ApoA-I deficiency increases cortical amyloid deposition, cerebral amyloid angiopathy, cortical and hippocampal astrogliosis, and amyloid-associated astrocyte reactivity in APP/PS1 mice

All procedures involving animals were approved by the Canadian Council of Animal Care and the University of British Columbia Committee on Animal Care. APP/PS1 mice (Jackson laboratories, B6.Cg-Tg(APPswe,PSEN1dE9)85Dbo/Mmjax, MMRRC stock no: 34832-JAX) on a C57Bl/6 background co-express two transgenes from the murine prion promoter: a chimeric mouse/human amyloid precursor protein (APP) cDNA containing the Swedish (K670 M/N671 L) mutations, and the human presenilin-1 (PS1) gene deleted for exon 9 [44]. APP/PS1 mice were first bred with apoA-I-deficient mice with targetted disruption in Apoa1(Jackson Laboratories, B6.129P2-Apoa1^tm1Unc/J, Stock no: 002055, also on a C57Bl/6 background) to produce an F1 generation hemizygous for both Apoa1^tm1Unc and APP/PS1 transgenes. These animals where then backcrossed to apoA-I knockouts (homozygous for Apoa1^tm1Unc) to produce F2 male and female mice of four genotypes: APP/PS1 mice hemizygous for Apoa1 (APP/PS1 apoA-I^HEM), APP/PS1 mice with complete Apoa1 deficiency (APP/PS1 apoA-I^KO), nontransgenic littermates hemizygous for Apoa1 (WT apoA-I^HEM), and nontransgenic littermates deficient in Apoa1 (WT apoA-I^KO). Although APP/PS1 mice on a pure C57Bl/6 background have an increased seizure risk, we selected this strain to maintain genetic homogeneity throughout this breeding strategy. Overall, 80% of the animals survived until the end of the experiment, with specific survival rates of 66% for APP/PS1 mice, 63% for APP/PS1 apoA-I^HEM mice, and 74% for APP/PS1 apoA-I^KO mice (Additional file 1: Figure S1a and b). While this breeding strategy was successful in generating N = 6–8 mice per group, insufficient animals survived to yield sex-specific cohorts. We therefore used mixed sexes, which is an acknowledged limitation of this study, yet tracking of individual animals throughout the study showed no clear sex bias throughout the results and justifies the use of pooled sexes.

Mice were fasted for 4 h prior to anesthetization by intraperitoneal injection of 20 mg/kg xylazine (Bayer) and 150 mg/kg ketamine (Bimeda-MTC). Blood was collected by cardiac puncture in ethylenediaminetetraacetic acid (EDTA)-containing syringes, centrifuged at 21,000g for 10 min at 4 °C, and the resulting plasma was stored at − 80 °C until use. Mice were then perfused for 6 min with ice-cold phosphate-buffered saline (PBS) containing 2500 U/L heparin at 6 mL/min. Brains were excised and bisected in the sagittal plane. A 2 × 5 mm piece of parietal cerebral cortex was removed and stored separately for RNA analysis. The piece of brain for RNA analysis and the remaining half-brain were snap-frozen on dry ice and stored at − 80 °C until use. The remaining half-brain was fixed in 4% paraformaldehyde (PFA) for 2 days at 4 °C followed by storage in PBS containing 30% sucrose and 0.1% sodium azide at 4 °C.

Plasma HDL cholesterol (HDL-C), low-density lipoprotein cholesterol (LDL-C), and total cholesterol levels were measured using Wako kits (Category no: 997-01301 for HDL-C, 993-00404 and 999-00504 for LDL-C, and 999-02601 for total cholesterol) as per the manufacturer’s directions adapted for 96-well microplates. Plasma samples were randomized, and the researcher performing the measurements was blinded to sample genotype. Plasma lipids were analyzed in N = 6–7 mice per genotype.

