Sex-dependent regulation of mucin gene transcription and airway secretion and mechanics following intra-airway IL-13 in mice with conditional loss of club cell Creb1

Mariana Sponchiado, Amy Fagan, Luz Mata, Angelina L. Bonilla, Pedro Trevizan-Baú, Sreekala Prabhakaran, Leah R. Reznikov
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Abstract

Introduction: Interleukin 13 (IL-13) is an important effector molecule in allergic asthma. IL-13-mediated mucin hypersecretion requires conversion of secretoglobin-positive club cells into goblet cells through suppression of forkhead box A2 (FOXA2) and induction of SAM pointed domain containing ETS transcription factor (SPDEF). IL-13-mediated mucin hypersecretion may also include modulation of purinergic and muscarinic receptors that control basal and stimulated mucin secretion. We recently found that the transcription factor cAMP response element-binding protein (Creb1) inhibits FOXA2 and modulates mucus secretion in mice.Methods: We tested the hypothesis that loss of club cell Creb1 mitigates the pro-mucin effects of IL-13. We challenged male and female mice with conditional loss of club cell Creb1 and wild type littermates with intra-airway IL-13 or vehicle. We also studied human “club cell-like” NCI-H322 cells.Results: Loss of club cell Creb1 augmented IL-13-mediated increases in mRNA for the gel-forming mucins Muc5ac and Muc5b and prevented IL-13-mediated decreases in muscarinic 3 receptor (M3R) mRNA in male airways. In female airways, loss of club cell Creb1 reduced M3R mRNA and significantly blunted IL-13-mediated increases in purinergic receptor P2Y2 (P2ry2) mRNA but did not impact Muc5ac and Muc5b mRNA. Despite changes in mucins and secretion machinery, goblet cell density following cholinergic stimulation was not impacted by loss of club cell Creb1 in either sex. IL-13 treatment decreased basal airway resistance across sexes in mice with loss of club cell Creb1, whereas loss of club cell Creb1 augmented IL-13-mediated increases in airway elastance in response to methacholine. NCI-H322 cells displayed IL-13 signaling components, including IL-13Rα1 and IL-4Rα. Pharmacologic inhibition of CREB reduced IL-13Rα1 mRNA, whereas recombinant CREB decreased IL-4Rα mRNA. Application of IL-13 to NCI-H322 cells increased concentrations of cAMP in a delayed manner, thus linking IL-13 signaling to CREB signaling.Conclusion: These data highlight sex-specific regulation of club cell Creb1 on IL-13-mediated mucin hypersecretion and airway mechanics.
俱乐部细胞 Creb1 条件性缺失小鼠气道内 IL-13 对粘蛋白基因转录、气道分泌和力学的性别依赖性调控
导言白细胞介素13(IL-13)是过敏性哮喘的重要效应分子。IL-13介导的粘蛋白高分泌需要通过抑制叉头盒A2(FOXA2)和诱导含ETS转录因子的SAM尖结构域(SPDEF)将分泌球蛋白阳性的会厌细胞转化为腺泡细胞。IL-13 介导的粘蛋白高分泌还可能包括对嘌呤能受体和毒蕈碱受体的调节,这些受体控制着基础和受刺激的粘蛋白分泌。我们最近发现,转录因子 cAMP 反应元件结合蛋白(Creb1)可抑制 FOXA2 并调节小鼠的粘液分泌:方法:我们测试了俱乐部细胞 Creb1 的缺失可减轻 IL-13 促粘液作用的假设。我们用气道内 IL-13 或药物挑战了条件性俱乐部细胞 Creb1 缺失的雄性和雌性小鼠以及野生型同窝小鼠。我们还研究了人类 "俱乐部细胞样 "NCI-H322细胞:结果:在男性气道中,会厌细胞 Creb1 的缺失增强了 IL-13 介导的凝胶形成粘蛋白 Muc5ac 和 Muc5b mRNA 的增加,并阻止了 IL-13 介导的毒蕈碱 3 受体(M3R)mRNA 的减少。在女性气道中,会厌细胞 Creb1 的缺失会降低 M3R mRNA,并显著减弱 IL-13 介导的嘌呤能受体 P2Y2 (P2ry2) mRNA 的增加,但不会影响 Muc5ac 和 Muc5b mRNA。尽管粘蛋白和分泌机制发生了变化,但胆碱能刺激后的鹅口疮细胞密度并没有因为雌雄鹅口疮细胞 Creb1 的缺失而受到影响。IL-13处理可降低俱乐部细胞Creb1缺失小鼠的基础气道阻力,而俱乐部细胞Creb1缺失可增强IL-13介导的气道弹性对甲氧胆碱反应的增加。NCI-H322 细胞显示了 IL-13 信号成分,包括 IL-13Rα1 和 IL-4Rα。药物抑制 CREB 可降低 IL-13Rα1 mRNA,而重组 CREB 可降低 IL-4Rα mRNA。对NCI-H322细胞施用IL-13可延迟增加cAMP浓度,从而将IL-13信号传导与CREB信号传导联系起来:这些数据强调了俱乐部细胞 Creb1 对 IL-13 介导的粘蛋白高分泌和气道力学的性别特异性调控。
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