Astrocytes have the capacity to act as antigen-presenting cells in the Parkinson’s disease brain

Human embryonic stem cell (ESC)-derived astrocytes [22] were expanded in Advanced DMEM/F12 (Thermo Fischer 12634-010) supplemented with 20 ng/ml Human Ciliary Neurotrophic Factor (CNTF) (Thermo Fischer), 1% penicillin streptavidin (Thermo Fischer 15140-122), 1% B27 supplement (Thermo Fischer 17504-044), 1% non-essential amino acids (Merc Millipore TMS001-C), and 1% l-glutamine (Thermo Fischer 25030-024). Cells were passaged using Trypsin-EDTA (Life technologies). Two weeks prior to the experiments, the media was changed to Neurobasal medium supplemented with 20 ng/ml CNTF, 1% penicillin streptavidin, 1% non-essential amino acids, 1% l-glutamine (Thermo Fischer 25030-024), and N2 supplements (Thermo Fischer 17502048). For experiments, the astrocytes were seeded at a concentration of 4500 cells/cm², resulting in a 40–50% confluence. Cells from 90 DIV to 120 DIV were used in the study.

Human adult microglia were isolated as described previously [23] (ethical number ANTJ 1988/3). Shortly, human brain tissue was obtained from the temporal lobe of three epilepsy patients undergoing surgery. A separate microglia culture was derived from each donor. The tissue was washed in PBS several times, and blood clots were removed using a Pasteur pipette. The tissue was then incubated with 0.5% trypsin and 25 μg/ml of DNase in PBS on shake for 30 min at 37 °C. The trypsin was inactivated using 10% fetal calf serum (FCS), and the tissue was dissociated using a mashing filter prior to centrifugation at 1200 rpm for 10 min. Thereafter, the cells and debris were resuspended in PBS and added to Percoll before centrifugation at ×31,000g for 30 min with no breaks at 4 °C. The top layer containing myelin was removed, and the middle layer consisting of microglia and oligodendrocytes was resuspended in PBS and centrifuged at 1200 rpm for 10 min. The cells were counted and cultured at a density of 2 × 10⁶ cells/ml in a T12.5 flask in MEM medium supplemented with 5% FCS, 0.1% glucose, 1% penicillin-streptomycin, and 1% glutamine. Following day, the floating cells (which are oligodendrocytes) were removed. The cells were passaged using 0.05% trypsin and 2 mM EDTA and cultured at a density of 50,000 cells/cm² for experiment.

Astrocyte and microglia cultures were exposed to 0.5 μM sonicated αSYN-F (Cy3 labeled or unlabeled), IFNγ (Thermo Fischer 100 U/ml for astrocytes and 25 U/ml for microglia), 0.5 μM αSYN-F + IFNγ, and 0.5 μM αSYN-M or were left untreated. After 7 days of exposure the cells were fixed or detached for further analyses.

Cells were fixed in 4% paraformaldehyde (PFA) in PBS and washed with PBS. Blocking and permeabilization were performed with 5% normal goat serum (NGS) and 0.1% triton in PBS for 30 min in RT. Primary antibodies were diluted in 0.5% NGS and 0.1% triton in PBS and added to the cells for 2 h at RT. Thereafter, cells were washed 3 times with PBS prior to incubation with secondary antibodies or dyes for 1 h at RT. After additional washes, the cells were mounted, using Ever Brite Hardset Mounting medium with or without DAPI (BioNordika). The cells were analyzed using the fluorescence microscope Observer and Z1 Zeiss and confocal images were taken using Zeiss LSM700. The primary antibodies used were CD68 (DAKO, m0841, Clone KP1, 1:200), MHC-II (DAKO M0775, 1:200), MHC-I (Abcam EMR8-5 1:100), PDL1-1 (Novus biologicals NBP-176769 1:200), LAMP-1 (Abcam ab24170 1:200), nestin (Millipore ABD69 1:200), vimentin (Millipore AB5733 1:200), GLAST (Novus biologicals NB100-1869 1:400), and ALDH1L1 (Novus biologicals NBP2-24143 1:400). The secondary antibodies and dyes used were Alexaflour 488 goat anti rabbit/mouse (Thermo Fischer, 1:200) and Alexaflour 555 goat anti rabbit/mouse (Thermo Fischer, 1:200). To stain the plasma membrane, cells were incubated with wheat germ agglutinin and Alexa Fluor® 350 Conjugate (Life technologies, 1:200) for 10 min.

