Multicentered prospective investigator initiated study to evaluate the clinical outcomes with extracorporeal cytokine adsorption device (CytoSorb®) in patients with sepsis and septic shock.

BACKGROUND: Sepsis is a severe clinical syndrome related to the host response to infection. The severity of infections is due to an activation cascade that will lead to an auto amplifying cytokine production: The cytokine storm. Hemoadsorption by CytoSorb® therapy is a new technology that helps to address the cytokine storm and to regain control over various inflammatory conditions. AIM: To evaluate prospectively CytoSorb® therapy used as an adjunctive therapy along with standard of care in septic patients admitted to intensive care unit (ICU).
METHODS: This was a prospective, real time, investigator initiated, observational multicenter study conducted in patients admitted to the ICU with sepsis and septic shock. The improvement of mean arterial pressure and reduction of vasopressor needs were evaluated as primary outcome. The change in laboratory parameters, sepsis scores [acute physiology and chronic health evaluation (APACHE II) and sequential organ failure assessment (SOFA)] and vital parameters were considered as secondary outcome. The outcomes were also evaluated in the survivor and non-survivor group. Descriptive statistics were used; a P value < 0.05 was considered to be statistically significant.
RESULTS: Overall, 45 patients aged ≥ 18 and ≤ 80 years were included; the majority were men (n = 31; 69.0%), with mean age 47.16 ± 14.11 years. Post CytoSorb® therapy, 26 patients survived and 3 patients were lost to follow-up. In the survivor group, the percentage dose reduction in vasopressor was norepinephrine (51.4%), epinephrine (69.4%) and vasopressin (13.9%). A reduction in interleukin-6 levels (52.3%) was observed in the survivor group. Platelet count improved to 30.1% (P = 0.2938), and total lung capacity count significantly reduced by 33% (P < 0.0001). Serum creatinine and serum lactate were reduced by 33.3% (P = 0.0190) and 39.4% (P = 0.0120), respectively. The mean APACHE II score was 25.46 ± 2.91 and SOFA scores was 12.90 ± 4.02 before initiation of CytoSorb® therapy, and they were reduced significantly post therapy (APACHE II 20.1 ± 2.47; P < 0.0001 and SOFA 9.04 ± 3.00; P = 0.0003) in the survivor group. The predicted mortality in our patient population before CytoSorb® therapy was 56.5%, and it was reduced to 48.8% (actual mortality) after CytoSorb® therapy. We reported 75% survival rate in patients given treatment in < 24 h of ICU admission and 68% survival rates in patients given treatment within 24-48 h of ICU admission. In the survivor group, the average number of days spent in the ICU was 4.44 ± 1.66 d; while in the non-survivor group, the average number of days spent in ICU was 8.5 ± 15.9 d. CytoSorb® therapy was safe and well tolerated with no adverse events reported.
CONCLUSION: CytoSorb® might be an effective adjuvant therapy in stabilizing sepsis and septic shock patients. However, it is advisable to start the therapy at an early stage (preferably within 24 h after onset of septic shock). ©The Author(s) 2021. Published by Baishideng Publishing Group Inc. All rights reserved.

Core Tip: This prospective, real time, observational multicenter study was conducted in 45 patients with sepsis and septic shock. Post therapy, 26 patients survived and dose reduction in norepinephrine, epinephrine and vasopressin was 51.4%, 69.4% and 13.9%, respectively. Interleukin-6 level reduction was 52.3%, and platelet count improved significantly to 30.1%. Mean acute physiology and chronic health evaluation and sequential organ failure assessment scores were reduced significantly. Predicted mortality before CytoSorb® therapy was 56.5%, and mortality reduced to 48.8% after CytoSorb® therapy. The survival rate in patients given treatment in < 24 h of intensive care unit admission was 75% and 68% when given within 24-48 h of intensive care unit admission. CytoSorb® therapy was safe and well tolerated with no adverse events reported.

INTRODUCTION

Sepsis is a life-threatening organ dysfunction caused by a dysregulated host response to infection with a high mortality rate, ranging from 30%-50% or more[1]. Extracorporeal cytokine hemoadsorption attenuates the overwhelming inflammatory response in sepsis and helps in immunomodulation[1,2]. Septic shock is defined as sepsis with hyperlactataemia and concurrent hypotension[3,4]. In intensive care units (ICUs), sepsis is a leading cause of death and the 11th leading cause of death overall. In India, more than one million estimated new cases of sepsis are treated in ICUs each year, accounting for one out of every four patients in the ICUs. A recent study conducted by the Indian Society of Critical Care across 17 states of India in 4209 patients (the Indian intensive care case mix and practice patterns study) reported mortality as high as 46% in patients with septic shock and 42.2% overall in septic patients, compared with 17.8% mortality for ICU patients who did not develop sepsis[5].

