Transition toward Human Cytomegalovirus Susceptibility in Early Human Embryonic Stem Cell-Derived Neural Precursors

Berger, Amnon A; Gil, Yaniv; Panet, Amos; Weisblum, Yiska; Oiknine‐Djian, Esther; Gropp, Michal; Steiner, Debora; Reubinoff, Benjamin; Wolf, Dana

doi:10.1128/jvi.01742-15

Cited by 16 publications

(23 citation statements)

References 51 publications

(60 reference statements)

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“…Fortunately, large populations of almost pure cell types can be generated using either embryonic stem (ES) cell or induced pluripotent stem cell (iPSC) technologies. Interestingly, NPCs derived from 10-week gestation tissue were substantially more permissive to infection (30) than either ES-or iPS-derived NPCs (31)(32)(33)(34)(35)(36)(37)(38); also our unpublished results). This suggests that the more primitive stage of development of the ES-and iPS-derived cells influences their interactions with the virus.…”

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confidence: 52%

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Human Cytomegalovirus Compromises Development of Cerebral Organoids

Brown

Rana

Jaeger

et al. 2019

J Virol

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Congenital human cytomegalovirus (HCMV) infection causes a broad spectrum of central and peripheral nervous system disorders, ranging from microcephaly to hearing loss. These ramifications mandate the study of virus-host interactions in neural cells. Neural progenitor cells are permissive for lytic infection. We infected two induced pluripotent stem cell (iPSC) lines and found these more primitive cells to be susceptible to infection but not permissive. Differentiation of infected iPSCs induced de novo expression of viral antigens. iPSCs can be cultured in three dimensions to generate cerebral organoids, closely mimicking in vivo development. Mock- or HCMV-infected iPSCs were subjected to a cerebral organoid generation protocol. HCMV IE1 protein was detected in virus-infected organoids at 52 days postinfection. Absent a significant effect on organoid size, infection induced regions of necrosis and the presence of large vacuoles and cysts. Perhaps more in parallel with the subtler manifestations of HCMV-induced birth defects, infection dramatically altered neurological development of organoids, decreasing the number of developing and fully formed cortical structure sites, with associated changes in the architectural organization and depth of lamination within these structures, and manifesting aberrant expression of the neural marker β-tubulin III. Our observations parallel published descriptions of infected clinical samples, which often contain only sparse antigen-positive foci yet display areas of focal necrosis and cellular loss, delayed maturation, and abnormal cortical lamination. The parallels between pathologies present in clinical specimens and the highly tractable three-dimensional (3D) organoid system demonstrate the utility of this system in modeling host-virus interactions and HCMV-induced birth defects. IMPORTANCE Human cytomegalovirus (HCMV) is a leading cause of central nervous system birth defects, ranging from microcephaly to hearing impairment. Recent literature has provided descriptions of delayed and abnormal maturation of developing cortical tissue in infected clinical specimens. We have found that infected induced pluripotent stem cells can be differentiated into three-dimensional, viral protein-expressing cerebral organoids. Virus-infected organoids displayed dramatic alterations in development compared to those of mock-infected controls. Development in these organoids closely paralleled observations in HCMV-infected clinical samples. Infection induced regions of necrosis, the presence of larger vacuoles and cysts, changes in the architectural organization of cortical structures, aberrant expression of the neural marker β-tubulin III, and an overall reduction in numbers of cortical structure sites. We found clear parallels between the pathologies of clinical specimens and virus-infected organoids, demonstrating the utility of this highly tractable system for future investigations of HCMV-induced birth defects.

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confidence: 52%

“…All of the infection studies performed to date on undifferentiated ES or iPS cells (including ours described herein) find both cell types to be essentially nonpermissive for infection, as measured by de novo expression of immediate early (IE) antigens (Ags) (31,33,35,37). However, the susceptibility to infection of these cells is much less clear.…”

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confidence: 96%

Human Cytomegalovirus Compromises Development of Cerebral Organoids

Brown

Rana

Jaeger

et al. 2019

J Virol

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“…This notion of a gradual release of viral restriction blocks along neuronal differentiation was corroborated by the transition to an increased susceptibility to HCMV during neural differentiation of ESCs into neural spheres [103]. Susceptibility to HCMV appeared to be correlated to expression of the platelet-derived growth factor receptor alpha (PDGFRα) [103]. Brown et al showed correspondingly a lack of permissiveness of iPSCs to HCMV, but also identified iPSCs to be susceptible to HCMV infection through positive staining for the input tegument proteins [104].…”

