Abstract
Background
Overt eosinophilic peritonitis (EP) is a relatively uncommon complication of peritoneal dialysis (PD), although not rare. Here we reported a case of EP relieved after changing dialysate.
Case presentation
A 28-year old male patient developed cloudy PD effluents within the first month after PD started. Cytological study of PD effluents showed elevated white blood cells and polynuclear cells. Bacteria culture of PD effluents repeated for several times were all negative, and no pathogen was found by metagenomics next generation sequencing (mNGS). Antibiotic therapy for 28-day was ineffective. Based on these and increased eosinophils in peritoneal fluid, he was finally diagnosed as EP. PD dialysate was changed (consists of the same buffer agent and electrolytes, but is packed in bags that do not contain PVC), and the patient’s PD effluent became clear. Of note, EP did not relapse 5 months later when the patient started to use the former PD solution again.
Conclusion
Although PD effluent turbidity almost always represents infectious peritonitis, there are other differential diagnoses including EP. For patients with cloudy fluid accompanied by mild symptoms who do not response to antibiotic therapy, it is reasonable to consider the possibility of this disease. EP tends to heal spontaneously, however, antihistamines or glucocorticoids are required sometimes to avoid catheter obstruction. For patients with no obvious incentives, replacement of dialysate may be useful.
Similar content being viewed by others
Background
Eosinophilic peritonitis (EP) was first reported in 1967 [1], which is usually a non-infectious peritoneal dialysis (PD) related peritonitis. The incidence of EP varies in the literature because of different diagnostic criteria [2,3,4,5], but generally showed a tendency to decrease. However, with the increased utilization of PD, the total number of patients with EP may still elevate. EP is often misdiagnosed as infective peritonitis because the two diseases have similar clinical symptoms and often overlap, which leads to the overuse of antibiotics, sometimes even results in serious complications and poor prognosis. Here we reported a case of EP manifested as cloudy PD effluent and relieved after changing peritoneal dialysate.
Case presentation
A 28-year old male patient developed end-stage kidney disease due to chronic glomerulonephritis and a double-cuff straight Tenckhoff peritoneal dialysis (PD) catheter was inserted on February 1, 2021. The patient received daytime ambulatory peritoneal dialysis (DAPD) since then. His PD regime included 2,000 ml of 1.5% PD solution (Dianeal 1.5%, Baxter, International Inc.) with a total dialysis dose of 8 L per day. His daily PD ultrafiltration volume was about 400 ml and urine output about 1,500 ml/24 h.
From February 18, 2021, the patient observed turbid PD effluent without abdominal pain, fever or decline of PD ultrafiltration volume. Dialysate effluent was obtained for laboratory evaluation including cytological study and bacterial culture. The cytological study showed a white blood cell (WBC) count of 1419 × 106/L, with 56.7% polynuclear cells, while the effluent culture was negative. He was diagnosed as PD-related peritonitis and received empirical antibiotic treatment by intraperitoneal injection of teicoplanine combined with third-generation cephalosporin and oral fluconazole for 14 days. The PD effluent was still cloudy. Other than that, the patient stated no discomfort. The effluent culture was repeated 5 days after the antibiotic application, but still negative. On March 2, 2021, the patient developed fever, and a dialysate effluent cytological study was repeated, which showed a WBC count of 2665 × 10^6/L, with 73.0% polynuclear cells. A complete blood count (CBC) was also performed this time which showed a WBC count of 6.5 × 10^9/L, with 65.3% neutrophils and 15.0% eosinophils. The patient was hospitalized on March 4, 2021.
The patient had a history of renal hypertension for 2 years. Irbesartan combined with amlodipine has been used since PD started and his blood pressure was well controlled. The patient also had anemia of CKD and Chronic Kidney Disease–Mineral and Bone Disorder (CKD-MBD). Home medications also included roxadustat, ferrous succinate and calcitriol. He had no history of tuberculosis or close contact with tuberculosis patients. He did not smoke, had no history of alcohol use, allergy and no previous surgeries except PD catheter insertion.
Physical examination on admission showed a body temperature of 38.5℃, a blood pressure of 113/80 mmHg, and a heart rate of 82 bpm. There was no purpura or rash. Pulmonary and cardiac auscultation was normal. The abdominal examination revealed no tenderness, guarding or rebound pain on palpation. There was no edema in both legs.