The cells were detached using Accutase (Thermo Fischer) and centrifuged in ×300g for 5 min. The pelleted cells were resuspended in staining buffer containing 2% FBS (BD Biosciences) and Versen (Thermo Fishcer) (1:1), before incubation with antibodies for 20 min in the dark. The following antibodies from BD Biosciences were used according to manufacturer’s instructions: APC mouse anti-human CD40 (555591), BV510 mouse anti-human CD80 (563084), PE mouse anti-human CD86 (555665), FITC mouse anti-human HLADR/DP/DQ (555558), PE-Cy7 mouse anti-human HLA-A/B/C (561349), and BV421 mouse anti-human PDL-1 (563738). The cells were washed and resuspended in Versen, and the fluorescence signal was examined with the machine flow cytometry Canto II (BD Biosciences). The flow cytometry data was analyzed using the FlowJo software (version 7.6.5; Tree Star, Ashland, OR) software.

Microglia cultures were detached using Accutase (Thermo Fischer) and centrifuged at ×300g for 5 min. The cells were incubated in blocking buffer (PBS, 10% normal human serum and normal mouse IgG (3 mg/ml)) for 30 min and centrifuged at ×300g for 5 min, before incubation with the antibodies for 20 min in the dark. The following antibodies from BD Biosciences were used according to the manufacturer’s instructions: APC mouse anti-human CD86 (BD Biosciences; 555660), FITC mouse anti-human HLA-DR/DP/DQ (BD Biosciences; 555558), BV786 mouse anti-human CD80 (BD Biosciences; 564159), PerCp mouse anti-human CD40 (Biolegend; 334316), and BV650 mouse anti-human HLA-A/B/C (BD Biosciences; 740407). The cells were washed and resuspended in 2 mM EDTA in PBS, and the fluorescence signal was examined and analyzed using the FACSAria Fusion (BD Biosciences). The data was analyzed using the FlowJo software (version 7.6.5; Tree Star, Ashland, OR) software.

We first sought to investigate if there was a correlation between PD pathology and the expression of MHC-II. The presence of Lewy body pathology in PD cases and the absence of pathology in the control cases were confirmed by staining brain sections with αSYN and p-αSYN antibodies (Fig. 1a). In order to investigate if the levels of MHC-II are different between PD brains and control brains, we performed immunostainings for MHC-II and p-αSYN. Quantifications of MHC-II IntDen (area × mean intensity) in mesencephalon demonstrated a significant increase of MHC-II expression in PD patients compared to healthy controls (Fig. 1b). Interestingly, we could observe a clear correlation between MHC-II expression and the presence of p-αSYN in the PD brains (Fig. 1c). Subsequently, we performed immunostainings for MHC-II in striatum to investigate if there was a correlation between MHC-II expression in different regions of the nigrostriatal pathway, which is heavily affected by αSYN pathology in PD. Indeed, we found a correlation of MHC-II expression between mesencephalon and striatum in the PD brains, but not in the control brains (Fig. 1d, e). To clarify whether the age of the patients had any impact on the MHC-II expression, we performed linear regression on the MHC-II and the age in the PD group and in the control group. Our analysis demonstrates that there is no correlation between age and the expression of MHC-II in the material included in this study (61–84 years of age) (Additional file 1 a and b).

