Introduction
The mortality associated with delayed or inappropriate initial management of peritonitis cases is unacceptably high worldwide. Even in state-of-the-art surgical emergency centers, mortality rates of up to 40% have been reported among peritonitis cases with established sepsis and septic shock [1‐6].
In the Sub-Saharan African region where most surgical centers have glaring healthcare resource gaps (namely: human resources, theatre space, and supplies as well as ICU space), outcomes of peritonitis are suboptimal, and saving especially those cases with advanced physiologic derangement is an enormous task [7‐9]. In this setting, therefore, the importance of early prognostic risk stratification to prioritize those at most risk of death for a prompt aggressive therapeutic approach cannot be overemphasized [10].
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Several prognostic scoring systems both specific and nonspecific have been validated for use in peritonitis such as the Mannheim Peritonitis Index (MPI) [11], The World Society of Emergency Surgery Sepsis Severity Score (WSESSSS) [12], the Predisposition, Infection Response Organ dysfunction score for Intra-Abdominal sepsis (PIRO-IAS) [13] and the APACHE II score [14‐16]. These tools, however, are not strictly preoperative, and/or bedside. Moreover, some require laboratory parameters that are not easily obtainable in resource-limited surgical emergency centers. These tools, therefore, play a limited role in early preoperative risk stratification as well as therapeutic decision-making for individual peritonitis patients. They have instead found roles in research and surgical audits [2].
The Sepsis 3 task force in 2016 recommended the use of the quick Sequential (Sepsis-related) Organ Function Assessment (qSOFA) criteria for quick, bedside triage of septic patients at risk of mortality [17], and indeed many surgical emergency centers in Uganda have since adopted this tool for early prognostication of sepsis-related conditions including peritonitis but this practice has not been backed by robust local evidence. Several observational studies in other centers have reported the qSOFA criteria to be specific but lack adequate sensitivity for identifying septic patients at risk of poor outcomes [18‐21]. Tolonen and colleagues in a study to evaluate the predictive abilities of several prognostic scoring systems for peritonitis outcomes found the qSOFA criteria to have a high specificity (95%) but very low sensitivity (37%) for peritonitis mortality [22].
Recently (2019), The world society of emergency surgery (WSES) designed the Physiologic Indicators for Prognosis in Abdominal Sepsis-score (PIPAS severity score) as a bedside early prognostic scoring tool for peritonitis mortality [10]. The tool has 8 variables obtainable from history and physical examination. Each variable is scored 0 or 1 with a maximum score of 8, the higher the score the worse the outcome. Sartelli and colleagues found the PIPAS severity score to have a good predictive ability for mortality of peritonitis in a mainly European cohort [10]. The performance of this tool is yet to be evaluated in our setting.
The qSOFA criteria and the PIPAS severity score tools are both easy to assess, strictly bedside, and have solely preoperative parameters, hence, have the potential to be practically useful for early prognostic evaluation for peritonitis but the predictive ability of these tools for in-hospital mortality of peritonitis in our setting is yet to be assessed and compared. We set out to assess and compare the discriminative ability of the PIPAS severity score and the qSOFA criteria for in-hospital mortality of peritonitis in a resource-limited tertiary center in Uganda.
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Method
The study design and setting
We conducted a prospective cohort study on peritonitis cases admitted to the surgical unit of Mulago National Referral Hospital (MNRH) for 9 months from 1st October 2020 to 31st of June 2021. MNRH is an 1800-bed capacity hospital located in Kampala, the capital city of Uganda. It is one of the national referral hospitals and doubles as the teaching hospital for Makerere university’s college of health sciences. The hospital’s accident and emergency (A&E) unit is an initial entry point for all trauma and non-trauma surgical emergencies. Here clinically suspected peritonitis cases are triaged, and those needing emergency surgical intervention are stabilized and then operated on before transfer to various surgical wards or to the ICU where appropriate for post-operative care and/or a further planned intervention or re-intervention.
