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患有多发性硬化症女性外周血白细胞中的男性微嵌合体。

Male microchimerism in peripheral blood leukocytes from women with multiple sclerosis.

作者信息

Bloch Evan M, Reed William F, Lee Tzong-Hae, Montalvo Leilani, Shiboski Stephen, Custer Brian, Barcellos Lisa F

机构信息

International Research and Training; Blood Systems Research Institute (BSRI); San Francisco, CA, USA.

出版信息

Chimerism. 2011 Jan;2(1):6-10. doi: 10.4161/chim.2.1.15151.

Abstract

BACKGROUND

Fetal microchimerism (F-MC), the persistence of fetal cells in the mother, is frequently encountered following pregnancy. The high prevalence of F-MC in autoimmune disease prompts consideration of the role for immune tolerance and regulation. This study examines the association between F-MC and multiple sclerosis (MS), an autoimmune disorder, of undetermined etiology.

RESULTS

21 out of 51 MS-positive subjects (41%) were classified as positive for F-MC; 4 of 22 (18%) of MS-negative sibling controls, were also positive for MC (p = 0.066). Unanticipated F-MC in controls lead to re-evaluation using 30 female singleton cord blood units (CBUs) as a biological control. Four CBUs were low-level positive.

STUDY DESIGN AND METHODS

Seventy-three female subjects were assigned to three groups according to disease status and pregnancy history: (1) MS positive (+) women with a history of one male pregnancy before symptom onset (n = 27); (2) MS negative (-) female siblings of MS(+) women with a history of one male pregnancy (n = 22); and (3) MS(+) women that reported never having been pregnant (n = 24). Ten micrograms of genomic DNA obtained from peripheral blood leukocytes of each subject were analyzed for F-MC using allele-specific real-time PCR targeting the SR-Y sequence on the Y-chromosome. MC classification was dichotomous (positive vs. negative) based on PCR results.

CONCLUSION

The association between F-MC and MS warrants further study to define this relationship. F-MC in women self-reporting as nulligravid, supports previous findings that a significant proportion of pregnancies go undetected. This lead to re-validation of a Y-chromosome based assay for F-MC detection.

摘要

背景

胎儿微嵌合体(F-MC),即胎儿细胞在母亲体内的持续存在,在妊娠后很常见。F-MC在自身免疫性疾病中的高患病率促使人们考虑其在免疫耐受和调节中的作用。本研究探讨了F-MC与病因不明的自身免疫性疾病——多发性硬化症(MS)之间的关联。

结果

51名MS阳性受试者中有21名(41%)被分类为F-MC阳性;22名MS阴性的同胞对照中有4名(18%)也为MC阳性(p = 0.066)。对照组中意外出现的F-MC导致使用30个女性单胎脐血单位(CBUs)作为生物学对照进行重新评估。4个CBUs为低水平阳性。

研究设计与方法

73名女性受试者根据疾病状态和妊娠史分为三组:(1)症状出现前有一次男性妊娠史的MS阳性(+)女性(n = 27);(2)有一次男性妊娠史的MS(+)女性的MS阴性(-)女性同胞(n = 22);以及(3)报告从未怀孕的MS(+)女性(n = 24)。使用针对Y染色体上SR-Y序列的等位基因特异性实时PCR分析从每个受试者外周血白细胞中获得的10微克基因组DNA,以检测F-MC。根据PCR结果,MC分类为二分法(阳性与阴性)。

结论

F-MC与MS之间的关联值得进一步研究以明确这种关系。自我报告为未孕女性中的F-MC支持了先前的发现,即很大一部分妊娠未被检测到。这导致对基于Y染色体的F-MC检测方法进行重新验证。

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