Moreover, the immunohistochemical staining showed that MHC-II co-localized with the astrocytic markers GLAST (Fig. 1f) and GFAP (Fig. 1g), as well as with the microglial marker Iba1 (Fig. 1h) in both PD and control brain sections, demonstrating that both microglia and astrocytes express MHC-II. To analyze the frequency of MHC-II expression in the various cell types, the respective overlaps of MHC-II with GLAST, GFAP, and Iba1 were quantified. In both PD and control brains, one third (35 and 31 %, respectively) of the MHC-II area overlapped with GLAST⁺ astrocytes (Fig. 1i). There was no significant difference in the total GLAST⁺ area between controls and patients, confirming GLAST expression by both nonreactive and reactive astrocytes (Additional file 2a). Moreover, 15% of the MHC-II area overlapped with reactive GFAP⁺ astrocytes in PD brains and 10% in control brains (Fig. 1j). Importantly, GFAP stains the cytoskeleton of the astrocyte, which only constitutes 15–20% of the cell [24]. Hence, the whole astrocyte is much bigger than the GFAP staining, and the overlap with MHC-II and GFAP will only reflect a proportion of the MHC-II expressing reactive astrocytes. In contrast to GLAST, there was an increase in GFAP⁺ area in PD patients compared to controls (Additional file 2 a). Double staining of GLAST and GFAP (Additional file 2b) show that the two markers overlap very little, which was expected since they label different parts of the astrocyte. While GFAP is a cytoskeleton protein, GLAST is expressed in the plasma membrane of the cells. Moreover, the expression levels of GFAP and GLAST vary between different astrocytic subclasses. Hence, the combined result from the MHC-II/GLAST and MHC-II/GFAP staining show that almost 50% of the MHC-II overlapped with either of the astrocytic markers. Both in PD and control brains, approximately one third (33% and 32%, respectively) of the MHC-II area overlapped with Iba1 (Fig. 1k). Similar to GFAP, the total Iba1 area was increased in PD patients, compared to controls (Additional file 2a). The remaining MHC positive cells (approximately 20%) may reflect MHC-II⁺ infiltrating immune cells and/or GLAST-GFAP-MHC-II+ astrocytes. Hence, although the expression of MHC II is increased in the PD brain, the overlap with astrocytic markers and microglial markers is not significantly different. The most likely explanation is that the same cells express MHCII in the healthy brain and in the PD brain, but that their expression level is higher in the PD brain.

Due to their myeloid origin, microglia cells have been addressed as the primary antigen-presenting cells in the brain. To investigate antigen presentation capacities of microglia in PD, adult human microglia were exposed to sonicated αSYN preformed fibrils (αSYN-F) (Fig. 2a). The β-sheet structure of the αSYN-F was assessed with ThT assay (Additional file 3a), and TEM was performed to compare the αSYN-F before and after the sonication (Additional file 3b-c). Immunostaining for the lysosomal marker CD68, a phagocytic marker specific for microglial cells, illustrated intracellular accumulation of αSYN 7 d after exposure (Fig. 2b). Flow cytometry analysis showed upregulation of surface expression of MHC-I and MHC-II and the co-stimulatory molecules CD80, CD86, and CD40 (Fig. 2c–g) upon treatment with IFNγ, verifying that the microglia were healthy and responded normally to surrounding inflammatory signals. However, exposure of the microglia to αSYN-F did not result in increased surface expression of MHC-I and MHC-II or any of the co-stimulatory molecules important for T-cell activation (Fig. 2c–g). These results indicate that microglia cells are not capable of activating T cells following exposure to αSYN-F.

Based on our findings that approximately half of the MHC-II-expressing cells in the PD brain are astrocytes, we next investigated whether astrocytes can act as antigen-presenting cells upon αSYN-F exposure. Subsequently, human astrocytes expressing the astrocytic markers GFAP, GLAST, ALDH1L1, vimentin, and S100β (Additional file 4) were exposed to αSYN-F for 7 days (Fig. 3a). Flow cytometry analysis revealed cell surface expression of MHC-II, MHC-I, and PDL-1 (Fig. 3b-d) upon stimulation with IFNγ. Interestingly, cell surface expression of the co-stimulatory molecules CD80, CD86, and CD40 (Fig. 3e–g) were only detected following exposure to sonicated αSYN-F. These results demonstrate that αSYN-F stimulate the astrocytes to express the co-stimulatory molecules necessary for professional APCs to activate CD4⁺ T cells.

