Grossmayer Gerhard E, Keppeler Hildegard, Boeltz Sebastian, Janko Christina, Rech Jürgen, Herrmann Martin, Lauber Kirsten, Muñoz Luis E
Department of Internal Medicine 3 - Rheumatology and Immunology, Universitätsklinikum Erlangen, Friedrich-Alexander-Universität Erlangen-Nürnberg, Erlangen, Germany.
Department of Internal Medicine II, University of Tübingen, Tübingen, Germany.
Front Immunol. 2018 Jan 17;8:1876. doi: 10.3389/fimmu.2017.01876. eCollection 2017.
Impaired clearance of dying and dead cells by professional and amateur phagocytes plays a crucial role in the etiology of systemic lupus erythematosus (SLE). While dying, cells expose and release a plethora of eat-me and find-me signals to ensure their timely removal before entering the dangerous stage of secondary necrosis. A well-described chemoattractant for macrophages is dying cell-derived lysophosphatidylcholine (LPC). However, its implications for and/or its association with SLE disease, so far, have not been examined. In the present study, we analyzed the LPC serum concentrations of patients with SLE and rheumatoid arthritis (RA). Subsequently, we examined if and to which extent the measured serum concentrations of LPC and an LPC-rich environment can impact the phagocytosis of necrotic cells.
Sera from patients with SLE, RA, and normal healthy donors (NHD) were characterized for several parameters, including LPC concentrations. Phagocytosis of dead cells by human macrophages in the presence of SLE and NHD sera was quantified. Additionally, the impact of exogenously added, purified LPC on phagocytosis was analyzed.
Patients with SLE had significantly increased LPC serum levels, and high serum LPC of SLE patients correlated significantly with impaired phagocytosis of dead cells in the presence of heat-inactivated serum. Phagocytosis in the presence of sera from NHD showed no correlation to LPC levels, but exogenous addition of purified LPC in the range as measured in SLE patients' sera led to a concentration-dependent decrease.
Our data show that high levels of LPC as observed in the sera of SLE patients have a negative impact on the clearance of dead cells by macrophages. Chemoattraction requires a concentration gradient. The higher the LPC concentration surrounding a dying or dead cell, the smaller the achievable gradient upon LPC release will be. Thus, it is feasible to assume that elevated LPC levels can interfere with the build-up of a local LPC gradient during cell death, and hence might play a role in the establishment and/or perpetuation of SLE disease.
专业和非专业吞噬细胞对濒死及死亡细胞的清除功能受损在系统性红斑狼疮(SLE)的病因学中起着关键作用。细胞在濒死时会暴露并释放大量“吃我”和“找到我”信号,以确保在进入继发性坏死的危险阶段之前被及时清除。一种已被充分描述的巨噬细胞趋化因子是濒死细胞衍生的溶血磷脂酰胆碱(LPC)。然而,其与SLE疾病的关系及关联,迄今为止尚未得到研究。在本研究中,我们分析了SLE患者和类风湿关节炎(RA)患者的血清LPC浓度。随后,我们研究了所测得的LPC血清浓度以及富含LPC的环境是否以及在何种程度上会影响坏死细胞的吞噬作用。
对SLE患者、RA患者及正常健康供体(NHD)的血清进行多项参数分析,包括LPC浓度。对人巨噬细胞在SLE和NHD血清存在下对死细胞的吞噬作用进行定量分析。此外,还分析了外源性添加的纯化LPC对吞噬作用的影响。
SLE患者的血清LPC水平显著升高,SLE患者的高血清LPC与热灭活血清存在时死细胞吞噬功能受损显著相关。NHD血清存在时的吞噬作用与LPC水平无相关性,但外源性添加SLE患者血清中所测范围内的纯化LPC会导致浓度依赖性降低。
我们的数据表明,SLE患者血清中观察到的高水平LPC对巨噬细胞清除死细胞有负面影响。趋化作用需要浓度梯度。濒死或死亡细胞周围的LPC浓度越高,LPC释放时可实现的梯度就越小。因此,可以合理推测升高的LPC水平可能会干扰细胞死亡期间局部LPC梯度的形成,从而可能在SLE疾病的发生和/或持续存在中起作用。
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