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Portuguese Journal of Nephrology & Hypertension

versão impressa ISSN 0872-0169

Port J Nephrol Hypert vol.34 no.1 Lisboa mar. 2020

https://doi.org/10.32932/pjnh.2020.04.057 

ORIGINAL ARTICLE

 

Predictors of peritonitis in peritoneal dialysis: experience during 3 decades

 

David Fiel, Joana Santos, Rita Vicente, Iolanda Santos, Beatriz Malvar, Rui Silva, Manuel Amoedo, Carlos Pires

Division of Nephrology, Hospital do Espírito Santo, Évora, Portugal

 

Correspondence to:

 

ABSTRACT

Introduction: Peritonitis is a common complication in peritoneal dialysis patients and a major cause for dropout. Systematic report and frequent trend analysis are thought to be major drivers for improvement in this area. The authors analysed peritonitis outcomes dating back over 20 years in a peritoneal dialysis unit of a central hospital. Methods: Retrospective study from 1993 to 2018: assessment of demographic, clinical and microbiological profiles of patients with peritonitis. We performed univariate and multivariate analysis (multiple logistic regression) to predict peritonitis risk factors, and survival analysis (Cox proportional hazards model) to determine the impact on outcomes (mortality and technique survival). Results: We included 225 patients, average age of 48.3±14.7 years, average time of follow‑up of 38±25 months, with a total of 221 episodes of peritonitis (0.31 peritonitis/patient.year), 76% resulting in cure. Most frequent agents were Staphylococci: Coagulase‑Negative (23%) and Staphylococcus aureus (19%, of which 24% were methicillin‑resistant). Gram‑negative infections led to higher rate of catheter removal, transfer to hemodialysis or death (49% of cases vs. 17% in Gram‑positive). Primary end‑point was death or transfer to hemodialysis, with a median time of 94 (min 4, max 94) and 66 (min 3, max 105) months, respectively. The occurrence of at least one peritonitis was the major variable that influenced transfer to hemodialysis (OR 3.94 [2.12 – 7.58], p < 0.001*], whereas an event in the first year also negatively affected the time to dialysis technique switch (median time 38.7 [26.2 – 58.4] vs. 67.8 [59.5 – 80.3] months, log‑rank = 0.02*), but without impact on mortality. Only the peritoneal dialysis modality (OR: automated peritoneal dialysis vs. continuous ambulatory peritoneal dialysis 0.38 [0.19‑0.74]) was predictive of peritonitis in multivariate analysis. Conclusions: In this single‑center long‑term analysis, where the rate of peritonitis was within recommended values, automated peritoneal dialysis seemed to have a protective impact. The number of peritonitis and peritonitis occurrence during the first year worsened technique survival, emphasizing early peritonitis prevention.

Keywords: Automated Peritoneal Dialysis; Continuous Ambulatory Peritoneal Dialysis; Peritonitis

 

INTRODUCTION

Peritoneal dialysis (PD) is one of the available treatments for end‑stage renal disease (ESRD) with some advantages when compared to its counterpart hemodialysis (HD), namely, more autonomous and self‑governing treatment, absence of a vascular access and its cannulation, no need for anticoagulation and even less mortality in the first years of treatment, as shown by Fenton et al.1 However, median time to technique dropout continues to be lower than expected. Long‑term exposition to conventional peritoneal dialysis solutions have been associated with an impairment in host cell defense, reduction in peritoneal mesothelial cell viability, and progressive peritoneal membrane injury and function loss.2 Furthermore, peritonitis is a common complication in patients undergoing PD and still a major cause of patient mortality and technique dropout.36

According to the ISPD Peritonitis Recommendations 2016, peritonitis is the direct or major contributing cause of death in around 16% of PD patients and may cause structural and functional alterations of the peritoneal membrane, eventually leading to membrane failure.7 Reported rates of PD peritonitis range widely from 0.06 to 1.66 episodes per patient‑year across different centers and countries.2

We are presenting the results of a retrospective study, designed to disclose peritonitis epidemiology, risk factors and outcomes dating back over 20 years in a PD unit of a central hospital in Portugal.

METHODS

General design

Following a retrospective, observational design, we assessed demographic, clinical and microbiological profiles of patients with peritonitis undergoing chronic PD in our center during the period between 1993 and 2018. The authors defined 2 main study variables: total number of peritonitis and peritonitis in the first year of PD. The main outcome variable was time until death or transfer to HD.

