Science and Research

Prenatal vitamin D supplementation mitigates inflammation-related alveolar remodeling in neonatal mice

The development of chronic lung disease in the neonate, also known as bronchopulmonary dysplasia (BPD), is the most common long-term complication in prematurely born infants. In BPD, the disease-characteristic inflammatory response culminates in nonreversible remodeling of the developing gas exchange area, provoked by the impact of postnatal treatments such as mechanical ventilation (MV) and oxygen treatment. To evaluate the potential of prenatal treatment regimens to modulate this inflammatory response and thereby impact the vulnerability of the lung toward postnatal injury, we designed a multilayered preclinical mouse model. After administration of either prenatal vitamin D-enriched (VitD+; 1,500 IU/g food) or -deprived (VitD-; <10 IU/kg) food during gestation in C57B6 mice (the onset of mating until birth), neonatal mice were exposed to hyperoxia (Fi(O(2)) = 0.4) with or without MV for 8 h at days 5-7 of life, whereas controls spontaneously breathed room air. Prenatal vitamin D supplementation resulted in a decreased number of monocytes/macrophages in the neonatal lung undergoing postnatal injury together with reduced TGF-β pathway activation. In consequence, neonatal mice that received a VitD+ diet during gestation demonstrated less extracellular matrix (ECM) remodeling upon lung injury, reflected by the reduction of pulmonary α-smooth muscle actin-positive fibroblasts, decreased collagen and elastin deposition, and lower amounts of interstitial tissue in the lung periphery. In conclusion, our findings support strategies that attempt to prevent vitamin D insufficiency during pregnancy as they could impact lung health in the offspring by mitigating inflammatory changes in neonatal lung injury and ameliorating subsequent remodeling of the developing gas exchange area.NEW & NOTEWORTHY Vitamin D-enriched diet during gestation resulted in reduced lung inflammation and matrix remodeling in neonatal mice exposed to clinically relevant, postnatal injury. The results underscore the need to monitor the subclinical effects of vitamin D insufficiency that impact health in the offspring when other risk factors come into play.

  • Waiden, J.
  • Heydarian, M.
  • Oak, P.
  • Koschlig, M.
  • Kamgari, N.
  • Hagemann, M.
  • Wjst, M.
  • Hilgendorff, A.

Keywords

  • Humans
  • Pregnancy
  • Female
  • Infant, Newborn
  • Animals
  • Mice
  • Animals, Newborn
  • *Lung Injury/metabolism
  • Vitamin D/pharmacology/metabolism
  • Lung/metabolism
  • *Bronchopulmonary Dysplasia/drug therapy/prevention & control/metabolism
  • *Pneumonia/metabolism
  • Inflammation/drug therapy/metabolism
  • *Hyperoxia/metabolism
  • *Vitamin D Deficiency/drug therapy/metabolism
  • Dietary Supplements
  • bronchopulmonary dysplasia
  • mechanical ventilation
  • oxygen toxicity
  • prenatal treatment
  • vitamin D
Publication details
DOI: 10.1152/ajplung.00367.2022
Journal: Am J Physiol Lung Cell Mol Physiol
Pages: L95-l103 
Number: 2
Work Type: Original
Location: CPC-M
Disease Area: DPLD
Partner / Member: HMGU
Access-Number: 37256661

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