The study population and sampling
We consecutively recruited patients who were 13 years or older, with the clinical diagnosis of peritonitis and admitted to the surgical unit of MNRH. A case of peritonitis was defined as clinical symptoms and signs (abdominal tenderness, guarding, and/or rigidity with or without imaging signs) suggestive of peritonitis, and evidence of peritoneal contamination confirmed intraoperatively by the primary surgeon. We excluded trauma patients who had peritonitis and concurrent major injuries to other regions of the body because of the likelihood of the latter having a significant impact on mortality outcome. Suspected peritonitis cases that were managed conservatively were also excluded as this group did not fully satisfy our case definition. The sample size for the study was estimated based on the formula suggested by Hajian-Tilaki (2014) for studies comparing the accuracy of two prognostic/diagnostic tools on the same study subjects [23]. We used the AUC for the PIPAS severity score from the previous study [10]. Assuming a detection of an effect size d = (AUC1-AUC2) of 10% with 95% confidence level and 80% power gave us a sample size of 91, we adjusted upwards of 15% for non-response or loss to follow-up cases to give us a sample size of approximately 136 study participants.
Study procedures and data collection
All study participants underwent the hospital’s routine initial resuscitation protocol for peritonitis which included: The correction of fluid and electrolyte deficits using intravenous fluids, nasogastric tube suctioning, urethral catheterization, and administration of broad-spectrum antibiotic therapy within 1 h of admission.
The assessment for the PIPAS severity score [10] and the qSOFA score [17] variables for each study participant was done after the initial resuscitation (within 1 h before anesthesia induction). These variables were: Age (in completed years), pre-existing medical conditions (i.e., history of Severe chronic kidney disease, severe cardiovascular disease, and malignancy), respiratory rate (breaths/minute), blood pressure (mmHg), peripheral blood oxygen saturation level (SpO2) in room air (percentages), and level of consciousness using both the AVPU (Alert/Verbal/Pain/Unresponsive) responsiveness scale and Glasgow Coma Scale (GCS). In addition, the sex of the study participant was also recorded.
Each case was followed up intraoperatively and then daily thereafter until their discharge from the hospital, or up to 30 days if in-hospital admission was longer than 30 days. In the follow-up evaluation, the data elements recorded for each study participant were: The time interval from admission to definitive intervention (laparotomy), the Source of peritoneal contamination (anatomic site), the need for reoperation (re-laparotomy), and the outcome at discharge (survivor or non-survivor). Those with in-hospital admission longer than 30 days were categorized as survivors.
Data management and analysis
All study data were entered in Epidata version 4.6 software (Epidata Association, Odense, Denmark), cleaned, and then exported to STATA version 16 for analysis.
Descriptive statistics were used to characterize our study population; continuous normally distributed variables were summarized into mean and standard deviation and in median and interquartile range if non-normally distributed, while categorical data were summarized into absolute frequencies, proportions, and percentages.
We used chi-square statistics or t-test to compare baseline characteristics among survivors and non-survivors of peritonitis cases. Binary logistic regression models PIPAS and qSOFA scores were created for predicting in-hospital mortality of peritonitis. Each model’s suitability was assessed using the Hosmer-Lemeshow goodness of fit test.
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The discriminative ability of the two tools (i.e., the PIPAS severity score and the qSOFA score tools) for in-hospital mortality of peritonitis were assessed using a non-parametric estimate of the Area Under the receiver operating characteristic Curves (AUC) with bootstrap resampling inference. The AUC of the tools was then compared using Delong’s method [24]. The optimum cut-off score (for each tool) for predicting in-hospital mortality of peritonitis was determined using Youden’s index. All statistical analyses were 2-sided (p < 0.05), with 95% confidence intervals using STATA version 16 (StataCorp, College Station, Texas, USA).
Results
Baseline characteristics of the study population
A total of 139 peritonitis patients were assessed, and 136 cases met the inclusion criteria for the study. The 3 cases excluded were (two clinically suspected peritonitis cases that were managed conservatively and one multiply injured patient with concurrent peritonitis) (Fig. 1).
