Effect of Selepressin vs Placebo on Ventilator- and Vasopressor-Free Days in Patients With Septic Shock

Laterre, Pierre‐François; Berry, Scott M.; Blemings, Allan; Carlsen, Jens; Dalmay, François; Graves, Todd L.; Jacobsen, Karsten; Lewis, Roger J.; Opal, Steven M.; Perner, Anders; Pickkers, Peter; Russell, James A.; Windeløv, Nis A.; Yealy, Donald M.; Asfar, Pierre; Bestle, Morten H.; Muller, Grégoire; Bruel, Cédric; Brulé, Noëlle; Decruyenaere, Johan; Dive, Alain-Michel; Dugernier, Thierry; Krell, Kenneth; Lefrant, Jean‐Yves; Mégarbane, Bruno; Mercier, Emmanuelle; Mira, Jean‐Paul; Quenot, Jean‐Pierre; Rasmussen, Bodil Steen; Thorsen-Meyer, Hans-Christian; Laenen, Margot Vander; Vang, Marianne L.; Vignon, Philippe; Vinatier, Isabelle; Wichmann, Sine; Wittebole, Xavier; Kjølbye, Anne Louise; Angus, Derek C.

doi:10.1001/jama.2019.14607

Cited by 100 publications

(88 citation statements)

References 26 publications

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“…Recently, the SEPSISACT study [50] compared with a randomized placebo-controlled trial the addition of selepressin to norepinephrine. This study was divided in two parts: the first was aimed at assessing the best-performing regimen of selepressin (between three dosing regimens of selepressin), and, in the second part, the authors compared this selepressin regimen to placebo.…”

Section: Vasopressin Analogues: Terlipressin and Selepressinmentioning

confidence: 99%

Vasopressin and its analogues in shock states: a review

Demiselle

Fage

Radermacher

et al. 2020

Ann. Intensive Care

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Activation of arginine-vasopressin is one of the hormonal responses to face vasodilation-related hypotension. Released from the post-pituitary gland, vasopressin induces vasoconstriction through the activation of V1a receptors located on vascular smooth muscle cells. Due to its non-selective receptor affinity arginine-vasopressin also activates V2 (located on renal tubular cells of collecting ducts) and V1b (located in the anterior pituitary and in the pancreas) receptors, thereby potentially promoting undesired side effects such as anti-diuresis, procoagulant properties due to release of the von Willebrand's factor and platelet activation. Finally, it also cross-activates oxytocin receptors. During septic shock, vasopressin plasma levels were reported to be lower than expected, and a hypersensitivity to its vasopressor effect is reported in such situation. Terlipressin and selepressin are synthetic vasopressin analogues with a higher affinity for the V1 receptor, and, hence, potentially less side effects. In this narrative review, we present the current knowledge of the rationale, benefits and risks of vasopressin use in the setting of septic shock and vasoplegic shock following cardiac surgery. Clearly, vasopressin administration allows reducing norepinephrine requirements, but so far, no improvement of survival was reported and side effects are frequent, particularly ischaemic events. Finally, we will discuss the current indications for vasopressin and its agonists in the setting of septic shock, and the remaining unresolved questions.

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Section: Vasopressin Analogues: Terlipressin and Selepressinmentioning

confidence: 99%

Vasopressin and its analogues in shock states: a review

Demiselle

Fage

Radermacher

et al. 2020

Ann. Intensive Care

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“…Up to April 30, 2020, we initially retrieved 807 records and 23 trials reporting on 4380 septic shock patients were eligible for final analysis (21 full-text articles and 2 abstracts). These papers were from Austria [ 30 ] ( n = 1), France [ 24 ] ( n = 1), Iran [ 22 ] ( n = 1), Czech Republic [ 16 ] ( n = 1), England [ 18 ] ( n = 1), Colombia [ 21 ] ( n = 1), Brazil [ 13 , 31 ] ( n = 2), India [ 15 , 32 ] ( n = 2), Italy [ 25 , 26 ] ( n = 2), the USA [ 23 , 33 ] ( n = 2), China [ 14 , 19 , 27 , 28 ] ( n = 4), and multi-country [ 4 , 11 , 17 , 20 , 34 ] ( n = 5). All these trials from ICUs were published from 2003 to 2019, and the mean age was from 47.53 to 72.83 years.…”

Section: Resultsmentioning

confidence: 99%

“…Nevertheless, achieving the target MAP may generally require high doses of NE, increasing the risk of myocardial, mesenteric, and digital ischemia as well as arrhythmias and mortality, etc. [ 4 , 5 ]. Regrettably, around 7% critically ill patients tend to be unresponsive to the increasing dose of NE (refractory shock) in spite of an early recognition, diagnosis, and treatment, with over 50% short-term mortality [ 6 ].…”

