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使用人源化抗CD2单克隆抗体Medi-507进行非清髓性预处理后,单倍体相合造血细胞移植受者的自然杀伤细胞恢复、嵌合状态、功能及识别情况

NK cell recovery, chimerism, function, and recognition in recipients of haploidentical hematopoietic cell transplantation following nonmyeloablative conditioning using a humanized anti-CD2 mAb, Medi-507.

作者信息

Koenecke Christian, Shaffer Juanita, Alexander Stephen I, Preffer Frederic, Dombkowski David, Saidman Susan L, Dey Bimalanghu, McAfee Steven, Spitzer Thomas R, Sykes Megan

机构信息

Department of Surgery, Massachusetts General Hospital/Harvard Medical School, Boston, Massachusetts 02129, USA.

出版信息

Exp Hematol. 2003 Oct;31(10):911-23. doi: 10.1016/s0301-472x(03)00224-8.

Abstract

OBJECTIVE

Natural killer (NK) cells kill allogeneic cells that lack a class I MHC ligand for clonally distributed killer inhibitory receptors (KIR). Following HLA-mismatched hematopoietic cell transplantation (HCT), donor NK cells might mediate graft-vs-host (GVH) reactions that promote donor chimerism and mediate anti-tumor effects. Additionally, recipient NK cells might mediate donor marrow rejection. We have developed a nonmyeloablative approach to haploidentical HCT involving recipient treatment with a T cell-depleting mAb, Medi-507, that can achieve donor engraftment and mixed hematopoietic chimerism without graft-vs-host disease (GVHD). Donor lymphocyte infusions (DLI) are later administered in an effort to achieve graft-vs-leukemia/lymphoma (GVL) effects without GVHD. It is unknown whether NK cell "tolerance" develops in human mixed chimeras.

METHODS

We have addressed these issues in 12 patients receiving Medi-507-based nonmyeloablative haploidentical HCT.

RESULTS

NK cells recovered relatively early, despite the presence of circulating anti-CD2 mAb, but the majority of initially recovering cells lacked CD2 expression. These NK cells showed a reduced capacity, compared to those from normal donors, to kill class I-deficient targets. No association was detected between KIR mismatches in the host-vs-graft (HVG) or GVH direction and graft or tumor outcomes in this small series. NK cell chimerism did not correlate with chimerism in other lineages in mixed chimeras. NK cell tolerance to the host was not observed in a patient with full donor chimerism. One patient developed NK cell reactivity against donor-derived lymphoblast targets after loss of chimerism, despite the absence of an HVG KIR mismatch.

CONCLUSION

Our results do not show an impact of NK cells on the outcome of nonmyeloablative, even T cell-depleted, HCT across haplotype barriers using an anti-CD2 mAb. Our data also raise questions about the applicability of observations made with NK cell clones to the bulk NK cell repertoire in humans.

摘要

目的

自然杀伤(NK)细胞可杀伤那些缺乏用于克隆性分布的杀伤抑制受体(KIR)的I类MHC配体的同种异体细胞。在HLA不匹配的造血细胞移植(HCT)后,供体NK细胞可能介导移植物抗宿主(GVH)反应,促进供体嵌合现象并介导抗肿瘤效应。此外,受体NK细胞可能介导供体骨髓排斥反应。我们已开发出一种非清髓性单倍体相合HCT方法,包括用一种耗竭T细胞的单克隆抗体Medi-507对受体进行治疗,该方法可实现供体植入和混合造血嵌合现象,且无移植物抗宿主病(GVHD)。随后给予供体淋巴细胞输注(DLI),以期在无GVHD的情况下实现移植物抗白血病/淋巴瘤(GVL)效应。尚不清楚在人类混合嵌合体中是否会产生NK细胞“耐受”。

方法

我们在12例接受基于Medi-507的非清髓性单倍体相合HCT的患者中解决了这些问题。

结果

尽管存在循环抗CD2单克隆抗体,NK细胞恢复相对较早,但最初恢复的细胞大多数缺乏CD2表达。与正常供体来源的NK细胞相比,这些NK细胞杀伤I类缺陷靶标的能力降低。在这个小样本系列中未检测到宿主与移植物(HVG)或GVH方向的KIR错配与移植物或肿瘤结局之间存在关联。NK细胞嵌合现象与混合嵌合体中其他谱系的嵌合现象不相关。在完全供体嵌合的患者中未观察到NK细胞对宿主的耐受。1例患者在嵌合现象消失后,尽管不存在HVG KIR错配,但仍产生了针对供体来源淋巴母细胞靶标的NK细胞反应性。

结论

我们的结果未显示NK细胞对使用抗CD2单克隆抗体跨越单倍型屏障进行的非清髓性(甚至是耗竭T细胞的)HCT结局有影响。我们的数据还对用NK细胞克隆所做观察结果应用于人类总体NK细胞库的适用性提出了疑问。

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