Immunofluorescence triple co-staining was performed to visualize endothelial cells (cluster of differentiation 31; CD31), amyloid beta plaques (X-34), and activated astrocytes (glial fibrillary acidic protein; GFAP) as follows. Cryoprotected half brains were sectioned at 40 μm on a Leica CM3050 Research Cryostat and stored in PBS containing 0.1% sodium azide until staining. Three sections from each half-brain were selected from the anterior to posterior hippocampus at 200-μm intervals and mounted on Superfrost Plus slides. Antigen retrieval was performed with citrate buffer (10 mM citric acid, 0.05% Tween 20, pH 6.0) at 95 °C for 5 min followed by washing with PBS, tissue permeabilization with 0.25% Triton X-100 in PBS for 30 min, and blocking with 5% donkey serum and 1% BSA and 0.3% Triton X-100 in PBS for 60 min. Sections were incubated in primary antibodies for CD31 (Abcam, ab28364, 1:200 dilution), GFAP Alexa Fluor 488 (eBiosceince, 53-9892-80 1:400 dilution), or ICAM-1 (R&D, AF796, 1:50 dilution) in 5% donkey serum, 1% BSA, and 0.3% Triton X-100 in PBS overnight at 4 °C. After washing with PBS, sections were incubated with secondary antibodies for 60 min at room temperature. Secondary antibodies were as follows: goat anti-rabbit Alexa Fluor 594 antibody (Life Tech, A11012, 1:600 dilution) to detect CD31 on its own and when co-stained with GFAP, goat anti-rabbit Alexa Fluor 647 antibody (Life Tech, A27040↗, 1:400 dilution) to detect CD31 co-stained with ICAM-1, and donkey anti-goat Alexa Fluor 594 antibody (Life Tech, A-11058, 1:400 dilution) to detect ICAM-1. Sections were then washed with PBS. Amyloid staining was subsequently performed with X-34 (Sigma-Aldrich, SML 1954, 2 μM in PBS-T) for 20–30 min followed by washing with 40% ethanol in PBS then PBS alone. Coverslips were mounted onto slides in prolong antifade (Invitrogen, P36970↗), and slides were stored at 4 °C until imaging with an Axio Scan.Z1 (Zeiss). Brain sections were randomized, and the researcher performing the staining was blinded to sample genotype. The cellular localization of ICAM-1 expression was visualized using an LSM 880 confocal laser scanning microscope (Zeiss).

Image analysis was performed with ImageJ (NIH) by a researcher blinded to sample genotype as illustrated in Additional file: Figure S2. Exported images for each channel were converted to 8-bit black and white images. The threshold for positive and negative pixels was manually determined for X-34 and GFAP images using histogram-based segmentation then applied to all of the images of that channel. Due to regional variation in CD31 staining, auto-local thresholding using the Bernsen method was performed on CD31 images. Cortical and hippocampal regions were manually selected and saved as “regions of interest” (ROIs) for each section. Total CD31, X-34, and GFAP-positive area was measured in the threshold segmented cortical and hippocampal ROIs and normalized to the total ROI area. Vascular GFAP was quantified as the GFAP-positive area associated with CD31 in each region whereby a mask of the segmented CD31 image for a section was created then applied to the segmented GFAP image of the same section. The GFAP-positive area within the CD31 mask was measured then normalized to the total CD31-positive area within the ROI. Plaque-associated GFAP was similarly quantified as the GFAP-positive area associated with X-34 in each region whereby a mask of the segmented X-34 image for a section was created then applied to the segmented GFAP image of the same section. The GFAP-positive area within the X-34 mask was measured then normalized to the total X-34-positive area within the ROI. 1

Total and vascular ICAM-1 quantification was performed using the same techniques as described above to measure total and vascular GFAP. Parenchymal ICAM-1-positive area was calculated as the difference between total and vascular ICAM-1-positive area in the cortical and hippocampal regions.

CAA was quantified using methods similar to that published in Nature Protocols by Wilcock et al. in 2006 [45], which has been used by many others [37, 46, 47] including in the study by Lefterov et al. using apoA-I-deficient APP/PS1 mice [34]. A mask containing areas of vascular amyloid was created by manually discriminating vascular amyloid from parenchymal plaques in segmented X-34 images based on morphology, as illustrated in Additional file 1: Figure S3. Identification of vascular versus parenchymal amyloid was performed on inverted images to ease visualization. These vascular amyloid masks were then applied back onto segmented X-34 images, and the percent positive area was measured and normalized to total area of the cortical ROI to give percent cortical CAA area. The X-34-positive area within the vascular amyloid mask was then used to create a new CAA mask. This CAA mask was then applied to a mask of vascular GFAP created as above. The vascular GFAP-positive area within the CAA mask was measured and normalized to CAA area to give the percent area of CAA associated with vascular GFAP.

The above analysis steps, excluding the drawing of cortical and hippocampal ROIs and vascular amyloid areas, were repeated for each section using an automated ImageJ macro. The full macro text for the imaging strategy is available in Additional file 2. Additional file 1: Figure S2 shows schematics illustrating the image analysis process. Analysis of vessel diameter and tortuosity was performed with Vesselucida 360 software (MBF Bioscience) using CD31 as the vessel marker. For amyloid staining, N = 4–5 animals per genotype were used, and for CD31, GFAP, and ICAM-1 staining, N = 5–6 animals per genotype were used.

