Maternal microchimerism in cord blood and risk of childhood‐onset type 1 diabetes

微嵌合体 医学 脐带血 1型糖尿病 优势比 人类白细胞抗原 数字聚合酶链反应 免疫学 胎儿 队列 脐带 内科学 怀孕 糖尿病 聚合酶链反应 抗原 内分泌学 遗传学 生物 基因
作者
German Tapia,Georgina Mortimer,Jody Ye,Benjamin T. Gillard,Saranna Chipper‐Keating,Karl Mårild,Marte K. Viken,Benedicte A. Lie,Geir Joner,Torild Skrivarhaug,Pål R. Njølstad,Ketil Størdal,Kathleen M. Gillespie,Lars C. Stene
出处
期刊:Pediatric Diabetes [Wiley]
被引量:7
标识
DOI:10.1111/pedi.12875
摘要

Background Maternal microchimerism (MMc), the transmission of small quantities of maternal cells to the fetus, is relatively common and persistent. MMc has been detected with increased frequency in the circulation and pancreas of type 1 diabetes (T1D) patients. We investigated for the first time whether MMc levels at birth predict future T1D risk. We also tested whether cord blood MMc predicted MMc in samples taken at T1D diagnosis. Methods Participants in the Norwegian Mother and Child Cohort study were human leukocyte antigen (HLA) class II typed to determine non-inherited, non-shared maternal alleles (NIMA). Droplet digital (dd) polymerase chain reaction (PCR) assays specific for common HLA class II NIMA (HLADQB1*03:01, *04:02, and *06:02/03) were developed and validated. MMc was estimated as maternal DNA quantity in the fetal circulation, by NIMA specific ddPCR, measured in cord blood DNA from 71 children who later developed T1D and 126 controls within the cohort. Results We found detectable quantities of MMc in 34/71 future T1D cases (48%) and 53/126 controls (42%) (adjusted odds ratio [aOR] 1.27, 95% confidence interval (CI) 0.68-2.36), and no significant difference in ranks of MMc quantities between cases and controls (Mann-Whitney P = .46). There was a possible association in the NIMA HLA-DQB1*03:01 subgroup with later T1D (aOR 3.89, 95%CI 1.05-14.4). MMc in cord blood was not significantly associated with MMc at T1D diagnosis. Conclusions Our findings did not support the hypothesis that the degree of MMc in cord blood predict T1D risk. The potential subgroup association with T1D risk should be replicated in a larger cohort.
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