Prenatal retinoid deficiency leads to airway hyperresponsiveness in adult mice
Felicia Chen, … , Loredana Quadro, Wellington V. Cardoso
Felicia Chen, … , Loredana Quadro, Wellington V. Cardoso
Published January 9, 2014
Citation Information: J Clin Invest. 2014;124(2):801-811. https://doi.org/10.1172/JCI70291.
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Research Article Pulmonology

Prenatal retinoid deficiency leads to airway hyperresponsiveness in adult mice

Abstract

There is increasing evidence that vitamin A deficiency in utero correlates with abnormal airway smooth muscle (SM) function in postnatal life. The bioactive vitamin A metabolite retinoic acid (RA) is essential for formation of the lung primordium; however, little is known about the impact of early fetal RA deficiency on postnatal lung structure and function. Here, we provide evidence that during murine lung development, endogenous RA has a key role in restricting the airway SM differentiation program during airway formation. Using murine models of pharmacological, genetic, and dietary vitamin A/RA deficiency, we found that disruption of RA signaling during embryonic development consistently resulted in an altered airway SM phenotype with markedly increased expression of SM markers. The aberrant phenotype persisted postnatally regardless of the adult vitamin A status and manifested as structural changes in the bronchial SM and hyperresponsiveness of the airway without evidence of inflammation. Our data reveal a role for endogenous RA signaling in restricting SM differentiation and preventing precocious and excessive SM differentiation when airways are forming.

Authors

Felicia Chen, Hector Marquez, Youn-Kyung Kim, Jun Qian, Fengzhi Shao, Alan Fine, William W. Cruikshank, Loredana Quadro, Wellington V. Cardoso

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Figure 3

VAD in utero results in aberrant airway SM differentiation in E14.5 lungs.

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VAD in utero results in aberrant airway SM differentiation in E14.5 lung...
(A) Diagram of experimental design. (B) HPLC measurements of total retinoid (RE and ROH) in E14.5 lung homogenates (ng/g) from WT and DKO mice in VAS and VAD groups. (C) qPCR of RARElacZ expression in lung homogenates (all mice were bred into a RARElacZ line). (DK) ISH of Tagln (DG) and Myh11 (HK) showing increased expression of SM markers in the proximal airways of VAD lungs (arrowheads), most prominent in DKO VAD lungs (G). Ectopic expression extended to the most distal airways (circled regions) in the VAD groups (red asterisks denote no or low signals). n = 6 per condition. *P < 0.05 compared with the VAS group. Scale bars: 150 μm (E) and 180 μm (J).