Fig. 1
Flow-chart showing recruitment of study participants into the study
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The 136 cases included in the study had a mean age of 34.4 years (SD: 14.5), The male-to-female ratio was 3:1. Open laparotomy was the source control procedure for all the 136 cases; 105 (77.2%) cases had laparotomy within 24 h of admission while the rest, 31 (22.8%) were operated on after 24 h of admission. Generalized peritoneal contamination occurred in 119 (87.5%) cases while 17 (12.5%) cases had localized peritoneal contamination. The commonest source of peritoneal contamination in this cohort was gastroduodenal perforation; (42.5% of cases) followed by appendiceal (17.6%) and small bowel perforations (16.2%).
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The overall in-hospital mortality in this cohort of peritonitis patients was 12.5% (17 cases). Fourteen cases (10.3%) required an un-planned re-operation due to persistent intra-abdominal sepsis. Table 1 summarizes the baseline characteristics of study participants.
Table 1
Baseline and clinical characteristics of study participants
Parameter
|
Total: n = 136 (100%) | Mortality |
p-value*
| |
|---|---|---|---|---|
No: n = 119 (87.5%) |
Yes: n = 17 (12.5%) | |||
Mean age: years (95% CI))
| 34.4 (31.9–26.9) | 32.9 (30.5–35.3) | 45.2 (35.6–54.7) | 0.002 |
Sex
| 0.335 | |||
Female | 35 (25.7) | 29 (82.9) | 6 (17.1) | |
Male | 101 (74.3) | 90 (89.1) | 11 (10.9) | |
Comorbidities
| ||||
Cardiovascular disease | 0.106 | |||
No | 134 (98.5) | 118 (88.1) | 16 (11.9) | |
Yes | 2 (1.5) | 1 (50.0) | 1 (50.0) | |
Chronic kidney disease | 0.106 | |||
No | 134 (98.5) | 118 (88.1) | 16 (11.9) | |
Yes | 2 (1.5) | 1 (50.0) | 1 (50.0) | |
Malignancy | < 0.0001 | |||
No | 130 (95.6) | 117 (90.0) | 13 (10.0) | |
Yes | 6 (4.4) | 2 (33.3) | 4 (66.7) | |
Preoperative clinical parameters
| ||||
sBP < 100mmHg | < 0.0001 | |||
No | 129 (94.9) | 119 (92.2) | 10 (7.8) | |
Yes | 7 (5.1) | 0 (0) | 7 (100) | |
RR > = 22 breaths/minute | 0.336 | |||
No | 28 (20.6) | 26 (92.9) | 2 (7.1) | |
Yes | 108 (79.4) | 93 (86.1) | 15 (13.9) | |
SpO2 < 90% | < 0.0001 | |||
No | 122 (89.7) | 115 (94.3) | 7 (5.7) | |
Yes | 14 (10.3) | 4 (28.6) | 10 (71.4) | |
AVPU scale not alert | < 0.0001 | |||
No | 127 (93.4) | 118 (92.9) | 9 (7.1) | |
Yes | 9 (6.6) | 1 (11.1) | 8 (88.9) | |
Mean hemoglobin level (g/dL) | 13.7 (13.2–14.2) | 14.0 (13.5–14.4) | 11.8 (10.6–13.1) | 0.002 |
White blood cell count (×109/L) | 0.094 | |||
< 4 | 11 (8.1) | 8 (72.7) | 3 (27.3) | |
4–12 | 78 (57.3) | 72 (92.3) | 6 (7.7) | |
> 12 | 47 (34.6) | 39 (83.0) | 8(17.0) | |
Mean platelet count (×103/uL) | 305.9 (283.4–328.4) | 313.6 (290.3–337.0) | 251.9 (174.5–329.4) | 0.073 |
Source of peritonitis
| 0.005 | |||
Gastroduodenal | 62 (45.6) | 57 (91.9) | 5 (8.1) | |
Small bowel | 22 (16.2) | 18 (81.8) | 4 (18.2) | |
Appendiceal | 24 (17.6) | 24 (100) | 0 (0) | |
Colonic | 12 (8.8) | 8 (66.7) | 4 (33.3) | |
Hepatobiliary | 1 (0.7) | 0 (0) | 1 (100) | |
Genitourinary | 2 (1.5) | 2 (100) | 0 (0) | |
Othersb | 13 (9.6) | 10 (76.9) | 3 (23.1) | |
Extend of peritonitis
| 0.096 | |||
Localised | 17 (12.5) | 17 (100) | 0 (0) | |
Generalised | 119 (87.5) | 102 (85.7) | 17 (14.3) | |
Reoperation
| 0.055 | |||
Yes | 14 (10.3) | 10 (71.4) | 4 (28.6) | |
No | 122 (89.7) | 109 (89.3) | 13 (10.7) | |
Prediction of peritonitis in-hospital mortality using the PIPAS severity score and the qSOFA score tools
The mean PIPAS severity score and qSOFA score for our peritonitis cohort were 1.1 (SD: 0.9) and 0.9 (SD: 0.6) respectively. The mean PIPAS severity score for males versus females were 1.1 (SD: 0.8) and 1.2 (SD: 1.1) respectively while the corresponding male versus female mean qSOFA scores were 0.9 (SD: 0.6) and 0.9 (SD: 0.7) respectively.