Study population

This study included all prevalent patients (under treatment for at least 3 months), older than 18 years who started PD therapy in our center from the 1st January 1993 until the 31st December 2016 and follow‑up until 31st December 2018.

Study variables

Demographic, clinical and microbiological profiles of patients with peritonitis were assessed by recovering data from the hospital's patient clinical database and from our PD unit patient local registry. The main study variables were I. the total number of peritonitis (0, 1, 2+) and II. any episode of peritonitis in the first year of PD. The main outcome variable was time until death or transfer to HD (primary).

We defined peritonitis according to standard ISPD rules.7 We recorded the main clinical and demographic variables with a potential association with clinical outcomes, including the risk of peritoneal infection (Table I).

 

 

Strategy of analysis and statistics

Primary univariate comparisons were produced using multiple logistic regression to predict peritonitis risk factors. Multivariate survival analysis was produced by the Cox proportional hazards model, controlling for other demographic, clinical or laboratory variables with an impact on the incidence of the outcome variables (mortality and technique survival). The R project® software was used for data management, with a significance level of 5%.

RESULTS

Population overview

We included 225 patients for analysis. The characteristics of the study population are represented in Table I. The average age was 48.3±14.7 years, with a predominance of the male gender (n=133, 59%). Most patients (71%) were undergoing continuous ambulatory peritoneal dialysis (CAPD) and 29% were being treated with automated peritoneal dialysis (APD) at the time of the peritonitis event. Average time of follow‑up was 38±25 months. Regarding the episodes of peritonitis, 221 events were registered in a total of 124 patients (0.31 peritonitis/patient.year), 76% resulting in cure.

Etiological peritonitis agents and outcomes

The results of the peritonitis etiological agents are depicted in Table II. The most frequent isolated agents in the peritoneal dwell were Staphylococci: Coagulase‑Negative Staphylococci in 23% of the cases and Staphylococcus aureus in 19% (of which 24% were methicillin‑resistant Staphylococcus aureus – MRSA). Pseudomonas and fungi are the most aggressive agents and their infection led to either removal of the peritoneal catheter, transfer to HD or death in 100% of cases.

Gram‑negative bacterial infections other than Pseudomonas, had a similar rate of cure as Gram‑positive (79 vs. 83%, p = 0.58, ns, qui2).

Differential analysis of epidemiological agents per decade of the studied period are represented in Graphic 1, where we can observe a trend towards an increase in relative frequency of Gram‑negative‑related peritonitis.

 

 

Predictors of peritonitis

Predictors of Peritonitis

Univariate analysis of possible predictors of peritonitis is presented in Table III. Patient characteristics such as the higher age (p = 0.03), etiology of chronic kidney disease (CKD) (p =0.012) and PD modality (p < 0.001) seem to be statistically significant as predictors of peritonitis.

However, when considering those variables in a multivariate model, only PD modality (OR: APD vs. CAPD 0.38 [0.19 – 0.74]) was predictor of peritonitis (Graphic 2).

 

 

Outcomes

Primary end‑points were occurrence of death or transfer to hemodialysis which occurred in 53 (24%) and 82 (36%) patients respectively. In the logistic regression model the occurrence of at least one peritonitis did not influence the probability of death (OR 0.55 [0.25 – 1.18], p = 0.13, ns). On the other hand, the presence of diabetes (OR 5.13 [2.41 – 11.3], p < 0.001) and aging (OR 1.05 per year [1.03 – 1.08], p < 0.001) have higher probability of outcome, whereas the era of PD initiation (2005‑2016 vs. 1993‑2004, OR: 0.20 [0.09 – 0.42], p < 0.001) shows the opposite tendency. – Graphic 3. On the other hand, peritonitis was the major variable that statistically influenced transfer to HD (OR 3.94 [2.12 – 7.58], p < 0.001*]– Graphic 4.

 

 

 

When we consider the time to event analysis, the median time to death was 93.9 months [IC95% 93 – 105] and transfer to HD was 66 months [IC95% 58 – 78]. Univariate Kaplan‑Meier estimates reveal that the occurrence of at least one peritonitis in the first year of treatment does not influence the time to death (log‑rank = 0.1, ns – Graphic 5a.) but indeed affects negatively the time to transfer to HD (median time 38.7 [26.2 – 58.4] vs. 67.8 [59.5 – 80.3] months, log‑rank= 0.02* – Graphic 5b).

