川崎病血管炎小鼠模型中 PAD2 和 PAD4 在心血管病变发展过程中的冗余作用

Talita P Domiciano, Youngho Lee, Thacyana T Carvalho, Daiko Wakita, Daisy Martinon, Prasant K Jena, Justyna Fert-Bober, Vanessa Borges, Timothy R Crother, Shuang Chen, Debbie Moreira, Jennifer E Van Eyk, Magali Noval Rivas, Moshe Arditi, Kenichi Shimada
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引用次数: 0

摘要

川崎病(KD)是儿童后天性心脏病的主要病因。虽然在急性川崎病期间循环中性粒细胞会增加和活化,但中性粒细胞和中性粒细胞胞外捕获物(NET)是否有助于川崎病的发病机制尚不清楚。肽基精氨酸脱氨酶 4(PAD4)是一种参与蛋白质瓜氨酸化的酶,对 NETs 的形成至关重要,它与多种疾病的发病机制有关。在此,我们利用乳杆菌细胞壁提取物(LCWE)诱导的 KD 脉管炎小鼠模型来确定 PAD4 在 KD 脉管炎中的作用。我们发现,泛 PADs 抑制剂 Cl-amidine 能显著减轻 LCWE 诱导的心血管病变,但中性粒细胞特异性 Padi4 KO 小鼠不会影响 KD 脉管炎的发展。虽然用氯胺酮体外处理高表达 Padi4 的巨噬细胞能抑制 IL-1β 的分泌,但巨噬细胞特异性 Padi4 KO 小鼠并不能减轻病变。Padi4-/-小鼠也会发生KD血管炎,PAD2抑制剂AFM30a能显著减轻Padi4-/-小鼠的KD血管炎,这表明PAD2在PAD4缺乏时具有代偿作用。我们还在具有组成型活性 NLRP3 炎症小体的巨噬细胞中发现了几种瓜氨酸化蛋白,它们受到氯脒(Cl-amidine)处理的抑制,这表明蛋白瓜氨酸化参与了 NLRP3 炎症小体的激活。这些数据表明,在这种小鼠 KD 脉管炎中,PAD4 依赖性 NETs 的形成起着不可或缺的作用,而 PAD2 和 PAD4 则起着多余的作用。克利脒降低小鼠 KD 血管炎严重程度的心脏保护作用不仅限于抑制 PAD4,还可能包括减少炎症小体通路中的瓜氨酸化。
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Redundant role of PAD2 and PAD4 in the development of cardiovascular lesions in a mouse model of Kawasaki Disease vasculitis
Kawasaki disease (KD) is the leading cause of acquired heart disease in children. While circulating neutrophils are increased and activated during acute KD, it is unclear whether neutrophils and neutrophil extracellular traps (NETs) contribute to the pathogenesis of KD. Peptidylarginine deiminase 4 (PAD4), an enzyme involved in protein citrullination and essential for NETs formation, is implicated in the pathogenesis of various diseases. Here, we used the Lactobacillus casei cell wall extract (LCWE)-induced mouse model of KD vasculitis to determine the contribution of PAD4 in KD vasculitis. We found that the pan-PADs inhibitor, Cl-amidine, significantly reduced LCWE-induced cardiovascular lesions, but neutrophil-specific Padi4 KO mice did not impact development of KD vasculitis. While in vitro treatment of macrophages, which highly express Padi4, with Cl-amidine inhibited IL-1βsecretion, macrophage-specific Padi4 KO mice did not reduce the lesions. Padi4-/- mice also developed KD vasculitis, AFM30a, a PAD2 inhibitor, significantly reduced KD vasculitis in Padi4-/- mice, indicating a compensatory role of PAD2 in PAD4 deficiency. We also identified several citrullinated proteins in macrophages with constitutively active NLRP3 inflammasome that were inhibited by Cl-amidine treatment, suggesting that protein citrullination participates in NLRP3 inflammasome activation. These data indicate a dispensable role for PAD4-dependent NETs formation, and a redundant role of PAD2 and PAD4 in this murine KD vasculitis. The cardioprotective effects of Cl-amidine to reduce the severity of murine KD vasculitis is not limited to PAD4 inhibition and may include decreased citrullination in the inflammasome pathway.
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