Kim Tae Woo, Lee Sung-Eun, Lim Ji-Young, Ryu Da-Bin, Jeon Young-Woo, Yoon Jae-Ho, Cho Byung-Sik, Eom Ki-Seong, Kim Yoo-Jin, Kim Hee-Je, Lee Seok, Cho Seok-Goo, Kim Dong-Wook, Lee Jong Wook, Min Woo-Sung, Min Chang-Ki
Department of Hematology, Seoul St. Mary's Hospital, College of Medicine, The Catholic University of Korea, Seoul, Korea.
Catholic Leukemia Research Institute, The Catholic University of Korea, Seoul, Korea.
Transpl Infect Dis. 2017 Feb;19(1). doi: 10.1111/tid.12643. Epub 2017 Jan 10.
Few studies have been performed to identify factors that are associated with an increased risk of infections during the neutropenic period in patients undergoing allogeneic stem cell transplantation (allo-SCT). The aim of this study was to identify the host immune cells responsible for infections before engraftment.
A total of 282 patients who underwent allo-SCT were enrolled. Peripheral blood samples were collected before conditioning therapy. Expression of CD161-expressing T cells, natural killer cells, and immature myeloid cells was analyzed by flow cytometry. Microbially and clinically defined infections and fevers of unknown origin as proposed by the Immunocompromised Host Society were included in this study.
The median age was 45 years (range, 16-68 years). Patients had various hematologic disorders and were transplanted from human leukocyte antigen (HLA)-matched siblings, unrelated donors, and familial HLA-mismatched donors. In univariate analysis, younger age and a familial HLA-mismatched donor were risk factors for the occurrence of infections. After adjusting for potential variables in univariate analysis, multivariate analyses revealed that a lower frequency of CD3 CD4 CD161 cells was significantly associated with the occurrence of neutropenic infections. An age of 35 years or younger and allografting from familial HLA-mismatched donors showed a trend toward higher infection rates.
Our data indicated that a lower frequency of CD3 CD4 CD161 T cells in peripheral blood before conditioning therapy was associated with a higher incidence of infection during the neutropenic period. These results suggest that recipient innate T cells with expression of C-type lectin CD161 can guard against infections before engraftment.
很少有研究致力于确定与异基因干细胞移植(allo-SCT)患者中性粒细胞减少期感染风险增加相关的因素。本研究的目的是确定移植前引发感染的宿主免疫细胞。
共纳入282例接受allo-SCT的患者。在预处理治疗前采集外周血样本。通过流式细胞术分析表达CD161的T细胞、自然杀伤细胞和未成熟髓样细胞的表达情况。本研究纳入了免疫受损宿主协会提出的微生物学和临床定义的感染以及不明原因发热。
中位年龄为45岁(范围16 - 68岁)。患者患有各种血液系统疾病,且供体来自人类白细胞抗原(HLA)匹配的同胞、无关供体以及家族性HLA不匹配的供体。单因素分析中,年龄较小和家族性HLA不匹配的供体是感染发生的危险因素。在对单因素分析中的潜在变量进行校正后,多因素分析显示CD3 CD4 CD161细胞频率较低与中性粒细胞减少期感染的发生显著相关。35岁及以下的年龄以及来自家族性HLA不匹配供体的同种异体移植显示出感染率较高的趋势。
我们的数据表明,预处理治疗前外周血中CD3 CD4 CD161 T细胞频率较低与中性粒细胞减少期感染发生率较高相关。这些结果表明,表达C型凝集素CD161的受体天然T细胞可在移植前预防感染。