The multivariate Cox proportional survival model reinforce the results obtained in the logistic regression, as diabetes (HR: 2.6 [1.5 – 4.5], p < 0.001), age ((HR: 1.03 per year [1.02 – 1.05], p < 0.001) and time of PD initiation (2005 – 16 vs. 1993 – 2004 HR: 0.38 [0.21 – 0.67], p < 0.001), influence the time to death. As for time to HD transfer, the influence of peritonitis in the first year maintains an important negative trend, although losing its statistical significance (HR: 1.60 [0.92 – 2.75], p = 0.09, ns), whereas the male gender remains a significant predictor (HR: 1.93 [1.20 – 3.11], p = 0.007).

DISCUSSION

Peritonitis Rate

In our analysis, the global rate of peritonitis was well within recommended values: 0.31 peritonitis/patient.year. Despite there being a substantial variation in the peritonitis rates reported by different countries, the ISPD 2016 Recommendations set an international goal of a total peritonitis rate no more than 0.5 episodes per year at risk.7

Peritonitis Agents

In the literature, the most common described pathogens responsible for PD related peritonitis are aerobic bacteria, such as coagulase‑negative staphylococcal species (eg, Staphylococcus epidermidis) that commonly colonize human skin and hands, and Staphylococcus aureus.

Together they are responsible for 50% or more of infections in most series.7,8 Our findings corroborate the former, as indeed the most frequent agents found were Coagulase‑Negative Staphylococci (23%) and Staphylococcus aureus (20%, with 5% MRSA).

Antibiotics are essential in the treatment of infectious diseases; however, their widespread abuse in medical care and outside human medicine has resulted in the development of (multi)drug resistance worldwide.2 Antibiotic resistance in microorganisms in Portugal was addressed by a retrospective unicenter PD peritonitis related study (1985 – 2010; 588 episodes), which encountered a total methicillin resistance in S. epidermidis of 7% and 2% for S. aureus.9 In our unit we also observed a relative increasing emergence of more virulent pathogens per decade of study such as Pseudomonas (8%), MRSA (5%) and other Gram negative (8%). This increase in frequency of methicillin‑resistant agents led our nephrologists to switch the peritonitis empirical antibiotic protocol from Cefazolin/Ceftazidime to Vancomycine/Ceftazidime, following ISPD Peritonitis Recommendations 2016.7 Regarding peritonitis prophylaxis protocols, we have followed ISPD recommendations, such strategies as Staph. Aureus carrier screening and treatment before catheter implantation, oral empirical antibiotic administration before the procedure as well as adoption of external orifice care guidelines, amongst others. Gram‑negative bacterial infections led to the removal of the peritoneal atheter, transfer to HD or death in 49% of cases (vs. 17% in Gram‑positive).

Regarding fungal peritonitis, reports vary widely, ranging from 1% to 15% of peritonitis episodes, but they are almost always associated with significant morbidity and higher mortality rate (up to 50%).2,10,11

We only assessed 2 cases (1%) and therefore our unit's peritonitis protocol does not include empirical antifungal treatment, despite worse outcome – both led to PD catheter removal and technique dropout.

Culture‑negative peritonitis still account for up to 12% of all peritonitis episodes.12 These may be owing to recent antibiotic exposure, suboptimal sample collection or culture methods, or because of unusual organisms such as fungi. Although they are rare, a delay in the diagnosis and implementation of appropriate treatment can result in adverse patient outcomes, including death.2 We obtained a higher number of negative cultures (n=33, 15%) than the international recommendations, probably because of technical problems during sample collection and processing. Since we obtained a cure rate of 97% in these cases (Table II), a fungal undiagnosed etiology renders less likely. As depicted in Graphic 1, in the first decade of study we obtained negative cultures in 33% of the cases; however, in the following two decades, this value lowered significantly to 21% and then 7%. We believe that the improvement of microbiological screening method quality as well as the growing dedication of our pathology department staff throughout time, allowed a steadily decrease in these numbers.

PD Modality

In our study, APD had a protective impact for peritonitis.

