control vector aav8 hsyn mcherry Search Results


aav8 camkiiamcherry  (Vector Biolabs)
95
Vector Biolabs aav8 camkiiamcherry
Aav8 Camkiiamcherry, supplied by Vector Biolabs, used in various techniques. Bioz Stars score: 95/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
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aav8-slu7  (PlasmidFactory gmbh)
90
PlasmidFactory gmbh aav8-slu7
Aav8 Slu7, supplied by PlasmidFactory gmbh, used in various techniques. Bioz Stars score: 90/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
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aav hsyn dio hm4d gi mcherry  (Addgene inc)
94
Addgene inc aav hsyn dio hm4d gi mcherry
Each coronal section represents a range of three sections relative to Bregma (B, in mm). Expression for each animal is plotted at 90% transparency and then per-animal expression is overlaid. Sections run anterior (top) to posterior (bottom). A) Expression map of <t>AAV-hSyn-DIO-hM4D(Gi)-mCherry</t> in VP following CAV2-Cre injections in NAcLSh (i.e., VP → NAcLSh inhibition animals; red). B) Expression map of AAV-hSyn-DIO-mCherry in VP (i.e., controls; black).
Aav Hsyn Dio Hm4d Gi Mcherry, 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
https://www.bioz.com/result/aav hsyn dio hm4d gi mcherry/product/Addgene inc
Average 94 stars, based on 1 article reviews
aav hsyn dio hm4d gi mcherry - by Bioz Stars, 2026-05
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virus strains aav8 camkiia hm4d gi mcherry addgene rrid addgene 50477 aav5 camkiia mcherry unc vector core  (Addgene inc)
96
Addgene inc virus strains aav8 camkiia hm4d gi mcherry addgene rrid addgene 50477 aav5 camkiia mcherry unc vector core
Each coronal section represents a range of three sections relative to Bregma (B, in mm). Expression for each animal is plotted at 90% transparency and then per-animal expression is overlaid. Sections run anterior (top) to posterior (bottom). A) Expression map of <t>AAV-hSyn-DIO-hM4D(Gi)-mCherry</t> in VP following CAV2-Cre injections in NAcLSh (i.e., VP → NAcLSh inhibition animals; red). B) Expression map of AAV-hSyn-DIO-mCherry in VP (i.e., controls; black).
Virus Strains Aav8 Camkiia Hm4d Gi Mcherry Addgene Rrid Addgene 50477 Aav5 Camkiia Mcherry Unc Vector Core, supplied by Addgene inc, used in various techniques. Bioz Stars score: 96/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
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Average 96 stars, based on 1 article reviews
virus strains aav8 camkiia hm4d gi mcherry addgene rrid addgene 50477 aav5 camkiia mcherry unc vector core - by Bioz Stars, 2026-05
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aav virus aav8 d377y mpsck9 vector biolabs aav 268246 chemicals  (Vector Biolabs)
94
Vector Biolabs aav virus aav8 d377y mpsck9 vector biolabs aav 268246 chemicals
Each coronal section represents a range of three sections relative to Bregma (B, in mm). Expression for each animal is plotted at 90% transparency and then per-animal expression is overlaid. Sections run anterior (top) to posterior (bottom). A) Expression map of <t>AAV-hSyn-DIO-hM4D(Gi)-mCherry</t> in VP following CAV2-Cre injections in NAcLSh (i.e., VP → NAcLSh inhibition animals; red). B) Expression map of AAV-hSyn-DIO-mCherry in VP (i.e., controls; black).
Aav Virus Aav8 D377y Mpsck9 Vector Biolabs Aav 268246 Chemicals, supplied by Vector Biolabs, 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
aav virus aav8 d377y mpsck9 vector biolabs aav 268246 chemicals - by Bioz Stars, 2026-05
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vectors aav8 tbg pi cre rbg  (Addgene inc)
96
Addgene inc vectors aav8 tbg pi cre rbg
Each coronal section represents a range of three sections relative to Bregma (B, in mm). Expression for each animal is plotted at 90% transparency and then per-animal expression is overlaid. Sections run anterior (top) to posterior (bottom). A) Expression map of <t>AAV-hSyn-DIO-hM4D(Gi)-mCherry</t> in VP following CAV2-Cre injections in NAcLSh (i.e., VP → NAcLSh inhibition animals; red). B) Expression map of AAV-hSyn-DIO-mCherry in VP (i.e., controls; black).
