app ki mice Search Results


app ps1 ki mice  (Oxford Instruments)
99
Oxford Instruments app ps1 ki mice
Selective attenuation of proinflammatory cytokines by MW150 administration in <t>APP/PS1</t> KI mice cortex. a 11–12-month-old wild type ( WT ) or APP/PS1 knock-in ( KI ) mice were treated with saline vehicle ( veh ) or 2.5 mg/kg MW150 by intraperitoneal injection (i.p.) once daily for 14 days. b IL-1β was increased in KI + veh mice compared to WT + veh mice ( p = 0.0012), and MW150 treatment of KI mice (KI + MW150) significantly attenuated IL-1β levels compared to KI + veh ( p = 0.0243) ( F (2,38) = 6.46; p = 0.004). c TNFα was elevated in KI + veh mice compared to WT + veh and attenuated in KI + MW150 mice compared to KI + veh; however, these changes were not significant ( F (2,38) = 1.11; p = 0.34). d IL-6 was slightly elevated in KI + veh compared to WT + veh mice, and there was no effect of MW150 treatment ( n = 11 WT + veh; n = 14 KI + veh; n = 14 KI + MW150). Data are mean ± SEM. Source data is available in Additional file : Table S1
App Ps1 Ki Mice, supplied by Oxford Instruments, used in various techniques. Bioz Stars score: 99/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
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Average 99 stars, based on 1 article reviews
app ps1 ki mice - by Bioz Stars, 2026-06
99/100 stars
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app ki mice  (Addgene inc)
94
Addgene inc app ki mice
Selective attenuation of proinflammatory cytokines by MW150 administration in <t>APP/PS1</t> KI mice cortex. a 11–12-month-old wild type ( WT ) or APP/PS1 knock-in ( KI ) mice were treated with saline vehicle ( veh ) or 2.5 mg/kg MW150 by intraperitoneal injection (i.p.) once daily for 14 days. b IL-1β was increased in KI + veh mice compared to WT + veh mice ( p = 0.0012), and MW150 treatment of KI mice (KI + MW150) significantly attenuated IL-1β levels compared to KI + veh ( p = 0.0243) ( F (2,38) = 6.46; p = 0.004). c TNFα was elevated in KI + veh mice compared to WT + veh and attenuated in KI + MW150 mice compared to KI + veh; however, these changes were not significant ( F (2,38) = 1.11; p = 0.34). d IL-6 was slightly elevated in KI + veh compared to WT + veh mice, and there was no effect of MW150 treatment ( n = 11 WT + veh; n = 14 KI + veh; n = 14 KI + MW150). Data are mean ± SEM. Source data is available in Additional file : Table S1
App Ki Mice, supplied by Addgene inc, used in various techniques. Bioz Stars score: 94/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
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Average 94 stars, based on 1 article reviews
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app nl-g-f mice  (BioResource International Inc)
90
BioResource International Inc app nl-g-f mice
Selective attenuation of proinflammatory cytokines by MW150 administration in <t>APP/PS1</t> KI mice cortex. a 11–12-month-old wild type ( WT ) or APP/PS1 knock-in ( KI ) mice were treated with saline vehicle ( veh ) or 2.5 mg/kg MW150 by intraperitoneal injection (i.p.) once daily for 14 days. b IL-1β was increased in KI + veh mice compared to WT + veh mice ( p = 0.0012), and MW150 treatment of KI mice (KI + MW150) significantly attenuated IL-1β levels compared to KI + veh ( p = 0.0243) ( F (2,38) = 6.46; p = 0.004). c TNFα was elevated in KI + veh mice compared to WT + veh and attenuated in KI + MW150 mice compared to KI + veh; however, these changes were not significant ( F (2,38) = 1.11; p = 0.34). d IL-6 was slightly elevated in KI + veh compared to WT + veh mice, and there was no effect of MW150 treatment ( n = 11 WT + veh; n = 14 KI + veh; n = 14 KI + MW150). Data are mean ± SEM. Source data is available in Additional file : Table S1
App Nl G F Mice, supplied by BioResource International Inc, used in various techniques. Bioz Stars score: 90/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
https://www.bioz.com/result/app nl-g-f mice/product/BioResource International Inc
Average 90 stars, based on 1 article reviews
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90/100 stars
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app saaki ki x htfrki ki  (Denali Therapeutics)
86
Denali Therapeutics app saaki ki x htfrki ki
Selective attenuation of proinflammatory cytokines by MW150 administration in <t>APP/PS1</t> KI mice cortex. a 11–12-month-old wild type ( WT ) or APP/PS1 knock-in ( KI ) mice were treated with saline vehicle ( veh ) or 2.5 mg/kg MW150 by intraperitoneal injection (i.p.) once daily for 14 days. b IL-1β was increased in KI + veh mice compared to WT + veh mice ( p = 0.0012), and MW150 treatment of KI mice (KI + MW150) significantly attenuated IL-1β levels compared to KI + veh ( p = 0.0243) ( F (2,38) = 6.46; p = 0.004). c TNFα was elevated in KI + veh mice compared to WT + veh and attenuated in KI + MW150 mice compared to KI + veh; however, these changes were not significant ( F (2,38) = 1.11; p = 0.34). d IL-6 was slightly elevated in KI + veh compared to WT + veh mice, and there was no effect of MW150 treatment ( n = 11 WT + veh; n = 14 KI + veh; n = 14 KI + MW150). Data are mean ± SEM. Source data is available in Additional file : Table S1
App Saaki Ki X Htfrki Ki, supplied by Denali Therapeutics, used in various techniques. Bioz Stars score: 86/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
https://www.bioz.com/result/app saaki ki x htfrki ki/product/Denali Therapeutics
Average 86 stars, based on 1 article reviews