Professional APCs have the ability to present antigens with both MHC-II and MHC-I molecules, enabling them to activate both CD4⁺ and CD8⁺ T cells. In order to investigate whether αSYN-F and MHC-I/II are in close proximity in the human astrocytes, we performed immunocytochemistry. In line with our recently published data [15], the human astrocytes accumulated large amounts of aggregated αSYN, while monomeric αSYN was rapidly degraded by the cells (Fig. 4a, b). In accordance with the flow cytometry data, the number of cells expressing MHC-II and MHC-I in control cultures and αSYN-F-exposed cultures was similar. Stimulation with IFNγ increased the number of MHC-II positive cells as well as the expression of MHC-I (Fig. 4a, b) and PDL-1 (Additional file 5). Interestingly, in the αSYN and αSYN + IFNγ-treated astrocyte cultures, the majority of αSYN aggregates were surrounded by MHC-II . The localization of MHC-II, forming a capsule around the deposited αSYN, was confirmed with confocal microscopy (Fig. 4c, c'). These data together with the flow cytometry results strongly suggest an involvement of the MHC-II pathway in astrocytes when exposed to αSYN-F. Furthermore, immunostainings revealed MHC-I expression in the proximity of the intracellular αSYN deposits and partial encapsulation of αSYN was also observed for MHC-I, using confocal microscopy (Fig. 4d, d'). Since both MHC-I and II co-localize with αSYN aggregates, astrocytes might process αSYN as an antigen through both pathways, which further proposes their role as antigen presenting-cells.

MHC-II molecules encounter their antigen in late endosomal, lysosomal vesicles and are then transported to the cell surface. To find out if the αSYN deposits that are surrounded by MHC-II are within the same cellular compartment, immunocytochemistry with the lysosomal marker LAMP-1 was performed. The immunostainings revealed that the ingested αSYN-F enter the endo-lysosomal pathway (Fig. 5a, b). The localization of the αSYN deposits within LAMP-1 positive vesicles was confirmed by confocal microscopy (Fig. 5c). To find out whether the intracellular MHC-II is also surrounded by LAMP-1 positive vesicles, human astrocytes treated with unlabeled αSYN-F were stained with MHC-II and LAMP-1. Confocal microscopy demonstrated that LAMP-1 positive vesicles indeed surrounded the MCH-II molecules in the αSYN-F-treated astrocytes (Fig. 5d, d').

Several studies have suggested that aggregated αSYN are transferred via tunneling nanotubes (TNTs) between astrocytes and between astrocyte and neurons [15, 25]. We wanted to explore whether MHC-II molecules also can spread between the human astrocytes and, if so, whether MHC-II and αSYN could be transported together from one cell to another. Immunostainings and confocal imaging showed that the MHC-II molecules were indeed transferred between the human astrocytes (Fig. 6a), suggesting that inflammatory molecules could be propagated from one astrocyte to another. Cell-to-cell transportation was detected in both control and αSYN-F exposed cultures. Additionally, confocal microscopy showed that the αSYN deposits surrounded by MHC-II also spread between the cells (Fig. 6b). These data suggest that the inflammation, as a part of the pathology, can spread from one astrocyte to another.

To examine whether astrocytes and CD4⁺ T cells are in direct contact with each other, human mesencephalon sections from PD post mortem brains were stained with specific antibodies to MHC-II, GFAP, and CD4. Infiltration of CD4⁺ T cells was observed in all the post mortem brain sections. Both perivascular and infiltrated T cells were demonstrated to be in contact with and closely surrounded by MHC-II expressing astrocytes (Fig. 7 a–c). Taken together, our data demonstrate that the astrocytes are capable of expressing all factors that are required for CD4⁺ T-cell activation, suggesting their involvement in T-cell activation during PD progression.

All data generated or analyzed during this study are included in this article.