Protein from half-brains was serially extracted to produce soluble and insoluble protein fractions. Half-brains were first homogenized with a Tissuemite homogenizer for 20 s in carbonate buffer (10 mmol/L carbonate, 50 mmol/L sodium chloride, cOmplete protease inhibitor tablet, pH 11.5) then sonicated. Homogenates were cleared by centrifugation at 12,500g for 45 min at 4 °C. The resulting supernatant was neutralized with 1.5 volumes Tris (1 mol/L Tris, pH 6.8) and labeled as the soluble fraction. The pellet was resuspended in 1 mL of guanidine hydrochloride (5 mol/L guanidine hydrochloride in 1 mol/L Tris, pH 8.0) by pipetting followed by rotation overnight at room temperature and labeled as the insoluble fraction. Soluble and insoluble extracts were stored at − 80 °C until use. Lysate protein concentrations were determined using the DC Protein assay kit (BioRad).

Human Aβ40 (KHB-3482, ThermoFisher, 1:20, 1:2500), human Aβ42 (KHB-3442, ThermoFisher, 1:40, 1:2500), and murine apoE (3752-1HP-2, ThermoFisher, 1:20, 1:200) levels were measured in carbonate soluble and guanidine hydrochloride insoluble half-brain lysates using commercial sandwich ELISA kits according to the manufacturer’s instructions. Murine GFAP (NS830, Millipore, 1:400), intercellular adhesion molecule 1 (ICAM-1) (ab100688, Abcam, 1:2), vascular cell adhesion molecule (VCAM-1) (ab100750, Abcam, 1:2000), platelet-derived growth factor receptor beta (PDGFRβ) (MBS919047, MyBioSource, 1:10), interleukin 1 beta (IL-1β) (K15245D, MesoScale Discovery, 1:2), and tau (K15121D, MesoScale Discovery, 1:50) levels were measured in carbonate soluble half-brain lysates using commercial sandwich or MesoScale Discovery ELISA kits according to the manufacturer’s instructions. Data points were interpolated from a standard curve using a 4-parameter nonlinear regression curve fitting and normalized to total soluble protein concentration. Brain lysates were randomized and the researcher performing the ELISAs was blinded to sample genotype. For apoE ELISA, N = 6 mice per genotype were used. For Aβ ELISA, N = 5–7 mice per genotype were used. For IL-1β, ICAM-1, VCAM-1, and PDGFRβ ELISA, N = 5–19 mice per genotype were used. For GFAP ELISA, N = 6–14 mice per genotype were used.

RNA was extracted from parietal cerebral cortices using Trizol (Invitrogen) and treated with DNaseI (Life Technologies) prior to cDNA synthesis. cDNA was generated using the Taqman Reverse Transcription Kit (ThermoFisher, N8080234). RT-qPCR was performed using the Light Cycler 96 Real-Time PCR System (Roche) and FastStart Essential DNA Green Master Mix (Roche). Expression of murine Abca1 (Fwd: CTGACCTATGTGCTGCCGTA; Rev.: GAGCCGGTCATCAATCTCAT) and murine Il1b (Fwd: TTGACGGACCCCAAAAGA; Rev.: CAGCTTCTCCACAGAGCCACA) were normalized to murine β-actin (Fwd: ACGGCCAGGTCATCACTATTG; Rev.: CAAGAAGGAAGGCTGGAAAAG). RNA homogenates were randomized, and the researcher performing the qRT-PCR was blinded to sample genotype. For Apoe and Il1b mRNA analyses, N = 7–12 mice per genotype were used.

All statistical analyses were performed with GraphPad Prism 7; p values < 0.05 were considered statistically significant. For the analysis of all non-amyloid data, statistical comparisons were made by two-way ANOVA considering APP/PS1 genotype as one factor and apoA-I genotype as a second factor (omnibus analysis) followed by Sidak’s multiple comparisons test if significant factor or interaction effects were observed. Analysis of Aβ levels, amyloid plaque area, and CAA were performed with unpaired t test or Mann-Whitney test for parametric and non-parametric data, respectively.

