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Medicina Interna

versão impressa ISSN 0872-671X

Medicina Interna vol.24 no.2 Lisboa jun. 2017

 

ARTIGOS ORIGINAIS / ORIGINAL ARTICLES

Pancreatite Hipertrigliceridémica: Tratamento Convencional Versus Troca Plasmática Terapêutica

Hypertriglyceridemic Pancreatitis: Conventional Treatment Versus Therapeutic Plasma Exchange

Diana M. Ferreira1, Filipe Lobo2, João Pedro Fonseca1, Patrícia A. Mendes1, António Aragão1, Manuela Ferreira3, Jorge Tomaz2, Armando de Carvalho1

11Internal Medicine Department, Centro Hospitalar e Universitário de Coimbra, Coimbra, Portugal
2Blood Bank and Transfusion Medicine Department, Centro Hospitalar e Universitário de Coimbra, Coimbra, Portugal
3Department and Gastroenterological Intensive Care Unit, Centro Hospitalar e Universitário de Coimbra, Coimbra, Portugal

Correspondência

 

RESUMO

Introdução:A pancreatite aguda (PA) por hipertrigliceridemia (HTG) pode ser tratada com troca plasmática terapêutica (TPT), com redução rápida dos valores de triglicerídeos. Contudo, não existem estudos comparativos definitivos que comprovem o real benefício desta terapêutica.

Objetivo: Comparação dos métodos de tratamento (troca plasmática terapêutica versus convencional) em doentes com PA HTG, durante um período de 12 anos (2000-2012).

Métodos: Estudo retrospetivo descritivo e inferencial de 37 doentes, avaliando: sexo, idade, antecedentes pessoais, gravidade, valores de TG e evolução consoante o tratamento (“TPT” ou terapêutica convencional “C”).

Resultados: Os dois grupos TPT e C mostraram-se homogéneos quanto ao sexo (p = 0,647), idade (43,5 ± 9,74 anos TPT versus 45,30 ± 9,90 anos C; p = 0.320), pancreatite prévia (40% TPT vs 40,7% C; p = 1,0) alcoolismo crónico (50% TPT vs 70,4% C; p = 0,275) e gravidade pelo score de APACHE II (p = 0,054) e Ranson às 48 horas (p = 0,258). Dos doentes 45,95% apresentava mais de um fator de risco secundário para HTG. O grupo TPT apresentou maiores valores de TG à admissão: 4850 ± 2802 mg/dL vs 1845 ± 1858 mg/dL (p = 0,001). Não se verificaram diferenças na duração do internamento 14,2 ± 6,8 dias vs 13,5 ± 9,0 dias (p = 0,56) ou na taxa de mortalidade (p = 0,47). À data de alta a redução dos TG foi superior no grupo TPT: 4433,70 ± 2896,08 mg/dL - 91,41% vs 1582,95 ± 2051,06 mg/dL – 83,92% (p = 0,002). De referir seis intercorrências minor durante a troca plasmática terapêutica.

Discussão/Conclusões: Apesar do viés de seleção (estudo retrospetivo), foi constatada uma maior redução dos TG por esta técnica. As intercorrências inerentes à técnica de troca plasmática terapêutica foram de simples resolução.

Palavras-chave:Doença Aguda; Hipertrigliceridémia/tratamento; Pancreatite/tratamento; Troca Plasmática.

 


ABSTRACT

 

Introduction:Acute pancreatitis (AP) induced by hypertriglyc-eridemia (HTG) can be treated with therapeutic plasma exchange (TPE), resulting in rapid reduction of triglyceride level. However, there are no definitive comparative studies that prove the real benefits of this therapy.

Objectives: Comparison of treatment methods (TPE versus conventional) in patients with HTG AP during a period of 12 years (2000-2012).

Methods:Retrospective, descriptive and inferential analysis of 37 patients, evaluating: gender, age, personal pathologic history, severity of disease, HTG values and evolution depending on treatment with therapeutic plasma exchange (“TPE”) or with conventional therapy (“C”).