The management of patients with septic shock includes early resuscitation with fluid and vasopressor therapy, support by mechanical ventilation, renal replacement therapy and appropriate antibiotic initiation[6]. An initial goal to treat patients with septic shock and sepsis is to maintain mean arterial pressure (MAP) and cardiac output. Patients who fail to respond to adequate fluid resuscitation are prescribed vasopressors [norepinephrine (NE), dopamine, epinephrine (E), vasopressin (V), phenylephrine] and inotropes (dobutamine, milrinone) in order to maintain hemodynamic parameters[7]. These agents help to maintain adequate blood pressure and organ perfusion. However, they can have substantial adverse effects like profound vasoconstriction, causing hypoperfusion and arrhythmic events[8]. Thus, their optimized use is crucial. CytoSorb® is an International Science Organization 10993 biocompatible device that is approved in the United States under International Science Organization 13485 certification. It is also approved as an extracorporeal cytokine adsorber in the European Union and marketed in 29 countries across the globe for all the indications that are associated with high cytokine levels[9-11]. It is a CE-approved hemoadsorption device designed to remove excess levels of inflammatory mediators like cytokines and other mid-molecular weight molecules through size selective removal and surface adsorption[12,13]. Unlike metabolic approaches to anti-inflammation, CytoSorb® is able to capture directly and reduce mid-molecular weight inflammatory mediators (approximately 10-60 kDa) in blood, including both pro- and anti-inflammatory cytokines, chemokines and bacterial exotoxins[14]. It is reported to work most effectively when treatment is initiated within 24 h of diagnosed sepsis[15]. As a result of adsorption of inflammatory metabolites like cytokines it is inferred that hemodynamic and metabolic stabilization will follow[16].

In addition to standard treatment, including renal replacement and cardiac support, recent studies showed promising results with the use of extracorporeal cytokine hemoadsorption therapy[17-20]. CytoSorb® therapy along with standard of care is also utilized in the treatment of allergic reactions, burn injuries, and liver and pulmonary failure. Other potential indications for use of CytoSorb® therapy are trauma, hemophagocytic lymphohistiocytosis, pancreatitis and rhabdomyolysis[21,22].

To date, scarce scientific evidence including few case series and randomized controlled trials are available on the use of CytoSorb® therapy[10,15]. An international registry of 22 countries on use of Cytosorb® therapy in 198 patients noted that sepsis was the most common indication for use of Cytosorb® therapy (n = 135) and reported improved interleukin (IL)-6 levels and improved actual mortality (AM, 65%) vs predicted mortality (PM, 78%) for these patients[10].

CytoSorb® has been used in India for several years. Therefore, the purpose of this prospective study was to collect data and evaluate the clinical outcomes with CytoSorb® therapy in patients with sepsis and septic shock.

MATERIALS AND METHODS

Study design

This was a prospective, real time, investigator initiated, observational, multicenter study conducted for 8 mo (including enrollment and completion) across four different tertiary care ICUs in India. The study protocol was approved by the local scientific and ethical committee. The study was conducted in compliance with the current International Council for Harmonization, Good clinical practice (ICH GCP), Schedule Y and Indian Council of Medical Research guidelines. A written informed consent was obtained from all the patients/relatives before initiating the therapy. The patients/ caretakers received information about the usage, advantages and disadvantages of treatment.

Inclusion/exclusion criteria

We enrolled patients admitted in the ICU with sepsis and septic shock who were initially managed for at least 6 h as recommended by the surviving sepsis guidelines[2]. Of these, we included those patients who had evidence of at least one new onset organ dysfunction during the course of sepsis.

Patients were excluded if: Diagnosed with septic shock for > 48 h; Had symptoms of uncontrolled hemorrhage in the last 24 h; Had more than three failed organs on presentation; Had received chemotherapy or radiation treatment within last 60 d; Diagnosed with chronic kidney disease stage 5 or end stage hepatic liver failure; Had a history of immunosuppressive disorders or admitted with acute coronary syndrome or life-threatening cardiac arrhythmia.