Section: Introductionmentioning

confidence: 99%

Non-catecholamine vasopressors in the treatment of adult patients with septic shock—evidence from meta-analysis and trial sequential analysis of randomized clinical trials

et al. 2020

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Background Norepinephrine (NE) has currently been the first-choice vasopressor in treating septic shock despite generally insufficient for patients with refractory septic shock. The aim of this update meta-analysis was to assess the safety and efficacy of a combination of non-catecholamine vasopressors (vasopressin/pituitrin/terlipressin/selepressin/angiotensin II) and NE versus NE in managing adult septic shock patients. Methods We conducted this study of literatures published from the inception to April 30, 2020, using PubMed, Embase, and the Cochrane Library databases without language restriction. Randomized controlled trials comparing NE with non-catecholamine vasopressors among adult septic shock patients were included in this meta-analysis. Pooled effects of relative risk (RR) or standard mean difference (SMD) and corresponding 95% confidence interval (CI) were calculated using a random-effects model. Results Twenty-three studies covering 4380 participants were finally enrolled. The combined analysis of non-catecholamine vasopressors resulted in a nonsignificant reduction in 90-day/ICU/hospital mortality except for a decreased in 28-day mortality (n = 4217; RR, 0.92; 95% CI 0.86–0.99; P = 0.02). This favorable result was subsequently verified by the subgroup analyses of low risk of bias studies (RR = 0.91, 95% CI = 0.84 to 0.98; P = 0.02) and catecholamine-resistant refractory shock patients group (RR, 0.84; 95% CI = 0.70–1.00; P = 0.048). The pooled analysis of non-catecholamine vasopressors showed a 14% higher success rate of shock reversal at 6 h, a 29% decreased risk of continuous renal replacement therapy, but a 51% increased risk of hyponatremia and a 2.43 times higher risk of digital ischemia. Besides, the pooled data showed that non-catecholamine vasopressors decreased heart rate (HR) (SMD, − 0.43; 95% CI − 0.66 – − 0.19; P < 0.001), serum creatinine (− 0.15; 95% CI − 0.29 – − 0.01; P = 0.04), and the length of mechanical ventilation (MV) (− 0.19; 95% CI − 0.31 – − 0.07; P < 0.01, but there was no significant difference in other parameters. Conclusions Current pooled results suggest that the addition of NE to non-catecholamine vasopressors was associated with a marginally significant reduction in 28-day mortality. Moreover, they were able to shorten the length of MV, improved renal function, decreased HR, and increased the 6-h shock reversal success rate at the expense of increased the risk of hyponatremia and digital ischemia.

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“…Many of these adaptive methodologies are applicable to clinical trials in critical care. Recent examples of adaptive design features in critical care include the RACE trial [37], an adaptive, dose-finding, phase 2 clinical trial of levocarnitine for septic shock, the SEPSIS-ACT trial of selepressin for septic shock [38], and the phase 3 PROSpect trial (NCT03896763). The PROSpect trial plans to randomize pediatric patients with ARDS to supine or prone positioning and low tidal volume or high-frequency ventilation, with adjustments in the enrollment ratios occurring every 100 patients.…”

Section: Bayesian Trial Analysismentioning

confidence: 99%

Contemporary strategies to improve clinical trial design for critical care research: insights from the First Critical Care Clinical Trialists Workshop

et al. 2020

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Background: Conducting research in critically-ill patient populations is challenging, and most randomized trials of critically-ill patients have not achieved pre-specified statistical thresholds to conclude that the intervention being investigated was beneficial. Methods: In 2019, a diverse group of patient representatives, regulators from the USA and European Union, federal grant managers, industry representatives, clinical trialists, epidemiologists, and clinicians convened the First Critical Care Clinical Trialists (3CT) Workshop to discuss challenges and opportunities in conducting and assessing critical care trials. Herein, we present the advantages and disadvantages of available methodologies for clinical trial design, conduct, and analysis, and a series of recommendations to potentially improve future trials in critical care. Conclusion: The 3CT Workshop participants identified opportunities to improve critical care trials using strategies to optimize sample size calculations, account for patient and disease heterogeneity, increase the efficiency of trial conduct, maximize the use of trial data, and to refine and standardize the collection of patient-centered and patientinformed outcome measures beyond mortality.

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Effect of Selepressin vs Placebo on Ventilator- and Vasopressor-Free Days in Patients With Septic Shock

Cited by 100 publications

References 26 publications

Vasopressin and its analogues in shock states: a review

Vasopressin and its analogues in shock states: a review

Non-catecholamine vasopressors in the treatment of adult patients with septic shock—evidence from meta-analysis and trial sequential analysis of randomized clinical trials

Contemporary strategies to improve clinical trial design for critical care research: insights from the First Critical Care Clinical Trialists Workshop

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