Vectors Aav8 Tbg Pi Cre Rbg, supplied by Addgene inc, used in various techniques. Bioz Stars score: 96/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
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vectors aav8 tbg pi cre rbg - by Bioz Stars, 2026-05
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gi o coupled dreadd vector aav8 hsyn dio hm4d gi mcherry plasmid 44362  (Addgene inc)
96
Addgene inc gi o coupled dreadd vector aav8 hsyn dio hm4d gi mcherry plasmid 44362
(a) Experimental diagram. Npas1-Cre-TdTomato mice received bilateral GPe injections <t>of</t> <t>Cre-dependent</t> <t>AAV8-hSyn-DIO-hM4D(Gi)-mCherry</t> or AAV8-hSyn-DIO-hM3D(Gq)-mCherry, with Cre-negative littermates serving as controls. All animals received C21 prior to testing, ensuring equivalent drug exposure across groups. Mice were tested on the elevated plus maze (EPM) 5 weeks post-surgery. Behavioral sessions were video-recorded for subsequent analysis. (b) Time spent in closed arms, center, and open arms during the EPM shows the expected preference for closed arms across all groups, with no effect of GPe NPAS1 manipulation on arm occupancy (two-way mixed ANOVA, maze compartment F (2,52) = 122.8, p = 2.003e-20; group F (2,26) = 1.546, p = 0.2319). (c) Number of open-arm entries does not differ across groups, indicating no effect of GPe NPAS1 manipulation on exploration of these areas (ANOVA, group F (2,26) = 1.048, p = 0.365). (d) Percent time spent in the open arms in the EPM is comparable across control, hM4D(Gi), and hM3D(Gq) mice, consistent with preserved global EPM performance (ANOVA, group F (2,55) = 0.4928, p = 0.6136). (e) Empirical cumulative distribution functions (ECDFs) of frame-wise horizontal movement in the open arms during the EPM show highly overlapping movement distributions across groups, illustrating the absence of gross shifts in locomotor behavior within high-risk regions of the maze. Pairwise Kolmogorov–Smirnov tests detected statistically significant but very small distributional differences (KS D = 0.02–0.05; FDR-corrected p < 0.001), consistent with negligible effect sizes that do not reflect meaningful differences in open-arm movement dynamics. (f) Distance traveled (two-way mixed ANOVA, group x time F (238,3094) = 0.8741, p = 0.9131), (g) speed (two-way mixed ANOVA, group x time F (238,3094) = 0.8742, p = 0.9129), and (h) acceleration (two-way mixed ANOVA, group x time F (238,3094) = 1.037, p = 0.3419) over time are comparable across control, hM4D(Gi), and hM3D(Gq) mice, indicating preserved global locomotor output across the session. Frame-wise polar histograms of heading direction during EPM show (i) control mice exhibit a modest but significant preference for a closed-arm-oriented heading (Rayleigh test, r = 0.005399, p = 0.001871). (j) hM4D(Gi) mice show a statistically significant, strong preferred closed arm heading (Rayleigh test, r = 0.01707, p = 1.225e-16). (k) In contrast, GPe NPAS1 hM4D(Gq) mice do not exhibit a statistically significant preferred heading orientation (Rayleigh test, r = 0.001264, p = 0.7505). (l) Pose features extracted from video tracking show bound box area across time was decreased for hM3D(Gq) mice compared to control mice across all EPM areas (two-way mixed ANOVA, group x time F (238,3094) = 1.180, p = 0.03497; post hoc control v hM3D(Gq) p = 0.03348). (m) Similarly, box aspect ratio over time was decreased for hM3D(Gq) mice compared to control mice (two-way mixed ANOVA, group x time F (238,3094) = 1.181, p = 0.03486; post hoc control v hM3D(Gq) p = 0.04464). (n) There were no group differences in the change in aspect ratio across time (two-way mixed ANOVA, group x time F (238,3094) = 0.08639, p = 0.06231). Dots represent individual data points, error bars or shaded bands represent standard error of the mean (SEM). For polar plots, 32 bins were computed to generate 11.25 degree bars for histogram densities.
