Microglial VPS35 deficiency impairs Aβ phagocytosis and Aβ-induced disease-associated microglia, and enhances Aβ associated pathology

VPS35^flox/flox (VPS35^f/f) mice were generated as previously described [15]. CX3CR1^Cre−ER and 5xFAD [B6SJL-Tg (APPSwFlLon, PSEN1 × M146L × L286V) 6799Vas/Mmjax] mice were purchased from the Jackson Laboratory (Stock No: 021160, MMRRC Stock No: 34840-JAX, respectively). Note that 5xFAD mice express mutant human amyloid beta precursor protein (APP) and human presenilin 1 (PSEN1), with a total of five mutations including the Swedish [K670N/M671L], Florida [I716V], and London [V717I] in APP and M146L and L286V in PSEN1 under the control of Thy1-promoter [21]. VPS35^f/f mice were crossed with CX3CR1^Cre−ER mice as described previously [15, 19], and then crossed with 5xFAD to generated VPS35^f/f:CX3CR1^Cre−ER:5xFAD. All mice were maintained in C57BL/6 strain background for > 6 generations. All mice were group-housed with no more than 5 per cage under a room with 12 h light/dark cycle with water and standard rodent chow diet. All experiments with animals were approved by the Institutional Animal Care and Use Committee at Case Western Reserve University.

At postnatal day of 15, 45, 75, mice were injected with100 mg/kg of tamoxifen (Sigma Millipore, catalog #T5648) dissolved in corn oil (Sigma Millipore, catalog #C8267) intraperitoneally for 3 times consecutive in 1-day intervals at each injection day (labeled as VPS35^CX3CR1:5xFAD). Unless indicated specifically, the age-matched control mice received same dose corn oil as vehicle by injection (labeled as Ctrl:5xFAD). All results were confirmed with tamoxifen injection in VPS35^f/f:5xFAD and CX3CR1^Cre−ER:5xFAD to eliminate the potential effects of tamoxifen.

All data were presented as mean ± SD. 5 or more brain slices from 3 or more mice in each group were used for immunohistochemical analyses. > 6 mice in each group were assigned for behavioral test. All immunofluorescence staining data were quantified by ImageJ software. Statistical analyses were performed using Prism 7 (GraphPad Software). For two independent data comparisons, unpaired Student’s t test was used to determine statically significance. The test was considered significant when P < 0.05.

Mice were anesthetized by 3% isoflurane and perfused with phosphate-buffered saline (PBS, 0.01 M, pH = 7.4), then followed by 4% paraformaldehyde (PFA), and brains were post-fix overnight with 4% PFA. Brain tissues were sectioned into 30 μm-thick free-floating coronal or sagittal sections with different purposes using a vibratome (Leica VT1000S). All brain slices were sequentially collected and stored at -20 °C in cryoprotectant solution (FD Section Storage Solution) for further staining.

Free-floating sections were washed in PBS (3–5 min, 3 times) and incubated in blocking buffer (0.03% Triton X-100, and 2% donkey serum in PBS) for 30 min. Then the slices were incubated in primary antibody for overnight at 4 °C, washed 3 time in PBS in the next day, followed by incubating in secondary antibodies for 2 h at room temperature. Primary antibodies used were as follows: anti-VPS35, generated by Xiong lab as previously described [8]; anti-Iba1, ab178846, Abcam; anti-Iba1, ab5076, Abcam; anti-OC, AB2286, Sigma-Aldrich; anti-6E10, 803015, Biolegend; anti-ATG9A, ab108338, Abcam; anti-RTN3, 12055-2-AP, Thermofisher; anti-GFAP, 12389, Cell Signaling; anti-APOE, K74180B, Menidian Life Science; anti-TMEM119, ab209064, Abcam; anti-LPL, ab21356, Abcam; anti-Trem2, MAB2056, Abnova; anti-Clec7A, mabg-mdect, InvivoGen.