Multiple risk factors for developing peritonitis have been identified, but there remains conflicting evidence on peritonitis risk between CAPD and APD in literature.13 There have been reports of lower14,15, similar1619, or higher20,21 peritonitis rates in patients treated with APD compared with CAPD, but the available evidence is predominantly based on observational studies, with only two small randomized controlled trials14,16 and a meta‑analysis of these trials22. In a large multicenter registry study with almost 7000 patients, Patrick G. Lan et al. demonstrated that PD modality was not associated with a patient's overall risk of developing peritonitis. However, they found that APD was associated with a lower risk of culture‑negative peritonitis, which was balanced by an increased risk of Gram‑negative peritonitis compared with CAPD.13 Most of these studies were conducted at different time periods (raising the possibility of vintage bias), involved small patient numbers and had low peritonitis event rates. They also had different center‑specific and patient‑specific factors (including medical comorbidities, prior RRT, and unit practices).13 This subject is also a matter of debate in the ISPD Peritonitis Recommendations 2016, where it is assumed that the published studies that compared APD and CAPD, so far, showed conflicting results. However, most of these studies were observational rather than randomized trials. At present, the choice of APD versus CAPD should not be based on the risk of peritonitis.7

CAPD and APD differ significantly in the frequency and method of making the connections and disconnections between the PD catheter and dialysate bags. This difference raises the question of whether one technique predisposes to or mitigates against the risk of the patient acquiring a peritoneal infection, due to contamination from repeated connections.23

The last two decades have witnessed a substantial change in PD practice. Understanding the different evolutions of the connection systems is critical when comparing peritonitis rates for PD patients during different periods. The connectology for CAPD has changed significantly over the years, from manually spiking bags with a separate connection and disconnecting with the dialysate bag and drain bag for each exchange to the twin bag systems that presently are standard.

The twin bag system is the only CAPD setup available today in most parts of the world and is the dominant reason for the reduction in risk for peritonitis in individuals undergoing PD.23 In our department, this method was implemented before the study period (1993); thus all patients were treated under such conditions, therefore not altering results.

Still regarding technique evolution, another important step was related to the introduction of more biocompatible solutions, which we started using in our unit gradually (between 2001 and 2004). However we didn't have this data recorded and this variable couldn't be accessed (as we also assume it to be a limitation of our study).

To mitigate this limitation, and other factors that possibly were not considered in this subject, we introduced a variable which tried to acknowledge technique evolution by splitting the time period in two halves (PD initiation period 1993 – 2004 vs. 2005 – 2016), being all patients in the former half already using these new biocompatible solutions.

Impact of peritonitis

In our research, the number of peritonitis did not correlate with an increased probability of death. However, the number of peritonitis did negatively impact technique survival, which was also worsened by peritonitis occurrence during the first treatment year, emphasizing the importance of early peritonitis prevention.

Regarding the matter of prevention, we consider that attention should be focused on the cumulative experience of the PD unit, improvement of PD technique and use of more functional equipment and more biocompatible solutions.

Study limitations

This study presents some significant limitations, including a single‑center retrospective design and a relatively small size of the sample, which may have limited the consistency of the results. For instance, of the 225 included patients, only 65 were on APD, which can introduce an interpretation bias of the results.

As mentioned before, the lack of data on the evolution of the PD technique itself, such as the precise moment of introduction of more biocompatible solutions, represents a limitation of our study.

Our multivariate model considered the most prominent confounding variables already known to influence the risk for peritonitis, but limited knowledge on the factors portending this complication add some uncertainty to the reliability of the analysis.

CONCLUSIONS

In sum, APD seems to have a protector impact for peritonitis, possibly due to the less risk of contamination of fewer connections, and the number of peritonitis but also peritonitis occurrence during the first treatment year worsened technique survival.

Our unit´s rate of peritonitis was found overall to be within internationally recommended values but we now emphasize to patients the importance of early (one‑year) peritonitis prevention.

 

References

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Correspondence to:

Hospital do Espírito Santo de Évora – Serviço de Nefrologia

Largo Senhor da Pobreza

7000‑811 Évora, Portugal

E‑mail: davidcarvalhofiel@gmail.com

 

Disclosure of potential conflicts of interest:none declared

 

Received for publication: Dec 11, 2019

Accepted in revised form: Feb 6, 2020

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