app saaki ki x htfrki ki - by Bioz Stars, 2026-06
86/100 stars
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app saa ki mice  (Jackson Laboratory)
86
Jackson Laboratory app saa ki mice
Selective attenuation of proinflammatory cytokines by MW150 administration in <t>APP/PS1</t> KI mice cortex. a 11–12-month-old wild type ( WT ) or APP/PS1 knock-in ( KI ) mice were treated with saline vehicle ( veh ) or 2.5 mg/kg MW150 by intraperitoneal injection (i.p.) once daily for 14 days. b IL-1β was increased in KI + veh mice compared to WT + veh mice ( p = 0.0012), and MW150 treatment of KI mice (KI + MW150) significantly attenuated IL-1β levels compared to KI + veh ( p = 0.0243) ( F (2,38) = 6.46; p = 0.004). c TNFα was elevated in KI + veh mice compared to WT + veh and attenuated in KI + MW150 mice compared to KI + veh; however, these changes were not significant ( F (2,38) = 1.11; p = 0.34). d IL-6 was slightly elevated in KI + veh compared to WT + veh mice, and there was no effect of MW150 treatment ( n = 11 WT + veh; n = 14 KI + veh; n = 14 KI + MW150). Data are mean ± SEM. Source data is available in Additional file : Table S1
App Saa Ki Mice, supplied by Jackson Laboratory, used in various techniques. Bioz Stars score: 86/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
https://www.bioz.com/result/app saa ki mice/product/Jackson Laboratory
Average 86 stars, based on 1 article reviews
app saa ki mice - by Bioz Stars, 2026-06
86/100 stars
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wt app ki mice  (Jackson Laboratory)
86
Jackson Laboratory wt app ki mice
Selective attenuation of proinflammatory cytokines by MW150 administration in <t>APP/PS1</t> KI mice cortex. a 11–12-month-old wild type ( WT ) or APP/PS1 knock-in ( KI ) mice were treated with saline vehicle ( veh ) or 2.5 mg/kg MW150 by intraperitoneal injection (i.p.) once daily for 14 days. b IL-1β was increased in KI + veh mice compared to WT + veh mice ( p = 0.0012), and MW150 treatment of KI mice (KI + MW150) significantly attenuated IL-1β levels compared to KI + veh ( p = 0.0243) ( F (2,38) = 6.46; p = 0.004). c TNFα was elevated in KI + veh mice compared to WT + veh and attenuated in KI + MW150 mice compared to KI + veh; however, these changes were not significant ( F (2,38) = 1.11; p = 0.34). d IL-6 was slightly elevated in KI + veh compared to WT + veh mice, and there was no effect of MW150 treatment ( n = 11 WT + veh; n = 14 KI + veh; n = 14 KI + MW150). Data are mean ± SEM. Source data is available in Additional file : Table S1
Wt App Ki Mice, supplied by Jackson Laboratory, used in various techniques. Bioz Stars score: 86/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
https://www.bioz.com/result/wt app ki mice/product/Jackson Laboratory
Average 86 stars, based on 1 article reviews
wt app ki mice - by Bioz Stars, 2026-06
86/100 stars
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app ki mice  (BioResource International Inc)
90
BioResource International Inc app ki mice
Selective attenuation of proinflammatory cytokines by MW150 administration in <t>APP/PS1</t> KI mice cortex. a 11–12-month-old wild type ( WT ) or APP/PS1 knock-in ( KI ) mice were treated with saline vehicle ( veh ) or 2.5 mg/kg MW150 by intraperitoneal injection (i.p.) once daily for 14 days. b IL-1β was increased in KI + veh mice compared to WT + veh mice ( p = 0.0012), and MW150 treatment of KI mice (KI + MW150) significantly attenuated IL-1β levels compared to KI + veh ( p = 0.0243) ( F (2,38) = 6.46; p = 0.004). c TNFα was elevated in KI + veh mice compared to WT + veh and attenuated in KI + MW150 mice compared to KI + veh; however, these changes were not significant ( F (2,38) = 1.11; p = 0.34). d IL-6 was slightly elevated in KI + veh compared to WT + veh mice, and there was no effect of MW150 treatment ( n = 11 WT + veh; n = 14 KI + veh; n = 14 KI + MW150). Data are mean ± SEM. Source data is available in Additional file : Table S1
App Ki Mice, supplied by BioResource International Inc, used in various techniques. Bioz Stars score: 90/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
https://www.bioz.com/result/app ki mice/product/BioResource International Inc
Average 90 stars, based on 1 article reviews
app ki mice - by Bioz Stars, 2026-06
90/100 stars
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cabp4 mouse gene knockout kit  (OriGene)
N/A
Cabp4 KN2 0 Mouse gene knockout kit via CRISPR non homology mediated
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pappa2 mouse gene knockout kit  (OriGene)
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Pappa2 KN2 0 Mouse gene knockout kit via CRISPR non homology mediated
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mouse nuclear factor kappa b2 elisa kit  (Innovative Research Inc)
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Mouse Nuclear Factor Kappa B2 ELISA Kit from Innovative Research is intended for the quantitative determination of Mouse Nuclear Factor Kappa B2 in biofluid samples, such as tissue homogenates, cell lysates and other biological fluids.
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mouse cabp4 activation kit by crispra  (OriGene)
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Cabp4 CRISPRa kit CRISPR gene activation of mouse calcium binding protein 4
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mouse pappa pappalysin 1 clia kit  (Elabscience)
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Image Search Results


