Pericardial & Mediastinal Fat-Associated Lymphoid Clusters are rapidly activated in an alkane induced model of Systemic Lupus Erythematosus

Karolina Bentkowska, Alex Hardgrave, Nadia Iqbal, Laura Gresty, Bethany Marsden, Sheila Macharia, Lucy Jackson-Jones
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Abstract

Abstract Systemic Lupus Erythematosus (SLE) is an autoimmune disease predominated by auto-antibodies that recognise cellular components. Pleural involvement is the most common SLE-related lung disease. Natural antibodies are rapidly secreted by innate-like B cells following perturbation of homeostasis and are important in the early stages of immune activation. The serous cavities are home to large numbers of innate-like B cells present both within serous fluid and resident within fat-associated lymphoid clusters (FALCs). FALCs are important hubs for B-cell activation and local antibody secretion within the body cavities. Patients with SLE can develop anti-phospholipid antibodies and in rare situations develop alveolar haemorrhage. Utilising delivery of the hydrocarbon oil pristane in C57BL/6 mice as a model of SLE we identify a rapid expansion of pleural cavity B cells as early as day 3 after intra-peritoneal pristane delivery. Following pristane delivery, pericardial B1 B cells are proliferative, express the plasma-cell surface marker CD138 and secrete both innate and class switched antibodies highlighting that this cavity niche may play an unrecognised role in the initiation of lupus pleuritis.
心包,纵隔脂肪相关淋巴细胞簇在烷烃诱导的系统性红斑狼疮模型中被迅速激活
系统性红斑狼疮(SLE)是一种以识别细胞成分的自身抗体为主的自身免疫性疾病。胸膜受累是最常见的slee相关肺部疾病。天然抗体由先天样B细胞在体内平衡紊乱后迅速分泌,在免疫激活的早期阶段起重要作用。浆液腔是大量先天样B细胞的家园,它们存在于浆液中,也存在于脂肪相关淋巴细胞簇(FALCs)中。FALCs是b细胞活化和体腔内局部抗体分泌的重要枢纽。SLE患者可产生抗磷脂抗体,并在极少数情况下发生肺泡出血。通过给C57BL/6小鼠注入烃类油嘌呤作为SLE模型,研究人员发现,早在给药后第3天,胸膜腔B细胞就迅速扩张。前列腺素输送后,心包B1 B细胞增殖,表达浆细胞表面标记物CD138,并分泌先天和类别转换抗体,这表明该腔位可能在狼疮性胸膜炎的发生中起着未被认识的作用。
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