1 Department of Tropical Pathology, 115374 Faculty of Tropical Medicine, Mahidol University , Ratchathewi, Bangkok 10400, Thailand.
2 Department of Microbiology and Immunology, 115374 Faculty of Tropical Medicine, Mahidol University , Ratchathewi, Bangkok 10400, Thailand.
Exp Biol Med (Maywood). 2018 Mar;243(5):395-407. doi: 10.1177/1535370218757458. Epub 2018 Feb 5.
Plasmodium falciparum, the most virulent malaria parasite species, causes severe symptoms especially acute lung injury (ALI), of which characterized by alveolar epithelium and endothelium destruction and accelerated to blood-gas-barrier breakdown. Parasitized erythrocytes, endothelial cells, monocytes, and cytokines are all involved in this mechanism, but hemozoin (HZ), the parasitic waste from heme detoxification, also mainly contributes. In addition, it is not clear why type II pneumocyte proliferation, alveolar restorative stage, is rare in malaria-associated ALI. To address this, in vitro culture of A549 cells with Plasmodium HZ or with interleukin (IL)-1β triggered by HZ and monocytes (HZ-IL-1β) was conducted to determine their alveolar apoptotic effect using ethidium bromide/acridine orange staining, annexin-V-FITC/propidium iodide staining, and electron mircroscopic study. Caspase recruitment domain-containing protein 9 ( CARD9), the apoptotic regulator gene, and IL-1β were quantified by reverse-transcriptase PCR. Junctional cellular defects were characterized by immunohistochemical staining of E-cadherin. The results revealed that cellular apoptosis and CARD9 expression levels were extremely high 24 h after induction by HZ-IL-1β when compared to the HZ- and non-treated groups. E-cadherin was markedly down-regulated by HZ-IL-1β and HZ treatments. CARD9 expression was positively correlated with IL-1β expression and the number of apoptotic cells. Interestingly, the localization of HZ in the vesicular surfactant of apoptotic pneumocyte was also identified and submitted to be a cause of alveolar resolution abnormality. Thus, HZ triggers monocytes to produce IL-1β and induces pneumocyte type II apoptosis through CARD9 pathway in association with down-regulated E-cadherin, which probably impairs alveolar resolution in malaria-associated ALI. Impact statement The present work shows the physical and immunomodulatory properties of hemozoin on the induction of pneumocyte apoptosis in relation to IL-1β production through the CARD9 pathway. This occurrence may be a possible pathway for the retardation of lung resolution leading to blood-gas-barrier breakdown. Our findings lead to the understanding of the host-parasite relationship focusing on the dysfunction in ALI induced by HZ, a possible pathway of the recovering lung epithelial retardation in malaria-associated ARDS.
恶性疟原虫(Plasmodium falciparum)是最具毒性的疟原虫物种,会导致严重的症状,尤其是急性肺损伤(ALI),其特征为肺泡上皮和内皮细胞破坏,并加速血-气屏障破裂。寄生红细胞、内皮细胞、单核细胞和细胞因子都参与了这一机制,但血红素(HZ),即血红素解毒产生的寄生虫废物,也起主要作用。此外,尚不清楚为什么在疟疾相关的 ALI 中,II 型肺泡细胞增生和肺泡修复阶段很少见。为了解决这个问题,通过使用溴化乙锭/吖啶橙染色、膜联蛋白-V-FITC/碘化丙啶染色和电子显微镜研究,对 A549 细胞进行了含有疟原虫 HZ 或由 HZ 和单核细胞触发的白细胞介素 (IL)-1β(HZ-IL-1β)的体外培养,以确定其肺泡凋亡效应。通过逆转录 PCR 定量检测凋亡调节基因 CARD9 和 IL-1β。通过 E-钙黏蛋白免疫组织化学染色来表征细胞连接缺陷。结果表明,与 HZ-和未处理组相比,诱导 24 小时后,HZ-IL-1β诱导的细胞凋亡和 CARD9 表达水平极高。HZ-IL-1β 和 HZ 处理明显下调 E-钙黏蛋白。CARD9 表达与 IL-1β 表达和凋亡细胞数量呈正相关。有趣的是,还鉴定了 HZ 在凋亡型 II 型肺泡细胞的囊泡表面活性剂中的定位,并将其作为肺泡修复异常的原因。因此,HZ 触发单核细胞产生 IL-1β,并通过 CARD9 途径诱导 II 型肺泡细胞凋亡,同时下调 E-钙黏蛋白,这可能会损害疟疾相关 ALI 中的肺泡修复。
影响评估
本工作显示了 HZ 通过 CARD9 途径诱导 IL-1β 产生与诱导型肺泡细胞凋亡有关的物理和免疫调节特性。这种发生可能是导致血-气屏障破裂的肺泡修复延迟的一种可能途径。我们的研究结果使人们对宿主-寄生虫关系有了更深的理解,重点关注 HZ 引起的 ALI 中的功能障碍,这可能是疟疾相关 ARDS 中肺上皮恢复延迟的一个可能途径。
