Cancer Vaccine Center and Departments of Medical Oncology and Biostatistics and Computational Biology, Dana-Farber Cancer Institute, Boston, Massachusetts 02115, USA.
Cancer Res. 2010 Feb 15;70(4):1344-55. doi: 10.1158/0008-5472.CAN-09-3143. Epub 2010 Feb 2.
Patients with chronic lymphocytic leukemia (CLL) who relapse after allogeneic transplant may achieve durable remission following donor lymphocyte infusion (DLI), showing the potency of donor-derived immunity in eradicating tumors. We sought to elucidate the antigenic basis of the effective graft-versus-leukemia (GvL) responses associated with DLI for the treatment of CLL by analyzing the specificity of plasma antibody responses developing in two DLI-treated patients who achieved long-term remission without graft-versus-host disease. By probing high-density protein microarrays with patient plasma, we discovered 35 predominantly intracellular antigens that elicited high-titer antibody reactivity greater in post-DLI than in pre-DLI plasma. Three antigens-C6orf130, MDS032, and ZFYVE19-were identified by both patients. Along with additional candidate antigens DAPK3, SERBP1, and OGFOD1, these proteins showed higher transcript and protein expression in B cells and CLL cells compared with normal peripheral blood mononuclear cells. DAPK3 and the shared antigens do not represent minor histocompatibility antigens, as their sequences are identical in both donor and tumor. Although ZFYVE19, DAPK3, and OGFOD1 elicited minimal antibody reactivity in 12 normal subjects and 12 chemotherapy-treated CLL patients, 5 of 12 CLL patients with clinical GvL responses were serologically reactive to these antigens. Moreover, antibody reactivity against these antigens was temporally correlated with clinical disease regression. These B-cell antigens represent promising biomarkers of effective anti-CLL immunity.
慢性淋巴细胞白血病 (CLL) 患者在异体移植后复发,可能会在供体淋巴细胞输注 (DLI) 后获得持久缓解,这表明供体来源的免疫在消除肿瘤方面具有强大的作用。我们试图通过分析两名接受 DLI 治疗并长期缓解且无移植物抗宿主病的患者的血浆抗体反应特异性,阐明与 DLI 治疗 CLL 相关的有效移植物抗白血病 (GvL) 反应的抗原基础。通过用患者血浆探测高密度蛋白质微阵列,我们发现了 35 种主要位于细胞内的抗原,这些抗原在 DLI 后比 DLI 前的血浆中产生了更高滴度的抗体反应性。两名患者都鉴定出了三种抗原-C6orf130、MDS032 和 ZFYVE19。除了其他候选抗原 DAPK3、SERBP1 和 OGFOD1 外,这些蛋白质在 B 细胞和 CLL 细胞中的转录和蛋白表达水平均高于正常外周血单核细胞。DAPK3 和共享抗原不是次要组织相容性抗原,因为它们在供体和肿瘤中是相同的。尽管 ZFYVE19、DAPK3 和 OGFOD1 在 12 名正常受试者和 12 名接受化疗的 CLL 患者中仅引起了最小的抗体反应性,但在 12 名具有临床 GvL 反应的 CLL 患者中有 5 名对这些抗原呈血清学反应。此外,针对这些抗原的抗体反应性与临床疾病消退具有时间相关性。这些 B 细胞抗原代表了有效的抗 CLL 免疫的有希望的生物标志物。