Selective attenuation of proinflammatory cytokines by MW150 administration in APP/PS1 KI mice cortex. a 11–12-month-old wild type ( WT ) or APP/PS1 knock-in ( KI ) mice were treated with saline vehicle ( veh ) or 2.5 mg/kg MW150 by intraperitoneal injection (i.p.) once daily for 14 days. b IL-1β was increased in KI + veh mice compared to WT + veh mice ( p = 0.0012), and MW150 treatment of KI mice (KI + MW150) significantly attenuated IL-1β levels compared to KI + veh ( p = 0.0243) ( F (2,38) = 6.46; p = 0.004). c TNFα was elevated in KI + veh mice compared to WT + veh and attenuated in KI + MW150 mice compared to KI + veh; however, these changes were not significant ( F (2,38) = 1.11; p = 0.34). d IL-6 was slightly elevated in KI + veh compared to WT + veh mice, and there was no effect of MW150 treatment ( n = 11 WT + veh; n = 14 KI + veh; n = 14 KI + MW150). Data are mean ± SEM. Source data is available in Additional file : Table S1

Journal: Journal of Neuroinflammation

Article Title: Retention of normal glia function by an isoform-selective protein kinase inhibitor drug candidate that modulates cytokine production and cognitive outcomes

doi: 10.1186/s12974-017-0845-2

Figure Lengend Snippet: Selective attenuation of proinflammatory cytokines by MW150 administration in APP/PS1 KI mice cortex. a 11–12-month-old wild type ( WT ) or APP/PS1 knock-in ( KI ) mice were treated with saline vehicle ( veh ) or 2.5 mg/kg MW150 by intraperitoneal injection (i.p.) once daily for 14 days. b IL-1β was increased in KI + veh mice compared to WT + veh mice ( p = 0.0012), and MW150 treatment of KI mice (KI + MW150) significantly attenuated IL-1β levels compared to KI + veh ( p = 0.0243) ( F (2,38) = 6.46; p = 0.004). c TNFα was elevated in KI + veh mice compared to WT + veh and attenuated in KI + MW150 mice compared to KI + veh; however, these changes were not significant ( F (2,38) = 1.11; p = 0.34). d IL-6 was slightly elevated in KI + veh compared to WT + veh mice, and there was no effect of MW150 treatment ( n = 11 WT + veh; n = 14 KI + veh; n = 14 KI + MW150). Data are mean ± SEM. Source data is available in Additional file : Table S1

Article Snippet: Fig. 6 Effect of MW150 treatment on microglia closely associated with Aβ plaques and microglia-internalized Aβ in the cortex of APP/PS1 KI mice. a Representative images of Imaris 3D reconstruction of plaques.

