<scp>RNA</scp>‐sequencing profiles hippocampal gene expression in a validated model of cancer‐induced depression

Nashed, Mina G.; Linher‐Melville, Katja; Frey, Benício N.; Singh, Gurmit

doi:10.1111/gbb.12323

Cited by 10 publications

(10 citation statements)

References 68 publications

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“…Several mRNA targets previously reported to be related to cancer- and drug-induced depression were affected by peripheral tumor in the present study, demonstrating parallel outcomes to those previously reported in SC tumor-bearing mice,20 with these effects being amplified in IF tumor-bearing mice. In particular, GluRs and glutamatergic modulators present on microglia (glutamate ionotropic receptor NMDA type subunit 2C [Grin2c], glutamate ionotropic receptor AMPA type subunit 4 [Gria4], gamma-aminobutyric acid type A receptor alpha 3 subunit [Gabra3], and glutamate metabotropic receptor 4 [Grm4]) were reduced across Pexidartinib- and control-treated IF and SC tumor groups, with the exception of increased Grin2c mRNA in IF tumor-bearing mice relative to sham.…”

Section: Resultssupporting

confidence: 89%

“…Isolated hippocampi were dissociated, preserved in RNAlater, and total RNA was isolated from each sample using the RNeasy Kit (Qiagen), as described previously 20. Briefly, eluates were DNase-treated using the DNA-free Kit (DNase Treatment and Removal Reagents; Ambion) and RNA quality/purity was quantitated using spectrophotometric analysis at OD 260 /OD 280 .…”

Section: Methodsmentioning

confidence: 99%

“…Relative mRNA levels were quantified using qPCR, adopted from previous reports 20. Briefly, cDNA was synthesized from 400 ng total RNA via reverse transcription using Superscript III kit (Life Technologies) and qPCR assays were performed for each target and reference gene per sample with SsoAdvanced Universal SYBR Green Supermix (BioRad).…”

Section: Methodsmentioning

confidence: 99%

“…Our lab recently developed a validated murine model of cancer-induced depression (CID) using 4T1 carcinoma cells, in which subcutaneous (SC) tumor burden was associated with increased depressive-like symptoms 19. RNA-sequencing and real-time RT-PCR analysis of hippocampi revealed considerable overlap between cancer-induced and positive control corticosterone-induced depressive states 20. Several of the validated hippocampal mRNA targets associated with the depressive-like state in tumor-bearing mice were ionotropic and metabotropic glutamate receptors (GluRs) and glutamatergic modulators,20 many of which are expressed or secreted by microglia (reviewed in Murugan et al21).…”

Section: Introductionmentioning

confidence: 99%

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<p>Activation of hippocampal microglia in a murine model of cancer-induced pain</p>

Miladinovic¹,

Sharma²,

Phan³

et al. 2019

JPR

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IntroductionPain is a common and debilitating comorbidity of metastatic breast cancer. The hippocampus has been implicated in nociceptive processing, particularly relating to the subjective aspect of pain. Here, a syngeneic mouse model was used to characterize the effects of peripheral tumors on hippocampal microglial activation in relation to cancer-induced pain (CIP).Materials and methodsMice were systemically treated with the colony-stimulating factor 1 receptor inhibitor Pexidartinib prior to intrafemoral (IF) or subcutaneous 4T1 carcinoma cell inoculation. Spontaneous and evoked nociceptive responses were quantitated throughout tumor development, and contralateral hippocampi were collected via endpoint microdissection for RNA analysis. Additionally, IF tumor-bearing animals were sacrificed on days 5, 10, 15, and 20 post 4T1 cell inoculation, and brain sections were immunofluorescently stained for Iba1, a marker of activated microglia.ResultsAblation of these neuroimmune cells with the CSF1R inhibitor Pexidartinib delayed the onset and severity of cancer-induced nociceptive behaviors in IF tumor-bearing animals, adding to the body of literature that demonstrates microglial contribution to the development and maintenance of CIP. Furthermore, in untreated IF tumor-bearing mice, nociceptive behaviors appeared to progress in parallel with microglial activation in hippocampal regions. Immunofluorescent Iba1+ microglia increased in the dentate gyrus and cornu ammonis 1 hippocampal regions in IF tumor-bearing animals over time, which was confirmed at the mRNA level using relevant microglial markers.ConclusionThis is the first experimental evidence to demonstrate the effects of peripheral tumor-induced nociception on hippocampal microglial activation. The increase in hippocampal microglia observed in the present study may reflect the emotional and cognitive deficits reported by patients with CIP.

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Section: Resultssupporting

confidence: 89%

Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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<p>Activation of hippocampal microglia in a murine model of cancer-induced pain</p>

Miladinovic¹,

Sharma²,

Phan³

et al. 2019

JPR

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“…27 Analysis was carried out using a web-based platform, the Galaxy Project, as previously described. 25,26 Briefly, the FastQC tool, Tophat, Cufflinks, and Cuffmerge were applied to evaluate the quality of sequencing, align reads to the human GRCh38/hg38 assembly, create assembled transcripts, and create a transcriptome assembly, respectively. Cuffdiff was then used to assess the transcript abundance in fragments per kilobase of transcript per million mapped reads (FPKM) and to identify the differentially expressed genes (DEGs) by merging the transcriptome assembly with individual aligned reads created by Tophat.…”

Section: Methodsmentioning

confidence: 99%

xCT knockdown in human breast cancer cells delays onset of cancer-induced bone pain

et al. 2019

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Cancers in the bone produce a number of severe symptoms including pain that compromises patient functional status, quality of life, and survival. The source of this pain is multifaceted and includes factors secreted from tumor cells. Malignant cells release the neurotransmitter and cell-signaling molecule glutamate via the oxidative stress-related cystine/glutamate antiporter, system xC−, which reciprocally imports cystine for synthesis of glutathione and the cystine/cysteine redox cycle. Pharmacological inhibition of system xC− has shown success in reducing and delaying the onset of cancer pain-related behavior in mouse models. This investigation describes the development of a stable siRNA-induced knockdown of the functional trans-membrane system xC− subunit xCT (SLC7A11) in the human breast cancer cell line MDA-MB-231. Clones were verified for xCT knockdown at the transcript, protein, and functional levels. RNAseq was performed on a representative clone to comprehensively examine the transcriptional cellular signature in response to xCT knockdown, identifying multiple differentially regulated factors relevant to cancer pain including nerve growth factor, interleukin-1, and colony-stimulating factor-1. Mice were inoculated intrafemorally and recordings of pain-related behaviors including weight bearing, mechanical withdrawal, and limb use were performed. Animals implanted with xCT knockdown cancer cells displayed a delay until the onset of nociceptive behaviors relative to control cells. These results add to the body of evidence suggesting that a reduction in glutamate release from cancers in bone by inhibition of the system xC− transporter may decrease the severe and intractable pain associated with bone metastases.

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Accumulation and neuroprotective effects of lithium on hepatocellular carcinoma mice model

Bgatova,

Obanina,

Taskaeva

et al. 2024

Behavioural Brain Research

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RNA‐sequencing profiles hippocampal gene expression in a validated model of cancer‐induced depression

Cited by 10 publications

References 68 publications

<p>Activation of hippocampal microglia in a murine model of cancer-induced pain</p>

<p>Activation of hippocampal microglia in a murine model of cancer-induced pain</p>

xCT knockdown in human breast cancer cells delays onset of cancer-induced bone pain

Accumulation and neuroprotective effects of lithium on hepatocellular carcinoma mice model

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