Sensitivity and specificity of phospho‐Ser129 α‐synuclein monoclonal antibodies

Delic, Vedad; Chandra, Sidhanth; Abdelmotilib, Hisham; Maltbie, Tyler; Wang, Shijie; Kem, Danielle; Scott, Hunter J.; Underwood, Rachel; Liu, Zhiyong; Volpicelli‐Daley, Laura A.; West, Andrew B.

doi:10.1002/cne.24468

Cited by 62 publications

(97 citation statements)

References 30 publications

(36 reference statements)

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“…Thereafter, the sections were washed three times for 20 min in 50 m m Tris-buffered saline (TBS; 50 m m Tris-HCl, pH 7.4, and 150 m m NaCl) and incubated in a blocking solution containing 10% normal goat serum (NGS) in TBS for 1 h. The sections were then incubated for 48 h in rabbit monoclonal anti-phosphorylated α-synuclein antibody (phospho-S129, clone EP1536Y, catalog number ab51253; Abcam) at a dilution of 1:1000 in 2% NGS in TBS. The sensitivity and specificity of this antibody was confirmed in a previous study ( Delic et al, 2018 ). Sections were then washed three times for 20 min each with TBS and incubated overnight at 4°C in 1.4 nm nanogold-conjugated goat anti-rabbit secondary antibody (Nanoprobes).…”

Section: Methodssupporting

confidence: 78%

Developmental Changes in Dendritic Spine Morphology in the Striatum and Their Alteration in an A53T α-Synuclein Transgenic Mouse Model of Parkinson’s Disease

Parajuli

Wako

Maruo

et al. 2020

eNeuro

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Section: Methodssupporting

confidence: 78%

Developmental Changes in Dendritic Spine Morphology in the Striatum and Their Alteration in an A53T α-Synuclein Transgenic Mouse Model of Parkinson’s Disease

Parajuli

Wako

Maruo

et al. 2020

eNeuro

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“…As has been reported by several other studies investigating alpha-synuclein PFF induced pathology (85)(86)(87)(88)(89)(90), we experienced issues with unequivocal identification of pathological alpha-synuclein aggregates using immunocytochemistry (Fig.S3), even after TritonX-1000 protein extraction, which should leave only insoluble inclusions (42,62,90). Although neural networks from the PFF condition consistently displayed positive immunolabeling of alphasynuclein phosphorylated at S129, unspecific labelling and background staining were also observed in control conditions, rendering the immunoassays inconclusive.…”

Section: Induction Of Pathology By Alpha-synuclein Pff Seedssupporting

confidence: 66%

Criticality as a measure of developing proteinopathy in engineered human neural networks

Heiney

et al. 2020

Preprint

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A patterned spread of proteinopathy represents a common characteristic of many neurodegenerative diseases. In Parkinson's disease (PD), misfolded forms of alpha-synuclein proteins aggregate and accumulate in hallmark pathological inclusions termed Lewy bodies and Lewy neurites, which seems to affect selectively vulnerable neuronal populations and propagate within interconnected neuronal networks. Research findings suggest that these proteinopathic inclusions are present at very early timepoints in disease development, even before strong behavioural symptoms of dysfunction arise, but that these underlying pathologies might be masked by homeostatic processes working to maintain the function of the degenerating neural circuits. This study investigates whether inducing the PD-related alpha-synuclein pathology in engineered human neural networks can be associated with changes in network function, and particularly with network criticality states. Self-organised criticality represents the critical point between resilience against perturbation and adaptational flexibility, which appears to be a functional trait in self-organising neural networks, both in vitro and in vivo. By monitoring the developing neural network activity through the use of multielectrode arrays (MEAs) for a period of three weeks following proteinopathy induction, we show that although this developing pathology is not clearly manifest in standard measurements of network function, it may be discerned by differences in network criticality states.