Study procedure

Before initiating the CytoSorb® therapy, the baseline patient data, including relevant demographic details, vital signs, clinical diagnosis, progression of clinical condition and laboratory parameters, were recorded in the case record form (CRF). To monitor the effects of CytoSorb therapy, all relevant parameters were recorded before and after the CytoSorb® treatment.

Primary outcomes

The following outcomes were considered as primary end points:

Change in vasopressor requirement: As per vasopressor or inotropic requirement, the MAP was targeted > 65 mmHg. Dose and number of drugs (i.e. NE, E and V) and change in MAP before and after CytoSorb® therapy were recorded.

Cytokine assay: Serum samples for multi cytokine assay (i.e. IL-1, IL-6) were collected pre-(baseline) and post-(after the last treatment) CytoSorb® therapy and analyzed in Syngene Lab (Bangalore, India). The post CytoSorb® samples were collected before disconnecting the device. Change in pre and post cytokine values were recorded in CRF.

Percentage reduction in vasopressor dose/cytokine level was calculated as (difference in average pre and average post vasopressor dose or cytokine level/average pre vasopressor dose or pre cytokine level dose) × 100. To monitor the vasopressor-MAP relationship, the MAP/NE ratio was used.

Secondary outcomes

Evaluation of laboratory parameters: We recorded the complete blood count and biochemistry test results both at baseline, during and at the completion of CytoSorb® therapy in the CRF. Change in laboratory parameter values for pre and post CytoSorb® therapy were evaluated.

Organ function

Acute physiology and chronic health evaluation (APACHE II) and Sequential organ failure assessment (SOFA) scores were recorded at baseline and post therapy. Vital parameters were recorded at baseline and on each day of CytoSorb® treatment. MAP, X–ray findings, ventilator requirement and oxygenation parameters (fraction of inspiration O2, alveolar oxygen partial pressure, partial pressure of carbon dioxide) were also documented in CRF. At the end of treatment, change in pre and post therapy values were calculated. APACHE-II calculator was used as a severity score and mortality estimation tool[23].

Survival outcomes

Survival outcomes were determined on the basis of length of patients’ stay in ICU (total number of days spent by the patient in ICU before, during and post CytoSorb® therapy) and mechanical ventilation/dialysis requirement (frequency at which the patients required mechanical ventilation and dialysis before and after the treatment).

Length of treatment

The duration of CytoSorb® treatment in hours and number of CytoSorb® devices used were decided as per the patient’s condition and clinical outcomes. We used a minimum of two devices for each patient. Each day one CytoSorb® device was used for 8-12 h in hemodialysis machine or for maximum of 24 h in continuous renal replacement therapy machines.

Safety evaluation

Any event that was not expected due to the course of disease and concurrent medications was recorded and evaluated.

Statistical analysis

A sample size calculation was not performed due to the exploratory character of the study. Data were primarily recorded in Microsoft Excel 2016. Data are summarized according to data distribution (normal or not-normal), and the appropriate parametric or non-parametric statistical tests were used to evaluate the difference in clinical outcomes and the change in clinical and laboratory parameters before and after CytoSorb® therapy. The level of significance was defined as P < 0.05.

RESULTS

Study population

A total of 45 patients aged ≥ 18 and ≤ 80 years were included in the study. Majority of the patients were men (n = 31; 69.0%) with mean age 47.16 ± 14.11 years. The mean age of women patients was 48.14 ± 19.04 years. Prior to CytoSorb® therapy, the percentage of patients who required mechanical ventilation and dialysis were 78% and 49%, respectively. The rest of the demographics are summarized in Table 1. Twenty-six patients (57.8%) survived the full course of CytoSorb® therapy, and 3 patients were lost to follow up.

Table 1

Baseline characteristics of all the patients before initiating the therapy

Baseline characteristics	Findings, mean ± SD
Age, yr	47.46 ± 15.56
Heart rate, beats/min	117 ± 22.05
MAP, mmHg	69.15 ± 9.19
GCS	9.04 ± 3.06
APACHE-II	25.46 ± 5.06
SOFA	12.90 ± 4.37
Leucocytes, µL	15311.44 ± 7140.54
Platelets, cells/mm3	139153.48 ± 89467.72
S. Creatinine, mg/dL	2.74 ± 1.72
S. Lactate, mmoL/L	4.61 ± 2.87
PaCO2	43.37 ± 18.22
PaO2	94.02 ± 49.09
FiO2	48.78 ± 43.28
PaO2/FiO2	118.6 ± 58.01

APACHE II: Acute physiology and chronic health evaluation; FiO2: Fraction of inspiration O2; GCS: Glasgow coma scale; MAP: Mean arterial pressure; SD: Standard deviation; SOFA: Sequential organ failure assessment; PaCO2: Partial pressure of carbon dioxide; PaO2: Alveolar oxygen partial pressure.

