A novel polyubiquitin chain linkage formed by viral Ubiquitin is resistant to host deubiquitinating enzymes

Author:

Negi Hitendra12,Reddy Pothula Purushotham3,Vengayil Vineeth34,Patole Chhaya3,Laxman Sunil3,Das Ranabir1ORCID

Affiliation:

1. National Center for Biological Sciences, TIFR, Bangalore, India

2. SASTRA University, Thirumalaisamudram, Thanjavur, India

3. Institute for Stem Cell Science and Regenerative Medicine (inStem), Bangalore, India

4. Manipal Academy of Higher Education, Manipal, India

Abstract

The Baculoviridae family of viruses encode a viral Ubiquitin (vUb) gene. Though the vUb is homologous to the host eukaryotic Ubiquitin (Ub), its preservation in the viral genome indicates unique functions that are not compensated by the host Ub. We report the structural, biophysical, and biochemical properties of the vUb from Autographa californica multiple nucleo-polyhedrosis virus (AcMNPV). The packing of central helix α1 to the beta-sheet β1–β5 is different between vUb and Ub. Consequently, its stability is lower compared with Ub. However, the surface properties, ubiquitination activity, and the interaction with Ubiquitin-binding domains are similar between vUb and Ub. Interestingly, vUb forms atypical polyubiquitin chain linked by lysine at the 54th position (K54), and the deubiquitinating enzymes are ineffective against the K54-linked polyubiquitin chains. We propose that the modification of host/viral proteins with the K54-linked chains is an effective way selected by the virus to protect the vUb signal from host DeUbiquitinases.

Publisher

Portland Press Ltd.

Subject

Cell Biology,Molecular Biology,Biochemistry

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