Results of laboratory tests and imaging study after admission are as follows: Cytological study of dialysate effluent showed a WBC count of 796.0 × 10^6/L, with 68.3% polynuclear cells. CBC showed WBC count 6.4 × 10^9/L (with 65.5% neutrophils and 14.9% eosinophils ), hemoglobin 87 g/L, and platelet count 220 × 10^9/L. Biochemical analysis revealed normal alanine aminotransferase and aspartate aminotransferase. Serum albumin was 32.4 g/L, and serum creatinine was 741 umol/L. His blood procalcitonin (1.5ng/ml) and C-reactive protein (CRP) (88.3 mg/l) were both high. Serum IgE was within normal range (60 IU/ml). During hospitalization, bacterial culture, Gram staining and acid fast bacilli staining of peritoneal dialysis effluents were all negative. Blood culture, detection of tuberculosis infected T cells, and tuberculosis antibody were negative as well. The G test of blood invasive fungi was 4.4pg/ml, and the GM test of blood invasive fungi was 0.07, both within normal range. Abdominal X-ray and CT scan did not show intra-abdominal free gas (Fig. 1).
Since the patient had fever and elevated blood eosinophils, dexamethasone (5 mg) was prescribed for one time, meanwhile, antibiotic therapy was continued, including intraperitoneal injection of teicoplanine and aminoglycosides (amikacin). The patient’s temperature returned to normal and his dialysis effluent went clear with WBC count of 131 × 10^6/L on March 5, 2021. Unfortunately, he observed turbid dialysate effluent again 4 days later. Still he denied abdominal pain or other discomfort. PD effluent cytological study showed a WBC count of 1228 × 10^6/L, with 81.9% polynuclear cells. Amikacin was replaced by imipenem/cliastatin and teicoplanine as well as fluconazol continued (antibiotics used during peritonitis are summarized in Table 1). However, the cloudy PD effluents did not improve, and the cytological study of effluents still showed elevated WBC counts (Fig. 2). Meanwhile, his blood CRP and procalcitonin decreased to normal, bacteria culture of PD effluents repeated for several times were all negative, and no pathogen was found by metagenomics next generation sequencing (mNGS). Considering that the proportion of blood eosinophils increased significantly during hospitalization (Fig. 3), we asked the laboratory to report the eosinophilic proportion of PD effluent (usually only the counts and proportion of polynuclear cells were reported), which showed that the proportion of eosinophils was as high as 71.2%, and exfoliated cells in PD effluent demonstrated an elevated eosinophils (Fig. 4). The patient was diagnosed as PD related EP, and antibiotics and fluconazol were discontinued. PD dialysate was changed to Daorun PD fluid (Wuhu Daorun Pharmaceutical Co., Ltd), which consists of the same buffer agent and electrolytes as Baxter fluid (Table 2), but is packed in bags that do not contain PVC, to see whether EP was caused by material of PD bags. The patient’s PD effluent went clear and the WBC counts of PD effluents decreased gradually (Fig. 2). The eosinophils in blood and PD effluents decreased as well (Fig. 3).
Since the new PD dialysate was not covered by his medical insurance, the patient decided to use Baxter’s PD solution again on August 2, 2021. His PD effluents were clear and cytological study of dialysate effluent showed normal WBC counts and proportions of polymorphonuclear cells and eosinophils during follow-up (Figs. 2 and 3).
Discussion and conclusions
EP is defined as the presence of more than 100 eosinophils/mm3 of PD effluent or as an eosinophil count > 10% of the total nonerythrocyte count [6]. This entity tends to occur shortly after PD is started, although it can develop as late as 1 ~ 2 years or more after dialysis [3, 7]. Our patient developed EP within the first month of the initiation of PD, which is consistent with that reported in the literature.
The main clinical presentation of EP is cloudy peritoneal dialysis fluid that is unresponsive to antibiotics. Usually, as in this case, other symptoms of peritonitis including abdominal pain, tenderness and rebound tenderness are mild or even absent, and dialysate culture is negative, which is helpful in its distinction from bacterial peritonitis [6]. However, as microbial-induced peritonitis is the most common cause of PD effluent turbidity, clinicians may still make an incorrect diagnosis of infectious peritonitis, which leads to the overuse of antibiotics and may result in adverse events and extra costs. Therefore, it is of importance that clinicians be aware of the possibility of EP in patients with asymptomatic fluid turbidity or patients with cloudy PD effluent but mild clinical symptoms.
