Abstract

The Yatapoxviruses encode a distinct class of secreted TNF-binding protein (TNF-BP) that resembles an MHC class I heavy chain but distinct from any other known TNF inhibitor. Characterization of these viral TNF inhibitors from Tanapox virus, Yaba monkey tumor virus (YMTV) and a closely related version from Swinepox virus revealed dramatically differential TNF binding specificities for different mammalian species. The Tanapox virus 2L protein (TPV-2L) formed inhibitory complexes with human TNF, and interacted with monkey and canine TNF with high affinity but rabbit TNF with low affinity. On the other hand, YMTV-2L bound human and monkey TNF with high affinity but rabbit TNF with only low affinity. The TNF-BP from swinepox virus (SPV003/148) only interacted with porcine TNF with high affinity. The observed TNF binding analysis mirrored the biological activity of these TNF-binding protein to block TNF-induced cellular cytolysis. TPV-2L and YMTV-2L also inhibited the human TNF-mediated signaling in cells but TPV-2L exhibited higher affinity for human TNF (KD, 43 pm) compared with monkey (KD, 120 pm) whereas for YMTV-2L, the affinities were reversed (human TNF KD, 440 pm; monkey TNF KD, 230 pm). The interaction domain of human TNF with TNF-binding proteins is significantly different from that of TNFRs, as determined using human TNF mutants. We conclude that these poxvirus TNF-binding proteins represent a new class of TNF inhibitors and are distinct from the viral TNF receptor homologues characterized to date.

Highlights

  • Tumor necrosis factor (TNF),2 secreted primarily by macrophages and monocytes, is a potent mediator cytokine of inflammation and the immune response to various pathogens [4, 5]

  • Among the poxvirus-encoded vTNFRs, two major categories have been described: the T2-like inhibitors encoded by leporipoxviruses and the cytokine response modifier (Crm)-like orthologs encoded by orthopoxviruses [8]

  • The vTNF-BP is encoded by ORF 2L, and related 2L ORFs are present in other members of this genus including Yaba-like disease virus (YLDV) and Yaba monkey tumor virus (YMTV), and 2L-like ORFs are found in swinepox virus (SPV) and deerpox virus (DPV) (24 –27)

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Summary

EXPERIMENTAL PROCEDURES

Recombinant human, rhesus monkey, canine, porcine, and murine TNF and human LT␣ were obtained from R&D biosystems. Soluble human TNFR1 and TNFR2 were obtained from BioSource International. Rabbit TNF was produced, concentrated and quantified using methods described previously [12]. Swinepox virus genomic DNA was provided from the laboratory of Dr Richard Moyer (UF, Gainesville). Human TNF mutants hTNFR32W-S86T and hTNFD143N-A145R were produced as described before [29, 30]

Cloning of Viral Genes for Expression in the Baculovirus System
Generation of Recombinant Baculoviruses
Protein Purification
Cytolytic Assays
Analysis of TNF Binding Specificity and Affinity Constants
Cell Assays and Immunoblotting
Porcine TNF
Findings
DISCUSSION
Full Text
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