Evaluation of primary outcomes

Vasopressor requirement: Table 2 shows the change in vasopressor drugs in the survivor group from the start after the termination of CytoSorb® therapy. Overall, before CytoSorb® therapy, 21 patients required NE, 4 patients were on E and 9 were on V. In general, there was a tendency of reduced need for vasopressors post CytoSorb® therapy, but it did not reach statistical significance. Amongst the patients in the non-survivor group, the use of vasopressor drugs increased or remained unchanged (data not shown).

Table 2

Percentage decrease in patients and vasopressor doses (survivors)

Vasopressor drug, µg/kg/min	Pre CytoSorb®, therapy patient number (n), dose (median)	Post CytoSorb® Therapy, patient number (n), dose (median)	% Decrease in dose	P value (dose)
Norepinephrine	21; 1	18; 0.45	43.3	0.160
Epinephrine	4; 0.055	1; 0.055	64.4	-
Vasopressin	9; 1.5	7; 1	15.4	0.816

Change in laboratory parameters in survivors (Table Total lymphocyte count reduced significantly at the end of the therapy. Serum creatinine and lactate levels also reduced significantly. There was no other significant change in any of the investigated parameters (Table 3).

Table 3

Change in laboratory parameters for survivors

Parameters	Pre CytoSorb ® therapy	Post CytoSorb ® therapy	P value
Hb, g/dL	10.01 ± 2.20	9.28 ± 1.53	0.1830
HCT, %	29.74 ± 8.4	25.75 ± 7.67	0.0909
Leucocytes, µL	16724 ± 5425	11215 ± 3317	0.00011
Platelets, cells/mm3	139256 ± 88029	181203 ± 181381	0.2938
S. Creatinine, mg/dL	3.13 ± 1.92	2.08 ± 1.02	0.01901
S. Lactate, mmol/L	4.75 ± 2.77	2.88 ± 2.39	0.01201
SGOT, U/L	488.44 ± 1570.42	369.95 ± 1134.74	0.7661
SGPT, U/L	192.72 ± 298.99	145.90 ± 236.97	0.5503
BUN, mg/dL	76.21 ± 61.88	62.39 ± 52.28	0.4076
Bilirubin, mg/dL	9.91 ± 36.77	8.35 ± 31.36	0.8730
Sodium, mmol/L	134.38 ± 25.69	134.32 ± 6.20	0.9908
Potassium, mmol/L	3.98 ± 0.95	3.73 ± 1.05	0.3723
Albumin, g/L	2.65 ± 0.93	2.71 ± 0.95	0.8261
Arterial pH	7.35 ± 0.100	7.36 ± 0.105	0.7291
Bicarbonate	24.89 ± 10.71	24.75 ± 9.21	0.9599

Significant value P < 0.05, all values are defined as mean ± SD.

BUN: Blood urea nitrogen; Hb: Hemoglobin; HCT: Hematocrit; SD: Standard deviation; SGOT: Serum glutamic oxaloacetic transaminase; SGPT: Serum glutamic-pyruvic transaminase.

There was some reduction in the inflammatory marker levels for both IL-1 and IL-6, but it did not reach statistical significance (Table 4).

Table 4

Cytokine assay results for survivors

Cytokine	Pre CytoSorb ® therapy, mean ± SD	Post CytoSorb ® therapy, mean ± SD	Percentage change	P value
IL1, pg/mL	10.74 ± 9.70	9.54 ± 9.66	11.11	0.5580
IL6, pg/mL	889.15 ± 1307.43	423.69 ± 1105.55	52.34	0.0792

IL: Interleukin.

Change in vital parameters in survivors (Table After CytoSorb® therapy, there was a 15.8% significant increase in MAP. Among non-survivors (n = 19) there was also a significant increase in MAP (from 69.56 ± 7.84 to 72.13 ± 13.2 mmHg, P = 0.036). Post CytoSorb® therapy, both heart rate and the Glasgow coma score improved significantly in the survivor group. The rest of the data for survivors are shown in Table 5.