Gi O Coupled Dreadd Vector Aav8 Hsyn Dio Hm4d Gi Mcherry Plasmid 44362, supplied by Addgene inc, used in various techniques. Bioz Stars score: 96/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
https://www.bioz.com/result/gi o coupled dreadd vector aav8 hsyn dio hm4d gi mcherry plasmid 44362/product/Addgene inc
Average 96 stars, based on 1 article reviews
gi o coupled dreadd vector aav8 hsyn dio hm4d gi mcherry plasmid 44362 - by Bioz Stars, 2026-05
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aav8 packaging vector paav2 8  (Addgene inc)
96
Addgene inc aav8 packaging vector paav2 8
(a) Experimental diagram. Npas1-Cre-TdTomato mice received bilateral GPe injections <t>of</t> <t>Cre-dependent</t> <t>AAV8-hSyn-DIO-hM4D(Gi)-mCherry</t> or AAV8-hSyn-DIO-hM3D(Gq)-mCherry, with Cre-negative littermates serving as controls. All animals received C21 prior to testing, ensuring equivalent drug exposure across groups. Mice were tested on the elevated plus maze (EPM) 5 weeks post-surgery. Behavioral sessions were video-recorded for subsequent analysis. (b) Time spent in closed arms, center, and open arms during the EPM shows the expected preference for closed arms across all groups, with no effect of GPe NPAS1 manipulation on arm occupancy (two-way mixed ANOVA, maze compartment F (2,52) = 122.8, p = 2.003e-20; group F (2,26) = 1.546, p = 0.2319). (c) Number of open-arm entries does not differ across groups, indicating no effect of GPe NPAS1 manipulation on exploration of these areas (ANOVA, group F (2,26) = 1.048, p = 0.365). (d) Percent time spent in the open arms in the EPM is comparable across control, hM4D(Gi), and hM3D(Gq) mice, consistent with preserved global EPM performance (ANOVA, group F (2,55) = 0.4928, p = 0.6136). (e) Empirical cumulative distribution functions (ECDFs) of frame-wise horizontal movement in the open arms during the EPM show highly overlapping movement distributions across groups, illustrating the absence of gross shifts in locomotor behavior within high-risk regions of the maze. Pairwise Kolmogorov–Smirnov tests detected statistically significant but very small distributional differences (KS D = 0.02–0.05; FDR-corrected p < 0.001), consistent with negligible effect sizes that do not reflect meaningful differences in open-arm movement dynamics. (f) Distance traveled (two-way mixed ANOVA, group x time F (238,3094) = 0.8741, p = 0.9131), (g) speed (two-way mixed ANOVA, group x time F (238,3094) = 0.8742, p = 0.9129), and (h) acceleration (two-way mixed ANOVA, group x time F (238,3094) = 1.037, p = 0.3419) over time are comparable across control, hM4D(Gi), and hM3D(Gq) mice, indicating preserved global locomotor output across the session. Frame-wise polar histograms of heading direction during EPM show (i) control mice exhibit a modest but significant preference for a closed-arm-oriented heading (Rayleigh test, r = 0.005399, p = 0.001871). (j) hM4D(Gi) mice show a statistically significant, strong preferred closed arm heading (Rayleigh test, r = 0.01707, p = 1.225e-16). (k) In contrast, GPe NPAS1 hM4D(Gq) mice do not exhibit a statistically significant preferred heading orientation (Rayleigh test, r = 0.001264, p = 0.7505). (l) Pose features extracted from video tracking show bound box area across time was decreased for hM3D(Gq) mice compared to control mice across all EPM areas (two-way mixed ANOVA, group x time F (238,3094) = 1.180, p = 0.03497; post hoc control v hM3D(Gq) p = 0.03348). (m) Similarly, box aspect ratio over time was decreased for hM3D(Gq) mice compared to control mice (two-way mixed ANOVA, group x time F (238,3094) = 1.181, p = 0.03486; post hoc control v hM3D(Gq) p = 0.04464). (n) There were no group differences in the change in aspect ratio across time (two-way mixed ANOVA, group x time F (238,3094) = 0.08639, p = 0.06231). Dots represent individual data points, error bars or shaded bands represent standard error of the mean (SEM). For polar plots, 32 bins were computed to generate 11.25 degree bars for histogram densities.
Aav8 Packaging Vector Paav2 8, supplied by Addgene inc, used in various techniques. Bioz Stars score: 96/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
https://www.bioz.com/result/aav8 packaging vector paav2 8/product/Addgene inc
Average 96 stars, based on 1 article reviews
aav8 packaging vector paav2 8 - by Bioz Stars, 2026-05
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aav8 mpcsk9 d377y  (Addgene inc)
93
Addgene inc aav8 mpcsk9 d377y
