The Z Proteins of Pathogenic but Not Nonpathogenic Arenaviruses Inhibit RIG-i-Like Receptor-Dependent Interferon Production

Xing, Junji; Ly, Hinh; Liang, Yuying

doi:10.1128/jvi.03349-14

Cited by 105 publications

(126 citation statements)

References 56 publications

(87 reference statements)

Supporting

Mentioning

117

Contrasting

Unclassified

Order By: Relevance

“…Using this approach, we have previously identified differences in the induction of cytokine responses to infection with TCRV or JUNV in macrophages, as well as differences in their influence on host cell apoptosis (Groseth et al, 2011;Wolff et al, 2013a). Other known differences that also might play a role for the virulence include receptor usage (Abraham et al, 2009), as well as the ability to engage in IFN antagonism (Xing et al, 2015). Previous studies have shown that TCRV lacks a novel NP-mediated anti-apoptotic function that was described for JUNV (Wolff et al, 2013a), and together with the observation that TCRV infection also induces severe cytopathic effects (CPEs) during infection in cell culture (Groseth et al, 2011), this suggests that cell death might be due at least in part to apoptotic responses.…”

Section: Introductionmentioning

confidence: 99%

The New World arenavirus Tacaribe virus induces caspase-dependent apoptosis in infected cells

Wolff

Groseth

Meyer

et al. 2016

Journal of General Virology

View full text Add to dashboard Cite

The Arenaviridae is a diverse and growing family of viruses that already includes more than 25 distinct species. While some of these viruses have a significant impact on public health, others appear to be non-pathogenic. At present little is known about the host cell responses to infection with different arenaviruses, particularly those found in the New World; however, apoptosis is known to play an important role in controlling infection of many viruses. Here we show that infection with Tacaribe virus (TCRV), which is widely considered the prototype for non-pathogenic arenaviruses, leads to stronger induction of apoptosis than does infection with its human-pathogenic relative Junín virus. TCRV-induced apoptosis occurred in several cell types during late stages of infection and was shown to be caspase-dependent, involving the activation of caspases 3, 7, 8 and 9. Further, UV-inactivated TCRV did not induce apoptosis, indicating that the activation of this process is dependent on active viral replication/transcription. Interestingly, when apoptosis was inhibited, growth of TCRV was not enhanced, indicating that apoptosis does not have a direct negative effect on TCRV infection in vitro. Taken together, our data identify and characterize an important virus-host cell interaction of the prototypic, non-pathogenic arenavirus TCRV, which provides important insight into the growing field of arenavirus research aimed at better understanding the diversity in responses to different arenavirus infections and their functional consequences.

show abstract

Section: Introductionmentioning

confidence: 99%

The New World arenavirus Tacaribe virus induces caspase-dependent apoptosis in infected cells

Wolff

Groseth

Meyer

et al. 2016

Journal of General Virology

View full text Add to dashboard Cite

show abstract

“…The generally innocuous nature of PICV is also supported by our recent molecular analysis of the viral gene products. We found that the Z proteins of all known human arenavirus pathogens, including the low-risk pathogen LCMV and the highly virulent pathogen Lassa fever virus (LASV), but not those of others such as PICV, can inhibit the RIG-I-like receptors (RLRs) (5). Therefore, we believe that PICV has a better biosafety profile than LCMV, but like LCMV, PICV can induce strong immune responses, especially cellular immunity (19,22).…”

mentioning

confidence: 99%

“…The arenavirus is composed of a total of four genes on two genomic RNA segments in opposite orientations (1). The Z protein, produced from the large (L) genomic segment, is a small RING domain-containing matrix protein that mediates virus budding, regulates viral RNA synthesis, and mediates host immune suppression (4,5). The large L protein (ϳ200 kDa), also encoded on the L segment, is the RNA-dependent RNA polymerase (RdRp), which is required for viral RNA synthesis (6).…”

mentioning

confidence: 99%

A Novel Live Pichinde Virus-Based Vaccine Vector Induces Enhanced Humoral and Cellular Immunity after a Booster Dose

