Adenovirus-Directed Ocular Innate Immunity: The Role of Conjunctival Defensin-like Chemokines (IP-10, I-TAC) and Phagocytic Human Defensin-{alpha}

doi:10.1167/iovs.05-0438

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(Investigative Ophthalmology and Visual Science. 2005;46:3657-3665.)
© 2005 by The Association for Research in Vision and Ophthalmology, Inc.
DOI: 10.1167/iovs.05-0438

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Adenovirus-Directed Ocular Innate Immunity: The Role of Conjunctival Defensin-like Chemokines (IP-10, I-TAC) and Phagocytic Human Defensin- ${alpha}$

Stephen A. K. Harvey,¹ Eric G. Romanowski,¹^,2 Kathleen A. Yates,¹^,2 and Y. Jerold Gordon¹^,2

^²From the Charles T. Campbell Laboratory and the ^¹Department of Ophthalmology, University of Pittsburgh, Pittsburgh, Pennsylvania.

PURPOSE. Adenovirus (Ad), a major cause of viral conjunctivitisworldwide, is controlled initially by the innate immune responseon the ocular surface. In the present study, cultured humanconjunctival epithelial cells were used to identify host genesresponsive to infection by a clinical isolate of Ad5, and theantiviral activity of some of their peptide products was investigated.

METHODS. Primary human conjunctival epithelial cells in culturewere infected with Ad5 at high (1.0), low (0.1), or zero (0.0)multiplicities of infection (MOI) and harvested at differenttimes after infection (1.5, 6, and 16 hours). Host gene expressionwas profiled with oligonucleotide microarrays (GeneChips; Affymetrix,Santa Clara, CA). Peptide products of interest were tested forantiviral activity in direct inhibition assays against respiratoryserotypes (Ad3, Ad5), ocular serotypes (Ad8, Ad19), and HSV-1.

RESULTS. At high MOI, viral infection suppressed the interferon(IFN)-mediated host antiviral response seen at low MOI. At 16hours after infection, 63 unique characterized transcripts wereidentified that were robustly and significantly suppressed byhigh MOI, (i.e., MOI [0.1]/MOI [0.1] $≥$ 2, P < 0.006). Of these,29 (46%) transcripts are involved in IFN signaling or are IFNor virus induced. This subset included CXCL10 and CXCL11, encodingIP-10 and I-TAC, respectively. These defensin-like chemokinesand human ${alpha}$ -defensin-1 directly inhibited Ad3 and Ad5 but notAd8 or Ad19.

CONCLUSIONS. In response to low-level Ad5 infection, conjunctivalepithelial cells showed upregulation of IFN-associated genes.The peptide products of two of these, IP-10 and I-TAC, are directlyactive against Ad3, and IP-10 is active against Ad5. The oculartropism of Ad8 and Ad19 may be due in part to their resistanceto these defensin-like chemokines.