Peritonitis survivors had a mean PIPAS severity score of 0.9 (SD: 05) compared to a mean PIPAS severity score of 2.8 (SD: 1.2) for non-survivors. Similarly, the mean qSOFA score for peritonitis survivors was 0.8 (SD: 0.4) versus 1.8 (SD: 1.0) for non-survivors.
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Logistic regression models for peritonitis mortality using only variables of each tool were both highly statistically significant with good fits (qSOFA: Hosmer-Lemeshow chi2 1.21, p = 0.997 and PIPAS: Hosmer-Lemeshow chi2 = 1.41, p = 0.495).
Table 2 shows the ability of the qSOFA and the PIPAS severity score tools to discriminate peritonitis survivors from non-survivors while Fig. 2 shows the comparative ROC curves. Overall, the PIPAS severity score tool had a significantly better discriminative ability for peritonitis in-hospital mortality than the qSOFA score tool (AUC = 0.893 CI 0.802–0.984) and AUC = 0.770, 95% CI (0.620–0.920) respectively, p = 0.047).
Table 2
Discriminative ability of the PIPAS severity score tool and the qSOFA for in-hospital mortality of peritonitis
Classifier (tool) | AUC | Bias | Bootstrap standard error | 95% confidence interval |
|---|---|---|---|---|
PIPAS severity score | 0.893 | < 0.0001 | 0.047 | 0.801–0.986 (N) 0.794–0.976 (P) 0.787–0.974 (BC) |
qSOFA score | 0.7701 | 0.00023 | 0.077 | 0.620–0.920 (N) 0.609–0.914 (P) 0.603–0.906 (BC) |
Fig. 2
Comparative ROC curves for the PIPAS severity score and the qSOFA score tool for predicting in-hospital mortality of peritonitis
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The best PIPAS severity score cut-off value for predicting in-hospital mortality of peritonitis was a score of 2 or more with a sensitivity of 76.5% and a Specificity of 93.3%. Similarly, the best qSOFA score cut-off value for predicting in-hospital mortality of peritonitis was a score of 2 or more with a sensitivity and specificity of 58.8% and 98.3% respectively (Table 3).
Table 3
Sensitivity and specificity values for various PIPAS severity score cut-off values for predicting in-hospital mortality of peritonitis
PIPAS severity score tool | qSOFA score tool | |||||
|---|---|---|---|---|---|---|
Cut-off scores | Sensitivity (%) | Specificity (%) | Youden’s index | Sensitivity (%) | Specificity (%) | Youden’s index |
≥ 0 score | 100 | 0.00 | 0.19 | 100 | 0.00 | - |
≥ 1 score | 100 | 19.3 | 0.19 | 88.2 | 19.3 | 0.08 |
≥ 2 scores* | 76.5 | 93.3 | 0.70 | 58.8 | 98.3 | 0.57 |
≥ 3 score | 70.6 | 99.2 | 0.70 | 29.4 | 100 | 0.29 |
≥ 4 score | 35.3 | 100 | 0.35 | - | - | - |
Discussion
This study compared the predictive ability of two bedside sepsis-related tools (the PIPAS severity score and the qSOFA criteria) for peritonitis in-hospital mortality in a real-time clinical setting of a low-resourced surgical emergency center. We would like to point out that, the successful application of these two tools in this study proves that both tools can be practically feasible even in a low resource setting.