Thioflavin S (Thio-s) staining was used for Aβ deposition assay as previously described with mini modification. Every fifth tissue section of five consecutive sagittal sections was collected for Immunofluorescence staining. The brain slices were washed with PBS for 3 times and incubated in 0.1% Thio-S solution for 10 min. Then the brain slices washed with a series of graded EtOH as follows: 95% EtOH for 3 min, 80% EtOH for 3 min. Finally, the brain slices washed by PBS for 3 times. All the brain slices were captured on a BZX slider scanner. The images were converted and adjusted to the same threshold to increase signal-to-noise ratio. Five sections per mice from ctrl:5xFAD (n = 10) and VPS35^CX3CR1:5xFAD (n = 9) were quantified. In brief, the area of cortex (CTX), hippocampus (HIP), subiculum (SUB) and thalamus (TH) were outlined and quantified. The plaque density (plaque⁺ area /5.5 µm²) was quantified by the National Institutes of Health ImageJ software.

For immunostaining analyses, the brain slices were collected every 5th brain slice from bregma to lambda in each mouse, and 3 mice from each group were quantified. For OC/6E10 quantification, the representative field in the somatosensory cortex and hippocampus were selected in matched area. The ROI (region of interest) area was defined as 638.9 μm × 638.9 μm and randomly selected by a blinded observer. The OC density was calculated as: Area_OC/Area_ROI × 100%. The plaque diffuseness index was calculated by (Area_60000000000 − Area_Thio-S)/ Area_60000000000, as described previously [22]. For quantification of Aβ-associated dystrophic neurites, the matched area in cortex and hippocampus were picked as previously described [23]. The selected areas containing the Aβ plaque core and the surrounding 50 μm in diameter were quantified. The percentage burden (% of pixels with positive staining for ATG9A and RTN3) were quantified in the Aβ-associated area, as described previously [22]. For Aβ associated microglia quantification, two representative brain regions, the somatosensory cortex and hippocampus, were chosen from each brain slice. The Aβ associated area was defined by a plaque centered circle within 50 μm in diameter, and the number of microglia within the circle was quantified by ImageJ. For disease associated microglia (DAM) quantification, the Aβ associated area and Aβ un-associated area were randomly selected from the matched regions in the somatosensory cortex, and the fluorescence of DAM marker(s) co-stained with Iba1 was quantified and normalized with the intensity of control group. For Aβ phagocytosis, the fluorescence intensity of Aβ, LPL, and Clec7a were quantified in injected site and un-injected site with match area in somatosensory cortex. For these analyses, five slices from medial to lateral in each mouse, and 3–6 mice from each group were quantified with ImageJ by a blind observer.

The brain homogenization from mouse cortex and hippocampus was obtained as previously described [24]. The frozen tissue (PBS buffer) was homogenized with Dounce homogenizers until no visible pieces were seen; centrifuged (12,000 g, 4 °C, 30 min); and the supernatants were collected for soluble Aβ Elisa analysis. The insoluble fraction by PBS buffer were further solubilized by adding 5 M Guanidine buffer at the same ratio and homogenized by sonication. The homogenates were blended at room temperature for 6 h, and the supernatants were collected for insoluble Aβ Elisa analysis. The concentrations of β-amyloids were measured by ELISA kits for human Aβ42 (Invitrogen, catalog # KHB3441), human Aβ40 (Invitrogen, catalog # KHB3481), and mouse Aβ40 (Invitrogen, Catalog # KMB3481), respectively, following the manufacture instruction.

Aβ42 (Bachem, catalog #H-1368) was purchased from AnaSpec and the pHrodo Red Zymosan Bioparticles was purchased from ThermoFisher (Catalog # P35364↗). The phagocytosis assay was performed as described previously [25]. Briefly, Aβ42 peptide was dissolved in 1% NH4OH at 1 mg/ml and sonicated. Lyophilized Aβ42 was further dissolved in water, filtered (0.22 mm), and incubated at 37 °C for 24 h before use. Mice were anesthetized with isoflurane, and they were mounted in a stereotaxic apparatus and injected with 1 μl of aged Aβ42 and same volume of Phred beads slowly (0.1 μl/min) into the cortex of control and VPS35^CX3CR1 mice according to mouse brain atlas [26, 27]. The coordinates relative to bregma for cortex injection was caudal: − 2.06 mm; lateral: +/− 1.5 mm; ventral: − 0.8 mm. The needle of microinjector was left at the injection site for 5 min to enable its diffusion, and slowly withdraw. The mice were sacrificed on day 7 after the injection.

