Reuthner K, Aubele P, Menhart K, Rath P, Harrer D C, Herr W, Hahn J, Vogelhuber M, Heudobler D, Lueke F, Reichle A, Grube M
Department of Internal Medicine III, Hematology and Oncology, University Hospital of Regensburg, Regensburg, Germany.
Medical Care Center (MVZ), Oncology, Hospital of Straubing, Straubing, Germany.
Front Pharmacol. 2024 Feb 20;15:1334233. doi: 10.3389/fphar.2024.1334233. eCollection 2024.
Targeted chemotherapy and immune checkpoint inhibitors (ICPi) have expanded the spectrum of therapies for patients with relapsed/refractory (r/r) Hodgkin's disease and significantly improved the proportion of patients with long-term disease control. However, there is no standardized therapeutic option in case of further progression. Recently, we demonstrated that therapy with MEPED (metronomic chemotherapy, everolimus, pioglitazone, etoricoxib, dexamethasone) is highly effective in patients with r/r Hodgkin's disease. The benefit after pre-treatment with ICPi has not been studied, yet. Here, we report a patient with progressive Hodgkin's disease on Pembrolizumab for the first time who achieved sustained complete remission (CR) after initiation of MEPED therapy. A 57-year-old patient was pre-treated with brentuximab vedotin for relapsed advanced Hodgkin's disease and had received Pembrolizumab for progression from November 2020 to July 2022. Due to further progression, MEPED therapy was started in August 2022 and continued until May 2023. It consisted of a strictly oral daily (28-day cycle) application of low-dose treosulfan 250 mg, everolimus 15 mg, pioglitazone 45 mg, etoricoxib 60 mg, and dexamethasone 0.5 mg. Treatment response was evaluated by F-18 FDG-PET/CT (PET/CT). CR was defined by a negative Deauville score (DS) of 1-3. Already 3 months after starting MEPED, a CR (DS: 3) was confirmed by PET/CT in November 2022. The next follow-up in May 2023 continued to show CR (DS: 3). The therapy was very well tolerated. No hematological or other organ toxicity was observed. However, in May 2023 the patient presented with leg edema and weight gain, most likely due to pioglitazone and the PET/CT revealed suspected everolimus-induced pneumonitis, so MEPED was discontinued and diuretic therapy and treatment with prednisolone was started with gradual dose reduction. This resulted in a rapid complete resolution of the symptoms. The next PET-CT in July 2023 continued to show CR (DS: 3) without evidence of pneumonitis. Currently, therapy with MEPED has not been resumed. In conclusion, we demonstrate for the first time that MEPED therapy is highly effective in a patient with Hodgkin's disease who has been refractory to ICPi. Sustained CR was achieved over 11 months after initiation of MEPED therapy. Further studies on a larger patient cohort should be performed.
靶向化疗和免疫检查点抑制剂(ICPi)扩大了复发/难治性(r/r)霍奇金淋巴瘤患者的治疗范围,并显著提高了长期疾病控制患者的比例。然而,在疾病进一步进展的情况下,尚无标准化的治疗方案。最近,我们证明了MEPED(节拍化疗、依维莫司、吡格列酮、依托考昔、地塞米松)治疗对r/r霍奇金淋巴瘤患者高度有效。此前尚未研究过ICPi预处理后的获益情况。在此,我们首次报告一例接受派姆单抗治疗后疾病进展的霍奇金淋巴瘤患者,在开始MEPED治疗后实现了持续完全缓解(CR)。一名57岁患者曾接受本妥昔单抗治疗复发的晚期霍奇金淋巴瘤,并于2020年11月至2022年7月因疾病进展接受派姆单抗治疗。由于疾病进一步进展,于2022年8月开始MEPED治疗并持续至2023年5月。该治疗方案包括每日严格口服(28天周期)低剂量曲奥舒凡250mg、依维莫司15mg、吡格列酮45mg、依托考昔60mg和地塞米松0.5mg。通过F-18 FDG-PET/CT(PET/CT)评估治疗反应。CR定义为Deauville评分(DS)为1-3分阴性。在开始MEPED治疗仅3个月后,2022年11月PET/CT证实达到CR(DS:3)。2023年5月的下一次随访仍显示为CR(DS:3)。该治疗耐受性良好。未观察到血液学或其他器官毒性。然而,2023年5月患者出现腿部水肿和体重增加,很可能是由于吡格列酮所致,且PET/CT显示疑似依维莫司诱导的肺炎,因此停用MEPED并开始利尿剂治疗和泼尼松龙治疗,逐渐减量。这导致症状迅速完全缓解。2023年7月的下一次PET-CT仍显示为CR(DS:3),且无肺炎证据。目前,尚未恢复MEPED治疗。总之,我们首次证明MEPED治疗对一名对ICPi耐药的霍奇金淋巴瘤患者高度有效。在开始MEPED治疗11个月后实现了持续CR。应针对更大规模的患者队列进行进一步研究。
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