Sepsis and Acute Pancreatitis in Tumor-Stage Mycosis Fungoides and Treatment with Brentuximab-Vedotin

M. Jost
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Abstract

Dear Editor, we report a case of a 67-year-old male patient who was first diagnosed with tumor-stage Mycosis Fungoides (MF) (T3N0M0B0a, clinical stage IIB – current ISCL/EORTC classification) in 2017. During the course of the disease of MF the patient was treated with bexarotene, gemcitabine and chlorambucil. All these treatments helped only short-term, quickly followed by relapses of the skin lesions. In September 2018, the patient developed a rapidly progressive disease with erythematous patches, plaques and ulcerated tumors (mSWAT 20) (Fig. 1). CD30 expression was determined in several skin biopsies, each with an expression rate of 2-5% (Fig. 1). Despite this relatively low amount, the tumor board decision was made favoring the monoclonal CD30-antibody Brentuximab-Vedotin (BV) application. In October 2018, BV was first administered with the maximum dose of 180 mg (1.8mg/kg of body weight). Five days after the infusion, the patient developed abdominal pain, diarrhea, chills and fever. Blood cultures were positive for Methicillin-Resistant Staphylococcus Aureus (MRSA) and a MRSA-sepsis was diagnosed. Intensive medical care was requiredand under symptomatic treatment, the patient recovered completely. Two months later – in December 2018 – the patient presented again in our department to evaluate the skin lesions, displaying a partial response (mSWAT 12) (Fig. 1). At this time, the sepsis was not considered in direct context with the medication. The patient had several ulcerations and had been a known MRSA-patient already before the initiation of the treatment. Therefore, the patient received BV for a second time in the total dose of 180 mg. Nine days after the infusion, abdominal pain with vomiting, diarrhea and unconsciousness occurred. The patient was readmitted to the intensive care unit and an acute pancreatitis was diagnosed (lipase 1502 U/l). Under symptomatic therapy and close monitoring, pancreatitis resolved within two weeks. BV is a CD30 antibody-drug conjugate. The cytotoxic component is monomethylauristatin E, a potent inhibitor of microtubule assembly [1]. It is approved for the treatment of patients with relapsed or refractory Hodgkin’s Lymphoma (HL), systemic Anaplastic Large-T-cell Lymphoma (sALCL) and in addition, for the treatment of CD30-positive Cutaneous T-cell Lymphoma (CTCL) [2]. This case report describes two serious complications after the administration of BV in the same patient. Both belong in the spectrum of rare to infrequent side effects. Awareness of the possibility of pancreatitis as a side effect of BV is essential, especially because it seems to occur not immediately but within days or weeks after the treatment application. The literature describes pancreatitis in patients with HL, ALCL and cutaneous Gamma Delta T-cell Lymphoma (GD-TCL) [3]. The onset of pancreatitis in most cases seems to be delayed with a range of 7-33 days [1,4]. In our patient the first symptoms presented nine days after the BV-administration. Acute pancreatitis can lead to fatal outcomes. BV reinduction should be carefully discussed. However, in patients without any other treatment options, it might be possible to reinduce BV without the risk of side effect recurrence [1,3].
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肿瘤期蕈样真菌病脓毒症和急性胰腺炎及Brentuximab-Vedotin治疗
亲爱的编辑,我们报告一例67岁男性患者,于2017年首次被诊断为肿瘤期蕈样真菌病(MF) (T3N0M0B0a,临床分期IIB -目前ISCL/EORTC分类)。在MF疾病过程中,患者接受贝沙罗汀、吉西他滨和氯霉素治疗。所有这些治疗都只是短期的,很快皮肤损伤就会复发。2018年9月,患者出现了快速进展的疾病,伴有红斑斑块、斑块和肿瘤溃疡(mSWAT 20)(图1)。在几次皮肤活检中检测到CD30表达,每次表达率为2-5%(图1)。尽管表达率相对较低,但肿瘤委员会还是决定支持单克隆CD30抗体Brentuximab-Vedotin (BV)应用。2018年10月,首次施用BV,最大剂量为180 mg (1.8mg/kg体重)。输液5天后,患者出现腹痛、腹泻、寒战和发热。血液培养阳性耐甲氧西林金黄色葡萄球菌(MRSA),诊断为MRSA败血症。病人在接受对症治疗后完全康复。两个月后,即2018年12月,患者再次来到我科评估皮肤病变,显示部分反应(mSWAT 12)(图1)。此时,脓毒症并未被认为与药物直接相关。患者有几处溃疡,在开始治疗之前已经是已知的mrsa患者。因此,患者第二次接受BV治疗,总剂量为180mg。输液后第9天出现腹痛并呕吐、腹泻、意识不清。患者再次入住重症监护室,诊断为急性胰腺炎(脂肪酶1502 U/l)。在对症治疗和密切监测下,胰腺炎在两周内消退。BV是一种CD30抗体-药物偶联物。细胞毒性成分是单甲月桂素E,一种有效的微管组装抑制剂[1]。它被批准用于治疗复发或难治性霍奇金淋巴瘤(HL)、全身性间变性大t细胞淋巴瘤(sALCL)以及cd30阳性皮肤t细胞淋巴瘤(CTCL)患者[2]。本病例报告描述了同一患者服用BV后的两个严重并发症。两者都属于罕见或不常见的副作用范围。认识到细菌性阴道炎作为细菌性阴道炎副作用的可能性是必要的,特别是因为它似乎不是立即发生,而是在治疗应用后的几天或几周内发生。文献报道了HL、ALCL和皮肤γ δ t细胞淋巴瘤(GD-TCL)患者的胰腺炎[3]。在大多数病例中,胰腺炎的发病似乎延迟了7-33天[1,4]。本例患者在bv给药后9天出现首次症状。急性胰腺炎可导致致命的后果。BV的再归纳应该仔细讨论。然而,在没有其他治疗选择的患者中,有可能在没有副作用复发风险的情况下重新诱导BV[1,3]。
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