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“…Sacino and colleagues cautioned that pSer129 antibodies (81A) can cross-react with neurofilament L in white matter tracts (150). Delic et al similarly observed nonspecific bands by Western blotting with all α-synuclein phosphoantibodies, and reported that the rabbit monoclonal anti-pSer129 antibody used here displays the highest sensitivity and specificity of commercially available anti-pSer129 antibodies; there are simply no better markers of α-synucleinopathy to date (47). It is also worth observing that, in those regions where the inclusions were quite dense per field of view (ie, more than one or two), statistically higher numbers of pSer129 + structures were always observed in the fibril-infused mice, confirming that our blinded interpretations of genuine α-synucleinopathic inclusions were indeed correct.…”

Section: α-Synuclein Fibril Infusions In the Murine Ob/ Aon Dramaticamentioning

confidence: 92%

“…Monoclonal mouse and rabbit antibodies raised against pSer129 were employed to visualize Lewy‐related pathology, as Ser129 phosphorylation of α‐synuclein is the most frequent posttranslational modification of this protein within Lewy aggregates . Manual counts of the number of pSer129 inclusions were performed on tissue sections stained with the mouse monoclonal antibody, as this antibody was employed before we found that the rabbit monoclonal was even better, as confirmed in a recent study . A blinded observer manually counted the total number of pSer129 + inclusions under 200× magnification (field of view = 447.1 μm × 337.0 μm) in 2–3 sagittal sections per animal.…”

Section: Methodsmentioning

confidence: 99%

The center of olfactory bulb‐seeded α‐synucleinopathy is the limbic system and the ensuing pathology is higher in male than in female mice

et al. 2019

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At early disease stages, Lewy body disorders are characterized by limbic vs. brainstem α‐synucleinopathy, but most preclinical studies have focused solely on the nigrostriatal pathway. Furthermore, male gender and advanced age are two major risk factors for this family of conditions, but their influence on the topographical extents of α‐synucleinopathy and the degree of cell loss are uncertain. To fill these gaps, we infused α‐synuclein fibrils in the olfactory bulb/anterior olfactory nucleus complex—one of the earliest and most frequently affected brain regions in Lewy body disorders—in 3‐month‐old female and male mice and in 11‐month‐old male mice. After 6 months, we observed that α‐synucleinopathy did not expand significantly beyond the limbic connectome in the 9‐month‐old male and female mice or in the 17‐month‐old male mice. However, the 9‐month‐old male mice had developed greater α‐synucleinopathy, smell impairment and cell loss than age‐matched females. By 10.5 months post‐infusion, fibril treatment hastened mortality in the 21.5‐month‐old males, but the inclusions remained centered in the limbic system in the survivors. Although fibril infusions reduced the number of cells expressing tyrosine hydroxylase in the substantia nigra of young males at 6 months post‐infusion, this was not attributable to true cell death. Furthermore, mesencephalic α‐synucleinopathy, if present, was centered in mesolimbic circuits (ventral tegmental area/accumbens) rather than within strict boundaries of the nigral pars compacta, which were defined here by tyrosine hydroxylase immunolabel. Nonprimate models cannot be expected to faithfully recapitulate human Lewy body disorders, but our murine model seems reasonably suited to (i) capture some aspects of Stage IIb of Lewy body disorders, which displays a heavier limbic than brainstem component compared to incipient Parkinson’s disease; and (ii) leverage sex differences and the acceleration of mortality following induction of olfactory α‐synucleinopathy.

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Sensitivity and specificity of phospho‐Ser129 α‐synuclein monoclonal antibodies

Cited by 62 publications

References 30 publications

Developmental Changes in Dendritic Spine Morphology in the Striatum and Their Alteration in an A53T α-Synuclein Transgenic Mouse Model of Parkinson’s Disease

Developmental Changes in Dendritic Spine Morphology in the Striatum and Their Alteration in an A53T α-Synuclein Transgenic Mouse Model of Parkinson’s Disease

Criticality as a measure of developing proteinopathy in engineered human neural networks

The center of olfactory bulb‐seeded α‐synucleinopathy is the limbic system and the ensuing pathology is higher in male than in female mice

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