(a) Experimental diagram. Npas1-Cre-TdTomato mice received bilateral GPe injections <t>of</t> <t>Cre-dependent</t> <t>AAV8-hSyn-DIO-hM4D(Gi)-mCherry</t> or AAV8-hSyn-DIO-hM3D(Gq)-mCherry, with Cre-negative littermates serving as controls. All animals received C21 prior to testing, ensuring equivalent drug exposure across groups. Mice were tested on the elevated plus maze (EPM) 5 weeks post-surgery. Behavioral sessions were video-recorded for subsequent analysis. (b) Time spent in closed arms, center, and open arms during the EPM shows the expected preference for closed arms across all groups, with no effect of GPe NPAS1 manipulation on arm occupancy (two-way mixed ANOVA, maze compartment F (2,52) = 122.8, p = 2.003e-20; group F (2,26) = 1.546, p = 0.2319). (c) Number of open-arm entries does not differ across groups, indicating no effect of GPe NPAS1 manipulation on exploration of these areas (ANOVA, group F (2,26) = 1.048, p = 0.365). (d) Percent time spent in the open arms in the EPM is comparable across control, hM4D(Gi), and hM3D(Gq) mice, consistent with preserved global EPM performance (ANOVA, group F (2,55) = 0.4928, p = 0.6136). (e) Empirical cumulative distribution functions (ECDFs) of frame-wise horizontal movement in the open arms during the EPM show highly overlapping movement distributions across groups, illustrating the absence of gross shifts in locomotor behavior within high-risk regions of the maze. Pairwise Kolmogorov–Smirnov tests detected statistically significant but very small distributional differences (KS D = 0.02–0.05; FDR-corrected p < 0.001), consistent with negligible effect sizes that do not reflect meaningful differences in open-arm movement dynamics. (f) Distance traveled (two-way mixed ANOVA, group x time F (238,3094) = 0.8741, p = 0.9131), (g) speed (two-way mixed ANOVA, group x time F (238,3094) = 0.8742, p = 0.9129), and (h) acceleration (two-way mixed ANOVA, group x time F (238,3094) = 1.037, p = 0.3419) over time are comparable across control, hM4D(Gi), and hM3D(Gq) mice, indicating preserved global locomotor output across the session. Frame-wise polar histograms of heading direction during EPM show (i) control mice exhibit a modest but significant preference for a closed-arm-oriented heading (Rayleigh test, r = 0.005399, p = 0.001871). (j) hM4D(Gi) mice show a statistically significant, strong preferred closed arm heading (Rayleigh test, r = 0.01707, p = 1.225e-16). (k) In contrast, GPe NPAS1 hM4D(Gq) mice do not exhibit a statistically significant preferred heading orientation (Rayleigh test, r = 0.001264, p = 0.7505). (l) Pose features extracted from video tracking show bound box area across time was decreased for hM3D(Gq) mice compared to control mice across all EPM areas (two-way mixed ANOVA, group x time F (238,3094) = 1.180, p = 0.03497; post hoc control v hM3D(Gq) p = 0.03348). (m) Similarly, box aspect ratio over time was decreased for hM3D(Gq) mice compared to control mice (two-way mixed ANOVA, group x time F (238,3094) = 1.181, p = 0.03486; post hoc control v hM3D(Gq) p = 0.04464). (n) There were no group differences in the change in aspect ratio across time (two-way mixed ANOVA, group x time F (238,3094) = 0.08639, p = 0.06231). Dots represent individual data points, error bars or shaded bands represent standard error of the mean (SEM). For polar plots, 32 bins were computed to generate 11.25 degree bars for histogram densities.
Aav8 Mpcsk9 D377y, supplied by Addgene inc, used in various techniques. Bioz Stars score: 93/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
https://www.bioz.com/result/aav8 mpcsk9 d377y/product/Addgene inc
Average 93 stars, based on 1 article reviews
aav8 mpcsk9 d377y - by Bioz Stars, 2026-05
93/100 stars
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aav8 hsyn dio hm4d gi mcherry titer 4 × 1012 vg ml  (Addgene inc)
93
Addgene inc aav8 hsyn dio hm4d gi mcherry titer 4 × 1012 vg ml
(a) Experimental diagram. Npas1-Cre-TdTomato mice received bilateral GPe injections <t>of</t> <t>Cre-dependent</t> <t>AAV8-hSyn-DIO-hM4D(Gi)-mCherry</t> or AAV8-hSyn-DIO-hM3D(Gq)-mCherry, with Cre-negative littermates serving as controls. All animals received C21 prior to testing, ensuring equivalent drug exposure across groups. Mice were tested on the elevated plus maze (EPM) 5 weeks post-surgery. Behavioral sessions were video-recorded for subsequent analysis. (b) Time spent in closed arms, center, and open arms during the EPM shows the expected preference for closed arms across all groups, with no effect of GPe NPAS1 manipulation on arm occupancy (two-way mixed ANOVA, maze compartment F (2,52) = 122.8, p = 2.003e-20; group F (2,26) = 1.546, p = 0.2319). (c) Number of open-arm entries does not differ across groups, indicating no effect of GPe NPAS1 manipulation on exploration of these areas (ANOVA, group F (2,26) = 1.048, p = 0.365). (d) Percent time spent in the open arms in the EPM is comparable across control, hM4D(Gi), and hM3D(Gq) mice, consistent with preserved global EPM performance (ANOVA, group F (2,55) = 0.4928, p = 0.6136). (e) Empirical cumulative distribution functions (ECDFs) of frame-wise horizontal movement in the open arms during the EPM show highly overlapping movement distributions across groups, illustrating the absence of gross shifts in locomotor behavior within high-risk regions of the maze. Pairwise Kolmogorov–Smirnov tests detected statistically significant but very small distributional differences (KS D = 0.02–0.05; FDR-corrected p < 0.001), consistent with negligible effect sizes that do not reflect meaningful differences in open-arm movement dynamics. (f) Distance traveled (two-way mixed ANOVA, group x time F (238,3094) = 0.8741, p = 0.9131), (g) speed (two-way mixed ANOVA, group x time F (238,3094) = 0.8742, p = 0.9129), and (h) acceleration (two-way mixed ANOVA, group x time F (238,3094) = 1.037, p = 0.3419) over time are comparable across control, hM4D(Gi), and hM3D(Gq) mice, indicating preserved global locomotor output across the session. Frame-wise