Dhanwani

Zhou

Huang

et al. 2016

J Virol

Self Cite

View full text Add to dashboard Cite

Pichinde virus (PICV) is a bisegmented enveloped RNA virus that targets macrophages and dendritic cells (DCs) early in infection and induces strong innate and adaptive immunity in mice. We have developed a reverse genetics system to produce live recombinant PICV (strain P18) with a trisegmented RNA genome (rP18tri), which encodes all four PICV gene products and as many as two foreign genes. We have engineered the vector to express the green fluorescent protein (GFP) reporter gene (abbreviated as G in virus designations) and either the hemagglutination (HA [H]) or the nucleoprotein (NP [P]) gene of the influenza A/PR8 virus. The trisegmented viruses rP18tri-G/H and rP18tri-G/P showed slightly reduced growth in vitro and expressed HA and NP, respectively. Mice immunized with rP18tri-G/H were completely protected against lethal influenza virus challenge even 120 days after immunization. These rP18tri-based vectors could efficiently induce both neutralizing antibodies and antigen-specific T cell responses via different immunization routes. Interestingly, the immune responses were significantly increased upon a booster dose and remained at high levels even after three booster doses. In summary, we have developed a novel PICV-based live vaccine vector that can express foreign antigens to induce strong humoral and cell-mediated immunity and is ideal for a primeand-boost vaccination strategy. IMPORTANCE We have developed a novel Pichinde virus (PICV)-based live viral vector, rP18tri, that packages three RNA segments and encodes as many as two foreign genes. Using the influenza virus HA and NP genes as model antigens, we show that this rP18tri vector can induce strong humoral and cellular immunity via different immunization routes and can lead to protection in mice. Interestingly, a booster dose further enhances the immune responses, a feature that distinguishes this from other known live viral vectors. In summary, our study demonstrates a unique feature of this live rP18tri vector to be used as a novel vaccine platform for a prime-and-boost vaccination strategy.A renaviruses are enveloped RNA viruses with a bisegmented genome and mostly use rodents as natural hosts. There are at least 27 members that are geographically, serologically, and phylogenetically divided into Old World and New World arenaviruses (1). The prototypic lymphocytic choriomeningitis virus (LCMV) infection of mice has long been used as a valuable model with which to study viral persistence and virus-induced immunity and immunopathology (2, 3). The arenavirus is composed of a total of four genes on two genomic RNA segments in opposite orientations (1). The Z protein, produced from the large (L) genomic segment, is a small RING domain-containing matrix protein that mediates virus budding, regulates viral RNA synthesis, and mediates host immune suppression (4, 5). The large L protein (ϳ200 kDa), also encoded on the L segment, is the RNA-dependent RNA polymerase (RdRp), which is required for viral RNA synthesis (6). The glycoprotein (GPC), encoded...

show abstract

“…аналогичным образом первичные макрофаги чело-века показывают более высокий уровень продукции интерлейкина-6, интерлейкина-10 и α-интерферона при инфицировании вирусом такарибе по сравнению с инфицированием патогенным для человека вирусом хунин [7]. показано, что Z-белок всех известных па-тогенных аренавирусов, в отличие от непатогенных, способен ингибировать активацию макрофагов [27]. поскольку макрофаги и дендритные клетки являют-ся антигенпрезентирующими клетками, играющими важную роль в формировании иммунного ответа, ингибирование этих клеток приводит к иммунной супрессии, которая во многом определяет патогенез вирусных геморрагических лихорадок [13].…”

unclassified

“…белок Z патогенных для человека арена-вирусов ингибируют рецепторы, индуцирующие образование интерферона [27]. процесс ингибиро-вания осуществляется в результате взаимодействия N-концевой последовательности белка Z (31 амино-кислотный остаток) и N-концевой последователь-ности соответствующего рецептора, что затрудняет связывание последнего с митохондриальным сиг-нальным белком.…”

unclassified

Molecular-Biological Peculiarities of Arenavirus Reproduction in Sensitive Cells

Сизикова¹,

Лебедев²,

Пантюхов³

et al. 2017

Problemy Osobo Opasnykh Infektsii

View full text Add to dashboard Cite

The Z Proteins of Pathogenic but Not Nonpathogenic Arenaviruses Inhibit RIG-i-Like Receptor-Dependent Interferon Production

Cited by 105 publications

References 56 publications

The New World arenavirus Tacaribe virus induces caspase-dependent apoptosis in infected cells

The New World arenavirus Tacaribe virus induces caspase-dependent apoptosis in infected cells

A Novel Live Pichinde Virus-Based Vaccine Vector Induces Enhanced Humoral and Cellular Immunity after a Booster Dose

Molecular-Biological Peculiarities of Arenavirus Reproduction in Sensitive Cells

Contact Info

Product

Resources

About