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白细胞介素-10具有抑制作用,而骨化三醇可恢复胎盘抗菌肽的基因表达。

IL-10 inhibits while calcitriol reestablishes placental antimicrobial peptides gene expression.

作者信息

Olmos-Ortiz Andrea, Noyola-Martínez Nancy, Barrera David, Zaga-Clavellina Verónica, Avila Euclides, Halhali Ali, Biruete Benjamín, Larrea Fernando, Díaz Lorenza

机构信息

Departamento de Biología de la Reproducción, Instituto Nacional de Ciencias Médicas y Nutrición Salvador Zubirán, Vasco de Quiroga No. 15, México City, Tlalpan 14000, Mexico.

Departamento de Inmunobioquímica, Instituto Nacional de Perinatología Isidro Espinosa de los Reyes, Montes Urales No. 800, México City, Col. Lomas de Virreyes 11000, Mexico.

出版信息

J Steroid Biochem Mol Biol. 2015 Apr;148:187-93. doi: 10.1016/j.jsbmb.2014.07.012. Epub 2014 Aug 1.

Abstract

IL-10 and calcitriol help to achieve a successful pregnancy by suppressing active maternal immunity; however, these factors exert opposite effects upon microbial infections. In the skin and immune cells, IL-10 downregulates β-defensins while calcitriol induces cathelicidin gene expression in various tissues including placenta. Though, the regulation of human placental β-defensins by IL-10 and calcitriol has not been studied. Therefore, we explored the regulation of these antimicrobial peptides expression in cultured placental cells by calcitriol and IL-10 alone and combined. Real time PCR showed that calcitriol stimulated, while IL-10 inhibited, β-defensins and cathelicidin gene expression (P<0.05). In coincubations studies, calcitriol was able to maintain antimicrobial peptides gene expression above control values, overriding IL-10 inhibitory effects. Calcitriol downregulated endogenous IL-10 secretion. Interestingly, calcitriol and TNF-α cooperatively enhanced β-defensins, while TNF-α reduced basal and calcitriol-stimulated cathelicidin gene expression. In summary, calcitriol and IL-10 exerted opposite effects on antimicrobial peptides expression in the human placenta, suggesting that unbalanced production of IL-10 and calcitriol could be deleterious to innate immune responses during gestation. Our results suggest that calcitriol enhancement of placental defenses involves two mechanisms: (1) downregulation of IL-10 secretion and (2) direct upregulation of β-defensins and cathelicidin gene expression. Considering that IL-10 and calcitriol differentially regulate the innate immune response in the placenta, in the case of an infection, calcitriol might restrict IL-10 permissive actions towards microbial invasion while restrains inflammation, allowing for pregnancy to continue in quiescence. These results strongly advice maternal vitamin D sufficiency during pregnancy.

摘要

白细胞介素-10(IL-10)和骨化三醇通过抑制母体活跃的免疫反应来助力实现成功妊娠;然而,这些因子对微生物感染却有着相反的作用。在皮肤和免疫细胞中,IL-10会下调β-防御素,而骨化三醇则会在包括胎盘在内的各种组织中诱导cathelicidin基因表达。不过,IL-10和骨化三醇对人胎盘β-防御素的调节作用尚未得到研究。因此,我们探究了骨化三醇和IL-10单独及联合作用对培养的胎盘细胞中这些抗菌肽表达的调节情况。实时聚合酶链反应(PCR)显示,骨化三醇刺激而IL-10抑制β-防御素和cathelicidin基因表达(P<0.05)。在共孵育研究中,骨化三醇能够使抗菌肽基因表达维持在高于对照值的水平,从而克服IL-10的抑制作用。骨化三醇下调内源性IL-10分泌。有趣的是,骨化三醇和肿瘤坏死因子-α(TNF-α)协同增强β-防御素,而TNF-α则降低基础及骨化三醇刺激的cathelicidin基因表达。总之,骨化三醇和IL-10对人胎盘中抗菌肽的表达产生相反作用,这表明IL-10和骨化三醇的不平衡产生可能对妊娠期间的固有免疫反应有害。我们的结果表明,骨化三醇增强胎盘防御涉及两种机制:(1)下调IL-10分泌;(2)直接上调β-防御素和cathelicidin基因表达。鉴于IL-10和骨化三醇对胎盘固有免疫反应的调节存在差异,在感染的情况下,骨化三醇可能会限制IL-10对微生物入侵的放任作用,同时抑制炎症,使妊娠在静止状态下得以继续。这些结果强烈建议孕期母亲保持充足的维生素D。

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