Results:Both groups TPE and C demonstrated homogeneity considering gender (p = 0.647), age (43.5 ± 9.74 years TPE vs 45.30 ± 9.90 years C; p = 0.320), prior AP episode (40% TPE vs 40.7% C; p = 1.0), chronic alcohol consumption (50% TPE vs 70.4% C; p = 0.275) and severity disease scores: APACHE II (p = 0.054) and Ranson (p = 0.258). More than one secondary HTG risk factor was presented in 45.95% of patients. TPE group presented higher TG levels at admission: 4850 ± 2802 mg/dL vs 1845 ± 1858 mg/dL (p = 0.001). No significant statistical differences were observed considering length of hospital stay [14.2 ± 6.8 days vs 13.5 ± 9.0 days (p = 0.56)] or mortality rate (p = 0.47). At discharge, TG reduction was greater in TPE group: 4433.70 ± 2896.08 mg/dL – 91.41% vs 1582.95 ± 2051.06 mg/dL – 83,92% (p = 0.002). Six minor complications associated to TPE occurred.

Discussion/Conclusion: Despite the selection bias (retrospective study), a greater TG reduction was observed with TPE technique. Complications associated with the technique were simple to resolve.

Keywords:: Acute Disease; Hypertriglyceridemia/therapy; Pancreatitis/therapy; Plasma Exchange.

 


 

Introduction

Acute pancreatitis (AP) is a potentially life-threatening condition, with a worldwide rising incidence. It is defined as an acute inflammatory process involving the pancreas, peripancreatic tissue and remote organ systems.1–4 The most prevalent causes are gallstone disease, alcohol abuse and hypertriglyceridemia (HTG), with HTG accounting for 1-7% of cases, depending on the series.3,5,6

It is commonly accepted that a triglyceride (TG) level > 1000 mg/dL (> 11.3 mmol/L) is necessary to trigger an AP. However, there is no clear threshold for TG level. TG levels between 500 and 1000 mg/dL should raise a high degree of suspicion, particularly if accompanied by lactescent serum, if the evaluation of TG level has been delayed or if there is no other obvious etiology.3,5–9

HTG can be either primary (rare cases of genetic determined dyslipidemias – Frederickson Classification I, IV and V) or secondary, usually multifactorial, consequent to an association of a large number of genetic polymorphisms, and lifestyle or acquired conditions (autoimmune disease, chronic kidney disease, diabetes mellitus, drugs, hypothyroidism, metabolic syndrome, obesity and pregnancy).1,3,8,10,11 The classic portrait of an AP induced by HTG is a patient with a preexisting lipid abnormality, along with the presence of a secondary factor (such as being a poorly controlled diabetic, the use of retinoids or other associated medications, alcohol abuse or pregnancy).4,5,8,12

The pathophysiologic mechanism by which HTG causes AP is still unclear. Several theories have been proposed, most of them describing free fatty acids as the cornerstone toxic molecule. Despite TG not being toxic themselves, they serve as a source of unsaturated fatty acids.3,5,7,8,13,14 Hence there was a need for development of treatment forms that promote rapid removal of excessive TG, contrasting with conventional treatment (pancreas rest, analgesia, supportive care for organ failure, and complications management). Even though the first case report of therapeutic plasma exchange (TPE) use in AP secondary to HTG dates of 1978, and most studies describe a rapid TG reduction (up to 60-80% after one or two sessions), it remains a poorly studied treatment.12,14–16 This is owing to its costs, poor accessibility and fear of potential complications, which limited the studies mostly to small case series and case reports, resulting in a weak recommendation in guidelines.1,7,10,12–14,16,17

Material and Methods

A retrospective, descriptive and inferential analysis was conducted, involving patients admitted to our Hospital (Hospitais da Universidade de Coimbra) from January 2000 to December 2012 (13-year period).

A control group (conservative treatment – “C”) was obtained through the analysis of the Hospital discharge documents database, selecting patients admitted to the Internal Medicine ward with the clinical diagnosis of AP, which corresponded to 347 patients. Exclusion criteria for the control group were: gallstone disease (identified in ultrasound imaging or other imaging exam), isolated alcohol abuse, potentially iatrogenic causes (such as post endoscopic retrograde cholangiopan- creatography – ERCP or associated to medications), idiopathic or not characterized etiology, TG < 500 mg/dL and patients submitted to TPE. A total of 27 patients were selected.

