Kawano Noriaki, Kuriyama Takuro, Yoshida Shuro, Kawano Sayaka, Yamano Yoshihisa, Marutsuka Kousuke, Minato Seiichirou, Yamashita Kiyoshi, Ochiai Hidenobu, Shimoda Kazuya, Ishikawa Fumihiko, Kikuchi Ikuo
Department of Internal Medicine, Miyazaki Prefectural Miyazaki Hospital.
J Clin Exp Hematop. 2017;56(3):135-144. doi: 10.3960/jslrt.56.135.
Although a humanized CCR4 antibody (mogamulizumab) was reported to be effective for refractory adult T-cell leukemia-lymphoma (ATL), several reports regarding the use of mogamulizumab before allo-hematopoietic stem cell transplantation (HSCT) strongly indicated a high incidence of severe acute graft-versus-host-disease (GVHD) and treatment-related mortality (TRM). We retrospectively analyzed nine aggressive-type ATL patients who underwent allo-HSCT at a single institution in Miyazaki from 2006.1.1 to 2015.7.31. Among nine ATL patients, three had used mogamulizumab before treatment with allo-HSCT because of the poor control of refractory ATL. All three patients were treated with four to eight cycles of mogamulizumab. The interval from last administration of mogamulizumab to allo-HSCT was two to five months. All three patients with prior mogamulizumab treatment developed mild-moderate acute GVHD (grade 2) 28, 34, or 40 days after allo-HSCT. Acute GVHD was controlled by prednisolone treatment. Two patients in complete remission before allo-HSCT exhibited relatively prolonged survival (survival rate, 66%). Moreover, one patient developed human T-cell leukemia virus type 1-associated myelopathy-mimicking myelitis at five months after allo-HSCT. In contrast, two of six ATL patients without a history of mogamulizumab use survived (survival rate 33%). Thus, in cases of mogamulizumab use before treatment with allo-HSCT for refractory ATL, an appropriately long interval from the last administration of mogamulizumab to allo-HSCT may be one of factors to reduce TRM by acute GVHD, and to subsequently enhance graft-versus-tumor effects in ATL cases. Furthermore, caution is needed when administering mogamulizumab before allo-HSCT for severe GVHD and TRM.
尽管据报道一种人源化CCR4抗体(莫加莫拉单抗)对难治性成人T细胞白血病-淋巴瘤(ATL)有效,但几份关于在异基因造血干细胞移植(HSCT)前使用莫加莫拉单抗的报告强烈表明,严重急性移植物抗宿主病(GVHD)和治疗相关死亡率(TRM)的发生率很高。我们回顾性分析了2006年1月1日至2015年7月31日在宫崎的一家机构接受异基因HSCT的9例侵袭性ATL患者。在9例ATL患者中,3例因难治性ATL控制不佳,在异基因HSCT治疗前使用了莫加莫拉单抗。所有3例患者均接受了4至8个周期的莫加莫拉单抗治疗。从最后一次使用莫加莫拉单抗到异基因HSCT的间隔时间为2至5个月。所有3例先前接受莫加莫拉单抗治疗的患者在异基因HSCT后28、34或40天出现轻至中度急性GVHD(2级)。急性GVHD通过泼尼松龙治疗得到控制。2例在异基因HSCT前完全缓解的患者生存时间相对延长(生存率66%)。此外,1例患者在异基因HSCT后5个月出现了类似1型人类T细胞白血病病毒相关脊髓病的脊髓炎。相比之下,6例无莫加莫拉单抗使用史的ATL患者中有2例存活(生存率33%)。因此,在难治性ATL的异基因HSCT治疗前使用莫加莫拉单抗的情况下,从最后一次使用莫加莫拉单抗到异基因HSCT的适当长间隔时间可能是降低急性GVHD导致的TRM并随后增强ATL病例中移植物抗肿瘤效应的因素之一。此外,在异基因HSCT前使用莫加莫拉单抗时,需要警惕严重GVHD和TRM。