胎盘疟疾中胎盘自噬受损。
Impaired placental autophagy in placental malaria.
作者信息
Dimasuay Kris Genelyn, Gong Lan, Rosario Fredrick, McBryde Emma, Spelman Tim, Glazier Jocelyn, Rogerson Stephen J, Beeson James G, Jansson Thomas, Devenish Rodney J, Boeuf Philippe
机构信息
Burnet Institute, Melbourne, Victoria, Australia.
Department of Medicine at the Peter Doherty Institute, University of Melbourne, Parkville, Victoria, Australia.
出版信息
PLoS One. 2017 Nov 10;12(11):e0187291. doi: 10.1371/journal.pone.0187291. eCollection 2017.
BACKGROUND
Placental malaria is a major cause of low birthweight, principally due to impaired fetal growth. Intervillositis, a local inflammatory response to placental malaria, is central to the pathogenesis of poor fetal growth as it impairs transplacental amino acid transport. Given the link between inflammation and autophagy, we investigated whether placental malaria-associated intervillositis increased placental autophagy as a potential mechanism in impaired fetal growth.
METHODS
We examined placental biopsies collected after delivery from uninfected women (n = 17) and from women with Plasmodium falciparum infection with (n = 14) and without (n = 7) intervillositis. Western blotting and immunofluorescence staining coupled with advanced image analysis were used to quantify the expression of autophagic markers (LC3-II, LC3-I, Rab7, ATG4B and p62) and the density of autophagosomes (LC3-positive puncta) and lysosomes (LAMP1-positive puncta).
RESULTS
Placental malaria with intervillositis was associated with higher LC3-II:LC3-I ratio, suggesting increased autophagosome formation. We found higher density of autophagosomes and lysosomes in the syncytiotrophoblast of malaria-infected placentas with intervillositis. However, there appear to be no biologically relevant increase in LC3B/LAMP1 colocalization and expression of Rab7, a molecule involved in autophagosome/lysosome fusion, was lower in placental malaria with intervillositis, indicating a block in the later stage of autophagy. ATG4B and p62 expression showed no significant difference across histological groups suggesting normal autophagosome maturation and loading of cargo proteins into autophagosomes. The density of autophagosomes and lysosomes in the syncytiotrophoblast was negatively correlated with placental amino acid uptake.
CONCLUSIONS
Placental malaria-associated intervillositis is associated with dysregulated autophagy that may impair transplacental amino acid transport, possibly contributing to poor fetal growth.
背景
胎盘疟疾是低出生体重的主要原因,主要是由于胎儿生长受限。绒毛间炎是对胎盘疟疾的局部炎症反应,在胎儿生长受限的发病机制中起核心作用,因为它会损害经胎盘的氨基酸转运。鉴于炎症与自噬之间的联系,我们研究了胎盘疟疾相关的绒毛间炎是否会增加胎盘自噬,这可能是胎儿生长受限的潜在机制。
方法
我们检查了分娩后从未感染疟疾的妇女(n = 17)以及感染恶性疟原虫且伴有(n = 14)和不伴有(n = 7)绒毛间炎的妇女的胎盘活检组织。采用蛋白质免疫印迹法和免疫荧光染色结合先进的图像分析技术,对自噬标志物(LC3-II、LC3-I、Rab7、ATG4B和p62)的表达、自噬体(LC3阳性斑点)和溶酶体(LAMP1阳性斑点)的密度进行定量分析。
结果
伴有绒毛间炎的胎盘疟疾与较高的LC3-II:LC3-I比值相关,提示自噬体形成增加。我们发现在伴有绒毛间炎的疟疾感染胎盘的合体滋养层中,自噬体和溶酶体的密度更高。然而,LC3B/LAMP1共定位似乎没有生物学上显著的增加,并且参与自噬体/溶酶体融合的分子Rab出现在伴有绒毛间炎的胎盘疟疾中表达较低,表明自噬后期存在阻滞。ATG4B和p62的表达在各组织学组之间没有显著差异,表明自噬体成熟正常且货物蛋白加载到自噬体中正常。合体滋养层中自噬体和溶酶体的密度与胎盘氨基酸摄取呈负相关。
结论
胎盘疟疾相关的绒毛间炎与自噬失调有关,这可能会损害经胎盘的氨基酸转运,可能导致胎儿生长受限。
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