The TPE group (TPE treatment - “TPE”), was obtained through the analysis of the Blood Bank and Transfusion Medicine Department TPE database, with identification of 11 patients. Exclusion criteria were the same as for the control group, except these patients had to have been treated with TPE. Patients submitted to TPE for any other condition were also excluded. A total of 10 patients were selected, submitted to a total of 23 sessions. In all TPE sessions albumin was used as fluid replacement and anticoagulation was obtained with citrate.

Both groups were included in the analysis, preserving the anonymity of the patients and considering: age, sex, previous pathologic conditions, medications, clinical presentation, severity score index of AP (Ranson’s criteria and APACHE II score - Acute Physiology and Chronic Health Disease Classification System II), blood analyses, including TG and total cholesterol levels, complications (associated or not to AP or its treatment), evolution and mortality.

Statistical analysis was performed using IBM SPSS Statistics 20.0®. Inferential analysis of nominal variables was performed according to Cochran rules, using Fisher’s exact test or chisquare test (?2). Continuous variables were tested for normality distribution with Shapiro-Wilk’s test. Analysis of continuous variables was performed with Mann-Whitney’s test (U– nonparametric test for non-normally distributed variables) or Student’s t test (t–parametric test for normally distributed variables, after assessment of equality of variances using Levene’s test). A p-value of less than 0.05 was considered to indicate statistical significance (type I error).

Results

As presented in Table 1 most of the patients were young (mean age of 44.81 ± 9.75 years), males (81.08%), frequently with prior diagnosis of lipid disorder (3 patients with known HTG hereditary syndromes, without specific Fredrickson classification – two in the TPE group and one in the C group). The most common secondary factors were alcohol consumption (64.86%), metabolic syndrome (45.95%) and type 2 diabetes mellitus (27.03%). Considering drugs as secondary factors for HTG, two patients where on beta-blockers (one in each group) and the remaining patients where on thiazide diuretics. One patient was diagnosed with HIV (human immunodeficiency virus) infection but only started antiretroviral treatment after the AP episode. Apart from body mass index (p = 0.041), the characteristics observed in Table 1 show homogeneity in both groups.

Table 2 shows the clinical presentation of the patients at admission (in all cases, the presentation in the emergency department). There were statistically significant differences in the evaluation of heart and respiratory rates (p = 0.017 and p=0.004 respectively). Although both parameters are important for the calculation of APACHE II Score, there is no statistically significant difference between the groups as seen in Table 3 (representing also other parameters related to the initial laboratory and clinical evaluation). Eight patients (all from the TPE group) were admitted to the Gastroenterology Intensive Care Unit (UCIGE), with a mean length of stay of 6.63 ± 3.78 days.

A total of 23 TPE sessions were performed (minimum of one session and maximum of four sessions), with the decrease in TG level being represented in Fig 1 (as well as TG variation of the C group and total cholesterol variation in both groups). Complications were identified in 26.09% (six patients) of all TPE sessions Table 4. All were quickly and effectively solved: an anxiety attack solved by stopping the session, paresthesia treated with calcium gluconate, urticaria treated with clemastine and treatment induced pain worsening treated with different analgesics. No other complications related to TPE were documented. TG levels after the first TPE cycle were only available for eight patients. For these eight patients, a single cycle of TPE was responsible for a TG lowering of 80.97% (TG values after one session: 635.88± 261.25 mg/dL).

 

 

A total of eleven patients were treated with fibrate drugs, with four from TPE group and seven from the C group. Fibrates were early introduced during treatment in six cases (two patients from TPE group and four from the C group).

One patient from the TPE group was discharged against medical advice, prior to optimal lipid care, and one patient (also from the TPE group) was transferred to another hospital (closer to the area of residence of the patient) to continue treatment.

