Interleukin-1β Transfer across the Blood–Brain Barrier in the Ovine Fetus

Author:

Sadowska Grazyna B1,Chen Xiaodi1,Zhang Jiyong1,Lim Yow-Pin2,Cummings Erin E1,Makeyev Oleksandr3,Besio Walter G3,Gaitanis John4,Padbury James F1,Banks William A5,Stonestreet Barbara S1

Affiliation:

1. Department of Pediatrics, The Alpert Medical School of Brown University, Women & Infants Hospital of Rhode Island, Providence, Rhode Island, USA

2. ProThera Biologics, Inc., Providence, Rhode Island, USA

3. Department of Electrical, Computer, and Biomedical Engineering, University of Rhode Island, Kingston, Rhode Island, USA

4. Department of Neurology, The Alpert Medical School of Brown University, Rhode Island Hospital, Providence, Rhode Island, USA

5. Division of Gerontology and Geriatric Medicine, Department of Medicine, Geriatric Research Educational, and Clinical Center, Veterans Affairs Puget Sound Health Care System, University of Washington, Seattle, Washington, USA

Abstract

Pro-inflammatory cytokines contribute to hypoxic–ischemic brain injury. Blood–brain barrier (BBB) dysfunction represents an important component of hypoxic–ischemic brain injury in the fetus. Hypoxic–ischemic injury could accentuate systemic cytokine transfer across the fetal BBB. There has been considerable conjecture suggesting that systemic cytokines could cross the BBB during the perinatal period. Nonetheless, evidence to support this contention is sparse. We hypothesized that ischemia–reperfusion increases the transfer of systemic interleukin-1β (IL-1β) across the BBB in the fetus. Ovine fetuses at 127 days of gestation were studied 4 hours after 30 minutes of bilateral carotid artery occlusion and compared with a nonischemic group. Recombinant ovine IL-1β protein was expressed from an IL-1β pGEX-2 T vector in E. coli BL-21 cells and purified. The BBB function was quantified in 12 brain regions using a blood-to-brain transfer constant with intravenous 125I-radiolabeled IL-1β (125I-IL-1β). Interleukin-1β crossed the intact BBB in nonischemic fetuses. Blood-to-brain transport of 125I-IL-1β was higher ( P < 0.05) across brain regions in fetuses exposed to ischemia–reperfusion than nonischemic fetuses. We conclude that systemic IL-1β crosses the intact fetal BBB, and that ischemia–reperfusion increases transfer of this cytokine across the fetal BBB. Therefore, altered BBB function after hypoxia–ischemia facilitates entry of systemic cytokines into the brain of the fetus.

Publisher

SAGE Publications

Subject

Cardiology and Cardiovascular Medicine,Clinical Neurology,Neurology

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