Table 5

Change in vital parameters in survivors

Parameters	Survivor group		P value
	Pre CytoSorb ® therapy, mean ± SD	Post CytoSorb ® therapy, mean ± SD
Heart rate, beats/min	118.57 ± 19.8	103.07 ± 19.38	0.00651
MAP, mmHg	68.61 ± 9.62	79.42 ± 9.05	0.00011
GCS	9.86 ± 2.34	12.20 ± 1.47	0.00011
PaCO2	43.32 ± 18.63	38.57 ± 11.66	0.2757
PaO2/FiO2	162.09 ± 82.99	161.20 ± 66.58	0.9704

Significant P value < 0.05.

All values are defined as mean ± SD. FiO2: Fraction of inspiration O2; GCS: Glasgow coma scale; MAP: Mean arterial pressure; PaCO2: Partial pressure of carbon dioxide; PaO2: Alveolar oxygen partial pressure; SD: Standard deviation.

Evaluation of secondary outcomes

Assessment of sepsis scores: Both APACHE II and SOFA scores were significantly reduced by the end of the treatment among survivors (Figure 1). Overall, there was a 20.7% reduction in APACHE II and 29.8% reduction in SOFA scores. In the non-survivor group, APACHE II scores increased from 26.5 ± 5.2 to 27.93 ± 5.2, and SOFA scores also increased from 13.56 ± 4.53 to 15.38 ± 4.29.

Figure 1

Sepsis scores in survivor group (pre and post CytosorbSignificant P values obtained for both acute physiology and chronic health evaluation (P < 0.0001) and sequential organ failure assessment scores (P = 0.0003). APACHE II: acute physiology and chronic health evaluation; SOFA: Sequential organ failure assessment scores.

Predicted mortality: The PM before CytoSorb® therapy was 56.5% in the overall population; the actual mortality after CytoSorb® therapy was 48.8% (Figure 2).

Figure 2

Predicted mortality vs actual mortality based on acute physiology and chronic health evaluation.

Initiation of CytoSorbIn most patients, treatment was commenced between 24-48 h after ICU admission (Figure 3). Only 3 patients among survivors and 1 in non-survivors received therapy within < 24 h, and in 16 cases treatment was started > 48 h after ICU.

Figure 3

Time of initiation of CytoSorb® therapy in survivors and non-survivors.

Overall, 50% (n = 8) of patients survived after 72 h of therapy. In the survivor group, the average number of days spent in ICU was 4.44 ± 1.66 d; while in the non-survivor group, it was 8.5 ± 15.9 d.

Evaluation of safety parameters: We could not observe any CytoSorb® related side effects or adverse events. There was no significant change in platelet or albumin levels (Table 3). Only 1 single patient showed clot formation in the device when used without heparin due to the clinical condition of the patient, which led to the stoppage of the therapy when used for the second time. One patient was diagnosed with ventricular tachycardia and needed injection of amiodarone.

DISCUSSION

Various adjuvant therapies are included in current treatment modalities for controlling cytokine storm; immunoglobulin therapy, endotoxin-binding polymyxin B hemoperfusion, dialysis and plasma filtration, etc. The mortality rate still remains high with these techniques[24-26]. Direct hemoperfusion using a polymyxin B endotoxin-adsorbing column was studied in clinical trials (ABDOMIX Study). The study could not confirm its clinical efficacy due to the nephrotoxic effects of the technique and associated high risks of cartridge clotting resulting in acute blood loss in patients admitted in ICU[27]. Similarly, anti-IL-1RA, anti-IL-1β, anti-tumor necrosis factor-α and anti-lipopolysaccharide showed disappointing results in both preclinical and clinical trials, despite their ability to reduce significantly serum cytokine concentrations[28,29]. A recent Cochrane review reported low-quality evidence for high-volume hemofiltration in the treatment of critically ill patients with sepsis and suggested that more multicenter randomized controlled trials are required before these therapies can be recommended for routine use[12].

Extracorporeal cytokine adsorption is a recent adjuvant alternative introduced into clinical practice less than a decade ago. Its aim was to reduce cytokine storm by the bulk removal of mediators of inflammation. Later, this treatment was reported as safe and well-tolerated in more than 300 human treatments in very sick patients with the worst forms of sepsis and lung injury, and to date, the treatment has emerged as the safest in nearly 1500 human treatments overall[30]. Though published data suggest that using CytoSorb® in conjunction with standard care including mechanical ventilation and dialysis may decrease the level of pro-inflammatory cytokines and improve hemodynamics in sepsis and septic shock, high-quality data from clinical trials are not available yet[16].