Discussion

This study included 37 patients (Table 1) most of them were young males, with prior diagnosis of lipid disorder. Seventeen patients had more than one secondary risk factor (45.95%), which demonstrates higher risk compared to other populations (data from a systematic study demonstrates accumulation of risk factors in 9.4% of the patients).7 All our other demographic data is coincident with previous studies (including a recent systematic review of 301 patients)7,16 and there are no statistically significant differences between the two groups (apart from body mass index, p = 0.041, but with both groups presenting overweight/obesity), demonstrating homogeneity between groups TPE and C.

At clinical presentation (Table 2), some differences between groups C and TPE are apparent, but merely considering heart rate and respiratory rate (p = 0.017 and p = 0.004). As AP usually presents as an acute onset of abdominal pain, homogeneity between groups was expected. Clinical signs and symptoms associated with initial laboratory evaluation (Table 3) allow calculation of scores like APACHE II and Ranson, that accurately predict outcome of patients with acute pancreatitis.18 Although there was no statistically significant differences between the scores of groups C and TPE (p=0.054 for APACHE II and p = 0.258 for Ranson) calculated scores should be analyzed in more detail. The group submitted to TPE presented APACHE II scores of 9.56 ± 4.82, much higher than the same value for C group – 6.55 ± 2.86, associated to a potentially higher hospital mortality. As the present study is retrospective, this type of bias was expected, as patients in worst clinical state are treated more aggressively and, therefore, most promptly selected for TPE (this kind of bias was present also in a systematic review of cases7). In this case, the low number of patients included in the study is probably the reason why there are no statistical differences.

Another expected bias is TG total level at admission. As previously stated, standard treatment of AP includes pancreas rest, analgesia, supportive care for organ failure, and management of complications. However, a rapid decrease in TG levels is essential to the successful management of HTG induced pancreatitis.10 Several studies report decreases in TG levels after only one session of TPE in up to 60% of patients, and up to 60- 80% in one or two sessions.3,7,10,12,16 Considering these results, a bias of selection of patients with high TG levels at admission to TPE is logical (as well as a selection bias for the patients admitted in the UCIGE). Similar reduction results were obtained in our study (Table 4), with decrease in TG up to 80.97% in one session (results considering data from eight patients) and up to 91.41% at the end of all sessions for patients submitted to more than one treatment (six patients). Similar results were obtained for total cholesterol level decrease. Regardless of selection bias and premature discharge of two patients in the TPE group (one patient against medical advice and one patient transferred to another hospital), the relative reduction achieved in the TPE treatment group was greater than in the conventional treatment group (p = 0.002 both in TG and total cholesterol levels reduction), demonstrating that TPE is a useful tool for achieving an early decrease of TG to safer levels. The benefits of this treatment acquire a greater importance given that some studies demonstrate that TG levels < 500 mg/dL represent a safe therapeutic target, not only to prevent AP recurrences, but also to prevent other clinical events (cardiovascular, diabetes and renal) and to reduce overall costs.12

Although TPE has proven effective in achieving significant reductions in TG levels, most studies are case reports and small case series. Randomized controlled trials are lacking and, consequently, guidelines such as the latest from the American Society for Apheresis classifies TPE as a category III indication in HTG induced AP.19 These studies are lacking not only because of the limited availability of this kind of treatment and low prevalence of the disease, but also because of the fear of potential complications. Some complications of TPE are bleeding/hematoma, catheter site infection, hemothorax, hypofibrinogenemia, hypotension, nausea, paresthesia (associated to the use of citrate as anticoagulation therapy and consequent hypocalcemia), pneumothorax, urticaria, vasovagal reactions and vomiting.17 However, studies have demonstrated that the occurrence of truly important complications is rare, and that most complications, like clinical manifestation of hypocalcemia by paresthesia is easily treated.6,10 This data is concurrent with that of our study, with only minor complications associated to TPE being documented.

It is also important to consider the length of the study (13 years), as it entails technological and practical changes that may represent a bias, not only in the rate of complications but also on the clinical evolution.