polar histograms of heading direction during EPM show (i) control mice exhibit a modest but significant preference for a closed-arm-oriented heading (Rayleigh test, r = 0.005399, p = 0.001871). (j) hM4D(Gi) mice show a statistically significant, strong preferred closed arm heading (Rayleigh test, r = 0.01707, p = 1.225e-16). (k) In contrast, GPe NPAS1 hM4D(Gq) mice do not exhibit a statistically significant preferred heading orientation (Rayleigh test, r = 0.001264, p = 0.7505). (l) Pose features extracted from video tracking show bound box area across time was decreased for hM3D(Gq) mice compared to control mice across all EPM areas (two-way mixed ANOVA, group x time F (238,3094) = 1.180, p = 0.03497; post hoc control v hM3D(Gq) p = 0.03348). (m) Similarly, box aspect ratio over time was decreased for hM3D(Gq) mice compared to control mice (two-way mixed ANOVA, group x time F (238,3094) = 1.181, p = 0.03486; post hoc control v hM3D(Gq) p = 0.04464). (n) There were no group differences in the change in aspect ratio across time (two-way mixed ANOVA, group x time F (238,3094) = 0.08639, p = 0.06231). Dots represent individual data points, error bars or shaded bands represent standard error of the mean (SEM). For polar plots, 32 bins were computed to generate 11.25 degree bars for histogram densities.
Aav8 Hsyn Dio Hm4d Gi Mcherry Titer 4 × 1012 Vg Ml, supplied by Addgene inc, used in various techniques. Bioz Stars score: 93/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
https://www.bioz.com/result/aav8 hsyn dio hm4d gi mcherry titer 4 × 1012 vg ml/product/Addgene inc
Average 93 stars, based on 1 article reviews
aav8 hsyn dio hm4d gi mcherry titer 4 × 1012 vg ml - by Bioz Stars, 2026-05
93/100 stars
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aav8  (Vector Biolabs)
95
Vector Biolabs aav8
(a) Experimental diagram. Npas1-Cre-TdTomato mice received bilateral GPe injections <t>of</t> <t>Cre-dependent</t> <t>AAV8-hSyn-DIO-hM4D(Gi)-mCherry</t> or AAV8-hSyn-DIO-hM3D(Gq)-mCherry, with Cre-negative littermates serving as controls. All animals received C21 prior to testing, ensuring equivalent drug exposure across groups. Mice were tested on the elevated plus maze (EPM) 5 weeks post-surgery. Behavioral sessions were video-recorded for subsequent analysis. (b) Time spent in closed arms, center, and open arms during the EPM shows the expected preference for closed arms across all groups, with no effect of GPe NPAS1 manipulation on arm occupancy (two-way mixed ANOVA, maze compartment F (2,52) = 122.8, p = 2.003e-20; group F (2,26) = 1.546, p = 0.2319). (c) Number of open-arm entries does not differ across groups, indicating no effect of GPe NPAS1 manipulation on exploration of these areas (ANOVA, group F (2,26) = 1.048, p = 0.365). (d) Percent time spent in the open arms in the EPM is comparable across control, hM4D(Gi), and hM3D(Gq) mice, consistent with preserved global EPM performance (ANOVA, group F (2,55) = 0.4928, p = 0.6136). (e) Empirical cumulative distribution functions (ECDFs) of frame-wise horizontal movement in the open arms during the EPM show highly overlapping movement distributions across groups, illustrating the absence of gross shifts in locomotor behavior within high-risk regions of the maze. Pairwise Kolmogorov–Smirnov tests detected statistically significant but very small distributional differences (KS D = 0.02–0.05; FDR-corrected p < 0.001), consistent with negligible effect sizes that do not reflect meaningful differences in open-arm movement dynamics. (f) Distance traveled (two-way mixed ANOVA, group x time F (238,3094) = 0.8741, p = 0.9131), (g) speed (two-way mixed ANOVA, group x time F (238,3094) = 0.8742, p = 0.9129), and (h) acceleration (two-way mixed ANOVA, group x time F (238,3094) = 1.037, p = 0.3419) over time are comparable across control, hM4D(Gi), and hM3D(Gq) mice, indicating preserved global locomotor output across the session. Frame-wise polar histograms of heading direction during EPM show (i) control mice exhibit a modest but significant preference for a closed-arm-oriented heading (Rayleigh test, r = 0.005399, p = 0.001871). (j) hM4D(Gi) mice show a statistically significant, strong preferred closed arm heading (Rayleigh test, r = 0.01707, p = 1.225e-16). (k) In contrast, GPe NPAS1 hM4D(Gq) mice do not exhibit a statistically significant preferred heading orientation (Rayleigh test, r = 0.001264, p = 0.7505). (l) Pose features extracted from video tracking show bound box area across time was decreased for hM3D(Gq) mice compared to control mice across all EPM areas (two-way mixed ANOVA, group x time F (238,3094) = 1.180, p = 0.03497; post hoc control v hM3D(Gq) p = 0.03348). (m) Similarly, box aspect ratio over time was decreased for hM3D(Gq) mice compared to control mice (two-way mixed ANOVA, group x time F (238,3094) = 1.181, p = 0.03486; post hoc control v hM3D(Gq) p = 0.04464). (n) There were no group differences in the change in aspect ratio across time (two-way mixed ANOVA, group x time F (238,3094) = 0.08639, p = 0.06231). Dots represent individual data points, error bars or shaded bands represent standard error of the mean (SEM). For polar plots, 32 bins were computed to generate 11.25 degree bars for histogram densities.
