Literature DB >> 35933637

Fetal Brain Damage in Human Fetuses with Congenital Cytomegalovirus Infection: Histological Features and Viral Tropism.

Giulia Piccirilli1, Liliana Gabrielli2, Maria Paola Bonasoni3, Angela Chiereghin1, Gabriele Turello1, Eva Caterina Borgatti4, Giuliana Simonazzi5, Silvia Felici1, Marta Leone4, Nunzio Cosimo Mario Salfi6, Donatella Santini7, Tiziana Lazzarotto1,4.   

Abstract

Human cytomegalovirus (HCMV) causes congenital neurological lifelong disabilities. To date, the neuropathogenesis of brain injury related to congenital HCMV (cCMV) infection is poorly understood. This study evaluates the characteristics and pathogenetic mechanisms of encephalic damage in cCMV infection. Ten HCMV-infected human fetuses at 21 weeks of gestation were examined. Specifically, tissues from different brain areas were analyzed by: (i) immunohistochemistry (IHC) to detect HCMV-infected cell distribution, (ii) hematoxylin-eosin staining to evaluate histological damage and (iii) real-time PCR to quantify tissue viral load (HCMV-DNA). The differentiation stage of HCMV-infected neural/neuronal cells was assessed by double IHC to detect simultaneously HCMV-antigens and neural/neuronal markers: nestin (a marker of neural stem/progenitor cells), doublecortin (DCX, marker of cells committed to the neuronal lineage) and neuronal nuclei (NeuN, identifying mature neurons). HCMV-positive cells and viral DNA were found in the brain of 8/10 (80%) fetuses. For these cases, brain damage was classified as mild (n = 4, 50%), moderate (n = 3, 37.5%) and severe (n = 1, 12.5%) based on presence and frequency of pathological findings (necrosis, microglial nodules, microglial activation, astrocytosis, and vascular changes). The highest median HCMV-DNA level was found in the hippocampus (212 copies/5 ng of human DNA [hDNA], range: 10-7,505) as well as the highest mean HCMV-infected cell value (2.9 cells, range: 0-23), followed by that detected in subventricular zone (1.7 cells, range: 0-19). These findings suggested a preferential viral tropism for both neural stem/progenitor cells and neuronal committed cells, residing in these regions, confirmed by the expression of DCX and nestin in 94% and 63.3% of HCMV-positive cells, respectively. NeuN was not found among HCMV-positive cells and was nearly absent in the brain with severe damage, suggesting HCMV does not infect mature neurons and immature neural/neuronal cells do not differentiate into neurons. This could lead to known structural and functional brain defects from cCMV infection.
© 2022. The Author(s).

Entities:  

Keywords:  Brain damage; Congenital infection; Cytomegalovirus; Human fetuses; Neural/neuronal cells; Viral tropism

Year:  2022        PMID: 35933637     DOI: 10.1007/s10571-022-01258-9

Source DB:  PubMed          Journal:  Cell Mol Neurobiol        ISSN: 0272-4340            Impact factor:   4.231


  71 in total

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Journal:  Kidney Int       Date:  1989-04       Impact factor: 10.612

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Journal:  J Virol       Date:  2015-08-19       Impact factor: 5.103

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Journal:  Biomaterials       Date:  2015-03-17       Impact factor: 12.479

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Authors:  Suresh B Boppana; Shannon A Ross; Karen B Fowler
Journal:  Clin Infect Dis       Date:  2013-12       Impact factor: 9.079

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Journal:  J Virol       Date:  2019-08-13       Impact factor: 5.103

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Journal:  Mol Biol Cell       Date:  2019-03-06       Impact factor: 4.138

7.  Association of LAG3 genetic variation with an increased risk of PD in Chinese female population.

Authors:  Wenyuan Guo; Miaomiao Zhou; Jiewen Qiu; Yuwan Lin; Xiang Chen; Shuxuan Huang; Mingshu Mo; Hanqun Liu; Guoyou Peng; Xiaoqin Zhu; Pingyi Xu
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Authors:  Xiao Chen; Dan-Bi Cho; Ping-Chang Yang
Journal:  N Am J Med Sci       Date:  2010-05

Review 10.  Nestin-expressing progenitor cells: function, identity and therapeutic implications.

Authors:  Aurora Bernal; Lorena Arranz
Journal:  Cell Mol Life Sci       Date:  2018-03-14       Impact factor: 9.261

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