Mucosal tolerance to E-selectin and response to systemic inflammation

Author:

Illoh, K.

Campbell, C.

Illoh, O.

Diehl, J.

Cherry, J.

Elkhaloun, A.

Chen, Y.

Hallenbeck, J.
Author Address

Univ Texas, Hlth Sci Ctr, Dept Neurol, Houston, TX 77030 USA. NINDS, SRA Int, NIH, Bethesda, MD USA. Univ Texas, Hlth Sci Ctr, Dept Pathol & Lab Med, Houston, TX 77030 USA. SAIC Frederick Inc, NCI, NIH, Frederick, MD USA. NHGRI, NIH, Bethesda, MD 20892 USA. NINDS, Stroke Branch, NIH, Bethesda, MD USA.;Illoh, K, Univ Texas, Hlth Sci Ctr, Dept Neurol, 6431 Fannin St,MSB 7-044, Houston, TX 77030 USA.;kachikwu.illoh@uth.tmc.edu

Abstract:

Mucosal tolerance to E-selectin has been shown to prevent stroke and reduce brain infarcts in experimental stroke models. However, the effective E-selectin dose range required to achieve mucosal tolerance and the precise mechanisms of neuroprotection remain unclear. We sought to examine the mechanisms of cytoprotection using gene expression profiling of tissues in the setting of mucosal tolerance and inflammatory challenge. Using spontaneously hypertensive rats (SHRs), we achieved immune tolerance with 0.1 to 5 mu g E-selectin per nasal instillation and observed a dose-related anti-E-selectin immunoglobulin G antibody production. We also show the distinct patterns of gene expression changes in the brain and spleen with the different tolerizing doses and lipopolysaccharide (LPS) exposure. Prominent differences were seen with such genes as insulin-like growth factors in the brain and downregulation of those encoding the major histocompatibility complex class I molecules in the spleen. In all, mucosal tolerance to E-selectin and subsequent exposure to LPS resulted in significant tissue changes. These changes, while giving an insight to the underlying mechanisms, serve as possible targets for future studies to facilitate translation to human clinical trials.

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