Modulation of neural stem/progenitor cell proliferation during experimental Herpes Simplex encephalitis is mediated by differential FGF-2 expression in the adult brain

Modulation of neural stem/progenitor cell proliferation during experimental Herpes Simplex encephalitis is mediated by differential FGF-2 expression in the adult brain

Neural stem cells (NSCs) respond to inflammatory cues induced during brain injury and are thought to be involved in recovery from brain damage. Little is known about NSC response during brain infections. The present study evaluated NSC proliferation during Herpes Simplex Virus-1 brain infection. Tot...

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Main Authors: Jessica H. Rotschafer, Shuxian Hu, Morgan Little, Melissa Erickson, Walter C. Low, Maxim C.J. Cheeran
Format: Article
Language:English
Published: Elsevier 2013-10-01
Series:Neurobiology of Disease
Subjects:
Herpes Simplex encephalitis
Neural stem cells
Proliferation
FGF-2
Adult neurogenesis
Online Access:http://www.sciencedirect.com/science/article/pii/S0969996113001605
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spelling doaj-8aeddbc86fb14215ab29abf3f4ba3a9c2021-03-22T12:40:03ZengElsevierNeurobiology of Disease1095-953X2013-10-0158144155Modulation of neural stem/progenitor cell proliferation during experimental Herpes Simplex encephalitis is mediated by differential FGF-2 expression in the adult brainJessica H. Rotschafer0Shuxian Hu1Morgan Little2Melissa Erickson3Walter C. Low4Maxim C.J. Cheeran5Department of Veterinary Population Medicine, University of Minnesota, St. Paul, MN 55108, USACenter for Infectious Diseases and Microbiology Translational Research, Department of Medicine, University of Minnesota, Minneapolis, MN 55455, USACenter for Infectious Diseases and Microbiology Translational Research, Department of Medicine, University of Minnesota, Minneapolis, MN 55455, USADepartment of Veterinary Population Medicine, University of Minnesota, St. Paul, MN 55108, USADepartment of Neurosurgery, University of Minnesota, Minneapolis, MN 55455, USA; Stem Cell Institute, University of Minnesota, Minneapolis, MN 55455, USADepartment of Veterinary Population Medicine, University of Minnesota, St. Paul, MN 55108, USA; Corresponding author at: 225 Veterinary Medical Center North, 1365 Gortner Ave, St. Paul, MN 55108, USA. Fax: +1 612 625 6241.Neural stem cells (NSCs) respond to inflammatory cues induced during brain injury and are thought to be involved in recovery from brain damage. Little is known about NSC response during brain infections. The present study evaluated NSC proliferation during Herpes Simplex Virus-1 brain infection. Total numbers of nestin(+) NSCs increased significantly in infected brains at 6 days post infection (p.i.). However, by 15 days p.i. the nestin(+) population decreased significantly below levels observed in uninfected brains and remained depressed through 30 days p.i. This initial increase in NSC population occurred concurrently with increased brain cell proliferation, which peaked at 3 days p.i. On closer examination, we found that while actively proliferating Sox2(+) NSCs increased in number at 6 days p.i., proliferating DCX(+) neuroblasts contributed to the increased response at 3 days p.i. However, overall proliferation decreased steadily from 15 days p.i. to below control levels. To determine the mechanisms involved in altering NSC proliferation, neurotrophin and growth factor expression profiles were assessed. FGF-2 gene expression increased at 5 days p.i. and was robustly down-regulated at 15 days p.i. (>1000-fold), which was further confirmed by increased FGF-2 immunostaining around the lateral ventricles. Furthermore, supplementing infected animals with recombinant FGF-2, at 15 days p.i., significantly increased the number of proliferating brain cells. These findings demonstrate that the temporal changes in NSC proliferation are mediated through the regulation of FGF-2 and that the NSC niche may benefit from supplementation with FGF-2 during HSV-1 brain infection.http://www.sciencedirect.com/science/article/pii/S0969996113001605Herpes Simplex encephalitisNeural stem cellsProliferationFGF-2Adult neurogenesis
collection DOAJ
language English
format Article
sources DOAJ
author Jessica H. Rotschafer
Shuxian Hu
Morgan Little
Melissa Erickson
Walter C. Low
Maxim C.J. Cheeran
spellingShingle Jessica H. Rotschafer
Shuxian Hu
Morgan Little
Melissa Erickson
Walter C. Low
Maxim C.J. Cheeran
Modulation of neural stem/progenitor cell proliferation during experimental Herpes Simplex encephalitis is mediated by differential FGF-2 expression in the adult brain
Neurobiology of Disease
Herpes Simplex encephalitis
Neural stem cells
Proliferation
FGF-2
Adult neurogenesis
author_facet Jessica H. Rotschafer
Shuxian Hu
Morgan Little
Melissa Erickson
Walter C. Low
Maxim C.J. Cheeran
author_sort Jessica H. Rotschafer
title Modulation of neural stem/progenitor cell proliferation during experimental Herpes Simplex encephalitis is mediated by differential FGF-2 expression in the adult brain
title_short Modulation of neural stem/progenitor cell proliferation during experimental Herpes Simplex encephalitis is mediated by differential FGF-2 expression in the adult brain
title_full Modulation of neural stem/progenitor cell proliferation during experimental Herpes Simplex encephalitis is mediated by differential FGF-2 expression in the adult brain
title_fullStr Modulation of neural stem/progenitor cell proliferation during experimental Herpes Simplex encephalitis is mediated by differential FGF-2 expression in the adult brain
title_full_unstemmed Modulation of neural stem/progenitor cell proliferation during experimental Herpes Simplex encephalitis is mediated by differential FGF-2 expression in the adult brain
title_sort modulation of neural stem/progenitor cell proliferation during experimental herpes simplex encephalitis is mediated by differential fgf-2 expression in the adult brain
publisher Elsevier
series Neurobiology of Disease
issn 1095-953X
publishDate 2013-10-01
description Neural stem cells (NSCs) respond to inflammatory cues induced during brain injury and are thought to be involved in recovery from brain damage. Little is known about NSC response during brain infections. The present study evaluated NSC proliferation during Herpes Simplex Virus-1 brain infection. Total numbers of nestin(+) NSCs increased significantly in infected brains at 6 days post infection (p.i.). However, by 15 days p.i. the nestin(+) population decreased significantly below levels observed in uninfected brains and remained depressed through 30 days p.i. This initial increase in NSC population occurred concurrently with increased brain cell proliferation, which peaked at 3 days p.i. On closer examination, we found that while actively proliferating Sox2(+) NSCs increased in number at 6 days p.i., proliferating DCX(+) neuroblasts contributed to the increased response at 3 days p.i. However, overall proliferation decreased steadily from 15 days p.i. to below control levels. To determine the mechanisms involved in altering NSC proliferation, neurotrophin and growth factor expression profiles were assessed. FGF-2 gene expression increased at 5 days p.i. and was robustly down-regulated at 15 days p.i. (>1000-fold), which was further confirmed by increased FGF-2 immunostaining around the lateral ventricles. Furthermore, supplementing infected animals with recombinant FGF-2, at 15 days p.i., significantly increased the number of proliferating brain cells. These findings demonstrate that the temporal changes in NSC proliferation are mediated through the regulation of FGF-2 and that the NSC niche may benefit from supplementation with FGF-2 during HSV-1 brain infection.
topic Herpes Simplex encephalitis
Neural stem cells
Proliferation
FGF-2
Adult neurogenesis
url http://www.sciencedirect.com/science/article/pii/S0969996113001605
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