Aav8, supplied by Vector Biolabs, used in various techniques. Bioz Stars score: 95/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
https://www.bioz.com/result/aav8/product/Vector Biolabs
Average 95 stars, based on 1 article reviews
aav8 - by Bioz Stars, 2026-05
95/100 stars
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aav gqdreadd aav8 hsyn dio hm3d gq mcherry  (Addgene inc)
95
Addgene inc aav gqdreadd aav8 hsyn dio hm3d gq mcherry
(a) Experimental diagram. Npas1-Cre-TdTomato mice received bilateral GPe injections <t>of</t> <t>Cre-dependent</t> <t>AAV8-hSyn-DIO-hM4D(Gi)-mCherry</t> or AAV8-hSyn-DIO-hM3D(Gq)-mCherry, with Cre-negative littermates serving as controls. All animals received C21 prior to testing, ensuring equivalent drug exposure across groups. Mice were tested on the elevated plus maze (EPM) 5 weeks post-surgery. Behavioral sessions were video-recorded for subsequent analysis. (b) Time spent in closed arms, center, and open arms during the EPM shows the expected preference for closed arms across all groups, with no effect of GPe NPAS1 manipulation on arm occupancy (two-way mixed ANOVA, maze compartment F (2,52) = 122.8, p = 2.003e-20; group F (2,26) = 1.546, p = 0.2319). (c) Number of open-arm entries does not differ across groups, indicating no effect of GPe NPAS1 manipulation on exploration of these areas (ANOVA, group F (2,26) = 1.048, p = 0.365). (d) Percent time spent in the open arms in the EPM is comparable across control, hM4D(Gi), and hM3D(Gq) mice, consistent with preserved global EPM performance (ANOVA, group F (2,55) = 0.4928, p = 0.6136). (e) Empirical cumulative distribution functions (ECDFs) of frame-wise horizontal movement in the open arms during the EPM show highly overlapping movement distributions across groups, illustrating the absence of gross shifts in locomotor behavior within high-risk regions of the maze. Pairwise Kolmogorov–Smirnov tests detected statistically significant but very small distributional differences (KS D = 0.02–0.05; FDR-corrected p < 0.001), consistent with negligible effect sizes that do not reflect meaningful differences in open-arm movement dynamics. (f) Distance traveled (two-way mixed ANOVA, group x time F (238,3094) = 0.8741, p = 0.9131), (g) speed (two-way mixed ANOVA, group x time F (238,3094) = 0.8742, p = 0.9129), and (h) acceleration (two-way mixed ANOVA, group x time F (238,3094) = 1.037, p = 0.3419) over time are comparable across control, hM4D(Gi), and hM3D(Gq) mice, indicating preserved global locomotor output across the session. Frame-wise polar histograms of heading direction during EPM show (i) control mice exhibit a modest but significant preference for a closed-arm-oriented heading (Rayleigh test, r = 0.005399, p = 0.001871). (j) hM4D(Gi) mice show a statistically significant, strong preferred closed arm heading (Rayleigh test, r = 0.01707, p = 1.225e-16). (k) In contrast, GPe NPAS1 hM4D(Gq) mice do not exhibit a statistically significant preferred heading orientation (Rayleigh test, r = 0.001264, p = 0.7505). (l) Pose features extracted from video tracking show bound box area across time was decreased for hM3D(Gq) mice compared to control mice across all EPM areas (two-way mixed ANOVA, group x time F (238,3094) = 1.180, p = 0.03497; post hoc control v hM3D(Gq) p = 0.03348). (m) Similarly, box aspect ratio over time was decreased for hM3D(Gq) mice compared to control mice (two-way mixed ANOVA, group x time F (238,3094) = 1.181, p = 0.03486; post hoc control v hM3D(Gq) p = 0.04464). (n) There were no group differences in the change in aspect ratio across time (two-way mixed ANOVA, group x time F (238,3094) = 0.08639, p = 0.06231). Dots represent individual data points, error bars or shaded bands represent standard error of the mean (SEM). For polar plots, 32 bins were computed to generate 11.25 degree bars for histogram densities.
