QIMR Centre for Immunotherapy and Vaccine Development, QIMR Berghofer Medical Research Institute, Brisbane, Australia.
South Australian Lung Transplant Unit, Department of Thoracic Medicine, Royal Adelaide Hospital, Adelaide, Australia.
Clin Infect Dis. 2019 Feb 1;68(4):632-640. doi: 10.1093/cid/ciy549.
Opportunistic infections including cytomegalovirus (CMV) are a major cause of morbidity and mortality in solid organ transplant (SOT) recipients. The recurrent and protracted use of antiviral drugs with eventual emergence of drug resistance represents a significant constraint to therapy. Although adoptive T-cell therapy has been successfully used in hematopoietic stem cell transplant recipients, its extension to the SOT setting poses a considerable challenge because of the inhibitory effects of immunosuppressive drugs on the virus-specific T-cell response in vivo and the perceived risk of graft rejection.
In this prospective study, 22 SOT recipients (13 renal and 8 lung and 1 heart transplants) with recurrent or ganciclovir-resistant CMV infection were recruited, and 13 of them were treated with in vitro-expanded autologous CMV-specific T cells. These patients were monitored for safety, clinical symptoms, and immune reconstitution.
Autologous CMV-specific T-cell manufacture was attempted for 21 patients, and was successful in 20. The use of this adoptive immunotherapy was associated with no therapy-related serious adverse events. Eleven (84%) of the 13 treated patients showed improvement in symptoms, including complete resolution or reduction in DNAemia and CMV-associated end-organ disease and/or the cessation or reduced use of antiviral drugs. Furthermore, four of these patients showed coincident increased frequency of CMV-specific T cells in peripheral blood after completion of T-cell therapy.
The data presented here demonstrate for the first time the clinical safety of CMV-specific adoptive T-cell therapy and its potential therapeutic benefit for SOT recipients with recurrent and/or drug-resistant CMV infection or disease.
ACTRN12613000981729.
机会性感染,包括巨细胞病毒(CMV),是实体器官移植(SOT)受者发病率和死亡率的主要原因。抗病毒药物的反复和长期使用,最终导致耐药性的出现,这对治疗构成了重大限制。虽然过继性 T 细胞疗法已成功应用于造血干细胞移植受者,但将其扩展到 SOT 环境中存在相当大的挑战,因为免疫抑制剂对体内病毒特异性 T 细胞反应的抑制作用以及对移植物排斥的感知风险。
在这项前瞻性研究中,招募了 22 名患有复发性或更昔洛韦耐药 CMV 感染的 SOT 受者(13 名肾移植、8 名肺移植和 1 名心脏移植),其中 13 名接受了体外扩增的自体 CMV 特异性 T 细胞治疗。这些患者的安全性、临床症状和免疫重建情况进行了监测。
尝试为 21 名患者制造自体 CMV 特异性 T 细胞,其中 20 名成功。这种过继免疫疗法的使用与无治疗相关的严重不良事件无关。在接受治疗的 13 名患者中,有 11 名(84%)患者的症状得到改善,包括 DNA 血症和 CMV 相关终末器官疾病的完全缓解或减少,以及抗病毒药物的停用或减少。此外,在 T 细胞治疗完成后,其中 4 名患者的外周血中 CMV 特异性 T 细胞的频率也同时增加。
这里提供的数据首次证明了 CMV 特异性过继性 T 细胞治疗的临床安全性及其对复发性和/或耐药性 CMV 感染或疾病的 SOT 受者的潜在治疗益处。
ACTRN12613000981729。
