Gemcitabine-induced thrombotic microangiopathy treated with eculizumab: a case report
Case Report

Gemcitabine-induced thrombotic microangiopathy treated with eculizumab: a case report

Lisa Van den Eeckhaut1^, Heidi Hannon1, Marie Schurgers1, Els Monsaert2, Kathleen Claes3,4

1Department of Nephrology, AZ Maria Middelares, Ghent, Belgium; 2Department of Gastroenterology, AZ Maria Middelares, Ghent, Belgium; 3Department of Nephrology and Renal Transplantation, University Hospital Leuven, Leuven, Belgium; 4Department of Microbiology, Immunology and Transplantation, KU Leuven, Leuven, Belgium

Contributions: (I) Conception and design: L Van den Eeckhaut, H Hannon; (II) Administrative support: L Van den Eeckhaut, H Hannon; (III) Provision of study materials or patients: L Van den Eeckhaut, H Hannon, K Claes; (IV) Collection and assembly of data: L Van den Eeckhaut, H Hannon, K Claes; (V) Data analysis and interpretation: L Van den Eeckhaut, H Hannon, K Claes; (VI) Manuscript writing: All authors; (VII) Final approval of manuscript: All authors.

^ORCID: 0000-0001-5869-5763.

Correspondence to: Lisa Van den Eeckhaut. Buitenring Sint-Denijs 30, 9000 Ghent, Belgium. Email: lvdeeckhaut@outlook.com.

Background: Gemcitabine is a broadly used chemotherapeutic agent that can cause a rare but life-threatening complication called thrombotic microangiopathy (TMA). Early recognition is crucial as therapy options are limited.

Case Description: We report the case of a 46-year-old patient with pancreatic adenocarcinoma who presented with severe anemia and thrombocytopenia as well as acute kidney injury. A diagnosis of gemcitabine-induced TMA was made. He became rapidly transfusion and dialysis dependent. Despite discontinuation of gemcitabine and treatment with high-dose corticotherapy as well as plasmapheresis, no improvement in both renal and hematological parameters was seen. Treatment with eculizumab was initiated. One week after the first administration, the patient no longer required packed cells nor platelet transfusions and one month later, dialysis could be discontinued. After five doses, treatment with eculizumab was stopped. Four months later, his serum creatinine was 1 mg/dL.

Conclusions: This case report illustrates the promising beneficial effects of eculizumab in gemcitabine-induced TMA, both regarding transfusion dependence as well as improvement in renal function, thereby allowing further therapy options in patients with an active malignancy.

Keywords: Gemcitabine-induced thrombotic microangiopathy; eculizumab; hemolytic uremic syndrome; case report


Submitted May 24, 2022. Accepted for publication Oct 21, 2022.

doi: 10.21037/jgo-22-509


Introduction

Thrombotic microangiopathy (TMA) is characterized by the triad of thrombocytopenia, microangiopathic hemolytic anemia and organ injury, including acute kidney injury. The classification of TMAs is constantly evolving with the greater understanding of the molecular basis and the role of complement dysregulation (1). Several drugs have been thought to have an association with TMA, although a definitive causality has been difficult to establish. Drug-induced TMA occurs through either immune-mediated damage or direct toxicity of the drug. Gemcitabine is a pyrimidine antimetabolite used for the treatment of several types of malignancies. The incidence of gemcitabine-induced TMA has been reported to be between 0.02% and 2.2% (2). Early recognition is crucial as mortality rates go up to 60% (3). Treatment of drug-induced TMA includes supportive therapy and withdrawal of the drug, but more specific therapy options are lacking (1). Several case reports have been published in which patients are treated with eculizumab, a monoclonal antibody directed against the complement protein C5, that has already been approved for the treatment of complement-mediated TMA (2-15). Our objective is to present a patient with gemcitabine-induced TMA who was successfully treated by eculizumab, and to review current literature regarding this topic. We present the following article in accordance with the CARE reporting checklist (available at https://jgo.amegroups.com/article/view/10.21037/jgo-22-509/rc).


