Glioma-mediated microglial activation promotes glioma proliferation and migration: roles of Na<sup>+</sup>/H<sup>+</sup>exchanger isoform 1

Zhu, Wen; Carney, Karen E.; Pigott, Victoria M.; Falgoust, Lindsay; Clark, Paul A.; Kuo, John S.; Sun, Dandan

doi:10.1093/carcin/bgw068

Cited by 55 publications

(46 citation statements)

References 56 publications

(85 reference statements)

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“…All these cell lines were developed through SV40 immortalization of human primary microglial cells, whereas a fraction of SV40-immortalized adult microglial cells were further engineered to express the human telomerase reverse transcriptase (hTERT) and reduce the proliferation rate [19]. To the best of our knowledge, two cell lines are commercially available, the human microglial clone 3 cell line, HMC3 [17,[20][21][22] and the "Immortalized Human Microglia -SV40", developed and distributed by Applied Biological Materials (Vancouver, Canada) [23][24][25][26][27][28]. The HMC3 has been recently authenticated by the American Type Culture Collection (ATCC®), a leading nonprofit organization in the authentication and distribution of biologic material, microorganisms, and standards.…”

Section: Introductionmentioning

confidence: 99%

The human microglial HMC3 cell line: where do we stand? A systematic literature review

Russo

Cappoli

Coletta

et al. 2018

J Neuroinflammation

151

130

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Microglia, unique myeloid cells residing in the brain parenchyma, represent the first line of immune defense within the central nervous system. In addition to their immune functions, microglial cells play an important role in other cerebral processes, including the regulation of synaptic architecture and neurogenesis. Chronic microglial activation is regarded as detrimental, and it is considered a pathogenic mechanism common to several neurological disorders. Microglial activation and function have been extensively studied in rodent experimental models, whereas the characterization of human cells has been limited due to the restricted availability of primary sources of human microglia. To overcome this problem, human immortalized microglial cell lines have been developed. The human microglial clone 3 cell line, HMC3, was established in 1995, through SV40-dependent immortalization of human embryonic microglial cells. It has been recently authenticated by the American Type Culture Collection (ATCC®) and distributed under the name of HMC3 (ATCC®CRL-3304). The HMC3 cells have been used in six research studies, two of which also indicated by ATCC® as reference articles. However, a more accurate literature revision suggests that clone 3 was initially distributed under the name of CHME3. In this regard, several studies have been published, thus contributing to a more extensive characterization of this cell line. Remarkably, the same cell line has been used in different laboratories with other denominations, i.e., CHME-5 cells and C13-NJ cells. In view of the fact that “being now authenticated by ATCC®” may imply a wider distribution of the cells, we aimed at reviewing data obtained with the human microglia cell line clone 3, making the readers aware of this complicated nomenclature. In addition, we also included original data, generated in our laboratory with the HMC3 (ATCC®CRL-3304) cells, providing information on the current state of the culture together with supplementary details on the culturing procedures to obtain and maintain viable cells.

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Section: Introductionmentioning

confidence: 99%

The human microglial HMC3 cell line: where do we stand? A systematic literature review

Russo

Cappoli

Coletta

et al. 2018

J Neuroinflammation

151

130

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“…NHE1 plays an important role in regulating microglial intracellular pH (pH i ) homeostasis, their activation, and migration (Boscia et al, 2016;Liu et al, 2010;Shi et al, 2013;Zhao et al, 2016;Zhu et al, 2016). In particular, NHE1 maintains optimal pH i to support NADPH oxidase (NOX) function during microglial activation (Lam et al, 2013).…”

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confidence: 99%

Selective role of Na⁺/H⁺ exchanger in Cx3cr1⁺ microglial activation, white matter demyelination, and post‐stroke function recovery