All male mice at the age of 3-MO (month) were used for behavior tests. Mice were transferred to the behavior test room 2 h before onset of behavior test to acclimate the environment. Before the onset of each trial, behavioral areas were sprayed with 75% ethanol. Unless otherwise noted, all behavioral trials were recorded using an overhead camera and analyzed by Etho Vision software (Etho Vision, Noldus). Mice were assigned and data quantified in double-blind method.

For open field test, each mouse was introduced into a chamber (50 × 50 × 20 cm, WxDxH) and allowed free move for 6 min. Total traveled distance and time in the inner zone were quantified. For depressive-like behavioral paradigms, force swimming test (FST), tail suspension test (TST) and sucrose preference test (SPT) were performed as previously described [28, 29]. Mice were recorded 6 min and quantified the mobility time in FST and TST, for the sucrose preference test, the mice were individually habituated to drink 2% (wt/vol) sucrose solution (dissolved in water) for 3 days, then mice were given access to the two pre-weighed bottles, one containing water and the other containing 2% sucrose solution. Bottle positions were changed every day and water and sucrose solution consumption was assessed daily for 4 days. The sucrose preference was quantified by the ratio of sucrose consumed over total solution consumed was used for measuring the sucrose preference. Y-Maze test, as previously described [30], each mouse was placed at the central of three opaque plastic arms and allowed to freely explore the three arms for 8 min. Total arm of entries and spontaneous alternation were quantified. For the Morris water maze (MWM), a circular water tank (diameter of 120 cm) fulfilled with water. The maze was equally divided into 4 quadrants, and one quadrant contain a platform with diameter of 10 cm as the escape platform. Then nontoxic white powder paints were added to the water to make the surface opaque to hide the escape platform. Mice were trained 4 trials per day with 20 min interval for 5 consecutive days. Mice were allowed to free search the escape platform for 60 s, at which point the experimenter would guide the animal to the escape platform if necessary, and the time latency will be quantified as 60 s. On the 6th day, the escape platform will be removed, and mice will have 60 s to swim. The swimming trajectories and the time spend in target quadrant will be recorded and quantified.

To investigate if microglial VPS35 deficiency contributes to the AD pathology, VPS35^CX3CR1:5xFAD mice were generated by crossing VPS35^f/f mice with CX3CR1^Cre−ER and 5xFAD mice (Additional file 1: Fig. S1a). The VPS35^CX3CR1:5xFAD mice were injected with tamoxifen or vehicle (as control) starting at age of P15 for three times as indicated in Additional file 1: Fig. S1b. At P90, mice were subjected to various tests, including brain pathology examinations and behavior assessment (Additional file 1: Fig. S1b). Notice that VPS35 was specifically knock out in the Iba1⁺ microglia cells in VPS35^CX3CR1:5xFAD brain, as compared with that in Ctrl:5xFAD mice (Additional file 1: Fig. S1c, d), verified the mouse identify. No difference in their body weights was detected between two group of mice at the age of 3 MO (Additional file 1: Fig. S1e).

It’s worth noting that the Thio-S positive plaque is the compact insoluble Aβ. To determine whether the soluble/ insoluble human Aβ and mouse Aβ levels are altered in 5XFAD brain by microglial VPS35 deficiency, we measured their levels by ELISA analysis. In line with the increased Aβ deposition, insoluble guanidine fraction of human Aβ40 and Aβ42 levels in cortex and hippocampus as well as the soluble PBS fraction of human Aβ42 levels in cortex were elevated in VPS35^CX3CR1:5xFAD mice (Fig. 1e–h). No difference was detected with the endogenous mouse Aβ40 levels in both cortex and hippocampus (Additional file 1: Fig. S2a, b). Together, these results suggest the Aβ deposition and Aβ levels were increased in VPS35^CX3CR1:5xFAD brain, indicating that the microglial VPS35 deficiency exacerbates Aβ pathology in 5XFAD mice.