The present study evaluated some aspects of the clinical outcomes with CytoSorb® device treatment along with current standard of care in management of sepsis and septic shock. We observed improved clinical outcomes of patients with septic shock in terms of reduced mortality as compared to predicted, improved hemodynamics as indicated by MAP, and reduced use of vasopressors and their doses.

We studied patients requiring increasing vasopressor dose to maintain MAP > 65 mmHg. In our study, MAP increased significantly during CytoSorb® therapy in both survivors and non-survivors. This improvement in MAP was accompanied by a non-significant reduction in vasopressor dose as also indicated by the increase in the MAP/NE ratio. These results are in accord with our previous study conducted in 10 ICU patients where an overall reduction in all the vasopressor drugs after CytoSorb® therapy was reported[31]. Of the nine patients who were given vasopressin, five were weaned off V, two had a reduced dose and two were on the same dose as before.

Our results were consistent with the results reported by a prospective single center study with 20 patients; wherein the CytoSorb® treatment included NE dose that was significantly reduced after 6 h (−0.4 µg/kg/min; P = 0.03) and 12 h (−0.6 µg/kg/min; P = 0.001). Shock reversal was achieved in 13 (65%) patients; 28 d survival was 45%. The study reported shock reversal in two-thirds of these patients after using CytoSorb® adsorption therapy[10]. The findings of our study are supported by some more recent case reports demonstrating that CytoSorb® might be an effective adjuvant therapy, decreasing vasopressor requirements and stabilizing hemodynamics of septic shock patients[15,31-35].

Cytokines play an important role in the pathophysiology of sepsis and other clinical conditions with systemic inflammation. An elevated circulating levels of pro-inflammatory cytokines causes dysregulation in immune response and results in multi organ failure causing prolonged ICU stay and high mortality in ICU patients[36,37]. Specifically, elevated serum IL-1 and IL-6 appear to correlate with sepsis severity and end-organ damage[38]. We performed a cytokine assay, and our results showed improved levels of IL-6 in survivor group.

In addition to all above parameters, our results showed significant reduction in laboratory parameters like total lung capacity count improved (P < 0.00001) and overall improvement in HR (P = 0.0065), Glasgow coma score (P < 0.0001) and other biomarkers like serum creatinine (P = 0.0190) and lactate (P = 0.0120). An insignificant improvement was seen in other parameters also (i.e. respiratory parameters, liver and kidney profile). There was significant reduction in the SOFA scores (P = 0.0003) in the survivor group. The current findings are well consistent with other published studies[33,39,40].

We also investigated the time of initiation of CytoSorb® (in less than 24 h or 48 h of admission in ICU). Although there was a tendency that survivors received therapy earlier compared to non-survivors, the numbers are very small to make firm conclusions regarding timing and outcome. Nevertheless, the tendency of this pattern provide some further support to those studies, which also reported that starting therapy within 24 h after the onset of septic shock is the most beneficial[16,24].

PM was 54% in survivor group and 60% in non-survivor group using acute APACHE II calculator[23]. However, the AM was 42%. Our findings are similar to those of Kogelmann et al[15] who used CytoSorb® as an adjunctive therapy in 26 critically ill patients with septic shock and in need of renal replacement therapy. They reported that AM was lower in the overall patient population than PM. The actual 28 d, ICU and hospital mortality was 61.54%, 73.08% and 80.77%, respectively. However, mortality as predicted by APACHE II score in the overall patient population was 89.9%. Another previously published study reported that hemoadsorption with CytoSorb® results in a decreased observed vs expected 28 d mortality in patients with septic shock, and the mean PM (based on SOFA) was 75% (95%CI: 71%-79%) while AM was found to be 48% (mean difference-27%, 95%CI: 38%-15%, P < 0.001)[11].

Regarding safety, our results provide further data that the therapy is safe, as we could not find any device related AE or laboratory deterioration. In fact, platelet count remained unchanged or rather slightly increased, rather than decreased. This is contrast with some other reports, where thrombocytopenia had been observed[41].