Considering the length of hospital stay and mortality, no statistically significant differences were achieved between both groups [p = 0.560 and p = 0.473 respectively (Table 4)]. These data are similar to a previous study, by Chen et al,20 that showed no clear benefit of apheresis in reducing severity and improving outcomes in AP.12,15,16 Nevertheless, it is important to emphasize that study presented similar bias and limitations as our present study: it is also a retrospective study, with small groups (60 patients treated with TPE; 34 patients treated otherwise) and single center experience (as it was designed for the evaluation of the clinical outcomes in HTG induced AP before and after the availability of apheresis at their institution). On the other hand, major AP complications (pancreatic pseudocyst and pancreatic abscess) were more commonly seen in the group treated with conventional therapy. Although the number of cases is too small in order to properly achieve definitive considerations, rapid removal of TG may reduce damage to the pancreas. Still, further studies are needed.

Many questions remain unanswered, not only considering the real benefit of the use of TPE, but also considering variations on the technique (a recent study found a significant reduced mortality using citrate anticoagulation as compared to heparin anticoagulation).3

Conclusions

Apart from the greater burden of secondary factors, our study reported a population that has general demographic data similar to what has been previously published in studies about AP induced by HTG. This can potentially illustrate greater incidence and/or more severe cases, conclusions that require further studies.

We also reported how therapeutic plasma exchange can effectively and quickly reduce TG levels, to a safe therapeutic target without major complications associated to the treatment. There was no statistically significant differences between patients treated with or without TPE, regarding length of hospital stay and mortality, but the small sample in this study may contribute to this result. Well design randomized controlled trials with an adequate sample size are necessary for further analyses and to determine the benefits of this procedure.

Acknowledgements

We gratefully acknowledge and thank Drs. João Casalta Lopes and Joana Parra for their expertise and skillful technical assistance.

 

References

1. Claudia Stefanutti, Serafina Di Giacomo, Antonio Vivenzio, Giancarlo Labbadia, Fabio Mazza, Giovanna D’Alessandri, et al. Therapeutic plasma exchange in patients with severe hypertriglyceridemia: a multicenter study. Artif Organs. 2009; 33:1096–1102.         [ Links ]

2. Kumaravel A, Stevens T, Papachristou GI, Muddana V, Bhatt A, Lee PJ, et al. Pancreas, biliary tract, and liver a model to predict the severity of acute pancreatitis based on serum level of amylase and body mass index. Clin Gastroenterol Hepatol. 2015;13:1496–501.         [ Links ]

3. Valdivielso P, Ramírez-Bueno A, Ewald N. Current knowledge of hypertriglyceridemic pancreatitis. Eur J Intern Med. 2014;25:689–94.         [ Links ]

4. Criddle DN. The role of fat and alcohol in acute pancreatitis: A dangerous liaison. Pancreatology. 2015;15:S6–12.         [ Links ]

5. Xiao-Li Zhang, Fei Li, Ya-Min Zhen, Ang Li, Yu Fang. Clinical Study of 224 Patients with Hypertriglyceridemia 2015. Chin Med J. 2015; 128:2045-9.         [ Links ]

6. Zeitler H, Balta Z, Klein B, Strassburg CP. Extracorporeal treatment in severe hypertriglyceridemia-induced pancreatitis. Ther Apher Dial. 2015; 19:405–10.         [ Links ]

7. Click B, Ketchum AM, Turner R, Whitcomb DC, Papachristou GI,Yadav D. The role of apheresis in hypertriglyceridemia-induced acute pancreatitis: A systematic review. Pancreatology. 2015;15:313–20.         [ Links ]

8. D, Pitchumoni CS. Hyperlipidemia in pancreatitis versus pancreatitis of hyperlipidemia. J Clin Gastroenterol. 2003;36:54–62.         [ Links ]

9. Berglund L, Brunzell JD, Goldberg AC, Goldberg IJ, Stalenhoef A. Treatment options for hypertriglyceridemia: from risk reduction to pancreatitis. Best Pract Res Clin Endocrinol Metab. 2014;28:423–37.         [ Links ]