The in-hospital mortality rate (12.5%) in this cohort of peritonitis patients is in the 10–20% range of peritonitis mortality generally reported in the sub-Saharan African region [25‐29] but still higher than those reported in the western world [5, 30]. The most likely explanation for this is the difference in the quality of the health care system that exists between these regions; the finding from the African surgical outcome study (ASOS) alluded to this difference [31].
We found the PIPAS severity score to have a significantly superior discriminative ability for in-hospital mortality of peritonitis than the qSOFA score tool. To the best of our knowledge, this is the first time these tools have been compared however, similar trends in the discriminative ability of these tools for peritonitis mortality have been reported in a couple of non-comparative studies. Sartelli and colleagues found a good discriminative ability of the PIPAS severity score tool for mortality among a large cohort of peritonitis patients (AUC = 0.85) [10]. One other study that evaluated the predictive ability of various scoring systems for mortality of peritonitis concluded that qSOFA has a fair discriminative ability (AUC = 0.723) [22].
Furthermore, we found the PIPAS severity score tool to have a higher sensitivity than the qSOFA criteria although the latter tool is more specific. Several recent observational studies have also indicated that qSOFA criteria have low sensitivity but high specificity for identifying septic patients who are at high risk of mortality[18‐22, 25]. The implication of this in practice is that the use of the qSOFA criteria as the sole initial prognostic tool for potentially septic patients would miss out on a significant number of otherwise high-risk patients for sepsis-related mortality. This is critical particularly in the management of peritonitis as the mortality associated with delayed and/or inappropriate management of these cases is extremely high [2, 10, 12].
The superiority of the PIPAS severity score tool over the qSOFA criteria both in terms of discriminative ability and sensitivity for predicting peritonitis mortality favors the former tool as the preferred initial prognostic screening tool for peritonitis.
This study had some limitations. First, it was a single tertiary center observation study. The population evaluated may be a lot sicker and biased towards poor outcomes owing to delays resulting from several levels of referral. The finding therefore may or may not be generalizable to those in lower-level surgical emergency centers. Secondly, we used qSOFA and PIPAS Severity score values that were assessed one time preoperatively to predict mortality outcomes in the study. A serial assessment including during the postoperative period would give added information including deaths attributable to postoperative complications (Additional file 1).
Conclusions
The in-hospital mortality in this cohort of peritonitis cases was high. The PIPAS severity score tool has a superior predictive ability for in-hospital mortality of peritonitis when compared to the qSOFA score tool. The PIPAS score cut-off value of 2 or more scores has a higher sensitivity than the qSOFA criteria however, the latter tool is more specific.
We recommend the use of the PIPAS severity score tool either alone or in combination with the qSOFA criteria as the initial prognostic tool for peritonitis in the emergency department. qSOFA should not be used as a lone initial prognostic tool for peritonitis due to its low sensitivity.
Acknowledgements
We acknowledge all healthcare providers working in their various capacities at the surgical unit of Mulago national referral hospital who were actively involved in the routine care of all patients (including patients who participated in this study).
Declarations
Ethics approval and consent to participate
The School of Medicine Research and Ethics committee of Makerere University (SoM-REC) and the Uganda National Council of Science and Technology (UNCST) approved the study. Written informed consent/assent was obtained from all patients and/or their caretakers before enrolment into the study. During the data collection process, COVID19 prevention guidelines for Uganda were strictly followed to prevent cross-infection among study patients, study assistants, and the caretakers of the study patients.
Consent for publication
Not applicable.
Competing interests
The authors declare they have no competing interests.
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