Techniques: Knock-In, Saline, Injection

No effect of MW150 on GFAP immunostaining. a Representative images of GFAP immunohistochemical (IHC) staining in cortex of WT or APP/PS1 KI mice treated with vehicle ( veh ) or MW150. b Digital quantification of GFAP in the cortex was done using the Aperio ScanScope with the entire cortex used as the region of interest. Quantification using the positive pixel algorithm showed a significant increase in GFAP staining in the KI + veh compared to WT + veh ( p < 0.0001). No significant difference was found between the KI + veh compared to the KI + MW150. (F2,41) = 34.66; p < 0.0001). ( n = 14 WT + veh; n = 14 KI + veh; n = 14 KI + MW150). Data are mean ± SEM. Source data is available in Additional file : Table S2

Journal: Journal of Neuroinflammation

Article Title: Retention of normal glia function by an isoform-selective protein kinase inhibitor drug candidate that modulates cytokine production and cognitive outcomes

doi: 10.1186/s12974-017-0845-2

Figure Lengend Snippet: No effect of MW150 on GFAP immunostaining. a Representative images of GFAP immunohistochemical (IHC) staining in cortex of WT or APP/PS1 KI mice treated with vehicle ( veh ) or MW150. b Digital quantification of GFAP in the cortex was done using the Aperio ScanScope with the entire cortex used as the region of interest. Quantification using the positive pixel algorithm showed a significant increase in GFAP staining in the KI + veh compared to WT + veh ( p < 0.0001). No significant difference was found between the KI + veh compared to the KI + MW150. (F2,41) = 34.66; p < 0.0001). ( n = 14 WT + veh; n = 14 KI + veh; n = 14 KI + MW150). Data are mean ± SEM. Source data is available in Additional file : Table S2

Article Snippet: Fig. 6 Effect of MW150 treatment on microglia closely associated with Aβ plaques and microglia-internalized Aβ in the cortex of APP/PS1 KI mice. a Representative images of Imaris 3D reconstruction of plaques.

Techniques: Immunostaining, Immunohistochemical staining, Immunohistochemistry, Staining

No effect of MW150 on IBA1 + microglia volume. a Representative 3D surface reconstructions of IBA1 + cells generated from confocal microscopic imaging using Imaris software. b Mean volume ± standard deviation (SD) of rendered IBA1 cells is shown for the APP/PS1 KI + veh and APP/PS1 KI + MW150 groups. Data represent mean of 3–4 independent z-stacks from each mouse. ( n = 11 KI + veh; n = 14 KI + MW150)

Journal: Journal of Neuroinflammation

Article Title: Retention of normal glia function by an isoform-selective protein kinase inhibitor drug candidate that modulates cytokine production and cognitive outcomes

doi: 10.1186/s12974-017-0845-2

Figure Lengend Snippet: No effect of MW150 on IBA1 + microglia volume. a Representative 3D surface reconstructions of IBA1 + cells generated from confocal microscopic imaging using Imaris software. b Mean volume ± standard deviation (SD) of rendered IBA1 cells is shown for the APP/PS1 KI + veh and APP/PS1 KI + MW150 groups. Data represent mean of 3–4 independent z-stacks from each mouse. ( n = 11 KI + veh; n = 14 KI + MW150)

Article Snippet: Fig. 6 Effect of MW150 treatment on microglia closely associated with Aβ plaques and microglia-internalized Aβ in the cortex of APP/PS1 KI mice. a Representative images of Imaris 3D reconstruction of plaques.

Techniques: Generated, Imaging, Software, Standard Deviation

No effect of MW150 on CD45 and CD68 immunostaining in the cortex. a Representative images of CD45 IHC in cortex of wild type ( WT ) or APP/PS1 KI mice treated with saline vehicle ( veh ) or MW150. Digital quantification of CD45 in the cortex was done using the Aperio ScanScope, and the positive pixel algorithm. b CD45 was significantly increased in the KI + veh compared to the WT + veh treated mice ( p < 0.0001), with no effect of MW150 treatment. ( F (2,42) = 211.08; p < 0.0001). c Representative images of CD68 IHC. d CD68 was significantly increased in the KI + veh compared to the WT + veh-treated mice ( p < 0.0001), with no effect of MW150 treatment. ( F (2,42) = 28.81; p < 0.0001). ( n = 14 WT + veh; n = 14 KI + veh; n = 14 KI + MW150). Data are mean ± SEM. Source data is available in Additional file : Table S2

