AVP histology and experiment timeline.

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AVP histology and experiment timeline. AVP histology and experiment timeline. A, Cre-dependent AAV (AAV-flex-taCasp3-TEVp) and location of bilateral BNST injection site; coordinates: AP –0.01 mm; ML ±0.75 mm; DV 4.8 mm; modified from Paxinos and Franklin (2012). Timeline of experimental manipulations. B, Example images of fluorescent in situ hybridization (ISH)-labeled BNST AVP cells and boxplot of cell number. Within the BNST, a significant decrease in AVP cell label was observed in both iCre+ male and female mice compared to iCre– control animals (males: p = 0.00014; females: p = 0.0025). iCre– (n = 13) and iCre+ (n = 11) males and iCre– (n = 13) and iCre+ (n = 8) females. C, Example images of fluorescent ISH-labeled accessory nucleus-AVP cells and boxplot of cell number. No significant AVP cell loss was observed between iCre+ and iCre– subjects (males: p = 0.98; females: p = 0.89). iCre– (n = 13) and iCre+ (n = 11) males and iCre– (n = 13) and iCre+ (n = 8) females. D, Example images of fluorescent ISH-labeled PVN and boxplot of image intensity (arbitrary units). iCre+ and iCre– subjects did not differ in PVN signal intensity (males: t(20) = 0.66, p = 0.947; females: p = 0.29). iCre– (n = 13) and iCre+ (n = 10) males and iCre– (n = 13) and iCre+ (n = 8) females. E, Example images of Nissl-stained BNST tissue and boxplot of cell number. No difference in BNST cell number between iCre+ and iCre– subjects was observed (males: p = 0.439; females: p = 0.44). iCre– (n = 6) and iCre+ (n = 9) males and iCre– (n = 8) and iCre+ (n = 6) females. In boxplots, dots indicate individual data points, bold horizontal lines illustrate the median, the areas above and below the lines show the 1st/3rd quartile. The vertical bars range from the minimal to the maximal values excluding outliers (±1.35 SDs from interquartile range). Images were taken at 10× for fluorescent material and 20× for Nissl-stained tissue. Scale bar = 50 µm; ** indicates significant effect of genotype, p < 0.005. Nicole Rigney et al. eNeuro 2019;6:ENEURO.0415-18.2019 ©2019 by Society for Neuroscience