de Silva Harini D, Ffrench Rosemary A, Korem Maya, Orlowski Eva, Curtis David J, Spencer Andrew, Avery Sharon, Patil Sushrut, Morrissey Catherine Orla
Burnet Institute Life Sciences Discipline Melbourne VIC Australia.
Department of Infectious Diseases Alfred Health and Monash University Melbourne VIC Australia.
Clin Transl Immunology. 2018 Oct 5;7(10):e1040. doi: 10.1002/cti2.1040. eCollection 2018.
Infections are a major cause of mortality after allogeneic haemopoietic stem cell transplantation (alloHSCT), and immune recovery is necessary for prevention. Novel transplant procedures have changed the epidemiology of infections but contemporary data on functional immune recovery are limited. In this pilot study, we aimed to measure immune recovery in the current era of alloHSCT.
Twenty, 13, 11, 9 and 9 alloHSCT recipients had blood collected at baseline (time of conditioning) and 3-, 6-, 9-, and 12-months post-alloHSCT, respectively. Clinical data were collected, and immune recovery was measured using immunophenotyping, lymphocyte proliferation, cytokine analysis and antibody isotyping.
Median absolute T- and B-cell counts were below normal from baseline until 9- to 12-months post-alloHSCT. Median absolute CD4 T-cell counts recovered at 12-months post-alloHSCT. Positive proliferative responses to , cytomegalovirus (CMV), Epstein-Barr virus (EBV), influenza and tetanus antigens were detected from 9 months. IL-6 was the most abundant cytokine in cell cultures. In cultures stimulated with CMV, EBV, influenza and tetanus peptides, the CD4 T-cell count correlated with IL-1β (=0.045) and CD8 T-cell count with IFNγ (=0.013) and IL-1β (=0.012). The NK-cell count correlated with IL-1β (=0.02) and IL-17a (=0.03). Median serum levels of IgG1, IgG2 and IgG3 were normal while IgG4 and IgA were below normal range throughout follow-up.
This pilot study demonstrates that immune recovery can be measured using CD4 T-cell counts, antigen stimulation and selected cytokines (IFNγ, IL-1β, IL-4, IL-6, IL-17, IL-21, IL-31) in alloHSCT recipients. While larger studies are required, monitoring immune recovery may have utility in predicting infection risk post-alloHSCT.
感染是异基因造血干细胞移植(alloHSCT)后死亡的主要原因,免疫恢复是预防感染所必需的。新型移植程序改变了感染的流行病学,但关于功能性免疫恢复的当代数据有限。在这项试点研究中,我们旨在测定当前alloHSCT时代的免疫恢复情况。
分别有20例、13例、11例、9例和9例alloHSCT受者在基线(预处理时)以及alloHSCT后3个月、6个月、9个月和12个月采集血液。收集临床数据,并使用免疫表型分析、淋巴细胞增殖、细胞因子分析和抗体分型来测定免疫恢复情况。
从基线到alloHSCT后9至12个月,T细胞和B细胞的绝对计数中位数均低于正常水平。CD4 T细胞的绝对计数中位数在alloHSCT后12个月恢复。从9个月起检测到对巨细胞病毒(CMV)、EB病毒(EBV)、流感和破伤风抗原的阳性增殖反应。IL-6是细胞培养物中最丰富的细胞因子。在用CMV、EBV、流感和破伤风肽刺激的培养物中,CD4 T细胞计数与IL-1β相关(r = 0.045),CD8 T细胞计数与IFNγ相关(r = 0.013)和IL-1β相关(r = 0.012)。自然杀伤细胞(NK)计数与IL-1β相关(r = 0.02)和IL-17a相关(r = 0.03)。在整个随访过程中,IgG1、IgG2和IgG3的血清水平中位数正常,而IgG4和IgA低于正常范围。
这项试点研究表明,可使用CD4 T细胞计数、抗原刺激和选定的细胞因子(IFNγ、IL-1β、IL-4、IL-6、IL-17、IL-21、IL-31)来测定alloHSCT受者的免疫恢复情况。虽然需要更大规模的研究,但监测免疫恢复可能有助于预测alloHSCT后的感染风险。