Journal: Journal of Neuroinflammation

Article Title: Retention of normal glia function by an isoform-selective protein kinase inhibitor drug candidate that modulates cytokine production and cognitive outcomes

doi: 10.1186/s12974-017-0845-2

Figure Lengend Snippet: No effect of MW150 on CD45 and CD68 immunostaining in the cortex. a Representative images of CD45 IHC in cortex of wild type ( WT ) or APP/PS1 KI mice treated with saline vehicle ( veh ) or MW150. Digital quantification of CD45 in the cortex was done using the Aperio ScanScope, and the positive pixel algorithm. b CD45 was significantly increased in the KI + veh compared to the WT + veh treated mice ( p < 0.0001), with no effect of MW150 treatment. ( F (2,42) = 211.08; p < 0.0001). c Representative images of CD68 IHC. d CD68 was significantly increased in the KI + veh compared to the WT + veh-treated mice ( p < 0.0001), with no effect of MW150 treatment. ( F (2,42) = 28.81; p < 0.0001). ( n = 14 WT + veh; n = 14 KI + veh; n = 14 KI + MW150). Data are mean ± SEM. Source data is available in Additional file : Table S2

Article Snippet: Fig. 6 Effect of MW150 treatment on microglia closely associated with Aβ plaques and microglia-internalized Aβ in the cortex of APP/PS1 KI mice. a Representative images of Imaris 3D reconstruction of plaques.

Techniques: Immunostaining, Saline

Effect of MW150 treatment on microglia closely associated with Aβ plaques and microglia-internalized Aβ in the cortex of APP/PS1 KI mice. a Representative images of Imaris 3D reconstruction of plaques. A region of interest ( ROI ) was generated by expanding the plaque volume by a 15 μm radius from the edge of the large plaques (larger than 10,000 voxels). This 3D ROI (shown in gray ) included the Aβ plaque, and a region near the plaque. IBA1 + cells in this ROI (shown in cyan ) were surface rendered to create a 3D volume of all IBA1 positive staining in the ROI. The IBA1 positive staining in the 3D ROI distinguishes plaque-associated microglia (shown in cyan ) compared to microglia away from plaques (shown in green ). b Volume of surface rendered IBA1 + cells within 15 μm radius around large plaques was significantly increased in KI + MW150 mice compared to KI + veh treatment ( p = 0.0397). c Representative image of microglia reconstruction with DAPI stained nuclei showing 6E10 staining within IBA1 + cell cytoplasm. d Microglia-internalized Aβ, as measured by 6E10 staining within surface rendered IBA1 + cells, was not significantly different between the KI + MW150 compared to KI + veh. ( n = 11 KI + veh; n = 14 KI + MW150). Data are mean ± SEM. Source data is available in Additional file : Table S3

Journal: Journal of Neuroinflammation

Article Title: Retention of normal glia function by an isoform-selective protein kinase inhibitor drug candidate that modulates cytokine production and cognitive outcomes

doi: 10.1186/s12974-017-0845-2

Figure Lengend Snippet: Effect of MW150 treatment on microglia closely associated with Aβ plaques and microglia-internalized Aβ in the cortex of APP/PS1 KI mice. a Representative images of Imaris 3D reconstruction of plaques. A region of interest ( ROI ) was generated by expanding the plaque volume by a 15 μm radius from the edge of the large plaques (larger than 10,000 voxels). This 3D ROI (shown in gray ) included the Aβ plaque, and a region near the plaque. IBA1 + cells in this ROI (shown in cyan ) were surface rendered to create a 3D volume of all IBA1 positive staining in the ROI. The IBA1 positive staining in the 3D ROI distinguishes plaque-associated microglia (shown in cyan ) compared to microglia away from plaques (shown in green ). b Volume of surface rendered IBA1 + cells within 15 μm radius around large plaques was significantly increased in KI + MW150 mice compared to KI + veh treatment ( p = 0.0397). c Representative image of microglia reconstruction with DAPI stained nuclei showing 6E10 staining within IBA1 + cell cytoplasm. d Microglia-internalized Aβ, as measured by 6E10 staining within surface rendered IBA1 + cells, was not significantly different between the KI + MW150 compared to KI + veh. ( n = 11 KI + veh; n = 14 KI + MW150). Data are mean ± SEM. Source data is available in Additional file : Table S3

Article Snippet: Fig. 6 Effect of MW150 treatment on microglia closely associated with Aβ plaques and microglia-internalized Aβ in the cortex of APP/PS1 KI mice. a Representative images of Imaris 3D reconstruction of plaques.

Techniques: Generated, Staining