Hematology Center, Beijing Key Laboratory of Pediatric Hematology Oncology; National Key Discipline of Pediatrics (Capital Medical University); Key Laboratory of Major Disease in Children, Ministry of Education; Beijing Children's Hospital, Capital Medical University, National Center for Children's Health, Beijing, 100045, People's Republic of China.
Hematologic Disease Laboratory, Beijing Pediatric Research Institute; Hematology Center, Beijing Key Laboratory of Pediatric Hematology Oncology; National Key Discipline of Pediatrics (Capital Medical University); Key Laboratory of Major Disease in Children, Ministry of Education; Beijing Children's Hospital, Capital Medical University, National Center for Children's Health, Beijing, 100045, People's Republic of China.
Clin Exp Med. 2023 Dec;23(8):4575-4583. doi: 10.1007/s10238-023-01210-1. Epub 2023 Oct 16.
To review and summarize the clinical features, treatment strategies, and prognosis of subcutaneous panniculitis-like T-cell lymphoma complicated with hemophagocytic lymphohistiocytosis (SPTCL-HLH). We searched the Web of Science, Embase, Cochrane Library, and PubMed databases. The keywords were subcutaneous panniculitis-like T-cell lymphoma and hemophagocytic lymphohistiocytosis or hemophagocytic syndrome. The patients were divided into a mutated group and a wild-type group based on the existence of HAVCR2 gene mutation. A total of 45 reports, including 63 patients with SPTCL-HLH, were included in the systematic review. Twelve patients detected gene mutations, including 11 with the HAVCR2 gene mutation and 1 with the STXBP2 gene mutation. Thirty-one patients were tested for autoantibodies. Compared with the wild-type group, patients in the mutated group were younger (p = 0.017), and the autoantibody-positive rate was higher (p = 0.006). The main treatment target of 17 patients was to control HLH, yielding an ORR of 88.2%. Two cases relapsed, and both were treated with corticosteroid monotherapy. The corticosteroid monotherapy experienced a higher recurrence rate than the corticosteroids plus other immunoregulatory agents therapy (66.7 vs. 0.0%, p = 0.029). Eighteen patients received initial anthracycline-based chemotherapy, and 50.0% reached remission. The ORR of initial chemotherapy aiming at controlling HLH was higher than those of anthracycline-based chemotherapy (p = 0.015). The ORR was higher in patients initially controlled for HLH versus chemotherapy without HLH control first (90.5 vs. 61.5%, p = 0.024). Interestingly, one patient with juvenile idiopathic arthritis developed SPTCL-HLH during tocilizumab therapy, discontinuing tocilizumab led to a remission of the disease spontaneously. Sixteen patients received stem cell transplantation (SCT). Fifteen patients, including 5 with relapsed/refractory SPTCL-HLH, responded well and survived after receiving SCT. One case who received a sibling-identical SCT relapsed. Further analysis revealed a homozygous HAVCR2 mutation with the donor. The 2-year overall survival (OS) was 91.0% ± 4.4%. There was a significant difference in the OS among patients of different age groups, and patients aged 40-60 had the lowest 2-year OS (66.7% ± 19.2%). Patients with HAVCR2 gene mutations are younger and more likely to be misdiagnosed with autoimmune diseases. Initial treatment of corticosteroids plus immunoregulatory agents attaches great significance to avoiding too aggressive therapies. Intensive anthracycline-based chemotherapy such as CHOP or CHOP-like regimens can also induce long-term remission for aggressive disease. SCT is still a reliable strategy currently. In addition, a watch and wait approach is recommended in patients with mild SPTCL-HLH caused by drugs. The occurrence of HLH does not necessarily mean a more rapidly progressive disease and worse prognosis in patients with SPTCL, but older patients with SPTCL-HLH may be associated with a lower survival rate.
回顾并总结皮下脂膜炎样 T 细胞淋巴瘤(SPTCL)合并噬血细胞性淋巴组织细胞增生症(HLH)的临床特征、治疗策略及预后。方法:我们检索了 Web of Science、Embase、Cochrane 图书馆和 PubMed 数据库,检索词为“皮下脂膜炎样 T 细胞淋巴瘤”和“噬血细胞性淋巴组织细胞增生症或噬血细胞综合征”。根据是否存在 HAVCR2 基因突变,将患者分为突变组和野生型组。系统评价共纳入 45 篇文献,包括 63 例 SPTCL-HLH 患者。12 例患者检测到基因突变,包括 11 例 HAVCR2 基因突变和 1 例 STXBP2 基因突变。31 例患者检测了自身抗体。与野生型组相比,突变型组患者更年轻(p=0.017),自身抗体阳性率更高(p=0.006)。17 例患者的主要治疗目标是控制 HLH,缓解率为 88.2%。2 例复发,均接受了皮质类固醇单药治疗。皮质类固醇单药治疗的复发率高于皮质类固醇联合其他免疫调节药物治疗(66.7% vs. 0.0%,p=0.029)。18 例患者接受初始蒽环类化疗,50.0%达到缓解。以控制 HLH 为初始化疗目标的缓解率高于以蒽环类化疗为初始化疗目标的缓解率(p=0.015)。与未首先控制 HLH 相比,首先控制 HLH 的患者缓解率更高(90.5% vs. 61.5%,p=0.024)。有趣的是,1 例幼年特发性关节炎患者在接受托珠单抗治疗期间发生 SPTCL-HLH,停用托珠单抗后疾病自发缓解。16 例患者接受了造血干细胞移植(SCT)。15 例患者,包括 5 例复发/难治性 SPTCL-HLH,在接受 SCT 后反应良好并存活。1 例接受同胞同基因 SCT 的患者复发。进一步分析显示,与供体存在纯合 HAVCR2 突变。2 年总生存率(OS)为 91.0%±4.4%。不同年龄组患者的 OS 存在显著差异,40-60 岁患者的 2 年 OS 最低(66.7%±19.2%)。HAVCR2 基因突变患者更年轻,更易误诊为自身免疫性疾病。初始皮质类固醇联合免疫调节药物治疗对避免过于激进的治疗具有重要意义。以 CHOP 或 CHOP 样方案为基础的强化蒽环类化疗也能诱导侵袭性疾病的长期缓解。SCT 目前仍然是一种可靠的策略。此外,对于药物引起的轻度 SPTCL-HLH 患者,建议采用观察等待的方法。HLH 的发生并不一定意味着 SPTCL 患者的疾病进展更快、预后更差,但年龄较大的 SPTCL-HLH 患者可能与生存率较低有关。