Biochemical analysis of total soluble and insoluble Aβ40 and Aβ42 pools in half-brain homogenates revealed no differences by apoA-I genotype, although soluble Aβ40, insoluble Aβ40, and insoluble Aβ42 were all very slightly and non-significantly increased in APP/PS1 apoA-I^KO vs. APP/PS1 apoA-I^HEM mice (Fig. 2g–j). The lack of a significant effect of apoA-I genotype on Aβ levels, despite the significant increase in cortical amyloid deposition, may be due to a region-specific effect of apoA-I on amyloid that is not detectable in crude half-brain homogenates. Indeed, immunofluorescence analysis (described above) confirms that apoA-I genotype influences amyloid plaque burden in the cortex but not in the hippocampus.

Although no significant differences in tau or p-tau were observed by APP/PS1 genotype, total tau levels (Fig. 2k) were significantly higher and p-tau levels (Fig. 2l) tended to be higher in apoA-I^KO mice compared to apoA-I^HEM mice (p = 0.041 and p = 0.054, respectively, by omnibus two-way ANOVA). ApoA-I genotype significantly interacted with APP/PS1 genotype with respect to p-tau (p = 0.023). Post-hoc Sidak’s multiple comparison tests revealed a nearly significant increase in total tau in APP/PS1 apoA-I^KO vs. APP/PS1 apoA-I^HEM mice (p = 0.063) and a significant increase in p-tau from 1.09 ng/mg in APP/PS1 apoA-I^KO to 1.40 ng/mg in APP/PS1 apoA-I^HEM (p = 0.026). Levels of p-tau showed a trend towards a reduction in APP/PS1 apoA-I^HEM vs. WT apoA-I^HEM mice (p = 0.099 by Sidak’s multiple comparisons test). The total tau to p-tau ratio was unaffected by loss of apoA-I (Fig. 2m).

We next investigated markers of inflammation expressed specifically by cells of the blood-brain barrier. PDGFRβ is a pericyte marker that is elevated in some cases of neuroinflammation [50]. We observed a significant interaction effect of APP/PS1 and apoA-I genotypes (p = 0.026 by omnibus two-way ANOVA) on PDGFRβ protein levels in the brain, where PDGFRβ protein tended to be elevated only in APP/PS1 apoA-I^KO mice compared to APP/PS1 apoA-I^HEM mice (p = 0.065 by Sidak’s multiple comparisons test) (Fig. 3c). Mean PDGFRβ levels were 5.03 ng/mg in WT apoA-I^HEM, 4.56 ng/mg in WT apoA-I^KO, 3.76 ng/mg in APP/PS1 apoA-I^HEM, and 5.61 ng/mg in APP/PS1 apoA-I^KO. To evaluate endothelial cell-specific inflammation, we measured protein levels of VCAM-1 in the brain. VCAM-1 is expressed on the cell surface of endothelial cells and assists in the adhesion of circulating immune cells to the vessel wall [11]. We found that VCAM-1 tended to be elevated in apoA-I^KO mice compared to apoA-I^HEM mice overall (p = 0.076 by omnibus two-way ANOVA) independent of APP/PS1 genotype (Fig. 3d). Together, these data suggest that loss of apoA-I can exacerbate neuroinflammation in APP/PS1 mice, particularly in cell types associated with the cerebrovasculature.

The effect of apoA-I genotype on total brain ICAM-1 levels was found to be region specific using immunofluorescence. Although we observed no significant differences in total cortical ICAM-1 staining by apoA-I genotype (Fig. 4b), total ICAM-1-positive area was increased in APP/PS1 apoA-I^KO compared to APP/PS1 apoA-I^HEM in the hippocampus, from 2.34% of hippocampal area to 4.67% (p = 0.001 by Sidak’s multiple comparisons test) (Fig. 4c). Interestingly, vascular-specific ICAM-1, measured as the ICAM-1-positive area associated with CD31, was significantly elevated in both cortex (Fig. 4d, e) and hippocampus (Fig. 4f, g) in APP/PS1 apoA-I^KO compared to APP/PS1 apoA-I^HEM. Cortical vascular ICAM-1 levels were 7.87% and 12.26% of CD31-positive area in APP/PS1 apoA-I^HEM and APP/PS1 apoA-I^KO, respectively (p = 0.001 by Sidak’s multiple comparisons test) (Fig. 4h, j) and hippocampal levels were 15.02% and 24.19% (p = 0.001 by Sidak’s multiple comparisons test) (Fig. 4k,m). Although no differences in parenchymal ICAM-1-positive area were observed in the absence of apoA-I (Fig. 4i, j), parenchymal ICAM-1-positive area was increased in the hippocampus from 2.19% of hippocampal area in APP/PS1 apoA-I^HEM to 4.41% in APP/PS1 apoA-I^KO (p = 0.001 by Sidak’s multiple comparisons test) (Fig. 4l, m).

