Porter D L, Luger S M, Duffy K M, Stadtmauer E A, Laport G, Schuster S J, Orloff G, Tsai D, McDaid K, Kathakali A, Leonard D G, Antin J H
Bone Marrow and Stem Cell Transplant Program, University of Pennsylvania Medical Center, Philadelphia 19104, USA.
Biol Blood Marrow Transplant. 2001;7(4):230-8. doi: 10.1053/bbmt.2001.v7.pm11349810.
Allogeneic donor leukocytes can be used after nonmyeloablative conditioning to exploit their graft-versus-tumor (GVT) activity in the setting of reduced conditioning-regimen toxicity. This approach may be particularly useful for patients who relapse after autologous stem cell transplantation (SCT). However, GVT activity, toxicity, and ability to establish mixed chimerism may differ in patients who were heavily pretreated prior to SCT compared with patients treated earlier in the course of their disease. We have performed a series of studies of nonmyeloablative allogeneic transplantation and present data on the subset of 14 patients treated for relapse after autologous SCT: 4 patients received no conditioning and unstimulated donor leukocyte infusions (DLI), 10 patients received conditioning with fludarabine and cyclophosphamide followed by unstimulated or granulocyte-colony-stimulating factor (G-CSF)-stimulated allogeneic peripheral blood stem cells (PBSCs), 4 patients received no graft-versus-host disease (GVHD) prophylaxis, and 10 patients received cyclosporine GVHD prophylaxis. All but 1 patient had sustained donor chimerism at least 30 days after allogeneic cell therapy (ACT), and 8 patients had more than 80% donor chimerism after ACT. Acute GVHD developed in 11 patients (grade III-IV, n = 6). Aplasia was more frequent in the patients receiving unstimulated PBSCs, despite the development of mixed chimerism. There were 6 complete responses and 4 partial responses; response was independent of conditioning and growth-factor stimulation of the donor graft. Five patients died of treatment-related causes and 4 patients died from progressive disease. Four patients remained alive 27 to 194 weeks (median, 66 weeks) after ACT. Prior autologous SCT may define a subset of patients at particularly high risk for GVHD and other toxicity after ACT. However, these data show that ACT with either DLI or G-CSF-stimulated blood cells results in direct GVT activity in some patients with Hodgkin's disease, myeloma, and non-Hodgkin's lymphoma, even after relapse from autologous SCT. Most patients developed donor chimerism with minimal conditioning. Alternative prophylactic regimens that control GVHD while maintaining GVT are needed to improve outcomes in these heavily pretreated patients.
在非清髓性预处理后可使用异基因供体白细胞,以在降低预处理方案毒性的情况下利用其移植物抗肿瘤(GVT)活性。这种方法对于自体干细胞移植(SCT)后复发的患者可能特别有用。然而,与疾病病程早期接受治疗的患者相比,在SCT前接受过大量预处理的患者的GVT活性、毒性以及建立混合嵌合体的能力可能有所不同。我们进行了一系列非清髓性异基因移植研究,并给出了14例自体SCT后复发接受治疗的患者亚组的数据:4例患者未接受预处理且输注未刺激的供体白细胞(DLI),10例患者接受氟达拉滨和环磷酰胺预处理,随后输注未刺激的或粒细胞集落刺激因子(G-CSF)刺激的异基因外周血干细胞(PBSC),4例患者未接受移植物抗宿主病(GVHD)预防,10例患者接受环孢素GVHD预防。除1例患者外,所有患者在异基因细胞治疗(ACT)后至少30天维持供体嵌合体状态,8例患者在ACT后供体嵌合体比例超过80%。11例患者发生急性GVHD(Ⅲ-Ⅳ级,n = 6)。尽管出现了混合嵌合体,但接受未刺激PBSC输注的患者中再生障碍性贫血更为常见。有6例完全缓解和4例部分缓解;缓解与供体移植物的预处理和生长因子刺激无关。5例患者死于治疗相关原因,4例患者死于疾病进展。4例患者在ACT后27至194周(中位值,66周)仍存活。既往自体SCT可能确定了一部分ACT后发生GVHD和其他毒性风险特别高的患者亚组。然而,这些数据表明,对于一些霍奇金淋巴瘤、骨髓瘤和非霍奇金淋巴瘤患者,即使在自体SCT复发后,采用DLI或G-CSF刺激的血细胞进行ACT也会产生直接的GVT活性。大多数患者在进行最小程度预处理后形成了供体嵌合体。需要能在维持GVT的同时控制GVHD的替代预防方案,以改善这些经过大量预处理患者的治疗结局。
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