Transcriptome Analyses in BV2 Microglial Cells Following Treatment with Amino-Terminal Fragments of Apolipoprotein E

Tanner B. Pollock; Giovan N. Cholico; Noail F. Isho; Ryan J. Day; Tarun Suresh; Erica S. Stewart; Madyson M. McCarthy; Troy T. Rohn

doi:10.3389/fnagi.2020.00256

Transcriptome Analyses in BV2 Microglial Cells Following Treatment with Amino-Terminal Fragments of Apolipoprotein E

Tanner B. Pollock
, Giovan N. Cholico
, Noail F. Isho
, Ryan J. Day
, Tarun Suresh
, Erica S. Stewart
, Madyson M. McCarthy
, Troy T. Rohn

Biological Sciences

Research output: Contribution to journal › Article › peer-review

8 Scopus citations

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Abstract

Despite the fact that harboring the apolipoprotein E4 (APOE4) allele represents the single greatest risk factor for late-onset Alzheimer’s disease (AD), the exact mechanism by which ApoE4 contributes to disease progression remains unknown. Recently, we demonstrated that a 151 amino-terminal fragment of ApoE4 (nApoE4_1–151) localizes within the nucleus of microglia in the human AD brain and traffics to the nucleus causing toxicity in BV2 microglia cells. In the present study, we examined in detail what genes may be affected following treatment by nApoE4_1–151. Transcriptome analyses in BV2 microglial cells following sublethal treatment with nApoE4_1–151 revealed the upregulation of almost 4,000 genes, with 20 of these genes upregulated 182- to 715-fold compared to untreated control cells. The majority of these 20 genes play a role in the immune response and polarization toward microglial M1 activation. As a control, an identical nApoE3_1–151 fragment that differed by a single amino acid at position 112 (Cys→Arg) was tested and produced a similar albeit lower level of upregulation of an identical set of genes. In this manner, enriched pathways upregulated by nApoE3_1–151 and nApoE4_1–151 following exogenous treatment included Toll receptor signaling, chemokine/cytokine signaling and apoptosis signaling. There were unique genes differentially expressed by at least two-fold for either fragment. For nApoE3_1–151, these included 16 times as many genes, many of which are involved in physiological functions within microglia. For nApoE4_1–151, on the other hand the number genes uniquely upregulated was significantly lower, with many of the top upregulated genes having unknown functions. Taken together, our results suggest that while nApoE3_1–151 may serve a more physiological role in microglia, nApoE4_1–151 may activate genes that contribute to disease inflammation associated with AD. These data support the hypothesis that the link between harboring the APOE4 allele and dementia risk could be enhanced inflammation through activation of microglia.

Original language	American English
Article number	256
Journal	Frontiers in Aging Neuroscience
Volume	12
Early online date	12 Aug 2020
DOIs	https://doi.org/10.3389/fnagi.2020.00256
State	Published - Aug 2020

Keywords

Alzheimer’s disease
apolipoprotein E4
BV2 cells
inflammation
M1 phenotype
microglia cells
RNA-seq
toxicity

EGS Disciplines

Biology
Neuroscience and Neurobiology

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10.3389/fnagi.2020.00256License: CC BY

https://scholarworks.boisestate.edu/bio_facpubs/624/License: CC BY

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@article{b6b609695ae94685b3cb4b1df874c822,

title = "Transcriptome Analyses in BV2 Microglial Cells Following Treatment with Amino-Terminal Fragments of Apolipoprotein E",

abstract = "Despite the fact that harboring the apolipoprotein E4 (APOE4) allele represents the single greatest risk factor for late-onset Alzheimer{\textquoteright}s disease (AD), the exact mechanism by which ApoE4 contributes to disease progression remains unknown. Recently, we demonstrated that a 151 amino-terminal fragment of ApoE4 (nApoE41–151) localizes within the nucleus of microglia in the human AD brain and traffics to the nucleus causing toxicity in BV2 microglia cells. In the present study, we examined in detail what genes may be affected following treatment by nApoE41–151. Transcriptome analyses in BV2 microglial cells following sublethal treatment with nApoE41–151 revealed the upregulation of almost 4,000 genes, with 20 of these genes upregulated 182- to 715-fold compared to untreated control cells. The majority of these 20 genes play a role in the immune response and polarization toward microglial M1 activation. As a control, an identical nApoE31–151 fragment that differed by a single amino acid at position 112 (Cys→Arg) was tested and produced a similar albeit lower level of upregulation of an identical set of genes. In this manner, enriched pathways upregulated by nApoE31–151 and nApoE41–151 following exogenous treatment included Toll receptor signaling, chemokine/cytokine signaling and apoptosis signaling. There were unique genes differentially expressed by at least two-fold for either fragment. For nApoE31–151, these included 16 times as many genes, many of which are involved in physiological functions within microglia. For nApoE41–151, on the other hand the number genes uniquely upregulated was significantly lower, with many of the top upregulated genes having unknown functions. Taken together, our results suggest that while nApoE31–151 may serve a more physiological role in microglia, nApoE41–151 may activate genes that contribute to disease inflammation associated with AD. These data support the hypothesis that the link between harboring the APOE4 allele and dementia risk could be enhanced inflammation through activation of microglia.",

keywords = "Alzheimer{\textquoteright}s disease, apolipoprotein E4, BV2 cells, inflammation, M1 phenotype, microglia cells, RNA-seq, toxicity",