We next used immunofluorescence to examine the association of CD31 and GFAP and observed a robust and statistically significant increase in the cerebrovascular area associated with GFAP in both the cortex and hippocampus of APP/PS1 apoA-I^KO mice compared to APP/PS1 apoA-I^HEM mice (p = 0.008, p = 0.007, respectively, by Sidak’s multiple comparisons test) (Fig. 5f–i). In addition, significant elevations were observed overall in APP/PS1 compared to WT mice (p < 0.0001 in the cortex by omnibus two-way ANOVA) and in apoA-I^KO compared to apoA-I^HEM mice (p = 0.025 and p = 0.049 in the cortex and hippocampus, respectively, by omnibus two-way ANOVA). Mean cortical vascular GFAP levels were elevated from 0.21% and 0.30% of CD31-positive vascular area in WT apoA-I^HEM and apoA-I^KO, respectively, to 1.80% in APP/PS1 apoA-I^HEM mice and 3.86% in APP/PS1 apoA-I^KO. In the hippocampus, mean vascular GFAP levels increased from 6.86%, 6.20%, and 5.20% in WT apoA-I^HEM, WT apoA-I^KO, and APP/PS1 apoA-I^HEM, respectively, to 10.86% in APP/PS1 apoA-I^KO. Strikingly, the elevation in vascular GFAP in apoA-I^KO mice was statistically more robust than the changes in total GFAP-positive area in both the cortex and the hippocampus. The total vascular area vessel thickness, and vessel tortuosity as defined by CD31 staining were all unchanged by apoA-I genotype in the cortex and the hippocampus (Additional file 1: Figure S4a-h).

Others have observed that genetically altering apoA-I levels in APP/PS1 mice affects spatial learning and memory, with increased apoA-I improving performance and loss of apoA-I worsening performance in the Morris Water Maze [34, 37]. We performed contextual and cued fear conditioning tests to evaluate fear memory (Additional file 1: Figure S5a and b). No significant genotype effects were observed with either test despite a trend towards reduced performance in both APP/PS1 vs. WT mice (p = 0.109) and in apoA-I^KO vs. apoA-I^HEM mice (p = 0.077) overall in the contextual fear conditioning test. Notably, the cohort of mice available for behavior testing was relatively small, particularly for the APP/PS1 apoA-I^KO group (n = 7); therefore, our behavior analysis was likely underpowered.

Additional file 1:Figure S1. Survival rates for (a) female and (b) male mice with known genotype upon death or experiment endpoint. Log-rank test p values are shown below graphs. Figure S2. Analysis strategy for histology. Images with bold, colored outlines indicate steps measuring percent positive area. Colored arrows between images indicate steps where the pixels positive in both images were combined into a new image. Figure S3. Morphological discrimination of vascular versus parenchymal amyloid for analysis of CAA area. Examples of inverted 8-bit X-34 images are shown with (right) and without (left) vascular (teal boxes) and parenchymal (green circles) amyloid indicated. Figure S4. Total vascular area was unchanged by APP/PS1 or apoA-I genotype. Vessel area (a, c), thickness (e, f) and tortuosity (g, h) as defined by immunofluorescent staining of CD31 in the (a, e, g) cortex and (c, f, h) hippocampus. (b, d) Representative images. Figure S5. Contextual and cued fear memory was not significantly affected by APP/PS1 or apoA-I genotype. Mice were trained to associate a context or auditory cue with a foot shock then tested for memory of the associated (a) context or (b) cue as measured by the time spent freezing Omnibus analyses of apoA-I and APP/PS1 genotype effects by two-way ANOVA are displayed as exact p values below graphs. Figure S6. Hypothalamic GFAP staining area was unaffected by apoA-I and APP/PS1 genotype. (a) GFAP staining area was visualized by immunofluorescence in the hypothalamus. (b) Representative image. For graphs in Figure S4, S5, and S6, points represent individual mice and bars represent mean values, circles represent female mice, squares represent male mice, and N = 5-23 mice per genotype. apoA-I, apolipoprotein A-I; HEM, hemizygous apoA-I genotype; KO, knockout apoA-I genotype; WT, wildtype APP/PS1 genotype; APP/PS1, transgenic APP/PS1 genotype; CD31, cluster of differentiation 21; GFAP, glial fibrillary acidic protein. (PDF 2870 kb)Additional file 2:Macro text for the quantification of total amyloid, GFAP, and vascular area, vascular astrogliosis, GFAP-associated plaques, CAA, and CAA-associated GFAP. (DOCX 22 kb)