Altered thymocyte and T cell development in neonatal mice with hyperoxia-induced lung injury

Author:

Angusamy Sowmya1,Mansour Tamer23,Abdulmageed Mohammed14,Han Rachel1,Schutte Brian C.2,LaPres John5,Harkema Jack R.6,Omar Said A.17

Affiliation:

1. Department of Pediatrics and Human Development College of Human Medicine, Division of Neonatology , Michigan State University , East Lansing, MI , USA

2. Microbiology and Molecular Genetics , Michigan State University , East Lansing, MI , USA

3. Department of Clinical Pathology , Mansoura University , Mansoura , Egypt

4. Department of Pediatrics, Faculty of Medicine , South Valley University , Qena , Egypt

5. Biochemistry and Molecular Biology , Michigan State University , East Lansing, MI , USA

6. Pathobiology and Diagnostic Investigation , Michigan State University , East Lansing, MI , USA

7. Regional Neonatal Intensive Care, Sparrow Health System , Lansing Michigan, 48912 MI , USA , Phone: +517-364-2670, Fax: +517-364-3994

Abstract

Abstract Background: The adaptive immune system of neonates is relatively underdeveloped. The thymus is an essential organ for adaptive T cell development and might be affected during the natural course of oxygen induced lung injury. The effect of prolonged hyperoxia on the thymus, thymocyte and T cell development, and its proliferation has not been studied extensively. Methods: Neonatal mice were exposed to 85% oxygen (hyperoxia) or room air (normoxia) up to 28 days. Flow cytometry using surface markers were used to assay for thymocyte development and proliferation. Results: Mice exposed to prolonged hyperoxia had evidence of lung injury associated alveolar simplification, a significantly lower mean weight, smaller thymic size, lower mean thymocyte count and higher percentage of apoptotic thymocytes. T cells subpopulation in the thymus showed a significant reduction in the count and proliferation of double positive and double negative T cells. There was a significant reduction in the count and proliferation of single positive CD4+ and CD8+ T cells. Conclusions: Prolonged hyperoxia in neonatal mice adversely affected thymic size, thymocyte count and altered the distribution of T cells sub-populations. These results are consistent with the hypothesis that prolonged hyperoxia causes defective development of T cells in the thymus.

Publisher

Walter de Gruyter GmbH

Subject

Obstetrics and Gynecology,Pediatrics, Perinatology and Child Health

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