The exact pathophysiological mechanisms or causes of EP are still not fully understood. In addition to increased eosinophils in PD effluent, it has been shown that 32 ~ 57% of patients with EP have elevated peripheral blood eosinophils as well [7,8,9]. Chan et al. [2] reported a higher mean serum IgE concentration in patients who experienced peritoneal eosinophilia than in those without. Our patient also showed significantly elevated peripheral blood eosinophils, although his serum IgE level was normal. These together strongly support the suggestion that EP is an allergic reaction that is not localized to the surface of the peritoneum. Several mechanisms have been suggested to cause this allergic reaction, including presence of air in the peritoneal cavity [10, 11], effect of dialysis solutions or dialysate additives such as antibiotics [9, 12, 13] and streptokinase [14], and even effect of oral drugs [15]. However, none of these could well explain the situation in our patient. Solary et al. [16] reported a case of EP caused by plasticizers in PD bags, whose cloudy dialysate disappeared after substituting glass bottles for plastic containers. However, what substances could be involved was unknown. Chan et al. [17]. reported a case of severe EP relieved by changing from Dianeal PD fluid (packed in bags made of PVC) to Stay-Safe Balance solution (Fresenius) (a low glucose degradation product solution at neutral PH). However, it is unclear whether the resolution of EP was due to the properties of the Stay-Safe Balance PD fluid or whether it was due to the difference in their materials used for the plastic container bags, as all components of the packaging for Stay-Safe Balance solution are made of PVC-free Biofne. Our patient’s EP relieved after changing to PD fluid containing the same buffer agent and electrolytes but packed in bags that do not contain PVC. Meanwhile, the peritoneal and blood eosinophils dropped to normal. Since hemodialysis using PVC tubing has been linked with blood eosinophilia [18], it is possible that PVC used as plasticizers can be released from PD bags under certain conditions, and cause EP in certain cases. However, since the number of eosinophils in dialysate was calculated rather late in this patient, it cannot be completely excluded that EP was caused by other factors such as antibiotics given for peritonitis, and that at the beginning cloudy dialysate was due to mild culture-negative infectious peritonitis.
EP often remits spontaneously, however, in some cases it may last for months or even recurrent, and antihistamine drugs or glucocorticoids are required, in case that the cloudy PD effluent block the PD tube. Our patient’s cloudy PD effluent had a transient improvement after intravenous injection of dexamethasone, suggesting that steroids are effective. However, it is still controversial how long they should be used. Some suggest that glucocorticoids should be used continuously for more than 4 weeks to reduce disease recurrence [7]. Meanwhile, in some cases, EP relieved promptly after steroids prescription and there was no recurrence following quick drug withdrawal. Our patient only received one single dose of dexamethasone and suffered relapse of cloudy PD effluent, but achieved sustained relief after changing dialysate. Of note, EP did not relapse 5 months later when the patient started to use Baxter’s PD solution again, which reminds us that transient replacement of dialysate may be useful for EP patients without drugs, infection, air entering the abdominal cavity or other obvious incentives.
Although PD effluent turbidity almost always represents microbial-induced peritonitis, there are other differential diagnoses including EP [19], which often occurs in the early stage of PD and is usually a benign disorder but unresponsive to routine antimicrobial therapy. For patients with cloudy fluid accompanied by mild symptoms who do not response to antibiotic therapy, it is reasonable to consider the possibility of EP [20]. EP tends to heal spontaneously, however, antihistamines or glucocorticoids are required sometimes. For patients with no obvious incentives, replacement of dialysate may be useful.
Availability of data and materials
The datasets used during the current study are available from the corresponding author on reasonable request.
Abbreviations
- EP:
-
Eosinophilic peritonitis
- PD:
-
Peritoneal dialysis
- mNGS:
-
Metagenomics next generation sequencing
- WBC:
-
White blood cell
- CBC:
-
Complete blood count
- CKD-MBD:
-
Chronic Kidney Disease–Mineral and Bone Disorder
- CRP:
-
C-reactive protein.
References
Lee S, Schoen I. Eosinophilia of peritoneal fluid and peripheral blood associated with chronic peritoneal dialysis. Am J Clin Pathol. 1967;47(5):638–40.
Chan MK, Chow L, Lam SS, Jones B. Peritoneal eosinophilia in patients on continuous ambulatory peritoneal dialysis: a prospective study. Am J Kidney Dis. 1988;11(2):180–3.
Fontan MP, Rodriguez-Carmona A, Galed I, Iglesias P, Villaverde P, Garcia-Ureta E. Incidence and significance of peritoneal eosinophilia during peritoneal dialysis-related peritonitis. Perit Dial Int. 2003;23(5):460–4.
Jo YI, Song JO, Park JH, Lee JH, Shin SK. Idiopathic eosinophilic peritonitis in continuous ambulatory peritoneal dialysis: experience with percutaneous catheter placement. Nephrol (Carlton). 2007;12(5):437–40.
Piraino BM, Silver MR, Dominguez JH, Puschett JB. Peritoneal eosinophils during intermittent peritoneal dialysis. Am J Nephrol. 1984;4(3):152–7.
Ejaz AA, Fitzpatrick PM, Durkin AJ, Wasiluk A, Haley WE, Goalen MJ, et al. Pathophysiology of peritoneal fluid eosinophilia in peritoneal dialysis patients. Nephron. 1999;81(2):125–30.
