul M, Grossman A. Vasopressors for the treatment of septic shock: systematic review and meta-analysis. PLoS One. 2015;10(8):e0129305.
²⁵
Serpa Neto A, Nassar AP, Cardoso SO, Manetta JA, Pereira VG, Espósito DC, et al. Vasopressin and terlipressin in adult vasodilatory shock: a systematic review and meta-analysis of nine randomized controlled trials. Crit Care. 2012;16(4):R154.
²⁶
Hissa PN, Hissa MR, Araújo PS. Análise comparativa entre dois escores na previsão de mortalidade em unidade de terapia intensiva. Rev Soc Bras Clin Med. 2013;11(1):21-6.
²⁷
Mehta S, Granton J, Gordon AC, Cook DJ, Lapinsky S, Newton G, Bandayrel K, Little A, Siau C, Ayers D, Singer J, Lee TC, Walley KR, Storms M, Cooper DJ, Holmes CL, Hebert P, Presneill J, Russell JA; Vasopressin and Septic Shock Trial (VASST) Investigators. Cardiac ischemia in patients with septic shock randomized to vasopressin or norepinephrine. Crit Care. 2013;17(3):R117.
²⁸
Gordon AC, Mason AJ, Thirunavukkarasu N, Perkins GD, Cecconi M, Cepkova M, Pogson DG, Aya HD, Anjum A, Frazier GJ, Santhakumaran S, Ashby D, Brett SJ; VANISH Investigators. Effect of Early Vasopressin vs Norepinephrine on Kidney Failure in Patients with Septic Shock: The VANISH Randomized Clinical Trial. JAMA. 2016;316(5):509-18.

Edited by

Responsible editor: Pedro Póvoa

Publication Dates

Publication in this collection
13 Dec 2018
Date of issue
Oct-Dec 2018

History

Received
19 Oct 2017
Accepted
13 June 2018

Este é um artigo publicado em acesso aberto (Open Access) sob a licença Creative Commons Attribution, que permite uso, distribuição e reprodução em qualquer meio, sem restrições desde que o trabalho original seja corretamente citado.

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[25] ²⁵
Serpa Neto A, Nassar AP, Cardoso SO, Manetta JA, Pereira VG, Espósito DC, et al. Vasopressin and terlipressin in adult vasodilatory shock: a systematic review and meta-analysis of nine randomized controlled trials. Crit Care. 2012;16(4):R154.

[26] ²⁶
Hissa PN, Hissa MR, Araújo PS. Análise comparativa entre dois escores na previsão de mortalidade em unidade de terapia intensiva. Rev Soc Bras Clin Med. 2013;11(1):21-6.

[27] ²⁷
Mehta S, Granton J, Gordon AC, Cook DJ, Lapinsky S, Newton G, Bandayrel K, Little A, Siau C, Ayers D, Singer J, Lee TC, Walley KR, Storms M, Cooper DJ, Holmes CL, Hebert P, Presneill J, Russell JA; Vasopressin and Septic Shock Trial (VASST) Investigators. Cardiac ischemia in patients with septic shock randomized to vasopressin or norepinephrine. Crit Care. 2013;17(3):R117.

[28] ²⁸
Gordon AC, Mason AJ, Thirunavukkarasu N, Perkins GD, Cecconi M, Cepkova M, Pogson DG, Aya HD, Anjum A, Frazier GJ, Santhakumaran S, Ashby D, Brett SJ; VANISH Investigators. Effect of Early Vasopressin vs Norepinephrine on Kidney Failure in Patients with Septic Shock: The VANISH Randomized Clinical Trial. JAMA. 2016;316(5):509-18.

Variables
Sex
Men	60
Woman	40
Age (years)
< 25	3.8
26 - 40	17.5
41-60	36.3
≥ 61	42.5
APACHE II
0 - 19	13.8
> 20	86.3
Infection sites
Abdominal	37.5
Pulmonary	30
Not informed^* * Patients had no defined infection focus or it was not possible to identify these data in the medical record. Results expressed as % or median.	18.8
Renal/urinary	6.3
Heart	2.5
Pelvic	2.5
Multiple organs	1.3
Skin	1.3
Low heart rate
Yes	53.7
No	46.3
Levels of SVO₂
Normal (68 - 77%)	2.5
Low	92.5
Not informed^* * Patients had no defined infection focus or it was not possible to identify these data in the medical record. Results expressed as % or median.	5
Mean blood pressure
Normal	55
Hypotension (< 65mmHg)	45
Lactate levels
Normal (1.0mmol/L to 1.8mmol/L)	22.5
High	73.8
Not informed	3.8
SOFA, p = 0.238
Survivors up to 72 hours	10
Deaths up to 72 hours	11

Results
Days of use of norepinephrine (dose of 1µg/kg/min^* * Unit referring to the dosage of medicines; )
1 - 5	66.3
6 - 20	31.3
21 - 30	2.5
Days of use of vasopressin (dose of 0.03 - 0.04 IU/min^* * Unit referring to the dosage of medicines; )
1 - 5	95
6 - 20^† † prescription authorized by the Drugs Commission of the Clinics Hospital of Porto Alegre;	5
Days of ICU stay
1 - 5	48.8
6 - 20	36.3
21 - 30	5.0
31 or more^‡ ‡ the length of hospital stay in the intensive care unit and the survival of patients over 30 days (maximum study period) cannot be stated. Results expressed as n (%).	10.0
Survival after vasopressin use 80 (%)
1 - 5 days	59 (73.8)
6 - 20 days	10 (12.5)
21 - 30 days	1 (1.3)
31 days or more^‡ ‡ the length of hospital stay in the intensive care unit and the survival of patients over 30 days (maximum study period) cannot be stated. Results expressed as n (%).	10 (12.5)
Evolution in 3 days after use of vasopressin (in relation to response to treatment with vasopressin) 80 (%)
Death	60 (75.0)
Improved	15 (18.8)
Worsened	4 (5.0)
Indifferent	1 (1.3)
Use of dobutamine
Yes	6.3
No	93.8
Use of auxiliary therapy
Total with at least one auxiliary therapy	98.8
Renal replacement	3.8
Invasive mechanical ventilation	3.8
Use of corticosteroids	5.0
Use of two auxiliary therapies	52.5
Use of three auxiliary therapies	33.7
Not informed	1.2
Period of introduction of vasopressin treatment
After 48 hours of onset of sepsis	36.3
Ignored	1.3
Hospital outcome (within 30 days)
Discharge	13.8
Death	86.2
Cause of death
Related to sepsis	76.3
Other reasons	12.5

Evolution 30 days after vasopressin use
Improved	47.4
Death	47.4
Worsened	5.2