Song

Wang

Pigott

et al. 2018

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Na /H exchanger (NHE1) activation is required for multiple microglial functions. We investigated effects of selective deletion of microglial Nhe1 in Cx3cr1-Cre ;Nhe1 mice on neuroinflammation and tissue repair after ischemic stroke. Infarct volume was similar in corn oil or tamoxifen (Tam)-treated mice at 48 hr and 14 days post-stroke. However, the Tam-treated mice showed significantly higher survival rate and faster neurological function recovery during day 1-14 post-stroke. Deletion of microglial Nhe1 prevented the elevation of CD11b /CD45 microglia in the ischemic hemisphere at day 3 post-stroke, but stimulated expression of Ym1, CD68, TGF-β, IL-10, decreased expression of CD86 and IL-1β, and reduced GFAP reactive astrocytes. Moreover, at day 14 post-stroke, enhanced white matter myelination was detected in the microglial Nhe1 deleted mice. In comparison, neuronal Nhe1-null mice (the CamKII-Cre ;Nhe1 mice) showed a significant reduction in both acute and subacute infarct volume, along with increased survival rate and moderate neurological function recovery. However, these neuronal Nhe1-null mice did not exhibit reduced activation of CD11b /CD45 microglia or CD11b /CD45 macrophages in the ischemic brains, and they exhibited no reductions in white matter lesions. Taken together, this study demonstrated that deletion of microglial and neuronal Nhe1 had differential effects on ischemic brain damage. Microglial NHE1 is involved in pro-inflammatory responses during post-stroke brain tissue repair. In contrast, neuronal NHE1 activation is directly associated with the acute ischemic neuronal injury but not inflammation. Our study reveals that NHE1 protein is a potential therapeutic target critical for differential regulation of ischemic neuronal injury, demyelination and tissue repair.

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“…Upregulation of the Na + /H + exchanger isoform 1 (NHE1), leading to increased intracellular sodium and increased intracellular pH, has been implicated in promoting glioma proliferation, invasion and resistance to temozolomide therapy[24, 25]. Another study demonstrated that in oligodendrogliomas, IDH-mutated and 1p/19q codeleted, the NHE1 on 1p is silenced, and proposes that this could be a major contributor to the low proliferation rates in these tumors[26].…”

Section: Discussionmentioning

confidence: 99%

Quantitative sodium imaging and gliomas: a feasibility study

et al. 2018

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Purpose: Recent advances in sodium brain MRI have allowed for increased signal-to-noise ratio, faster imaging and the ability of differentiating intracellular from extracellular sodium concentration, opening a new window of opportunity for clinical application. In gliomas there are significant alterations in sodium metabolism, including increase in total sodium concentration and extracellular volume fraction. The purpose of this study is to assess the feasibility of using sodium MRI quantitative measurements to evaluate gliomas. Methods: Eight patients with treatment naïve gliomas were scanned at 3 Tesla with a homemade 1H/23Na head coil, generating maps of pseudo-intracellular sodium concentration (C1), pseudo-extracellular volume fraction (α2), apparent intracellular sodium concentration (aISC) and apparent total sodium concentration (aTSC). Measurements were made within the contralateral normal appearing putamen, contralateral normal appearing white matter (NAWM) and in solid tumor regions (area of T2-FLAIR abnormality, excluding highly likely areas of edema, cysts, or necrosis). Paired samples t-test were performed comparing NAWM and putamen and between NAWM and solid tumor. Results: Normal appearing putamen demonstrated significantly higher values for aTSC, aISC, C1 (p<0.001), and α2 (p=0.002) when compared to NAWM. Mean average of all solid tumors, when compared to NAWM, demonstrated significantly higher values of aTSC and α2 (p<0.001), and significantly lower values of aISC (p=0.02), There was no significant difference between the values of C1 (p=0.19). Conclusion: Quantitative sodium measurements can be done in glioma patients and also has provided further evidence that total sodium and extracellular volume fraction are increased in gliomas.

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Glioma-mediated microglial activation promotes glioma proliferation and migration: roles of Na⁺/H⁺exchanger isoform 1

Cited by 55 publications

References 56 publications

The human microglial HMC3 cell line: where do we stand? A systematic literature review

The human microglial HMC3 cell line: where do we stand? A systematic literature review

Selective role of Na⁺/H⁺ exchanger in Cx3cr1⁺ microglial activation, white matter demyelination, and post‐stroke function recovery

Quantitative sodium imaging and gliomas: a feasibility study

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Glioma-mediated microglial activation promotes glioma proliferation and migration: roles of Na+/H+exchanger isoform 1

Cited by 55 publications

References 56 publications

The human microglial HMC3 cell line: where do we stand? A systematic literature review

The human microglial HMC3 cell line: where do we stand? A systematic literature review

Selective role of Na+/H+ exchanger in Cx3cr1+ microglial activation, white matter demyelination, and post‐stroke function recovery

Quantitative sodium imaging and gliomas: a feasibility study

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Product

Resources

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Glioma-mediated microglial activation promotes glioma proliferation and migration: roles of Na⁺/H⁺exchanger isoform 1

Selective role of Na⁺/H⁺ exchanger in Cx3cr1⁺ microglial activation, white matter demyelination, and post‐stroke function recovery