Drury Broc, Chuah Cher S, Hall Rebecca, Hardisty Gareth R, Rossi Adriano G, Ho Gwo-Tzer
Edinburgh IBD Science Unit, Centre for Inflammation Research, University of Edinburgh, Edinburgh, UK.
Gastro Hep Adv. 2023 Mar 23;2(6):788-798. doi: 10.1016/j.gastha.2023.03.022. eCollection 2023.
Inflammatory bowel disease (IBD) is associated with increased circulating damage-associated molecular patterns, in particular, the highly pro-inflammatory mitochondrial DNA (mtDNA). Here, we study the importance of blood neutrophils in mtDNA release via neutrophil extracellular trap (NET) formation and mitochondrial NETosis, where neutrophils specifically expulse mtDNA as potential targetable biological pathways.
We investigated the roles of A23187 (a known NET stimulant), granulocyte macrophage stimulating factor, lipopolysaccharide (LPS), and human IBD plasma in their ability to induce NET formation, mitochondrial NETosis, mtDNA, and total DNA release from human blood neutrophils; and the evidence for increased NET formation in IBD.
We demonstrated that NET formation resulted in significant DNA ( < .0001) and mtDNA release ( < .0001) with long DNA fragments (>1000 base pairs) with NETs containing high levels of mtDNA. Using previously described in vitro conditions for mitochondrial NETosis, granulocyte macrophage stimulating factor + LPS triggered neutrophil mtDNA release at lower levels but not NETosis. LPS alone can trigger neutrophilic DNA release without NET formation. Heterologous coculture with plasma from patients with active IBD (vs remission [n = 6/group]) were not associated with significantly higher levels of NETs and mtDNA release. During coculture with active IBD plasma (vs remission), citrullinated histone 3 (CitH3) (a NETs biomarker) levels were significantly lower ( < .001). Similarly, CitH3 levels were lower in stool supernatants of patients with active IBD vs remission (n = 19/12, = .0001). Stool CitH3 negatively correlates with stool calprotectin, a biomarker for gut inflammation (r = -0.47, = .03).
Hence, although blood neutrophils remain an important source of circulating mtDNA with defined mechanisms for release via NET formation and during neutrophil activation, our data do not support excessive systemic NET formation as a dominant underpinning pathobiological process in IBD.
炎症性肠病(IBD)与循环中损伤相关分子模式增加有关,尤其是促炎作用很强的线粒体DNA(mtDNA)。在此,我们研究血液中性粒细胞在通过中性粒细胞胞外陷阱(NET)形成和线粒体NETosis释放mtDNA过程中的重要性,中性粒细胞在此过程中特异性排出mtDNA,这可能是潜在的可靶向生物学途径。
我们研究了A23187(一种已知的NET刺激剂)、粒细胞巨噬细胞刺激因子、脂多糖(LPS)和人类IBD血浆在诱导人类血液中性粒细胞形成NET、线粒体NETosis、释放mtDNA和总DNA方面的作用;以及IBD中NET形成增加的证据。
我们证明NET形成导致显著的DNA释放(P<0.0001)和mtDNA释放(P<0.0001),释放的DNA片段较长(>1000个碱基对),且NETs中含有高水平的mtDNA。使用先前描述的线粒体NETosis体外条件,粒细胞巨噬细胞刺激因子+LPS可触发较低水平的中性粒细胞mtDNA释放,但不会触发NETosis。单独的LPS可触发嗜中性粒细胞DNA释放而不形成NET。与活动期IBD患者的血浆(与缓解期患者相比[n = 6/组])进行异源共培养,NETs和mtDNA释放水平并未显著升高。在与活动期IBD血浆共培养期间(与缓解期相比),瓜氨酸化组蛋白3(CitH3)(一种NETs生物标志物)水平显著降低(P<0.001)。同样,活动期IBD患者粪便上清液中的CitH3水平低于缓解期患者(n = 19/12,P = 0.0001)。粪便CitH3与肠道炎症生物标志物粪便钙卫蛋白呈负相关(r = -0.47,P = 0.03)。
因此,虽然血液中性粒细胞仍然是循环mtDNA的重要来源,且存在通过NET形成和中性粒细胞激活释放mtDNA的明确机制,但我们的数据不支持过度的全身NET形成是IBD主要的病理生物学过程基础。
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