Sukocheva Olga A, Manavis Jim, Kok Tuck-Weng, Turra Mark, Izzo Angelo, Blumbergs Peter, Marmion Barrie P
Q Fever Research Group (1993-2009), Hanson Institute, Adelaide, South Australia.
School of Health Sciences, Flinders University, Bedford Park, South Australia.
BMC Infect Dis. 2016 Apr 18;16:165. doi: 10.1186/s12879-016-1497-z.
In a previous study of a Q fever outbreak in Birmingham, our group identified a non-infective complex of Coxiella burnetii (C.b.) antigens able to survive in the host and provoked aberrant humoral and cell-mediated immunity responses. The study led to recognition of a possible pathogenic link between C.b. infection and subsequent long-term post Q fever fatigue syndrome (QFS). This report presents an unusually severe case of C.b. antigen and DNA detection in post-mortem specimens from a patient with QFS.
We report a 19-year old female patient who became ill with an acute unexplained febrile encephalitis-like illness, followed by increasingly severe multisystem dysfunction and death 10 years later. During life, extensive clinical and laboratory investigations from different disciplinary stand points failed to deliver a definitive identification of a cause. Given the history of susceptibility to infection from birth, acute fever and the diagnosis of "post viral syndrome", tests for infective agents were done starting with C.b. and Legionella pneumophila. The patient had previously visited farms a number of times. Comprehensive neuropathological assessment at the time of autopsy had not revealed gross or microscopic abnormalities. The aim was to extend detailed studies with the post-mortem samples and identify possible factors driving severe disturbance of homeostasis and organ dysfunction exhibited by the course of the patient's ten-year illness. Immunohistochemistry for C.b. antigen and PCR for DNA were tested on paraffin embedded blocks of autopsy tissues from brain, spleen, liver, lymph nodes (LN), bone marrow (BM), heart and lung. Standard H&E staining of brain sections was unrevealing. Immuno-staining analysis for astrocyte cytoskeleton proteins using glial fibrillary acidic protein (GFAP) antibodies showed a reactive morphology. Coxiella antigens were demonstrated in GFAP immuno-positive grey and white matter astrocytes, spleen, liver, heart, BM and LN. PCR analysis (COM1/IS1111 genes) confirmed the presence of C.b. DNA in heart, lung, spleen, liver & LN, but not in brain or BM.
The study revealed the persistence of C. b. cell components in various organs, including astrocytes of the brain, in a post-infection QFS. The possible mechanisms and molecular adaptations for this alternative C.b. life style are discussed.
在先前一项关于伯明翰Q热暴发的研究中,我们的团队鉴定出一种能在宿主体内存活的伯氏考克斯体(C.b.)非感染性抗原复合物,该复合物引发了异常的体液免疫和细胞介导免疫反应。该研究使人们认识到C.b.感染与后续长期Q热后疲劳综合征(QFS)之间可能存在致病联系。本报告介绍了一例在一名QFS患者尸检标本中C.b.抗原和DNA检测结果异常严重的病例。
我们报告一名19岁女性患者,她最初患有一种病因不明的急性发热性脑炎样疾病,10年后出现日益严重的多系统功能障碍并死亡。在其生前,从不同学科角度进行的广泛临床和实验室检查均未能明确病因。鉴于该患者自出生起就易受感染,且有急性发热及 “病毒后综合征” 的诊断,故从检测C.b.和嗜肺军团菌开始进行感染因子检测。该患者此前曾多次到访农场。尸检时进行的全面神经病理学评估未发现大体或微观异常。目的是对尸检样本进行详细研究,并确定在患者十年病程中导致体内稳态严重紊乱和器官功能障碍的可能因素。对取自脑、脾、肝、淋巴结(LN)、骨髓(BM)、心脏和肺的尸检组织石蜡包埋块进行C.b.抗原免疫组织化学检测和DNA聚合酶链反应(PCR)检测。脑切片的标准苏木精-伊红(H&E)染色未发现异常。使用胶质纤维酸性蛋白(GFAP)抗体对星形胶质细胞骨架蛋白进行免疫染色分析显示出反应性形态。在GFAP免疫阳性的灰质和白质星形胶质细胞、脾、肝及心脏、BM和LN中均检测到考克斯体抗原。PCR分析(COM1/IS1111基因)证实心脏、肺、脾、肝和LN中存在C.b. DNA,但脑和BM中未检测到。
该研究揭示了在感染后QFS中,C.b.细胞成分在包括脑星形胶质细胞在内的各种器官中的持续存在。文中讨论了这种C.b.另类生活方式的可能机制和分子适应性。
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