Section: The Infection Of Pluripotent Stem Cell-based Models Of Humanmentioning

confidence: 87%

“…Due to their similarity to cells in the developing neural tube, they are suggestive of the presence of a cellular harbor at a very primitive neuronal developmental stage for virus persistence along further neuronal differentiation stages [101]. This notion of a gradual release of viral restriction blocks along neuronal differentiation was corroborated by the transition to an increased susceptibility to HCMV during neural differentiation of ESCs into neural spheres [103]. Susceptibility to HCMV appeared to be correlated to expression of the platelet-derived growth factor receptor alpha (PDGFRα) [103].…”

Section: The Infection Of Pluripotent Stem Cell-based Models Of Humanmentioning

confidence: 89%

Pluripotent Stem Cell-Based Models: A Peephole into Virus Infections during Early Pregnancy

Claus

Jung

Hübschen

2020

Cells

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The rubella virus (RV) was the first virus shown to be teratogenic in humans. The wealth of data on the clinical symptoms associated with congenital rubella syndrome is in stark contrast to an incomplete understanding of the forces leading to the teratogenic alterations in humans. This applies not only to RV, but also to congenital viral infections in general and includes (1) the mode of vertical transmission, even at early gestation, (2) the possible involvement of inflammation as a consequence of an activated innate immune response, and (3) the underlying molecular and cellular alterations. With the progress made in the development of pluripotent stem cell-based models including organoids and embryoids, it is now possible to assess congenital virus infections on a mechanistic level. Moreover, antiviral treatment options can be validated, and newly emerging viruses with a potential impact on human embryonal development, such as that recently reflected by the Zika virus (ZIKV), can be characterized. Here, we discuss human cytomegalovirus (HCMV) and ZIKV in comparison to RV as viruses with well-known congenital pathologies and highlight their analysis on current models for the early phase of human development. This includes the implications of their genetic variability and, as such, virus strain-specific properties for their use as archetype models for congenital virus infections. In this review, we will discuss the use of induced pluripotent stem cells (iPSC) and derived organoid systems for the study of congenital virus infections with a focus on their prominent aetiologies, HCMV, ZIKV, and RV. Their assessment on these models will provide valuable information on how human development is impaired by virus infections; it will also add new insights into the normal progression of human development through the analysis of developmental pathways in the context of virus-induced alterations. These are exciting perspectives for both developmental biology and congenital virology.

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“…Progenitors of the myeloid lineage are hosts for latent HCMV, and differentiation to macrophages or dendritic cells results in reactivation of the virus. Recently, Berger et al investigated the transition from restriction of HCMV infection in human embryonic stem cells (hESC) toward susceptibility in hESC-derived neural precursors [36]. Using protocols for controlled induction of differentiation of hESC into neural precursors, they discovered PDGFR-/ as a determinant of HCMV susceptibility.…”

Section: Cell Differentiationmentioning

confidence: 99%

Herpesviruses and Their Host Cells: A Successful Liaison

Adler

Christine

Adler

2017

Trends in Microbiology

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During a long history of coevolution, herpesviruses have reached a fine-tuned balance with their hosts, allowing them to successfully persist and spread to new hosts without causing too much damage. Only under certain circumstances, as in neonates or immunocompromised individuals, they may cause serious diseases. The delicate balance between herpesviruses and their hosts results from interactions of a great variety of viral and cellular factors which together shape the tropism for a particular host, tissue, or cell. Understanding these interactions will provide insight into the viral life cycle and cell biology in general. Moreover, it will also facilitate comprehension of herpesvirus pathogenesis, enabling the development of new strategies to combat herpesviruses in cases where they cause disease.

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Transition toward Human Cytomegalovirus Susceptibility in Early Human Embryonic Stem Cell-Derived Neural Precursors

Cited by 16 publications

References 51 publications

Human Cytomegalovirus Compromises Development of Cerebral Organoids

Human Cytomegalovirus Compromises Development of Cerebral Organoids

Pluripotent Stem Cell-Based Models: A Peephole into Virus Infections during Early Pregnancy

Herpesviruses and Their Host Cells: A Successful Liaison

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