Case presentation

We report the case of a 46-year-old male patient with stage IV pancreatic adenocarcinoma who received neoadjuvant gemcitabine—nab-paclitaxel and underwent a pancreaticosplenectomy followed by adjuvant gemcitabine—nab-paclitaxel. The cumulative dose of gemcitabine was 27,500 mg and nab-paclitaxel 3,437.5 mg. Five days after the eighth cycle of chemotherapy, the patient presented at the Emergency Department with fatigue, recurrent epistaxis, headache and anorexia. Clinical examination showed a weakened and pale patient, with a normal blood pressure. Biochemically, we noticed severe anemia (hemoglobin of 6.4 g/dL), thrombocytopenia (26.000×103/mm3), signs of hemolysis [increased lactate dehydrogenase (LDH) of 956 U/L, low haptoglobin of <0.10 g/L] and an acute kidney injury (creatinine level of 1.88 mg/dL corresponding with an estimated glomerular filtration rate (eGFR) according to the Cockcroft-Gault equation of 42 mL/min/1.73 m2 with baseline creatinine level of 0.79 mg/dL). White blood cell count was normal. Direct Coombs test was negative and peripheral blood smear showed the presence of schistocytes confirming the diagnosis of TMA. Reticulocyte level was initially decreased, probably as a result of bone marrow suppression due to recent chemotherapy. During the follow-up time the reticulocyte level was elevated. Testing for C3, C4, fibrinogen, prothrombin time (PT) and activated partial thromboplastin time (aPTT) were normal (0.94 g/L, 0.2 g/L, 280 mg/dL, 72% and 31.9 s respectively). Quantitative analysis of the complement alternative pathway [complement factor H (CFH), complement factor I (CFI), CD46/membrane cofactor protein (MCP), anti-factor H antibodies, ratio of degradation product of factor B and factor B (FBb/FB ratio)] demonstrated normal values. Urinalysis showed proteinuria and hematuria. The patient was started on high doses of intravenous corticotherapy (methylprednisolone 80 mg daily) as well as on daily plasmapheresis, which was discontinued when ADAMTS13 deficiency was excluded (ADAMTS13 activity was 77%) and no improvement was seen after two days. Based on some supporting evidence showing a reduction of the concentration of ultra-large von Willebrand factor (VWF) multimers in vitro and in an animal model in thrombotic thrombocytopenic purpura (TTP), as well as a resolution of abnormal electrocardiogram (ECG) findings in a patient with ponatinib-associated drug-induced TMA affecting the coronary microvasculature, a trial with N-acetylcysteine (NAC; 8,000 mg daily after a loading dose of 12,000 mg) was done (16-18). Unfortunately, again without result and NAC was discontinued after two days. The patient’s condition rapidly deteriorated and he became transfusion and dialysis dependent (due to volume overload and anuria). The required vaccinations before treatment with eculizumab were given. Access to eculizumab was granted through the company’s Global Access to Medicines Program, and started four days after submitting a request. Treatment with eculizumab was initiated 19 days after presentation at a dose of 900 mg IV weekly for four doses, followed by 1,200 mg IV for the fifth dose. The second dose needed to be postponed by one week due to an abdominal infection, with improvement after empiric antibiotic therapy with broad-spectrum antibiotics (piperacillin-tazobactam). After only one cycle, the patient no longer required platelet and packed cells transfusion. CH50 level was low (7 U/mL), suggesting an effective complement inhibition. One month after the initiation of eculizumab, dialysis could be discontinued (Figure 1). The patient received five doses of eculizumab in total. Unfortunately, he developed progressive oncological disease necessitating second line chemotherapy. Second line treatment with liposomal irinotecan and 5-fluorouracil (modified de Gramont) was initiated. Creatinine level normalized to 1 mg/dL corresponding with an eGFR of 90 mL/min/1.73 m2.

Figure 1 Trend of hemoglobin (g/dL), platelet count (×103/mm3) and serum creatinine (mg/dL) with eculizumab. Black full arrow indicates presentation at the Emergency Department (day 1). Dashed arrows indicate administration of eculizumab (day 20, 30, 37, 44 and 52). Green full arrow indicates last transfusion of packed cells (day 28). Purple full arrow indicates last transfusion of platelets (day 28). Orange full arrows indicate initiation (day 16) and discontinuation (day 49) of hemodialysis.

All procedures performed in this study were in accordance with the ethical standards of the institutional and/or national research committee(s) and with the Declaration of Helsinki (as revised in 2013). Written informed consent was obtained from the patient for publication of this case report and the accompanying image. A copy of the written consent is available for review by the editorial office of this journal.


Discussion

Eculizumab is a recombinant humanized monoclonal antibody that binds to C5 and prevents the formation of the proinflammatory C5a and membrane attack complex C5b9 in the alternative pathway of the complement system, thereby inhibiting inappropriate systemic coagulation (1,5). It has been approved for the treatment of complement-mediated TMA (1).