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Each coronal section represents a range of three sections relative to Bregma (B, in mm). Expression for each animal is plotted at 90% transparency and then per-animal expression is overlaid. Sections run anterior (top) to posterior (bottom). A) Expression map of AAV-hSyn-DIO-hM4D(Gi)-mCherry in VP following CAV2-Cre injections in NAcLSh (i.e., VP → NAcLSh inhibition animals; red). B) Expression map of AAV-hSyn-DIO-mCherry in VP (i.e., controls; black).

Journal: bioRxiv

Article Title: Circuit directionality for motivation: lateral accumbens-pallidum, but not pallidum-accumbens, connections regulate motivational attraction to reward cues

doi: 10.1101/474387

Figure Lengend Snippet: Each coronal section represents a range of three sections relative to Bregma (B, in mm). Expression for each animal is plotted at 90% transparency and then per-animal expression is overlaid. Sections run anterior (top) to posterior (bottom). A) Expression map of AAV-hSyn-DIO-hM4D(Gi)-mCherry in VP following CAV2-Cre injections in NAcLSh (i.e., VP → NAcLSh inhibition animals; red). B) Expression map of AAV-hSyn-DIO-mCherry in VP (i.e., controls; black).

Article Snippet: The inhibition group received 0.6 µl of AAV-hSyn-DIO-hM4D(Gi)-mCherry (n = 12, AAV5, UNC Vector Core; n = 4, AAV8, Addgene) in the VP and 1.0 µl CAV-Cre or CAV-Cre-GFP in the NAcLSh.

Techniques: Expressing, Inhibition

(a) Experimental diagram. Npas1-Cre-TdTomato mice received bilateral GPe injections of Cre-dependent AAV8-hSyn-DIO-hM4D(Gi)-mCherry or AAV8-hSyn-DIO-hM3D(Gq)-mCherry, with Cre-negative littermates serving as controls. All animals received C21 prior to testing, ensuring equivalent drug exposure across groups. Mice were tested on the elevated plus maze (EPM) 5 weeks post-surgery. Behavioral sessions were video-recorded for subsequent analysis. (b) Time spent in closed arms, center, and open arms during the EPM shows the expected preference for closed arms across all groups, with no effect of GPe NPAS1 manipulation on arm occupancy (two-way mixed ANOVA, maze compartment F (2,52) = 122.8, p = 2.003e-20; group F (2,26) = 1.546, p = 0.2319). (c) Number of open-arm entries does not differ across groups, indicating no effect of GPe NPAS1 manipulation on exploration of these areas (ANOVA, group F (2,26) = 1.048, p = 0.365). (d) Percent time spent in the open arms in the EPM is comparable across control, hM4D(Gi), and hM3D(Gq) mice, consistent with preserved global EPM performance (ANOVA, group F (2,55) = 0.4928, p = 0.6136). (e) Empirical cumulative distribution functions (ECDFs) of frame-wise horizontal movement in the open arms during the EPM show highly overlapping movement distributions across groups, illustrating the absence of gross shifts in locomotor behavior within high-risk regions of the maze. Pairwise Kolmogorov–Smirnov tests detected statistically significant but very small distributional differences (KS D = 0.02–0.05; FDR-corrected p < 0.001), consistent with negligible effect sizes that do not reflect meaningful differences in open-arm movement dynamics. (f) Distance traveled (two-way mixed ANOVA, group x time F (238,3094) = 0.8741, p = 0.9131), (g) speed (two-way mixed ANOVA, group x time F (238,3094) = 0.8742, p = 0.9129), and (h) acceleration (two-way mixed ANOVA, group x time F (238,3094) = 1.037, p = 0.3419) over time are comparable across control, hM4D(Gi), and hM3D(Gq) mice, indicating preserved global locomotor output across the session. Frame-wise polar histograms of heading direction during EPM show (i) control mice exhibit a modest but significant preference for a closed-arm-oriented heading (Rayleigh test, r = 0.005399, p = 0.001871). (j) hM4D(Gi) mice show a statistically significant, strong preferred closed arm heading (Rayleigh test, r = 0.01707, p = 1.225e-16). (k) In contrast, GPe NPAS1 hM4D(Gq) mice do not exhibit a statistically significant preferred heading orientation (Rayleigh test, r = 0.001264, p = 0.7505). (l) Pose features extracted from video tracking show bound box area across time was decreased for hM3D(Gq) mice compared to control mice across all EPM areas (two-way mixed ANOVA, group x time F (238,3094) = 1.180, p = 0.03497; post hoc control v hM3D(Gq) p = 0.03348). (m) Similarly, box aspect ratio over time was decreased for hM3D(Gq) mice compared to control mice (two-way mixed ANOVA, group x time F (238,3094) = 1.181, p = 0.03486; post hoc control v hM3D(Gq) p = 0.04464). (n) There were no group differences in the change in aspect ratio across time (two-way mixed ANOVA, group x time F (238,3094) = 0.08639, p = 0.06231). Dots represent individual data points, error bars or shaded bands represent standard error of the mean (SEM). For polar plots, 32 bins were computed to generate 11.25 degree bars for histogram densities.

