Distinct neural stem cell tropism, early immune activation, and choroid plexus pathology following coxsackievirus infection in the neonatal central nervous system

Puccini, Jenna M.; Ruller, Chelsea; Robinson, Scott M.; Knopp, Kristeene A.; Buchmeier, Michael J.; Doran, Kelly S.; Feuer, Ralph

doi:10.1038/labinvest.2013.138

Cited by 19 publications

(20 citation statements)

References 59 publications

(90 reference statements)

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“…We previously determined that proliferating neural stem and progenitor cells grown in the subventricular zone of the neonatal brain or grown in culture were preferentially targeted by CVB3 [10], [11], [16], [14], [26]. Furthermore, CVB3 reduced the levels of neurogenesis and altered brain development in a neonatal model of viral infection [15].…”

Section: Resultsmentioning

confidence: 99%

“…This model seems to mirror the late consequences of childhood doxorubicin-induced cardiotoxicity observed in humans which manifests in weakening of the myocardium, an attenuation of cardiac pump performance, and progression towards congestive heart failure. Since previous studies described preferential CVB3 infection of progenitor cells in the CNS [10], [11], [15], [16], [26] and bone marrow [17], we investigated the effect of CVB3 on CPCs in the developing heart. We established a mouse model of juvenile CVB3 infection and observed that not only did CVB3 productively infect CPCs, but infection caused a sustained reduction in the CPC pool into adulthood.…”

Section: Introductionmentioning

confidence: 99%

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The Impact of Juvenile Coxsackievirus Infection on Cardiac Progenitor Cells and Postnatal Heart Development

et al. 2014

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Coxsackievirus B (CVB) is an enterovirus that most commonly causes a self-limited febrile illness in infants, but cases of severe infection can manifest in acute myocarditis. Chronic consequences of mild CVB infection are unknown, though there is an epidemiologic association between early subclinical infections and late heart failure, raising the possibility of subtle damage leading to late-onset dysfunction, or chronic ongoing injury due to inflammatory reactions during latent infection. Here we describe a mouse model of juvenile infection with a subclinical dose of coxsackievirus B3 (CVB3) which showed no evident symptoms, either immediately following infection or in adult mice. However following physiological or pharmacologically-induced cardiac stress, juvenile-infected adult mice underwent cardiac hypertrophy and dilation indicative of progression to heart failure. Evaluation of the vasculature in the hearts of adult mice subjected to cardiac stress showed a compensatory increase in CD31+ blood vessel formation, although this effect was suppressed in juvenile-infected mice. Moreover, CVB3 efficiently infected juvenile c-kit+ cells, and cardiac progenitor cell numbers were reduced in the hearts of juvenile-infected adult mice. These results suggest that the exhausted cardiac progenitor cell pool following juvenile CVB3 infection may impair the heart's ability to increase capillary density to adapt to increased load.

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Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

The Impact of Juvenile Coxsackievirus Infection on Cardiac Progenitor Cells and Postnatal Heart Development

et al. 2014

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“…Many of these recombinant viral constructs have proven to be quite stable, although the loss of the foreign insert can appear in the viral population within five passages, depending upon the size of the insert, nucleotide sequence, nature of the gene, and passage conditions. The utilization of these rCVBs in tissue culture and in vivo have clarified questions regarding viral tropism (Feuer, Pagarigan et al, 2005) (Puccini, Ruller et al, 2014), activation of the adaptive immune response against infection (Kemball, Harkins et al, 2009), mechanisms of virulence and disease (Zeng, Chen et al, 2013), and possible uses of CVB as therapeutic/vaccine vectors (Kim, Kim et al, 2012) (Miller, Geng et al, 2009). …”

Section: Introductionmentioning

confidence: 99%

“…The recruitment of these novel myeloid cells was preceded by the induction of CCL12, a chemokine known to attract monocytic cells (Sarafi, Garcia-Zepeda et al, 1997) and fibrocytes (Moore, Murray et al, 2006). Although epithelial cells appeared spared from infection, CVB induced significant acute damage in the choroid plexus (Puccini, Ruller et al, 2014). Also, infected nestin + myeloid cells were shown to migrate into the CNS and assist in virus dissemination.…”

Section: Introductionmentioning

confidence: 99%

“…Utilizing our in vivo model of CNS infection, unique host immune gene expression changes were observed for CVB compared to a different neurotropic virus - LCMV - an arenavirus considered to activate the prototypical immune response in the host (Puccini, Ruller et al, 2014). CCL12, CCL7, CCL4, CXCL4, and CCL2 were upregulated at early time points following CVB infection.…”

Section: Introductionmentioning

confidence: 99%

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Recent progress in understanding coxsackievirus replication, dissemination, and pathogenesis

et al. 2015

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Coxsackieviruses (CVs) are relatively common viruses associated with a number of serious human diseases, including myocarditis and meningo-encephalitis. These viruses are considered cytolytic yet can persist for extended periods of time within certain host tissues requiring evasion from the host immune response and a greatly reduced rate of replication. A member of Picornaviridae family, CVs have been historically considered non-enveloped viruses – although recent evidence suggest that CV and other picornaviruses hijack host membranes and acquire an envelope. Acquisition of an envelope might provide distinct benefits to CV virions, such as resistance to neutralizing antibodies and efficient nonlytic viral spread. CV exhibits a unique tropism for progenitor cells in the host which may help to explain the susceptibility of the young host to infection and the establishment of chronic disease in adults. CVs have also been shown to exploit autophagy to maximize viral replication and assist in unconventional release from target cells. In this article, we review recent progress in clarifying virus replication and dissemination within the host cell, identifying determinants of tropism, and defining strategies utilized by the virus to evade the host immune response. Also, we will highlight unanswered questions and provide future perspectives regarding the potential mechanisms of CV pathogenesis.

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Roles of the Choroid Plexus in CNS Infections

Schwerk

Tenenbaum

Schroten

2020

Physiology in Health and Disease

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Distinct neural stem cell tropism, early immune activation, and choroid plexus pathology following coxsackievirus infection in the neonatal central nervous system

Cited by 19 publications

References 59 publications

The Impact of Juvenile Coxsackievirus Infection on Cardiac Progenitor Cells and Postnatal Heart Development

The Impact of Juvenile Coxsackievirus Infection on Cardiac Progenitor Cells and Postnatal Heart Development

Recent progress in understanding coxsackievirus replication, dissemination, and pathogenesis

Roles of the Choroid Plexus in CNS Infections

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