TMA occurring in a patient with a malignancy can be both malignancy or drug-induced. The exact pathophysiology of gemcitabine-induced TMA is not well established. In a recent retrospective study, deposits of C5b9 in kidney biopsies suggest an at least partial role of complement activation, which may result from a direct endothelial toxicity of the drug (4). This could also explain why treatment with eculizumab is potentially successful in this setting. Apart from drug-induced TMA through direct endothelial damage (type 1, dose dependent) or immune-mediated through the development of drug-dependent autoantibodies (type 2, none-dose dependent), the malignancy itself can also cause TMA (paraneoplastic TMA) (19). This can arise from metastases in the microvasculature or direct invasion of tumor cells in the bone marrow (2). In this case, it was more likely that the cause was drug-induced. At the time when the patient developed TMA, he showed no signs of progressive disease. It was only after discontinuation of chemotherapy and during eculizumab treatment that the patient showed disease progression. Furthermore, paraneoplastic TMA usually does not respond well to eculizumab and would more likely improve when there is a good response to chemotherapy (19). Also, paraneoplastic TMA is most frequently seen in metastatic disease (91.8%), which was not the case in our patient (20). Gemcitabine has shown to have a causal association with TMA (1). Although TMA caused by nab-paclitaxel has been rarely reported, its potential role in causing drug-induced TMA cannot be denied. A recent article suggests a potential drug interaction between nab-paclitaxel and gemcitabine thereby increasing the risk of developing gemcitabine-induced TMA (21).

Aside from permanent discontinuation of gemcitabine and supportive care, the optimal treatment is not known (4). The use of eculizumab in gemcitabine-induced TMA is limited probably due to several factors. Firstly, optimal timing and exact duration of treatment as well as dose intervals to keep patients in remission is unknown. Secondly, treatment with eculizumab comes at a high cost (2). Thirdly, the impact of complement mediated treatment on tumor progression is not known. However, if it could keep the patient off dialysis, it might be more cost efficient than suspected and impose a significant impact on the patient’s quality of life. Therefore, one could speculate that eculizumab should be instituted without delay, after balancing the patient’s life expectancy and performance status against the risks of eculizumab (e.g., infectious complications) and benefits of improving TMA. Currently in Belgium, eculizumab in drug-induced TMA is not reimbursed.

Current evidence is limited to case reports and case series. To our knowledge, 15 publications (including this case report) have described 33 patients in total with gemcitabine-induced TMA treated with eculizumab (2-15). Table 1 illustrates the demographic factors and outcome parameters of these cases. A renal response and hematological response were seen in 26 patients (79%) and 28 patients (85%) respectively. Even though these findings seem promising, they should be interpreted with caution. Firstly, there might be publication bias. Secondly, a contributing role is suspected in hematological response when chemotherapy is temporarily discontinued. Also, the interpretation of these results is limited by the heterogeneity of patient characteristics and small population groups. Furthermore, it cannot be excluded that patients showed a late response to treatment discontinuation while already receiving eculizumab. Unfortunately, we do not have data on complement activation (C5b9) or complement deposition in a renal biopsy because an elevated level would have added to the case of treatment with complement inhibition. Finally, it is to be suspected that the mortality rates of gemcitabine-induced TMA are inseparably related to the prognosis of the underlying malignancy.