Journal: bioRxiv

Article Title: External Globus Pallidus Arkypallidal Circuit Dynamics Gate Risk-Taking Behavior

doi: 10.64898/2026.03.20.713182

Figure Lengend Snippet: (a) Experimental diagram. Npas1-Cre-TdTomato mice received bilateral GPe injections of Cre-dependent AAV8-hSyn-DIO-hM4D(Gi)-mCherry or AAV8-hSyn-DIO-hM3D(Gq)-mCherry, with Cre-negative littermates serving as controls. All animals received C21 prior to testing, ensuring equivalent drug exposure across groups. Mice were tested on the elevated plus maze (EPM) 5 weeks post-surgery. Behavioral sessions were video-recorded for subsequent analysis. (b) Time spent in closed arms, center, and open arms during the EPM shows the expected preference for closed arms across all groups, with no effect of GPe NPAS1 manipulation on arm occupancy (two-way mixed ANOVA, maze compartment F (2,52) = 122.8, p = 2.003e-20; group F (2,26) = 1.546, p = 0.2319). (c) Number of open-arm entries does not differ across groups, indicating no effect of GPe NPAS1 manipulation on exploration of these areas (ANOVA, group F (2,26) = 1.048, p = 0.365). (d) Percent time spent in the open arms in the EPM is comparable across control, hM4D(Gi), and hM3D(Gq) mice, consistent with preserved global EPM performance (ANOVA, group F (2,55) = 0.4928, p = 0.6136). (e) Empirical cumulative distribution functions (ECDFs) of frame-wise horizontal movement in the open arms during the EPM show highly overlapping movement distributions across groups, illustrating the absence of gross shifts in locomotor behavior within high-risk regions of the maze. Pairwise Kolmogorov–Smirnov tests detected statistically significant but very small distributional differences (KS D = 0.02–0.05; FDR-corrected p < 0.001), consistent with negligible effect sizes that do not reflect meaningful differences in open-arm movement dynamics. (f) Distance traveled (two-way mixed ANOVA, group x time F (238,3094) = 0.8741, p = 0.9131), (g) speed (two-way mixed ANOVA, group x time F (238,3094) = 0.8742, p = 0.9129), and (h) acceleration (two-way mixed ANOVA, group x time F (238,3094) = 1.037, p = 0.3419) over time are comparable across control, hM4D(Gi), and hM3D(Gq) mice, indicating preserved global locomotor output across the session. Frame-wise polar histograms of heading direction during EPM show (i) control mice exhibit a modest but significant preference for a closed-arm-oriented heading (Rayleigh test, r = 0.005399, p = 0.001871). (j) hM4D(Gi) mice show a statistically significant, strong preferred closed arm heading (Rayleigh test, r = 0.01707, p = 1.225e-16). (k) In contrast, GPe NPAS1 hM4D(Gq) mice do not exhibit a statistically significant preferred heading orientation (Rayleigh test, r = 0.001264, p = 0.7505). (l) Pose features extracted from video tracking show bound box area across time was decreased for hM3D(Gq) mice compared to control mice across all EPM areas (two-way mixed ANOVA, group x time F (238,3094) = 1.180, p = 0.03497; post hoc control v hM3D(Gq) p = 0.03348). (m) Similarly, box aspect ratio over time was decreased for hM3D(Gq) mice compared to control mice (two-way mixed ANOVA, group x time F (238,3094) = 1.181, p = 0.03486; post hoc control v hM3D(Gq) p = 0.04464). (n) There were no group differences in the change in aspect ratio across time (two-way mixed ANOVA, group x time F (238,3094) = 0.08639, p = 0.06231). Dots represent individual data points, error bars or shaded bands represent standard error of the mean (SEM). For polar plots, 32 bins were computed to generate 11.25 degree bars for histogram densities.

Article Snippet: The Gi/o-coupled DREADD vector AAV8-hSyn-DIO-hM4D(Gi)-mCherry (plasmid #44362) and the Gq-coupled DREADD vector AAV8-hSyn-DIO-hM3D(Gq)-mCherry (plasmid #44361) were obtained from Addgene.

Techniques: Control