10. Galán Carrillo I, Demelo-Rodriguez P, Rodríguez Ferrero ML, Anaya F. Double filtration plasmapheresis in the treatment of pancreatitis due to severe hypertriglyceridemia. J Clin Lipidol. 2015;9:698–702.         [ Links ]

11. Toth PP, Grabner M, Ramey N, Higuchi K. Clinical and economic outcomes in a real-world population of patients with elevated triglyceride levels. Atherosclerosis. 2014;237:790–7.         [ Links ]

12. Scherer J, Singh V, Pitchumoni CS, Yadav D. Issues in hypertriglyceridemic pancreatitis - an update. J Clin Gastroenterol. 2014 ; 48: 195–203.         [ Links ]

13. Valme U De, Valme HU De, Intensivos UDC. Uso de la plasmaféresis en la pancreatitis aguda hipertrigliceridémica Plasmapheresis in hypertriglyceridemic acute pancreatitis. Med Intensiva. 2015 ;39:387-8.         [ Links ]

14. Maher NG, Ramaswamykanive H. Case report use of plasmapheresis in managing the diagnostic dilemma of symptomatic hypertriglyceridemia. Case Rep Gastrointest Med. 2012;2012:501373.         [ Links ]

15. Lalastra CS, Hernández ET, Vicente VM, Castellanos MM, Concepción M, et al. Pancreatitis aguda por hipertrigliceridemia. Gastroenterol Hepatol. 2013;36:274–9.         [ Links ]

16. Ramírez-Bueno A, Salazar-Ramírez C, Cota-Delgado F, De La Torre-Prados M V, Valdivielso P. Plasmapheresis as treatment for hyperlipidemic pancreatitis. Eur J Intern Med. 2014;25:160–3.         [ Links ]

17. Winters JL. Plasma exchange: concepts, mechanisms, and an overview of the American Society for Apheresis guidelines. Hematol Am Soc Hematol Educ Program. 2012;2012:7-12.         [ Links ]

18. Suvarna R, Pallipady A, Bhandary N, Hanumanthappa H. The clinical prognostic indicators of acute pancreatitis by APAChe II Scoring. J Clin Diagn Res. 2011;5:459–63.         [ Links ]

19. Schwartz J, Winters JL, Padmanabhan A, Balogun RA, Delaney M, Linenberger ML, et al. Guidelines on the use of therapeutic apheresis in clinical practice-evidence-based approach from the Writing Committee of the American Society for Apheresis: the sixth special issue. J Clin Apher. 2013;28:145-284.         [ Links ]

20. Chen JH, Yeh JH, Lai HW, Liao CS. Therapeutic plasma exchange in patients with hyperlipidemic pancreatitis. World J Gastroenterol. 2004;10:2272-4.         [ Links ]

 

Correspondência: Diana M. Ferreira diana.c.marquesferreira@gmail.com
Internal Medicine Department, Centro Hospitalar e Universitário de Coimbra, Coimbra, Portugal
Praceta Prof. Mota Pinto, 3000-075 COIMBRA

 

Presentations/Apresentações: This work was presented in the XXII Nacional Congress of Internal Medicine / V Iberian Congress of Internal Medicine, posteriorly being proposed to article writing.

Conflicts of interest: The authors have no conflicts of interest to declare.

Financing Support: This work has not received any contribution, grant or scholarship.

Confidentiality of Data: The authors declare that they have followed the protocols of their work center on the publication of data from patients.

Protection of Human and Animal Subjects: The authors declare that the procedures followed were in accordance with the regulations of the relevant clinical research ethics committee and with those of the Code of Ethics of the World Medical Association (Declaration of Helsinki).

Conflitos de Interesse: Os autores declaram a inexistência de conflitos de interesse na realização do presente trabalho.

Fontes de Financiamento: Não existiram fontes externas de financiamento para a realização deste artigo.

Direito à Privacidade e Consentimento Informado: Os autores declaram que nenhum dado que permita a identificação do doente aparece neste artigo.

Protecção de Seres Humanos e Animais: Os autores declaram que não foram realizadas experiências em seres humanos ou animais.

 

Recebido: 15/12/2016

Aceite: 01/03/2017

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