Department of Bone Marrow Transplantation, University Hospital Essen, Essen, Germany.
Institute for Transfusion Medicine, University Hospital Essen, Essen, Germany.
Front Immunol. 2020 Jan 10;10:3027. doi: 10.3389/fimmu.2019.03027. eCollection 2019.
HLA-E is a member of the non-classical HLA molecules and by interaction with activating or inhibitory receptors of NK and T cells, HLA-E can lead to immune activation or suppression context-dependently. Recently, the non-classical HLA molecules gain more attention in the setting of allogeneic hematopoietic stem cell transplantation (HSCT). Most studies so far have focused on the two most frequent genotypes (HLA-E01:01 and HLA-E01:03) and investigated their potential association with clinical endpoints of HSCT, like graft-versus-host disease (GvHD), relapse, and overall survival (OS). However, these studies have produced inconsistent results regarding the role of HLA-E and the clinical endpoints after HSCT. We therefore here investigate the amount of soluble HLA-E (sHLA-E) in patients following HSCT and relate this to the clinical endpoints after HSCT. In univariate analysis, we observe a significant association of reduced levels of sHLA-E with severe acute GvHD, extended chronic GvHD and with inferior OS. Using receiver operating characteristic analyses specific thresholds obtained 1, 2, or 3 month(s) after HSCT were identified being indicative for severe acute GvHD, extended chronic GvHD, or inferior OS. In sub-group analyses, this effect can be confirmed in patients not treated with ATG, but is derogated in ATG-treated patients. Notably, we could not detect any association of the course of sHLA-E levels post-HSCT with the three most frequent HLA-E genotypes (HLA-E*01:03/01:03, HLA-E01:01/01:01, HLA-E01:01/01:03). However, with regard to 5-year-OS there was an association of HLA-E01:03 homozygosity with inferior OS. Taking ATG-treatment, recipient and donor HLA-E genotypes into consideration among other well-known risk factors, the sHLA-E status was found as an independent predictor for the development of extended cGvHD and inferior OS following HSCT irrespective of the sHLA-E thresholds. These findings shed some light on the possible impact of reduced sHLA-E levels after HSCT on GvHD and OS. Thus, sHLA-E appears to be a novel promising candidate for the prediction of clinical HSCT outcome with regards to extended cGvHD and OS.
HLA-E 是一种非经典 HLA 分子,通过与 NK 和 T 细胞的激活或抑制受体相互作用,HLA-E 可以根据上下文导致免疫激活或抑制。最近,非经典 HLA 分子在异基因造血干细胞移植(HSCT)中受到了更多的关注。到目前为止,大多数研究都集中在两种最常见的基因型(HLA-E01:01 和 HLA-E01:03)上,并研究了它们与 HSCT 的临床终点(如移植物抗宿主病[GvHD]、复发和总生存[OS])之间的潜在关联。然而,这些研究对于 HLA-E 及其在 HSCT 后的临床终点的作用产生了不一致的结果。因此,我们在这里研究了 HSCT 后患者可溶性 HLA-E(sHLA-E)的含量,并将其与 HSCT 后的临床终点联系起来。在单因素分析中,我们观察到 sHLA-E 水平降低与严重急性 GvHD、扩展慢性 GvHD 和 OS 降低显著相关。使用接收者操作特征分析,在 HSCT 后 1、2 或 3 个月获得了特定的阈值,这些阈值可用于指示严重急性 GvHD、扩展慢性 GvHD 或 OS 降低。在亚组分析中,在未接受 ATG 治疗的患者中可以证实这种影响,但在接受 ATG 治疗的患者中则被削弱。值得注意的是,我们没有检测到 HSCT 后 sHLA-E 水平的变化与三种最常见的 HLA-E 基因型(HLA-E*01:03/01:03、HLA-E01:01/01:01、HLA-E01:01/01:03)之间有任何关联。然而,在 5 年 OS 方面,HLA-E01:03 纯合子与 OS 降低有关。在考虑到 ATG 治疗、受者和供者 HLA-E 基因型等其他已知危险因素的情况下,sHLA-E 状态被发现是 HSCT 后发生扩展 cGvHD 和 OS 降低的独立预测因子,与 sHLA-E 阈值无关。这些发现为 HSCT 后 sHLA-E 水平降低对 GvHD 和 OS 的可能影响提供了一些线索。因此,sHLA-E 似乎是一种新的有前途的候选物,可以预测与扩展 cGvHD 和 OS 相关的 HSCT 临床结局。
