Determination of Critical Requirements for Classical Swine Fever Virus NS2-3-Independent Virion Formation

Dubrau, D.; Schwindt, S.; Klemens, O.; Bischoff, HA; Tautz, Norbert

doi:10.1128/jvi.00679-19

Cited by 4 publications

(1 citation statement)

References 45 publications

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“…It was reported that the introduction of an internal ribosome entry site (IRES) or ubiquitin (Ubi) coding sequence between the NS2 and NS3 coding sequences cannot lead to the loss of viral infectious particles, indicating that the uncleavage NS2–NS3 is highly conservative and is a key factor for the formation of pestivirus virions [ 57 , 60 ]. To determine the conservation of NS2–NS3 in the pestivirus genus, Dubrau et al evaluated the NS2 and NS3 mutants (2/T444-V and 3/M132-A) of CSFV, a virus in the same genus as BVDV [ 61 ]. These mutants encode ubiquitin between NS2 and NS3 (NS2-Ubi-NS3) and internal IRES (NS2-IRES-NS3), respectively.…”

Section: Non-structural Proteinsmentioning

confidence: 99%

Non-structural proteins of bovine viral diarrhea virus

et al. 2022

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Bovine viral diarrhea virus (BVDV) belongs to the family Flaviviridae genus pestivirus. The viral genome is a single-stranded, positive-sense RNA that encodes four structural proteins (i.e., C, Erns, E1, and E2) and eight non-structural proteins (NSPs) (i.e., Npro, p7, NS2, NS3, NS4A, NS4B, NS5A, and NS5B). Cattle infected with BVDV exhibit a number of different clinical signs including diarrhea, abortion, and other reproductive disorders which have a serious impact on the cattle industry worldwide. Research on BVDV mainly focuses on its structural protein, however, progress in understanding the functions of the NSPs of BVDV has also been made in recent decades. The knowledge gained on the BVDV non-structural proteins is helpful to more fully understand the viral replication process and the molecular mechanism of viral persistent infection. This review focuses on the functions of BVDV NSPs and provides references for the identification of BVDV, the diagnosis and prevention of Bovine viral diarrhea mucosal disease (BVD-MD), and the development of vaccines.

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Section: Non-structural Proteinsmentioning

confidence: 99%

Non-structural proteins of bovine viral diarrhea virus

et al. 2022

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Classical swine fever virus: the past, present and future

et al. 2020

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Downstream Sequences Control the Processing of the Pestivirus E ^rns -E1 Precursor

Bintintan

Meyers

2020

J Virol

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Like other enveloped viruses pestiviruses employ cellular proteases for processing of their structural proteins. While typical signal peptidase cleavage motifs are present at the carboxyterminus of the signal sequence preceding Erns, and the E1/E2 and E2/P7 sites, the Erns-E1 precursor is cleaved by signal peptidase at a highly unusual structure, in which the transmembrane sequence upstream of the cleavage site is replaced by an amphipathic helix. As shown before, the integrity of the amphipathic helix is crucial for efficient processing. The data presented here demonstrate that also the E1 sequence downstream of this cleavage site is important for the cleavage. Carboxyterminal truncation of the E1 moiety as well as internal deletions in E1 reduced the cleavage efficiency to less than 30% of the wt level. Moreover, the C-terminal truncation by more than 30 amino acids resulted in strong secretion of the uncleaved fusion proteins. The reduced processing and increased secretion was even observed when 10 to 5 aminoterminal residues or E1 were left whereas extensions by 1 or 3 E1 residues resulted in reduced processing but no significantly increased secretion. In contrast to the E1 sequences, a 10 amino acid c-myc tag fused to the Erns C-terminus had only marginal effect on secretion but was also not processed efficiently. Mutation of the von Heijne sequence upstream of E2 not only blocked the cleavage between E1 and E2 but also prevented the processing between Erns and E2. Thus, processing at the ErnsE1 site is a highly regulated process. IMPORTANCE Cellular signal peptidase (SPase) cleavage represents an important step in maturation of viral envelope proteins. Fine tuning of this system allows for establishment of concerted folding and processing processes in different enveloped viruses. We report here on SPase processing of the Erns-E1-E2 glycoprotein precursor of pestiviruses. Erns-E1 cleavage is delayed and only executed efficiently when the complete E1 sequence is present. C-terminal truncation of the Erns-E1 precursor impairs processing and leads to significant secretion of the protein. The latter is not detected when internal deletions preserving the E1 carboxyterminus are introduced, but also these constructs show impaired processing. Moreover, Erns-E1 is only processed after cleavage at the E1/E2 site. Thus, processing of the pestiviral glycoprotein precursor by SPase is done in an ordered way and depends on the integrity of the proteins for efficient cleavage. The functional importance of this processing scheme is discussed in the paper.

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Determination of Critical Requirements for Classical Swine Fever Virus NS2-3-Independent Virion Formation

Cited by 4 publications

References 45 publications

Non-structural proteins of bovine viral diarrhea virus

Non-structural proteins of bovine viral diarrhea virus

Classical swine fever virus: the past, present and future

Downstream Sequences Control the Processing of the Pestivirus E ^rns -E1 Precursor

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Determination of Critical Requirements for Classical Swine Fever Virus NS2-3-Independent Virion Formation

Cited by 4 publications

References 45 publications

Non-structural proteins of bovine viral diarrhea virus

Non-structural proteins of bovine viral diarrhea virus

Classical swine fever virus: the past, present and future

Downstream Sequences Control the Processing of the Pestivirus E rns -E1 Precursor

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Product

Resources

About

Downstream Sequences Control the Processing of the Pestivirus E ^rns -E1 Precursor