Xu Y, Gao C, Xu J, Chen N. Successful treatment of idiopathic eosinophilic peritonitis by oral corticosteroid therapy in a continuous ambulatory peritoneal Dialysis patient. Case Rep Nephrol Dial. 2015;5(2):130–4.
Oh SY, Kim H, Kang JM, Lim SH, Park HD, Jung SS, et al. Eosinophilic peritonitis in a patient with continuous ambulatory peritoneal dialysis (CAPD). Korean J Intern Med. 2004;19(2):121–3.
Rosner MH, Chhatkuli B. Vancomycin-related eosinophilic peritonitis. Perit Dial Int. 2010;30(6):650–2.
Daugirdas JT, Leehey DJ, Popli S, Hoffman W, Zayas I, Gandhi VC, et al. Induction of peritoneal fluid eosinophilia and/or monocytosis by intraperitoneal air injection. Am J Nephrol. 1987;7(2):116–20.
Fourtounas C, Dousdampanis P, Hardalias A, Liatsikos E, Vlachojannis JG. Eosinophilic peritonitis following air entrapment during peritoneoscopic insertion of peritoneal dialysis catheters. Semin Dial. 2008;21(2):180–2.
Hsu CY, Lee DJ, Lin SH. Severe eosinophilic peritonitis caused by intraperitoneal vancomycin administration. Clin Nephrol. 2021;96(3):184–7.
Wong PN, Mak SK, Lee KF, Fung LH, Wong AK. A prospective study of vancomycin-(Vancoled-)induced chemical peritonitis in CAPD patients. Perit Dial Int. 1997;17(2):202–4.
Rathi M. Intraperitoneal streptokinase use-associated eosinophilic peritonitis. Saudi J Kidney Dis Transpl. 2015;26(1):128–31.
Minato S, Miyazawa H, Kitano T, Shindo M, Ito K, Ueda Y, et al. Eosinophilic peritonitis induced by sucroferric oxyhydroxide. Perit Dial Int. 2020;40(4):419–21.
Solary E, Cabanne JF, Tanter Y, Rifle G. Evidence for a role of plasticizers in ‘eosinophilic’ peritonitis in continuous ambulatory peritoneal dialysis. Nephron. 1986;42(4):341–2.
Chan Z, Hui YH, Wong SSH. Resolution of severe eosinophilic peritonitis in a patient on continuous ambulatory peritoneal dialysis by changing from Dianeal peritoneal dialysis solution to stay-safe balance solution: a case report. BMC Nephrol. 2022;23(1):149.
Bommer J, Ritz E, Andrassy K. Necrotizing dermatitis resulting from hemodialysis with polyvinylchloride tubing. Ann Intern Med. 1979;91(6):869–70.
Rocklin MA, Teitelbaum I. Noninfectious causes of cloudy peritoneal dialysate. Semin Dial. 2001;14(1):37–40.
Keane WF, Bailie GR, Boeschoten E, Gokal R, Golper TA, Holmes CJ, et al. Adult peritoneal dialysis-related peritonitis treatment recommendations: 2000 update. Perit Dial Int. 2000;20(4):396–411.
Acknowledgements
Not applicable.
Funding
This study was supported by funding for Clinical Trials from the Affiliated Drum Tower Hospital, Medical School of Nanjing University (2021-LCYJ-PY-12). They provided financial support for metagenomics next generation sequencing.
Author information
Authors and Affiliations
Contributions
QYZ collected the clinical data and wrote the manuscript; YYX and MZ collected and analyzed the data; CMJ revised the manuscript. All authors read and approved the final manuscript.
Corresponding author
Ethics declarations
Ethics approval and consent to participate
Not applicable.
Consent for publication
The patient gave us written consent for publication of his details and images.
Competing interests
The authors declare that they have no competing interests.
Additional information
Publisher’s Note
Springer Nature remains neutral with regard to jurisdictional claims in published maps and institutional affiliations.
Rights and permissions
Open Access This article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons licence, and indicate if changes were made. The images or other third party material in this article are included in the article's Creative Commons licence, unless indicated otherwise in a credit line to the material. If material is not included in the article's Creative Commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this licence, visit http://creativecommons.org/licenses/by/4.0/. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated in a credit line to the data.
About this article
Cite this article
Qingyan, Z., Yangyang, X., Miao, Z. et al. Peritoneal dialysis related eosinophilic peritonitis: a case report and review of the literature. BMC Nephrol 24, 10 (2023). https://doi.org/10.1186/s12882-022-03027-8
Received:
Accepted:
Published:
DOI: https://doi.org/10.1186/s12882-022-03027-8