author = "Pollock, \{Tanner B.\} and Cholico, \{Giovan N.\} and Isho, \{Noail F.\} and Day, \{Ryan J.\} and Tarun Suresh and Stewart, \{Erica S.\} and McCarthy, \{Madyson M.\} and Rohn, \{Troy T.\}",

note = "Publisher Copyright: {\textcopyright} Copyright {\textcopyright} 2020 Pollock, Cholico, Isho, Day, Suresh, Stewart, McCarthy and Rohn.",

year = "2020",

month = aug,

doi = "10.3389/fnagi.2020.00256",

language = "American English",

volume = "12",

}

TY - JOUR

T1 - Transcriptome Analyses in BV2 Microglial Cells Following Treatment with Amino-Terminal Fragments of Apolipoprotein E

AU - Pollock, Tanner B.

AU - Cholico, Giovan N.

AU - Isho, Noail F.

AU - Day, Ryan J.

AU - Suresh, Tarun

AU - Stewart, Erica S.

AU - McCarthy, Madyson M.

AU - Rohn, Troy T.

PY - 2020/8

Y1 - 2020/8

N2 - Despite the fact that harboring the apolipoprotein E4 (APOE4) allele represents the single greatest risk factor for late-onset Alzheimer’s disease (AD), the exact mechanism by which ApoE4 contributes to disease progression remains unknown. Recently, we demonstrated that a 151 amino-terminal fragment of ApoE4 (nApoE41–151) localizes within the nucleus of microglia in the human AD brain and traffics to the nucleus causing toxicity in BV2 microglia cells. In the present study, we examined in detail what genes may be affected following treatment by nApoE41–151. Transcriptome analyses in BV2 microglial cells following sublethal treatment with nApoE41–151 revealed the upregulation of almost 4,000 genes, with 20 of these genes upregulated 182- to 715-fold compared to untreated control cells. The majority of these 20 genes play a role in the immune response and polarization toward microglial M1 activation. As a control, an identical nApoE31–151 fragment that differed by a single amino acid at position 112 (Cys→Arg) was tested and produced a similar albeit lower level of upregulation of an identical set of genes. In this manner, enriched pathways upregulated by nApoE31–151 and nApoE41–151 following exogenous treatment included Toll receptor signaling, chemokine/cytokine signaling and apoptosis signaling. There were unique genes differentially expressed by at least two-fold for either fragment. For nApoE31–151, these included 16 times as many genes, many of which are involved in physiological functions within microglia. For nApoE41–151, on the other hand the number genes uniquely upregulated was significantly lower, with many of the top upregulated genes having unknown functions. Taken together, our results suggest that while nApoE31–151 may serve a more physiological role in microglia, nApoE41–151 may activate genes that contribute to disease inflammation associated with AD. These data support the hypothesis that the link between harboring the APOE4 allele and dementia risk could be enhanced inflammation through activation of microglia.

AB - Despite the fact that harboring the apolipoprotein E4 (APOE4) allele represents the single greatest risk factor for late-onset Alzheimer’s disease (AD), the exact mechanism by which ApoE4 contributes to disease progression remains unknown. Recently, we demonstrated that a 151 amino-terminal fragment of ApoE4 (nApoE41–151) localizes within the nucleus of microglia in the human AD brain and traffics to the nucleus causing toxicity in BV2 microglia cells. In the present study, we examined in detail what genes may be affected following treatment by nApoE41–151. Transcriptome analyses in BV2 microglial cells following sublethal treatment with nApoE41–151 revealed the upregulation of almost 4,000 genes, with 20 of these genes upregulated 182- to 715-fold compared to untreated control cells. The majority of these 20 genes play a role in the immune response and polarization toward microglial M1 activation. As a control, an identical nApoE31–151 fragment that differed by a single amino acid at position 112 (Cys→Arg) was tested and produced a similar albeit lower level of upregulation of an identical set of genes. In this manner, enriched pathways upregulated by nApoE31–151 and nApoE41–151 following exogenous treatment included Toll receptor signaling, chemokine/cytokine signaling and apoptosis signaling. There were unique genes differentially expressed by at least two-fold for either fragment. For nApoE31–151, these included 16 times as many genes, many of which are involved in physiological functions within microglia. For nApoE41–151, on the other hand the number genes uniquely upregulated was significantly lower, with many of the top upregulated genes having unknown functions. Taken together, our results suggest that while nApoE31–151 may serve a more physiological role in microglia, nApoE41–151 may activate genes that contribute to disease inflammation associated with AD. These data support the hypothesis that the link between harboring the APOE4 allele and dementia risk could be enhanced inflammation through activation of microglia.

KW - Alzheimer’s disease

KW - apolipoprotein E4

KW - BV2 cells

KW - inflammation

KW - M1 phenotype

KW - microglia cells

KW - RNA-seq

KW - toxicity

UR - https://www.scopus.com/pages/publications/85089999032

U2 - 10.3389/fnagi.2020.00256

DO - 10.3389/fnagi.2020.00256

M3 - Article

VL - 12

JO - Frontiers in Aging Neuroscience

JF - Frontiers in Aging Neuroscience

M1 - 256

ER -

Transcriptome Analyses in BV2 Microglial Cells Following Treatment with Amino-Terminal Fragments of Apolipoprotein E

Abstract

Keywords

EGS Disciplines

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