The extracellular Aβ deposition is also often associated GFAP positive (+) reactive astrocytes in brains of AD patients and animal models [21, 24, 36]. We thus performed co-immunostaining analysis using antibodies against GFAP and ApoE, an AD risk gene that is also highly expressed in astrocytes [37, 38]. Indeed, a marked increase in GFAP⁺ astrocytes was detected in VPS35^CX3CR1:5xFAD cortex (Additional file 1: Fig. S3a, b). However, the plaque associated GFAP⁺ astrocytes (or the number of astrocytes per plaque) in the VPS35^CX3CR1:5xFAD cortex were comparable to that of control: 5XFAD (Additional file 1: Fig. S3d). Notice that the ApoE⁺ astrocytes and the ApoE⁺Thio-S⁺ plaques were both elevated in the VPS35^CX3CR1:5xFAD cortex (Additional file 1: Fig. S3a, c, e). These results suggest an increased reactive astrogliosis in VPS35^CX3CR1:5xFAD cortex, in line with the view for the elevated Aβ deposition.

Additional file 1: Figure S1. Mouse breeding and experimental protocol. a Breeding schematic to obtain VPS35^f/f:CX3CR1^Cre−ER:5xFAD mice. b Schematic illustrating TMX injection and behavioral testing timeline. Tamoxifen (100 mg/kg) was administered (i.p.) into VPS35^f/f:CX3CR1^Cre−ER:5xFAD mice [as mutants (VPS35^CX3CR1:5XFAD)]. In addition, tamoxifen was injected to VPS35^f/f:5xFAD or vehicle (Corn oil) was injected to VPS35^f/f:CX3CR1^Cre−ER:5xFAD mice [as controls (Ctrl:5XFAD)]. c Double immunostaining analysis for Iba1 (green) and VPS35 (Red) immunostaining. Scale bar = 10 μm. d Quantitative analysis of relative microglial VPS35 intensity compared with Ctrl: 5xFAD mice. (n = 3 per group, mean ± SD, **, P < 0.01, Student’s t test) e Weight analysis was conducted in 3 months Ctrl:5XFAD and VPS35^CX3CR1:5XFAD mice. (n = 7 per group, mean ± SD). Figure S2. No difference detected in endogenous mouse Aβ40 levels in microglial VPS35 deficient 5XFAD brain. a, b Expression of endogenous mouse Aβ40 level (n = 3 per group, mean ± SD, N.S., P > 0.05, Student’s t test). Figure S3. Increased reactive astrocytes in microglial VPS35 deficient 5XFAD brain. a Co-immunostaining of GFAP (green), ApoE (red) and Thio-S (gray) in the cortex of Ctrl:5XFAD and VPS35^CX3CR1:5XFAD mice. b–e Quantification of GFAP⁺ cell density, ApoE⁺ cell density, average ApoE fluorescence intensity per astrocyte and relative ApoE⁺Thio-S⁺ density in the cortex of Ctrl:5XFAD and VPS35^CX3CR1:5XFAD mice (n = 5 per group, mean ± SD, **, P < 0.01, Student’s t test). Figure S4. Increased branch number and soma volume in microglial VPS35 deficient 5XFAD brain. a Representative image for Aβ un-associated microglia and 3D reconstitution was performed with Imaris. Scale bar = 10 μm. b, c Quantitative analysis branch number and soma volume of Aβ un-associated microglia in Ctrl:5XFAD and VPS35^CX3CR1:5XFAD mice (n = 5 per group, mean ± SD, **, P < 0.01, Student’s t test).