Multipotent adult progenitor cells prevent functional impairment and improve development in inflammation driven detriment of preterm ovine lungs.

Neuen, Sophie M L; Ophelders, Daan R M G; Widowski, Helene; Hütten, Matthias C; Brokken, Tim; van Gorp, Charlotte; Nikkels, Peter G J; Severens-Rijvers, Carmen A H; Sthijns, Mireille M J P E; van Blitterswijk, Clemens A; Troost, Freddy J; LaPointe, Vanessa L S; Jolani, Shahab; Seiler, Christof; Pillow, J Jane; Delhaas, Tammo; Reynaert, Niki L; Wolfs, Tim G A M

Neuen, Sophie M L; Ophelders, Daan R M G; Widowski, Helene; Hütten, Matthias C; Brokken, Tim; van Gorp, Charlotte; Nikkels, Peter G J; Severens-Rijvers, Carmen A H; Sthijns, Mireille M J P E; van Blitterswijk, Clemens A; Troost, Freddy J; LaPointe, Vanessa L S; Jolani, Shahab; Seiler, Christof; Pillow, J Jane; Delhaas, Tammo; Reynaert, Niki L; Wolfs, Tim G A M.

Afiliación

Neuen SML; Department of Pediatrics, Maastricht University Medical Center, MosaKids Children's Hospital, Maastricht, the Netherlands.
Ophelders DRMG; GROW Research Institute for Oncology and Reproduction, Maastricht University, Maastricht, the Netherlands.
Widowski H; Department of Pediatrics, Maastricht University Medical Center, MosaKids Children's Hospital, Maastricht, the Netherlands.
Hütten MC; GROW Research Institute for Oncology and Reproduction, Maastricht University, Maastricht, the Netherlands.
Brokken T; Department of Pediatrics, Maastricht University Medical Center, MosaKids Children's Hospital, Maastricht, the Netherlands.
van Gorp C; GROW Research Institute for Oncology and Reproduction, Maastricht University, Maastricht, the Netherlands.
Nikkels PGJ; Department of BioMedical Engineering, Maastricht University, Maastricht, the Netherlands.
Severens-Rijvers CAH; Department of Pediatrics, Maastricht University Medical Center, MosaKids Children's Hospital, Maastricht, the Netherlands.
Sthijns MMJPE; GROW Research Institute for Oncology and Reproduction, Maastricht University, Maastricht, the Netherlands.
van Blitterswijk CA; Department of Pediatrics, Maastricht University Medical Center, MosaKids Children's Hospital, Maastricht, the Netherlands.
Troost FJ; GROW Research Institute for Oncology and Reproduction, Maastricht University, Maastricht, the Netherlands.
LaPointe VLS; Department of Pediatrics, Maastricht University Medical Center, MosaKids Children's Hospital, Maastricht, the Netherlands.
Jolani S; GROW Research Institute for Oncology and Reproduction, Maastricht University, Maastricht, the Netherlands.
Seiler C; Department of Pathology, University Medical Center Utrecht, Utrecht, the Netherlands.
Pillow JJ; GROW Research Institute for Oncology and Reproduction, Maastricht University, Maastricht, the Netherlands.
Delhaas T; Department of Pathology, Maastricht University Medical Center, Maastricht, the Netherlands.
Reynaert NL; Food Innovation and Health, Department of Human Biology, Maastricht University, Venlo, the Netherlands.
Wolfs TGAM; NUTRIM Institute of Nutrition and Translational Research in Metabolism, Maastricht University, Maastricht, the Netherlands.

Regen Ther ; 27: 207-217, 2024 Dec.

Article en En | MEDLINE | ID: mdl-38576851

ABSTRACT

ABSTRACT

Background:

Perinatal inflammation increases the risk for bronchopulmonary dysplasia in preterm neonates, but the underlying pathophysiological mechanisms remain largely unknown. Given their anti-inflammatory and regenerative capacity, multipotent adult progenitor cells (MAPC) are a promising cell-based therapy to prevent and/or treat the negative pulmonary consequences of perinatal inflammation in the preterm neonate. Therefore, the pathophysiology underlying adverse preterm lung outcomes following perinatal inflammation and pulmonary benefits of MAPC treatment at the interface of prenatal inflammatory and postnatal ventilation exposures were elucidated.

Methods:

Instrumented ovine fetuses were exposed to intra-amniotic lipopolysaccharide (LPS 5 mg) at 125 days gestation to induce adverse systemic and peripheral organ outcomes. MAPC (10 × 106 cells) or saline were administered intravenously two days post LPS exposure. Fetuses were delivered preterm five days post MAPC treatment and either killed humanely immediately or mechanically ventilated for 72 h.

Results:

Antenatal LPS exposure resulted in inflammation and decreased alveolar maturation in the preterm lung. Additionally, LPS-exposed ventilated lambs showed continued pulmonary inflammation and cell junction loss accompanied by pulmonary edema, ultimately resulting in higher oxygen demand. MAPC therapy modulated lung inflammation, prevented loss of epithelial and endothelial barriers and improved lung maturation in utero. These MAPC-driven improvements remained evident postnatally, and prevented concomitant pulmonary edema and functional loss.

Conclusion:

In conclusion, prenatal inflammation sensitizes the underdeveloped preterm lung to subsequent postnatal inflammation, resulting in injury, disturbed development and functional impairment. MAPC therapy partially prevents these changes and is therefore a promising approach for preterm infants to prevent adverse pulmonary outcomes.

Palabras clave

Bronchopulmonary dysplasia; Postnatal ventilation; Prenatal inflammation; Preterm birth; Stem cell therapy

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