This study has certain limitations. The sample size is relatively small, several circumstances were not standardized and there was no control group. Detailed hemodynamic evaluation and conventionally used inflammatory markers, such as C-reactive protein or procalcitonin, were not measured. However, a very recent retrospective, propensity score matched study reported very positive results on around 100 patients without measuring inflammatory markers[11].

CONCLUSION

Overall, the current study showed improvement in hemodynamic stability and organ function and reduction in IL-6 levels. Our results provide further support to the notion that outcomes are better if cytokine adsorption (CytoSorb®) is initiated early after the onset of septic shock. We can also conclude that we could not find any treatment related AE. Further, studies should be performed to help us to identify the appropriate patient population and timing of therapy and also to test the positive results of retrospective and observational studies, just like the current results, in the setting of randomized clinical trials.

ARTICLE HIGHLIGHTS

Research background

Sepsis is one of the oldest and most elusive syndromes in medicine, and yet it remains the most significant unmet medical need. In India, more than one million estimated new cases of sepsis are treated in intensive care units (ICUs) each year. CytoSorb® is an International Science Organization 10993 biocompatible device that is approved in the United States under International Science Organization 13485 certification. It is also approved as an extracorporeal cytokine adsorber in the European Union and marketed in 29 countries. In this study, clinical outcomes of patients with septic shock were assessed in terms of reduced mortality as compared to predicted, improved hemodynamics as indicated by mean arterial pressure (MAP) and reduced use of vasopressors and their doses.

Research motivation

Sepsis and septic shock is the leading cause of death among hospitalized patients. CytoSorb® therapy showed promising results in hyperinflammatory condition of critically ill septic patients. This study was conducted to evaluate clinical outcomes in these patients. This study will help clinicians to evaluate the use of CytoSorb® therapy for the patients considering clinical outcomes like MAP and use of vasopressors drugs.

Research objectives

The objective of the study was to evaluate CytoSorb® use as an adjunctive therapy along with the standard of care. The study showed improvement in hemodynamic stability and organ function and reduction in interleukin-6 levels.

Research methods

This was a prospective, real time, investigator initiated, observational multicenter study conducted in the patients admitted to the ICU with sepsis and septic shock. The improvement of MAP and reduction of vasopressor needs were evaluated as primary outcome. The change in laboratory parameters, sepsis scores [acute physiology and chronic health evaluation (APACHE II) and sequential organ failure assessment (SOFA)] and vital parameters were considered as secondary outcome. The outcomes were also evaluated in the survivor and non-survivor group. Descriptive statistics were used; a P value < 0.05 was considered to be statistically significant.

Research results

A total of 45 patients aged ≥ 18 and ≤ 80 years were included; a majority were men (n = 31; 69.0%) with mean age; 47.16 ± 14.11 years. Post CytoSorb® therapy, 26 patients survived and 3 patients were lost to follow-up. In the survivor group, the percentage dose reduction in vasopressor was NE (51.4%), E (69.4%) and V (13.9%). A reduction in interleukin-6 levels (52.3%) was observed in the survivor group. Platelet count improved to 30.1% (P = 0.2938), total lung capacity count significantly reduced by 33% (P < 0.0001). Serum creatinine and serum lactate were reduced by 33.3% (P = 0.0190) and 39.4% (P = 0.0120), respectively. The mean APACHE II score was 25.46 ± 2.91, and SOFA scores was 12.90 ± 4.02 before initiation of CytoSorb® therapy and reduced significantly post therapy (APACHE II 20.1 ± 2.47; P < 0.0001 and SOFA 9.04 ± 3.00; P = 0.0003) in the survivor group. The predicted mortality in our patient population before CytoSorb® therapy was 56.5%, and it reduced to 48.8% (actual mortality) after CytoSorb® therapy. We reported 75% survival rate in patients given treatment in < 24 h of ICU admission and 68% survival rates in patients given treatment within 24-48 h of ICU admission. In the survivor group, the average number of days spent by patients in ICU was 4.44 ± 1.66 d; while in the non-survivor group, the average number of days spent by patients in ICU was 8.5 ± 15.9 d. CytoSorb® therapy was safe and well tolerated with no adverse events reported.

Research conclusions

Early initiation of CytoSorb® therapy significantly improves clinical outcomes.

Research perspectives

In the future, adding a standard of control group and conducting a study that is powered to compare the time of initiation of CytoSorb® therapy will be necessary.

ACKNOWLEDGEMENTS

The authors acknowledge Mr. Pradeep Yanamala and Dr Vikram Shetty for end-to-end coordination.