Table 1

Publications of eculizumab treatment for gemcitabine-induced TMA

Study Year Patient Age/malignancy type Unsuccessful treatments prior to eculizumab Doses of eculizumab Renal response to eculizumab Hematological response to eculizumab
Al Ustwani et al. (5) 2014 1 75/lung Drug cessation 8 Yes Yes
2 70/pancreatic Drug cessation, corticotherapy 6 Yes Yes
3 73/cholangio Drug cessation 6 Yes NA
4 69/lung Plasmapheresis 5 Yes Yes
Starck et al. (6) 2014 5 45/duodenal Drug cessation, plasmapheresis, Rituximab 4 Yes Yes
Rogier et al. (7) 2016 6 68/pancreatic Drug cessation, plasmapheresis 7 Yes Yes
Nanjappa et al. (8) 2017 7 56/pancreatic Drug cessation, plasmapheresis NA No Yes
Facchini et al. (3) 2017 8 3/medulloblastoma Rituximab, defibrotide, immunoglobulins, plasmapheresis 7 Yes Yes
Gosain et al. (9) 2017 9 54/pancreatic Plasmapheresis NA Yes Yes
López Rubio et al. (10) 2017 10 74/pancreatic Drug cessation, plasmapheresis 7 Yes Yes
Krishnappa et al. (11) 2018 11 64/pancreatic Plasmapheresis, drug cessation 18b Yes Yes
Martin et al. (12) 2019 12 56/pancreatic Corticotherapy, plasmapheresis 10b Yes Yes
Daviet et al. (13) 2019 13 53–68/pancreatic and lungc Plasmapheresis (n=4), drug cessation (n=1) NA Yes Yes
14 53–68/pancreatic and lungc Plasmapheresis (n=4), drug cessation (n=1) NA No Yes
15 53–68/pancreatic and lungc Plasmapheresis (n=4), drug cessation (n=1) NA No Yes
16 53–68/pancreatic and lungc Plasmapheresis (n=4), drug cessation (n=1) NA No Yes
17 53–68/pancreatic and lungc Plasmapheresis (n=4), drug cessation (n=1) NA No No
Burns et al. (14) 2020 18 39/pancreatic Drug cessation 1 Yes Yes
Sethi et al. (2) 2021 19 67/pancreatic Drug cessation NA Yes NA
Efe et al. (15) 2021 20 29/cholangio Drug cessation 6 Yes Yes
Grall et al. (4) 2021 21 36/ovarian Drug cessation ± plasmapheresisa 4 Yes Yes
22 64/ovarian Drug cessation ± plasmapheresisa 3 No No
23 54/pancreatic Drug cessation ± plasmapheresisa 22 Yes Yes
24 69/pancreatic Drug cessation ± plasmapheresisa 3 No No
25 64/ovarian Drug cessation ± plasmapheresisa 7 Yes Yes
26 68/pancreatic Drug cessation ± plasmapheresisa 14 Yes Yes
27 59/lung Drug cessation ± plasmapheresisa 5 Yes Yes
28 57/lung Drug cessation ± plasmapheresisa 4 Yes Yes
29 52/uterine Drug cessation ± plasmapheresisa 2 Yes Yes
30 50/pancreatic Drug cessation ± plasmapheresisa 2 Yes Yes
31 56/ovarian Drug cessation ± plasmapheresisa 3 Yes Yes
32 55/ovarian Drug cessation ± plasmapheresisa 4 Yes Yes
Van den Eeckhaut et al. (present study) 2022 33 46/pancreatic Drug cessation, corticotherapy, plasmapheresis, N-acetylcysteine 5 Yes Yes

a, five patients received plasmapheresis, not mentioned which patients; b, not explicitly reported; number of doses was estimated based on reported schedule of eculizumab; c, not further specified. NA, not available.

Nonetheless, this case reports adds to limited literature on the successful use of terminal complement blockade by eculizumab for gemcitabine-induced TMA, with improvement in hematological and renal outcomes. Furthermore, as our case illustrates, our patient became independent of dialysis with a major effect on quality of life. It also highlights the importance of accurate diagnosis of TMA when a patient treated with chemotherapy presents with progressive acute kidney injury, hemolysis and thrombocytopenia.


Conclusions

This case report shows promising beneficial effects of eculizumab in gemcitabine-induced TMA, regarding transfusion dependence as well as improvement in renal function. It also shows that larger controlled studies are needed to confirm these effects.


Acknowledgments

Funding: None.


Footnote

Reporting Checklist: The authors have completed the CARE reporting checklist. Available at https://jgo.amegroups.com/article/view/10.21037/jgo-22-509/rc

Conflicts of Interest: All authors have completed the ICMJE uniform disclosure form (available at https://jgo.amegroups.com/article/view/10.21037/jgo-22-509/coif). KC has received consultancy fees from Alexion, Astellas, Sanofi. The other authors have no conflicts of interest to declare.

Ethical Statement: The authors are accountable for all aspects of the work in ensuring that questions related to the accuracy or integrity of any part of the work are appropriately investigated and resolved. All procedures performed in this study were in accordance with the ethical standards of the institutional and/or national research committee(s) and with the Declaration of Helsinki (as revised in 2013). Written informed consent was obtained from the patient for publication of this case report and the accompanying image. A copy of the written consent is available for review by the editorial office of this journal.

Open Access Statement: This is an Open Access article distributed in accordance with the Creative Commons Attribution-NonCommercial-NoDerivs 4.0 International License (CC BY-NC-ND 4.0), which permits the non-commercial replication and distribution of the article with the strict proviso that no changes or edits are made and the original work is properly cited (including links to both the formal publication through the relevant DOI and the license). See: https://creativecommons.org/licenses/by-nc-nd/4.0/.


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Cite this article as: Van den Eeckhaut L, Hannon H, Schurgers M, Monsaert E, Claes K. Gemcitabine-induced thrombotic microangiopathy treated with eculizumab: a case report. J Gastrointest Oncol 2022;13(6):3314-3320. doi: 10.21037/jgo-22-509

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